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Nutrition in Cancer Care (PDQ®): Supportive care - Health Professional Information [NCI]

This information is produced and provided by the National Cancer Institute (NCI). The information in this topic may have changed since it was written. For the most current information, contact the National Cancer Institute via the Internet web site at http://cancer.gov or call 1-800-4-CANCER.

Nutrition in Cancer Care

Overview

Nutrition plays major (but not always fully understood) roles in many aspects of cancer development and treatment.[1] Malnutrition is a common problem in cancer patients that has been recognized as an important component of adverse outcomes, including increased morbidity and mortality and decreased quality of life. Weight loss has been identified as an indicator of poor prognosis in cancer patients.[2] It has been shown that at the time of diagnosis, 80% of patients with upper gastrointestinal cancer and 60% of patients with lung cancer have already experienced a significant weight loss,[3] generally defined as at least a 10% loss of body weight in 6 months' time.[4] Good nutrition practices can help cancer patients maintain weight and the body's nutrition stores, offering relief from nutrition impact symptoms and improving quality of life.[5] Poor nutrition practices, which can lead to undernutrition, can contribute to the incidence and severity of treatment side effects and increase the risk of infection, thereby reducing chances for survival.[6] Nutrition impact symptoms are those symptoms that impede oral intake. They include, but are not limited to, anorexia, nausea, vomiting, diarrhea, constipation, stomatitis, mucositis, dysphagia, alterations in taste and smell, pain, depression, and anxiety.[7] Early recognition and detection of risk for malnutrition through nutrition screening followed by comprehensive assessments is increasingly recognized as imperative in the development of standards of quality of care in oncology practices.[2] Undesirable weight gain may be an effect of chemotherapy treatment for early-stage cancers, possibly resulting from decreases in resting metabolism.[8] Consequently, the eating practices of individuals diagnosed with cancer should be assessed throughout the continuum of care to reflect the changing goals of nutritional therapy.

Nutritional status is often jeopardized by the natural progression of neoplastic disease. (Refer to the Tumor-Induced Effects on Nutritional Status section.) Alterations in nutritional status begin at diagnosis, when psychosocial issues may also adversely affect dietary intake, and proceed through treatment and recovery. Protein-calorie malnutrition (PCM) is the most common secondary diagnosis in individuals diagnosed with cancer, stemming from the inadequate intake of carbohydrate, protein, and fat to meet metabolic requirements and/or the reduced absorption of macronutrients. PCM in cancer results from multiple factors most often associated with anorexia, cachexia, and the early satiety sensation frequently experienced by individuals with cancer. These factors range from altered tastes to a physical inability to ingest or digest food, leading to reduced nutrient intake. Cancer-induced abnormalities in the metabolism of the major nutrients also increase the incidence of PCM. Such abnormalities may include glucose intolerance and insulin resistance, increased lipolysis, and increased whole-body protein turnover. If left untreated, PCM can lead to progressive wasting, weakness, and debilitation as protein synthesis is reduced and lean body mass is lost, possibly leading to death.[9]

Anorexia, the loss of appetite or desire to eat, is typically present in 15% to 25% of all cancer patients at diagnosis and may also occur as a side effect of treatments. Anorexia is an almost universal side effect in individuals with widely metastatic disease [10,11] because of physiologic alterations in metabolism during carcinogenesis. (Refer to the Tumor-induced Effects on Nutritional Status section.) Anorexia can be exacerbated by chemotherapy and radiation therapy side effects such as taste and smell changes, nausea, and vomiting. Surgical procedures, including esophagectomy and gastrectomy, may produce early satiety, a premature feeling of fullness.[4] Depression, loss of personal interests or hope, and anxious thoughts may be enough to bring about anorexia and result in PCM.[3] Evidence-based recommendations have been published describing various approaches to the problems of cancer-related fatigue, anorexia, depression, and dyspnea.[12] Other systemic or local effects of cancer or its treatment that may affect nutritional status include hypermetabolism, sepsis, malabsorption, and obstructions.[9]

Anorexia can hasten the course of cachexia,[3] a progressive wasting syndrome evidenced by weakness and a marked and progressive loss of body weight, fat, and muscle. Cachexia is estimated to be the immediate cause of death in 20% to 40% of cancer patients; it can develop in individuals who appear to be eating adequate calories and protein but have primary cachexia whereby tumor-related factors prevent maintenance of fat and muscle. Particularly at risk are patients with diseases of the gastrointestinal tract.

The etiology of cancer cachexia is not entirely understood. Cachexia can manifest in individuals with metastatic cancer as well as in individuals with localized disease. Several theories suggest that cachexia is caused by a complex mix of variables, including tumor-produced factors and metabolic abnormalities.[11] The basal metabolic rate in cachectic individuals is not adaptive, that is, it may be increased, decreased, or normal.[13] Some individuals do respond to nutrition therapy, but most will not see a complete reversal of the syndrome, even with aggressive therapy.[6] Thus, the most prudent and advantageous approach to cachexia is the prevention of its initiation through nutrition monitoring and nutrition intervention.[14]

Reference citations in some PDQ Supportive and Palliative Care information summaries may include links to external Web sites that are operated by individuals or organizations for the purpose of marketing or advocating the use of specific treatments or products. These reference citations are included for informational purposes only. Their inclusion should not be viewed as an endorsement of the content of the Web sites or of any treatment or product by the PDQ Supportive and Palliative Care Editorial Board or the National Cancer Institute (NCI).

In this summary, unless otherwise stated, evidence and practice issues as they relate to adults are discussed. The evidence and application to practice related to children may differ significantly from information related to adults. When specific information about the care of children is available, it is summarized under its own heading.

References:

1. Reeves GK, Pirie K, Beral V, et al.: Cancer incidence and mortality in relation to body mass index in the Million Women Study: cohort study. BMJ 335 (7630): 1134, 2007.
2. McMahon K, Decker G, Ottery FD: Integrating proactive nutritional assessment in clinical practices to prevent complications and cost. Semin Oncol 25 (2 Suppl 6): 20-7, 1998.
3. Bruera E: ABC of palliative care. Anorexia, cachexia, and nutrition. BMJ 315 (7117): 1219-22, 1997.
4. Rivadeneira DE, Evoy D, Fahey TJ 3rd, et al.: Nutritional support of the cancer patient. CA Cancer J Clin 48 (2): 69-80, 1998 Mar-Apr.
5. American Cancer Society.: Nutrition for the Person with Cancer: A Guide for Patients and Families. Atlanta, Ga: American Cancer Society, Inc., 2000.
6. Vigano A, Watanabe S, Bruera E: Anorexia and cachexia in advanced cancer patients. Cancer Surv 21: 99-115, 1994.
7. Wojtaszek CA, Kochis LM, Cunningham RS: Nutrition impact symptoms in the oncology patient. Oncology Issues 17 (2): 15-7, 2002.
8. Harvie MN, Campbell IT, Baildam A, et al.: Energy balance in early breast cancer patients receiving adjuvant chemotherapy. Breast Cancer Res Treat 83 (3): 201-10, 2004.
9. Shils ME: Nutrition and diet in cancer management. In: Shils ME, Olson JA, Shike M, et al., eds.: Modern Nutrition in Health and Disease. 9th ed. Baltimore, Md: Williams & Wilkins, 1999, pp 1317-47.
10. Langstein HN, Norton JA: Mechanisms of cancer cachexia. Hematol Oncol Clin North Am 5 (1): 103-23, 1991.
11. Tisdale MJ: Cancer cachexia. Anticancer Drugs 4 (2): 115-25, 1993.
12. Dy SM, Lorenz KA, Naeim A, et al.: Evidence-based recommendations for cancer fatigue, anorexia, depression, and dyspnea. J Clin Oncol 26 (23): 3886-95, 2008.
13. Ottery FD: Cancer cachexia: prevention, early diagnosis, and management. Cancer Pract 2 (2): 123-31, 1994 Mar-Apr.
14. Zeman FJ: Nutrition and cancer. In: Zeman FJ: Clinical Nutrition and Dietetics. 2nd ed. New York, NY: Macmillan Pub . Co, 1991, pp 571-98.

Tumor-induced Effects on Nutritional Status

Nutritional status can be compromised in direct response to tumor-induced alterations in metabolism. Also known as cachexia, this condition is one of advanced protein-calorie malnutrition and is characterized by involuntary weight loss, muscle wasting, and decreased quality of life.[1,2] Tumor-induced weight loss occurs frequently in patients with solid tumors of the lung, pancreas, and upper gastrointestinal tract and less often in patients with breast cancer or lower gastrointestinal cancer. Although anorexia may also be present, the energy deficit alone does not explain the pathogenesis of cachexia. Several factors have been proposed.[3] Mediators including cytokines, neuropeptides, neurotransmitters, and tumor-derived factors are postulated to contribute to this syndrome.[4] Products of host tissues, such as tumor necrosis factor-α, interleukin-1, interleukin-6, interferon-γ, and leukemia inhibitor factor, as well as tumor products that have a direct catabolic effect on host tissues, such as lipid-mobilizing factor and proteolysis-inducing factor (not established as definite in humans), have all been identified as mediators of this complex syndrome.[3] Altered metabolism of fats, proteins, and carbohydrates is evident in cancer patients with cachexia. Tumors may induce impaired glucose uptake and glucose oxidation, leading to an increased glycolysis.[5] Weight loss can occur from a decrease in energy intake, an increase in energy expenditure, or a combination of the two. Although anorexia is a common symptom of cancer patients, studies have shown that increased caloric intake either by the oral route or by supplementation with total parenteral nutrition has failed to counteract the wasting process. This supports the theory that the aberrant metabolic rate is the direct response by the tumor and the immune system to disrupt the pathways that regulate the homeostatic loop of body-weight regulation.[4]

Current studies suggest that the basal metabolic rate serves as a possible prognostic indicator of survival. As cancer progresses, the basal metabolic rate declines and cachexia occurs, reducing long-term survival.[6] Although alterations in overall basal metabolic rates have not been observed by some,[7] increased basal metabolic rates have been reported in pediatric,[8] breast,[9] lung,[8] malnourished,[10] and other [11] cancer patient populations; however, the discrepancy may be related to the stage of cancer progression.[12] Nutritional support therapies aimed at preserving lean muscle mass and subcutaneous adipose stores despite this altered metabolic rate may ultimately improve patients' quality of life and impact overall survival.

Although an individual's nutritional status may be compromised initially by the diagnosis of cancer, thorough nutritional screening procedures and the timely implementation of nutritional therapies may markedly improve the patient's outcome. Symptoms and side effects may sometimes be managed by a combination of dietary and pharmacologic interventions.

Several approaches to the treatment of cancer cachexia have been reported, and a variety of agents have been studied for their effects on appetite and weight. The decision to use pharmacological treatment to improve a patient's appetite should be based on the patient's desires, current medical condition, and life expectancy. Table 1 lists several medications that have been proposed to treat the symptoms of cancer cachexia.[13] However, the management of cachexia remains a complex challenge, and integrated multimodal treatment targeting the different factors involved has been proposed. In a phase III study, patients were randomly assigned to receive megestrol acetate, eicosapentaenoic acid, L-carnitine, thalidomide, or megestrol acetate plus L-carnitine and thalidomide. Interim analysis of 125 patients suggested the most effective treatment would be a combination regimen. The optimal combination is the goal of ongoing research.[14]

Table 1. Commonly Prescribed Medications

Drug Category Common Drugs Used Comments
EPA = eicosapentaenoic acid; TNF-alpha = tumor necrosis factor-alpha; U.S. FDA = United States Food and Drug Administration.
Progestational agents megestrol acetate Multiple investigations report appetite stimulant activity and weight gain with use. Body composition of weight gain indicates increased body fat stores instead of lean body tissue. Increased risk of thromboembolism with doses >800 mg/day is an apparent trend. Studies suggest improved effectiveness in patients with better digestive function; therefore, targeted nutritional strategies such as digestive enzymes or elemental diets may be useful.[13,15]
medroxyprogesterone
Glucocorticoids dexamethasone Mechanism of appetite stimulation is unknown but likely related to anti-inflammatory and euphoric actions. Studies report positive but short-lived effects on clinical outcomes such as appetite and quality of life, with minimal or no effect on weight gain. Risk of adverse effects such as muscle wasting and immunosuppression limit use for long-term use for appetite stimulation.[13,16]
methylprednisolone
prednisolone
Cannabinoids dronabinol Inconsistent evidence of clinical effectiveness in cancer patients. Studies of dronabinol alone or with megestrol acetate have not shown superior benefit in promoting weight gain and appetite.[13,17,18,19,20]
Antihistamines cyproheptadine Not studied well in cancer patients. A randomized placebo-controlled trial in patients with advanced cancer reported no difference in weight changes and progressive weight loss in both groups. Sedation is a frequent adverse effect that may limit usefulness in cancer patients.[13,21]
Antidepressants/ antipsychotics mirtazapine Clinical data supporting routine use in cancer patients are lacking. Further studies are needed.[16]
olanzapine
Anti-inflammatory agents thalidomide All have been shown to decrease TNF-alpha. Mixed results in clinical trials regarding weight gain and appetite stimulation. One published randomized placebo-controlled trial evaluated the safety and efficacy of thalidomide, 200 mg daily, in patients with advanced pancreatic cancer and weight loss of at least 10% of premorbid weight. Thalidomide group showed a significant difference in weight loss compared with the placebo group, indicating the drug's ability to safely decrease weight loss and loss of lean body mass in the patients studied.[22]Preliminary clinical studies and laboratory studies of the polyunsaturated fatty acid EPA have suggested a benefit to cancer patients; however, subsequent large comparative studies failed to reproduce this benefit.[23,24]
pentoxifylline
melatonin
omega 3 fatty acids (EPA)
Metabolic inhibitors hydrazine sulfate Not approved by the U.S. FDA for marketing in the United States.[16]
Anabolic agents oxandrolone Used in an attempt to stimulate muscle anabolism. Limited published reports of successful appetite stimulation in cancer patients.[16]
nandrolone decanoate
fluoxymesterone

Weight loss associated with cancer and its treatment may be secondary to a host of symptoms and side effects. Early intervention using appropriate nutrition and pharmacologic symptom-management strategies can keep weight loss at bay. The drug categories typically used to manage these symptoms and side effects include the following:[25]

  • Prokinetic agents (e.g., metoclopramide hydrochloride).
  • Antiemetic agents (e.g., phenothiazines, butyrophenones, substituted benzamides, serotonin antagonists, benzodiazepines, corticosteroids, anticholinergics, and cannabinoids).
  • Antidiarrheal agents (e.g., bulk-forming agents, antimotility agents, and codeine derivatives).
  • Pancreatic enzymes.
  • Laxatives (e.g., stool softeners, stimulants, bulk-forming agents, hyperosmotic laxatives, and saline laxatives).
  • Agents for oral care (e.g., saliva stimulants, cleansing agents, antifungal agents, topical anesthetics, mouthwashes, and healing/coating agents).
  • Pain medications (e.g., nonopioid analgesics, nonsteroidal anti-inflammatory drugs, and opioids).

(Refer to the Nutrition Screening and Assessment section and the Nutritional Suggestions for Symptom Management section.)

References:

1. Tisdale MJ: Biology of cachexia. J Natl Cancer Inst 89 (23): 1763-73, 1997.
2. Strasser F, Bruera ED: Update on anorexia and cachexia. Hematol Oncol Clin North Am 16 (3): 589-617, 2002.
3. Tisdale MJ: Pathogenesis of cancer cachexia. J Support Oncol 1 (3): 159-68, 2003 Sep-Oct.
4. Ramos EJ, Suzuki S, Marks D, et al.: Cancer anorexia-cachexia syndrome: cytokines and neuropeptides. Curr Opin Clin Nutr Metab Care 7 (4): 427-34, 2004.
5. Gambardella A, Tortoriello R, Tagliamonte MR, et al.: Metabolic changes in elderly cancer patients after glucose ingestion. The role of tumor necrosis factor-alpha. Cancer 79 (1): 177-84, 1997.
6. Jatoi A, Daly BD, Hughes V, et al.: The prognostic effect of increased resting energy expenditure prior to treatment for lung cancer. Lung Cancer 23 (2): 153-8, 1999.
7. Ottery FD: Cancer cachexia: prevention, early diagnosis, and management. Cancer Pract 2 (2): 123-31, 1994 Mar-Apr.
8. den Broeder E, Oeseburg B, Lippens RJ, et al.: Basal metabolic rate in children with a solid tumour. Eur J Clin Nutr 55 (8): 673-81, 2001.
9. Kutynec CL, McCargar L, Barr SI, et al.: Energy balance in women with breast cancer during adjuvant treatment. J Am Diet Assoc 99 (10): 1222-7, 1999.
10. Gambardella A, Tortoriello R, Pesce L, et al.: Intralipid infusion combined with propranolol administration has favorable metabolic effects in elderly malnourished cancer patients. Metabolism 48 (3): 291-7, 1999.
11. Bosaeus I, Daneryd P, Svanberg E, et al.: Dietary intake and resting energy expenditure in relation to weight loss in unselected cancer patients. Int J Cancer 93 (3): 380-3, 2001.
12. Pi-Sunyer FX: Overnutrition and undernutrition as modifiers of metabolic processes in disease states. Am J Clin Nutr 72 (2 Suppl): 533S-7S, 2000.
13. Murphy S, Von Roenn JH: Pharmacological management of anorexia and cachexia. In: McCallum PD, Polisena CG, eds.: The Clinical Guide to Oncology Nutrition. Chicago, Ill: The American Dietetic Association, 2000, pp 127-33.
14. Mantovani G, Macciò A, Madeddu C, et al.: Randomized phase III clinical trial of five different arms of treatment for patients with cancer cachexia: interim results. Nutrition 24 (4): 305-13, 2008.
15. Deutsch J, Kolhouse JF: Assessment of gastrointestinal function and response to megesterol acetate in subjects with gastrointestinal cancers and weight loss. Support Care Cancer 12 (7): 503-10, 2004.
16. Mattox TW: Treatment of unintentional weight loss in patients with cancer. Nutr Clin Pract 20 (4): 400-10, 2005.
17. Jatoi A, Yamashita J, Sloan JA, et al.: Does megestrol acetate down-regulate interleukin-6 in patients with cancer-associated anorexia and weight loss? A North Central Cancer Treatment Group investigation. Support Care Cancer 10 (1): 71-5, 2002.
18. Ulutin HC, Arpaci F, Pak Y: Megestrol acetate for cachexia and anorexia in advanced non-small cell lung cancer: a randomized study comparing two different doses. Tumori 88 (4): 277-80, 2002 Jul-Aug.
19. Jatoi A, Windschitl HE, Loprinzi CL, et al.: Dronabinol versus megestrol acetate versus combination therapy for cancer-associated anorexia: a North Central Cancer Treatment Group study. J Clin Oncol 20 (2): 567-73, 2002.
20. Strasser F, Luftner D, Possinger K, et al.: Comparison of orally administered cannabis extract and delta-9-tetrahydrocannabinol in treating patients with cancer-related anorexia-cachexia syndrome: a multicenter, phase III, randomized, double-blind, placebo-controlled clinical trial from the Cannabis-In-Cachexia-Study-Group. J Clin Oncol 24 (21): 3394-400, 2006.
21. Kardinal CG, Loprinzi CL, Schaid DJ, et al.: A controlled trial of cyproheptadine in cancer patients with anorexia and/or cachexia. Cancer 65 (12): 2657-62, 1990.
22. Gordon JN, Trebble TM, Ellis RD, et al.: Thalidomide in the treatment of cancer cachexia: a randomised placebo controlled trial. Gut 54 (4): 540-5, 2005.
23. Jatoi A: Fish oil, lean tissue, and cancer: is there a role for eicosapentaenoic acid in treating the cancer anorexia/weight loss syndrome? Crit Rev Oncol Hematol 55 (1): 37-43, 2005.
24. Fearon KC, Barber MD, Moses AG, et al.: Double-blind, placebo-controlled, randomized study of eicosapentaenoic acid diester in patients with cancer cachexia. J Clin Oncol 24 (21): 3401-7, 2006.
25. Kennedy LD: Common supportive drug therapies used with oncology patients. In: McCallum PD, Polisena CG, eds.: The Clinical Guide to Oncology Nutrition. Chicago, Ill: The American Dietetic Association, 2000, pp 168-81.

Nutrition Implications of Cancer Therapies

The nutritional status of patients diagnosed with cancer entering the treatment process varies. Not everyone begins therapy with anorexia, weight loss, and other symptoms of nutritional problems. For patients who have such symptoms, however, anticancer therapies can complicate the treatment and expected recovery. Many individuals also present with preexisting comorbid diseases and illnesses that further complicate their treatment. Surgery, chemotherapy, and radiation can have a direct (or mechanical) and/or an indirect (or metabolic) negative effect on nutritional status. The success of the anticancer therapy will be influenced by a patient's ability to tolerate therapy, which will, in turn, be affected by nutritional status preceding treatment. The treating clinician should assess baseline nutritional status (see the Nutrition Screening and Assessment section) and be aware of the possible implications of the various therapies. Patients receiving aggressive cancer therapies typically need aggressive nutrition management.

Surgery

Surgery is often the primary treatment modality for cancer. Approximately 60% of individuals diagnosed with cancer will have some type of cancer-related surgery.[1] Malnourished surgical patients are at increased risk for postoperative morbidity and mortality. Steps should be taken to attempt to correct nutritional macronutrient and micronutrient deficiencies before surgery if time permits.[2] This involves identification and assessment of the problem, with the possible use of oral liquid nutritional supplements, enteral or parenteral nutritional support, and/or use of pharmacologic therapies to stimulate the appetite (see the Tumor-Induced Effects on Nutritional Status section).[2]

Depending on the procedure, surgery can cause mechanical or physiologic barriers to adequate nutrition, such as a short gut that results in malabsorption after bowel resection.[2] In addition to these mechanical barriers, surgery frequently imposes an immediate metabolic response that increases the energy needs and changes the nutrient requirements necessary for wound healing and recovery at a time when baseline needs and requirements are often not being met.

The following sections highlight various surgical issues for specific cancers. Nutritional complications are usually most notable and severe with cancerous growths and anticancer therapy involving the alimentary canal.

Head and neck cancers

Alcohol abuse is a major risk factor for cancer in the head and neck region and can itself lead to malnutrition.[3] Cancer occurring in this region coupled with curative or palliative surgery can alter a patient's ability to speak, chew, salivate, swallow, smell, taste, and/or see.[2] Treatment for head and neck cancer can have a profound negative effect on nutritional status.

Nutrition assessment is advised at the initial visit. Clinicians should anticipate additional complicating factors such as the side effects of combined modality therapy (chemotherapy and radiation therapy),[4] as well as the increased nutritional requirements for withstanding these therapies. Because head and neck cancer patients are often malnourished at diagnosis and will undergo therapies that may directly affect their ability to eat, many of these individuals have enteral feeding tubes placed prophylactically before undergoing surgery.[2]

Gastrointestinal cancers

Surgery may take a tremendous toll on the body, but it has reduced mortality and morbidity from gastrointestinal cancers.[2] Anticancer therapy for aerodigestive cancers (e.g., esophageal, gastric, pancreatic, liver, gallbladder, bile duct, and small and large intestine) can result in gastric paresis, alterations in digestion, malabsorption of nutrients, hyperglycemia, elevated lipid levels, hepatic encephalopathy, fluid and electrolyte imbalance, anastomotic and chyle leaks, dumping syndrome, and vitamin and mineral deficiencies.[2] The use of enteral nutritional support is common in the treatment of gastrointestinal cancers. The feeding tube may be placed in the stomach (gastrostomy) or down into the jejunum (jejunostomy).[2,5]

Additional complications and side effects from surgical oncology

Many individuals experience fatigue, pain, and loss of appetite and are unable to consume their regular diet as the result of surgery.[2] Prompt nutritional therapy can help relieve or reduce these problems. Avoiding carbonated or known gas-producing foods will help, as will altering the fiber content in the diet to encourage bowel regularity. A well-balanced diet that contains the recommended amounts of essential nutrients and calories will help promote good wound healing. Finally, proper nutrition and adequate rest may help prevent or treat fatigue.

Chemotherapy

In 2000, more than 90 different chemotherapy agents were approved for use. These agents are divided into several functional categories. Chemotherapy agents can be used in combination or as single agents, depending on the disease type and health condition of the individual.[6]

Unlike surgery and radiation therapy, cancer chemotherapy is a systemic treatment (not a localized treatment) that affects the whole body (not just a specific part).[7] Consequently, there are potentially more side effects with chemotherapy than with surgery and radiation therapy. The most commonly experienced nutrition-related side effects are anorexia, taste changes, early satiety, nausea, vomiting, mucositis/esophagitis, diarrhea, and constipation (see the Nutritional Suggestions for Symptom Management section). Because side effects of chemotherapy, as well as the cancer itself, can greatly affect nutritional status, healthcare providers need to anticipate possible problems and educate the patient about them [7] in an effort to prevent malnutrition and weight loss (see the Nutrition Screening and Assessment section). Malnutrition and weight loss can affect a patient's ability to regain health and acceptable blood counts between chemotherapy cycles; this can directly affect the patient's ability to stay on treatment schedules, which is important in achieving a successful outcome.

Nutritional support or high-calorie/high-protein liquid supplements may be used in an effort to maintain adequate calorie and nutrient intake. Special formulas are available for people with secondary medical conditions such as hyperglycemia or compromised renal function.

Radiation Therapy

Nutritional support during radiation therapy is vital. The effect of radiation therapy on healthy tissue in the treatment field can produce changes in normal physiologic function that may ultimately diminish a patient's nutritional status by interfering with ingestion, digestion, or absorption of nutrients. Medications such as pilocarpine (Salagen) may be useful in treating the xerostomia (dry mouth) that accompanies radiation therapy. This medicine may reduce the need for artificial saliva agents or other oral comfort agents such as hard candy or sugarless gum.

The side effects of radiation therapy depend on the area irradiated, total dose, fractionation, duration, and volume irradiated. Most side effects are acute, begin around the second or third week of treatment, and diminish 2 or 3 weeks after radiation therapy is completed. Some side effects can be chronic and continue or occur after treatment has been completed.[8]

Individuals receiving radiation therapy to any part of the gastrointestinal tract are more susceptible to nutrition-related side effects.[9] Patients most at risk for developing nutrition-related side effects are those whose cancers involve the aerodigestive tract, including the head and neck, lungs, esophagus, cervix, uterus, colon, rectum, and pancreas. Patients who are receiving radiation therapy to the head and neck region may present to radiation therapy with preexisting malnutrition secondary to an inability to ingest foods because of the disease itself or because of surgery to treat the disease. Many of these patients have a history of high alcohol intake, which also places them at a higher nutritional risk. These individuals are generally at the greatest risk for developing significant nutrition problems and severe weight loss.[10] In a placebo-controlled, double-blind randomized study of 57 patients receiving radiation therapy for head/neck and lung cancer, megestrol acetate (MA) was administered at a dose of 800 mg per day. Patients who received MA demonstrated significant advantages in weight maintenance and some aspects of quality of life.[11]

Nutrition intervention is based on symptom management. Patients who maintain good nutrition are more likely to tolerate the side effects of treatment. Adequate calories and protein can help maintain patient strength and prevent body tissues from further catabolism. Individuals who do not consume adequate calories and protein use stored nutrients as an energy source, which leads to protein wasting and further weight loss.

Some of the more common nutrition-related side effects caused by irradiation to the head and neck include taste alterations or aversions, odynophagia (pain produced by swallowing), xerostomia, thick saliva, mucositis, dysphagia, and stricture of the upper esophagus.[4] Thoracic irradiation may be associated with esophagitis, dysphagia, or esophageal reflux. Diarrhea, nausea, vomiting, enteritis, and malabsorption of nutrients are possible side effects of pelvic or abdominal radiation.[12] (See the Nutritional Suggestions for Symptom Management section.) A prospective, randomized study of patients with colorectal cancer receiving radiation therapy demonstrated that concurrent individualized dietary counseling can improve patients' nutritional intake, status, and quality of life. These improvements, in turn, may reduce radiation-induced morbidity.[13] Patients receiving high-dose radiation or bone marrow transplant should consult with a dietician.

Suggestions for appropriate dietary modifications based on nutrition-related symptoms are widely available for patient and healthcare professional use. For a full listing of dietary suggestions see the Tumor-Induced Effects on Nutritional Status section. A list of appropriate references is also included below.

Many patients who are undergoing radiation therapy will benefit from nutritional supplements between meals.[14] Aggressive nutritional support is indicated when oral intake alone fails to maintain an individual's weight. Tube feedings are used more frequently than parenteral nutrition, primarily to preserve gastrointestinal function. Tube feedings are usually well tolerated, pose less risk to the patient than parenteral feedings, and are more cost effective. Numerous studies demonstrate the benefit of enteral feedings initiated at the onset of treatment, specifically treatment to head and neck regions, before significant weight loss has occurred.[15,16,17]

Many nutrition-related side effects result from radiation therapy. Quality of life and nutritional intake can be improved by managing these side effects through appropriate medical nutritional therapy and dietary modifications.

Immunotherapy

Monoclonal antibodies, which are used to block cancer-cell receptors for growth-stimulating factors, may cause a cascade of symptoms; however, the symptoms most likely to impact nutritional status are fever, nausea, vomiting, and diarrhea.[1] Interferon (a nonspecific immunotherapy) has had the noted nutrition-related side effects of anorexia, nausea, vomiting, and fatigue.[1] Interleukin-2, approved by the U.S. Food and Drug Administration for the single-agent treatment of metastatic renal cell cancer, can also cause symptoms such as fatigue, nausea, vomiting, and diarrhea.[1,18] Response to interleukin-2 treatment varies; some patients gain weight, and some require nutritional support.[18] However, most patients taking interleukin gain weight. Finally, granulocyte-macrophage colony-stimulating factor, a very common therapy used to increase the production of white blood cells, may also cause fever, nausea, vomiting, and diarrhea.[1]

If ignored, these symptoms can cause gradual or drastic weight loss (depending on the severity of the symptoms), which may lead to malnutrition. Malnutrition can complicate the expected healing and recovery process (see the Nutritional Suggestions for Symptom Management section).

Hemopoietic and Peripheral Blood Stem Cell Transplantation

Hemopoietic and stem cell transplant patients have special nutritional requirements.[19] Before their transplant, patients receive high-dose chemotherapy and may also be treated with total-body irradiation (TBI).[20] These treatments, in addition to medications used during transplantation, frequently result in nutritional side effects, which may affect patients' ability to consume an adequate diet. The goal of nutritional support should be the maintenance of nutritional status and protein stores. In addition, transplant patients are at very high risk for neutropenia, an abnormally small number of neutrophils in the blood, that makes them susceptible to multiple infections.[21,22]

To reduce the risk of infections related to stem cell transplantation, most healthcare setting guidelines recommend only cooked and processed foods and restrict raw vegetables and fresh fruits that could cause a food-related infection. Specific dietary restrictions and their duration depend on the type of transplant and the cancer site. In addition to specific dietary restrictions, food safety guidelines should be reviewed and stressed with all transplant patients.

The chemotherapy regimen and complications associated with the transplant may result in numerous problems that adversely affect nutritional intake and status.[23] During the transplant process, patients may experience nutrition-related side effects such as taste changes, oral dryness, thick saliva, mouth and throat sores, nausea and vomiting, diarrhea, constipation, lack of appetite/weight loss, and weight gain. Often during the first few weeks posttransplant, patients are fed intravenously to ensure that they receive sufficient calories, protein, vitamins, minerals, and fluids.[24]

Many patients experience mouth and throat sores 2 to 4 weeks after transplantation. Mucositis is the general term that refers to the erythema, swelling, and ulceration of the intraoral soft-tissue structures and the oral and esophageal mucosa in response to the cytotoxic effect of radiation therapy and high-dose chemotherapy. Mouth and throat sores can make eating and swallowing difficult. TBI may also cause dryness of the mouth, temporarily alter the taste of food, and/or cause thick saliva to form in the mouth and throat. Nausea and vomiting are common problems experienced by transplant patients. Nausea and vomiting may be caused by TBI, chemotherapy, and some medications. TBI, chemotherapy, infection, depression, and fatigue can cause a decrease in appetite and weight loss. Lack of appetite may continue to be a problem long after discharge from the hospital. Patients may also experience gastrointestinal problems such as diarrhea and constipation that could be caused by TBI, chemotherapy, gastrointestinal graft-versus-host disease, infection, and some medications.[25,26]

References:

1. American Cancer Society Web Site. Atlanta, Ga: American Cancer Society, 2012. Available online. Last accessed January 5, 2012.
2. McGuire M: Nutritional care of surgical oncology patients. Semin Oncol Nurs 16 (2): 128-34, 2000.
3. Allison G, Dixon D, Eldridge B, et al.: Nutrition implications of surgical oncology. In: McCallum PD, Polisena CG, eds.: The Clinical Guide to Oncology Nutrition. Chicago, Ill: The American Dietetic Association, 2000, pp 79-89.
4. Laurell G, Kraepelien T, Mavroidis P, et al.: Stricture of the proximal esophagus in head and neck carcinoma patients after radiotherapy. Cancer 97 (7): 1693-700, 2003.
5. Persson CR, Johansson BB, Sjöden PO, et al.: A randomized study of nutritional support in patients with colorectal and gastric cancer. Nutr Cancer 42 (1): 48-58, 2002.
6. Eldridge B: Chemotherapy and nutrition implications. In: McCallum PD, Polisena CG, eds.: The Clinical Guide to Oncology Nutrition. Chicago, Ill: The American Dietetic Association, 2000, pp 61-9.
7. Fishman M, Mrozek-Orlowski M, eds.: Cancer Chemotherapy Guidelines and Recommendations for Practice. 2nd ed. Pittsburgh, Pa: Oncology Nursing Press, 1999.
8. Donaldson SS: Nutritional consequences of radiotherapy. Cancer Res 37 (7 Pt 2): 2407-13, 1977.
9. Unsal D, Mentes B, Akmansu M, et al.: Evaluation of nutritional status in cancer patients receiving radiotherapy: a prospective study. Am J Clin Oncol 29 (2): 183-8, 2006.
10. Chencharick JD, Mossman KL: Nutritional consequences of the radiotherapy of head and neck cancer. Cancer 51 (5): 811-5, 1983.
11. McQuellon RP, Moose DB, Russell GB, et al.: Supportive use of megestrol acetate (Megace) with head/neck and lung cancer patients receiving radiation therapy. Int J Radiat Oncol Biol Phys 52 (5): 1180-5, 2002.
12. Polisena CG: Nutrition concerns with the radiation therapy patient. In: McCallum PD, Polisena CG, eds.: The Clinical Guide to Oncology Nutrition. Chicago, Ill: The American Dietetic Association, 2000, pp 70-8.
13. Ravasco P, Monteiro-Grillo I, Vidal PM, et al.: Dietary counseling improves patient outcomes: a prospective, randomized, controlled trial in colorectal cancer patients undergoing radiotherapy. J Clin Oncol 23 (7): 1431-8, 2005.
14. McCarthy D, Weihofen D: The effect of nutritional supplements on food intake in patients undergoing radiotherapy. Oncol Nurs Forum 26 (5): 897-900, 1999.
15. Tyldesley S, Sheehan F, Munk P, et al.: The use of radiologically placed gastrostomy tubes in head and neck cancer patients receiving radiotherapy. Int J Radiat Oncol Biol Phys 36 (5): 1205-9, 1996.
16. Heymsfield SB, Greenwood T, Roongpisuthipong C: Dietetics and enteral nutrition: past, present, and future. J Am Diet Assoc 85 (6): 667-8, 1985.
17. Beer KT, Krause KB, Zuercher T, et al.: Early percutaneous endoscopic gastrostomy insertion maintains nutritional state in patients with aerodigestive tract cancer. Nutr Cancer 52 (1): 29-34, 2005.
18. Samlowski WE, Wiebke G, McMurry M, et al.: Effects of total parental nutrition (TPN) during high-dose interleukin-2 treatment for metastatic cancer. J Immunother 21 (1): 65-74, 1998.
19. Charuhas PM: Bone marrow transplantation. In: Skipper A, ed.: Dietitian's Handbook of Enteral and Parenteral Nutrition. 2nd ed. Gaithersburg, Md: Aspen Publishers, 1998, pp 273-94.
20. Johns A: Overview of bone marrow and stem cell transplantation. J Intraven Nurs 21 (6): 356-60, 1998 Nov-Dec.
21. Ninin E, Milpied N, Moreau P, et al.: Longitudinal study of bacterial, viral, and fungal infections in adult recipients of bone marrow transplants. Clin Infect Dis 33 (1): 41-7, 2001.
22. Jantunen E, Ruutu P, Piilonen A, et al.: Treatment and outcome of invasive Aspergillus infections in allogeneic BMT recipients. Bone Marrow Transplant 26 (7): 759-62, 2000.
23. Roberts SR: Bone marrow and peripheral blood stem cell transplantation. In: Lysen LK, ed.: Quick Reference to Clinical Dietetics. Gaithersburg, Md: Aspen Publishers, Inc, 1997, pp 162-8.
24. Weisdorf SA, Schwarzenberg SJ: Nutritional support of bone marrow transplantation recipients. In: Forman SJ, Blume KG, Thomas ED, eds.: Bone Marrow Transplantation. Boston, Mass: Blackwell Scientific Publications, 1994, pp 327-36.
25. Charuhas PM: Medical nutrition therapy in bone marrow transplantation. In: McCallum PD, Polisena CG, eds.: The Clinical Guide to Oncology Nutrition. Chicago, Ill: The American Dietetic Association, 2000, pp 90-8.
26. Shapiro TW, Davison DB, Rust DM, eds.: A Clinical Guide to Stem Cell and Bone Marrow Transplantation. Boston, Mass: Jones and Bartlett Publishers, 1997.

Nutrition Therapy

Nutrition Screening and Assessment

Nutrition in cancer care embodies prevention of disease, treatment, cure, or supportive palliation. Caution should be exercised when considering alternative or unproven nutritional therapies during all phases of cancer treatment and supportive palliation, as these diets may prove harmful. Patient nutritional status plays an integral role in determining not only risk of developing cancer but also risk of therapy-related toxicity and medical outcomes. Whether the goal of cancer treatment is cure or palliation, early detection of nutritional problems and prompt intervention are essential.

The original principles of nutrition care for people diagnosed with cancer were developed in 1979 [1] and are still very relevant today. Proactive nutritional care can prevent or reduce the complications typically associated with the treatment of cancer.[1]

Many nutritional problems stem from local effects of the tumor. Tumors in the gastrointestinal tract, for example, can cause obstruction, nausea, vomiting, impaired digestion, and/or malabsorption. In addition to the effects of the tumor, marked alterations in normal metabolism of carbohydrates, protein, and/or fats can occur.[2]

The nutritional prognostic indicators most recognized as being predictive of poor outcome include weight loss, wasting, and malnutrition. In addition, significant weight loss at the time of diagnosis has been associated with decreased survival and reduced response to surgery, radiation therapy, and/or chemotherapy.[3]

Malnutrition and accompanying weight loss can be part of an individual's presentation or can be caused or aggravated by treatments for the disease. Identification of nutrition problems and treatment of nutrition-related symptoms have been shown to stabilize or reverse weight loss in 50% to 88% of oncology patients.[4]

Screening and nutrition assessment should be interdisciplinary; the healthcare team (e.g., physicians, nurses, registered dietitians, social workers, psychologists) should all be involved in nutritional management throughout the continuum of cancer care.[5]

A number of screening and assessment tools are currently available for use in nutritional assessment. Examples of these tools include the Prognostic Nutrition Index,[6,7] delayed hypersensitivity skin testing, institution-specific guidelines, and anthropometrics. Each of these tools can help identify persons at nutritional risk; unfortunately, the values obtained using such tools can be altered by the hydration status and the immune compromise frequently found in individuals diagnosed with cancer. In addition, each of these objective measures can carry a cost in terms of laboratory or practitioner time. One author has provided a useful overview of assessment procedures for advanced cancer patients.[8]

Another example of a screening and assessment procedure is the Patient-Generated Subjective Global Assessment (PG-SGA). Based on earlier work on a protocol called Subjective Global Assessment (SGA),[9] the PG-SGA is an easy-to-use and inexpensive approach in identifying individuals at nutritional risk and in triaging for subsequent medical nutritional therapy in a variety of clinical settings.[10,11] The individual and/or caretaker complete sections on weight history, food intake, symptoms, and function. A member of the healthcare team evaluates weight loss, disease, and metabolic stress and performs a nutrition-related physical examination. A score is generated from the information collected. The need for nutrition intervention is determined according to the score.

Bioelectrical impedance analysis (BIA) is also used to assess nutritional status, as determined by body composition.[12] The BIA measures electrical resistance on the basis of lean body mass and body fat composition. Single BIA measures show body cell mass, extracellular tissue, and fat as a percent of ideal, whereas sequential measurements can be used to show body composition changes over time. Because of cost and accessibility, BIA is currently in limited use and often unavailable in most ambulatory settings.

Taste and smell defects are common in cancer patients and may affect nutritional status. The relative importance of chemosensory changes to the etiology of malnutrition was assessed in 66 patients with advanced cancer. Some degree of chemosensory abnormality was reported by 86% of patients; approximately one-half of patients reported interference with enjoying favorite foods. Poor appetite, nausea, early satiety, and chemosensory abnormalities presented concurrently. These findings were significantly related to decreased energy intake. Further research is required to design nutritional interventions for these chemosensory problems.[13]

Because nutritional status can quickly become compromised from illness and decreased dietary intake, and because nutritional well-being plays an important role in treatment and recovery from cancer, early screening and intervention as well as close monitoring and evaluation throughout all phases of cancer treatment and recovery are imperative in the pursuit of health for the individual with cancer.

Goals of Nutrition Therapy

Optimal nutritional status is an important goal in the management of individuals diagnosed with cancer. Although nutrition therapy recommendations may vary throughout the continuum of care, maintenance of adequate intake is important. Therefore, a waiver from most dietary restrictions observed during religious holidays is granted for those undergoing active treatment. Individuals with cancer are encouraged to speak to their religious leaders regarding this matter before a holiday.

Whether patients are undergoing active therapy, recovering from cancer therapy, or in remission and striving to avoid cancer recurrence, the benefit of optimal caloric and nutrient intake is well documented.[14,15,16]

The goals of nutrition therapy are to accomplish the following:

  • Prevent or reverse nutrient deficiencies.
  • Preserve lean body mass.
  • Help patients better tolerate treatments.
  • Minimize nutrition-related side effects and complications.
  • Maintain strength and energy.
  • Protect immune function, decreasing the risk of infection.
  • Aid in recovery and healing.
  • Maximize quality of life.

Patients with advanced cancer can receive nutritional support even when nutrition therapy can do little for weight gain.[17,18] Such support may help accomplish the following:

  • Lessen side effects.
  • Reduce risk of infection (if given enterally).
  • Reduce asthenia.
  • Improve well-being.

In individuals with advanced cancer, the goal of nutrition therapy should not be weight gain or reversal of malnutrition, but rather comfort and symptom relief.[19]

Nutrition continues to play an integral role for individuals whose cancer has been cured or who are in remission.[20] A healthy diet helps prevent or control comorbidities such as heart disease, diabetes, and hypertension. Following a healthful nutrition program might help prevent another malignancy from developing.

Methods of Nutrition Care

As outlined above, individuals diagnosed with cancer are at risk for malnutrition resulting from the disease itself; from anticancer therapy such as surgery, radiation, or pharmacologic therapy; and/or from anorexia due to emotional turmoil. The following sections highlight the benefits, contraindications, methods of administration, and home care issues for all forms of nutrition support—oral, enteral, and parenteral.

The preferred method of nutrition support is via the oral route, with the use of dietary modifications to reduce the symptoms associated with cancer treatments. Enteral nutrition is indicated when the gastrointestinal (GI) tract is functional but oral intake is insufficient to meet nutritional requirements. Common situations in which enteral nutrition may be needed include malignancies of the head and neck regions, esophagus, and stomach. When the GI tract is dysfunctional, total parenteral nutrition (TPN) or enteral nutrition may be indicated; however, the widespread use of TPN is controversial because little evidence of improved survival has been demonstrated in patients with advanced cancer.[21] Parenteral nutrition has been shown to be beneficial in only a small group of patients—specifically, postoperative patients who are being aggressively treated and who have demonstrated a positive response rate. One study [22] reported that patients with GI cancer benefited from perioperative support with TPN, with one-third fewer complications and decreased mortality.

Oral nourishment

Optimal nutrition can improve the clinical course, outcome, and quality of life of patients undergoing treatment for cancer.[23] Virtually every cancer patient could benefit from consultation with a registered dietitian or physician to formulate a plan for nutrition and to begin meal planning. Oral nutrition, or eating by mouth, is the preferred method of feeding and should be used whenever possible. Appetite stimulants may be used to enhance the enjoyment of foods and to facilitate weight gain in the presence of significant anorexia.[24]

Recommendations during treatment may focus on eating foods that are high in energy, protein, and micronutrients to help maintain nutritional status. This may be especially true for individuals with early satiety, anorexia, and alteration in taste, xerostomia, mucositis, nausea, or diarrhea. Under most of these circumstances, eating frequently and including high-energy and high-protein snacks may help overall intake.[25]

At-risk individuals who may benefit from nutritional support might have one or more of the following characteristics:[26]

  • Low body weight, as defined by less than 80% of ideal weight or recently experienced unintentional weight loss of more than 10% of usual weight.
  • Malabsorption of nutrients due to disease, short bowel syndrome, or anticancer therapy.
  • Fistulas or draining abscesses.
  • Inability to eat or drink for more than 5 days.
  • Moderate or high nutritional risk status as determined by screening or an assessment tool.
  • The ability to demonstrate competencies for discharge planning on nutritional support (both individual and caregiver).

Although the many benefits of achieving good nutritional status via nutritional support can clearly be detailed, the disadvantages or questionable benefits of nutritional support must also be considered. The debate regarding the effect of nutritional support on tumor growth has not been settled;[27] though quality of life is usually improved with better nutritional status, the actual impact of nutritional support on longevity has yet to be definitively determined.[27]

Once the degree of malnutrition has been assessed, the decision to offer nutritional support and which form of support to utilize must be determined by the healthcare professional and other parties involved. Enteral and parenteral nutritional support offers viable options to reduce the risk of debilitating malnutrition and interruptions in anticancer therapy that may influence outcome. Each form of nutritional support has advantages and disadvantages. It is critical to thoroughly evaluate the diagnosis, prognosis, degree of malnutrition, function of the gut, and ease of delivery before embarking on the plan of nutritional support. Caution must also be exercised to avoid refeeding syndrome, the metabolic complication that is caused by rapid repletion of potassium, phosphorous, and magnesium in a severely malnourished or cachectic patient.[26]

The following sections highlight the benefits, contraindications, methods of administration, formulas, and home care issues for both enteral and parenteral nutrition.

Enteral nutrition

The benefits of enteral nutrition, or tube feeding, are that it continues to use the gut, has fewer complications such as infection and organ malfunction, is often easier to administer, and is cheaper than parenteral nutrition.[26,27,28,29] In addition, nutrients are metabolized and utilized more efficiently by the body.

Specific disease and condition-related indications for use consist of a diagnosis of a cancer of the alimentary canal (in particular, head and neck, esophageal, gastric, or pancreatic cancers) and severe complications/side effects from chemotherapy and/or radiation that are seriously jeopardizing the treatment plan of an individual already suffering from malnutrition.[26]

Contraindications for enteral nutritional support include a malfunctioning gastrointestinal tract, malabsorptive conditions, mechanical obstructions, severe bleeding, severe diarrhea, intractable vomiting, gastrointestinal fistulas in locations difficult to bypass with an enteral tube, inflammatory bowel processes such as prolonged ileus and severe enterocolitis, and/or an overall health prognosis not consistent with aggressive nutrition therapy.[26] Thrombocytopenia and general pancytopenic conditions following anticancer treatments may also prevent placement of an enteral tube.

Prospective Assessment

Several effective methods for the delivery of enteral nutritional support or tube feedings exist. An approximation of how long nutritional support will be needed is critical, however, to determine the most appropriate delivery route. Nasogastric, nasoduodenal, or nasojejunal methods are best for short-term support (<2 weeks).[29] The endpoint of delivery—the stomach, the duodenum, or jejunum—is determined by the risk of aspiration, with nasojejunal feeds recommended for individuals with aspiration risk. If the person with cancer is at very high risk for aspiration, enteral nutritional support may be contraindicated and parenteral nutrition should be considered. Also, immune-compromised individuals with mucositis, esophagitis, and/or herpetic, fungal, or candidiasis lesions in the mouth or throat may not be able to tolerate the presence of a nasogastrointestinal tube.

Tubes are constructed from silicone or polyurethane and can vary in length from 30 to 43 inches, with the shorter tubes used for nasogastric feedings. The diameters range from 5F to 16F catheters. Tubes may have weighted tips to help passage through the gut.

Percutaneous endoscopic gastrostomy tubes (PEGs) and percutaneous endoscopic jejunostomy tubes (PEJs) are generally used for long-term enteral feedings (>2 weeks).[29] The placement further down in the gastrointestinal tract has a number of advantages: the diameter of the tube is larger (15F-24F catheters), which allows easier and faster passage of formulas and medications; the risk for aspiration is lower because of the decreased chance of migration of the tube up into the esophagus; the risk for sinusitis or nasoesophageal erosion is lower; and this route is more convenient and aesthetically pleasing to the individual because of the ability to conceal the tube.[29] People anticipating long-term support may also consider a skin-level button gastrostomy or jejunostomy.

Assessment of need and ease of delivery are best done early. If the malnourished individual requires surgery for an unrelated event, a PEG or PEJ may be placed at that time to avoid an additional procedure.

Infusion Methods and Formulas

Enteral nutrition or tube feedings can be delivered at various rates. When possible, the bolus method is preferable because it mimics normal feeding, requires less time and equipment, and offers greater flexibility to the patient.[29] The following is a summary of infusion possibilities:[29]

Continuous or cyclic drip feeding

  • Caloric/nutrient and free-water requirements need to be determined first to plan rate and time recommendations.
  • Enteral feeding pumps provide reliable, constant infusion rates and decrease the risk of gastric retention.
  • Assuming that no compounding factors are present, feeding into the stomach (25–30 cc/h) can start at a higher rate than feeding into the jejunum (10 cc/h); rates can be increased, with tolerance, every 4 to 6 hours until the rate reaches that needed to deliver the required caloric/nutrient needs.
  • Continuous feeds can be cycled to run at night to allow greater flexibility and comfort. If it is physically possible, these nocturnal feeds can allow daytime oral or bolus feedings to meet nutritional goals and provide a more normal lifestyle.

Bolus and intermittent feeding

  • Caloric/nutrient and free-water requirements need to be determined to plan the feeding schedule.
  • Bolus feedings can be offered several times (3–6 times) each day; as much as 250 to 500 cc can be given over 10 to 15 minutes.
  • Bolus feeding should be used ONLY when the endpoint of the tube is in the stomach; it should NEVER be used when feedings are delivered into the duodenum or jejunum. This precaution protects against gastric distention and dumping.
  • A gravity drip from a bag or syringe with a slow push can be used to administer the formula.
  • Diarrhea is a common side effect of this infusion method but can be controlled with a change in formula, additions to the formula, and a change in the amount of formula given over a finite period of time.

After the infusion method has been determined, a formula needs to be selected. There are many formulas on the market, ranging from elemental preparations of predigested nutrients to more complete and complex formulas that mimic oral nutrition intake. Specialized formulas are available for specific health conditions such as diabetes mellitus and compromised renal function. Modular formulas that are not nutritionally complete but add specific nutrients such as protein, fat, and carbohydrate are also available. These preparations can be added to an existing formula to provide additional benefit.

Glutamine, an amino acid, is a key energy source for the gut and has been shown to help maintain gut health and integrity and to protect the gut from damage from radiation and chemotherapy.[29,30] The use of supplemental glutamine in tube feedings in addition to L-arginine and omega-3 fatty acids is gaining popularity. These potentially beneficial nutrients are now available in formulas and as oral supplements. More research needs to be done, however, to thoroughly evaluate the benefits and possible disadvantages.

When a formula is being chosen, the institution nutrition formulary for available preparations, modular formulas, and additions such as glutamine or fiber should be considered. Consideration should also be given to the patient's medical condition, gastrointestinal function, and financial resources.

Transition to Home

A significant number of patients using enteral nutritional support in the hospital are discharged to home while still on therapy. This can be done successfully and requires that the following conditions are met:[29]

  • The patient and/or caregiver is given enough time for education and is proficient in the use of the tubes, site care, and the use of the pump.
  • The patient is discharged to a safe and clean environment.
  • Regular medical follow-up is arranged to ensure appropriate function of the feeding tube and optimization of the nutrition plan.

Parenteral nutrition

Parenteral nutrition may be indicated in select individuals who are unable to use the oral or enteral route (i.e., those who have a nonfunctioning gut), such as those with obstruction, intractable nausea and/or vomiting, short-bowel syndrome, or ileus. Additional inclusive conditions common in the cancer population are severe diarrhea/malabsorption, severe mucositis or esophagitis, high-output gastrointestinal fistulas that cannot be bypassed by enteral intubation, and/or severe preoperative malnutrition.[27,29]

Contraindications for use of parenteral nutrition are a functioning gut, a need for nutritional support for a duration less than 5 days, an inability to obtain intravenous (IV) access, and poor prognosis not warranting aggressive nutritional support.[27,29] Additional conditions that should cause hesitation are the following: patient or caregiver does not want parenteral nutrition, patient is hemodynamically unstable or has profound metabolic and/or electrolyte disturbances, and/or patient is anuric without dialysis.[27,29]

Prospective Assessment

If parenteral nutrition is determined to be beneficial, the two venous access sites are central and peripheral. Cancer patients usually have central IV catheters to accommodate multiple IV therapies. If this is not the case, a peripheral catheter can be placed, although care must be taken to avoid overuse of the peripheral accesses with nutritional support and anticancer therapies. Numerous peripheral infusions and venesections can result in vessel sclerosis. The following discussion highlights both types of access:[27,29]

Central venous catheters

  • May utilize single-, double-, or triple-lumen catheters for delivery of medication, blood and blood products, and parenteral nutrition without interruption.
  • Placement of lines should be done by an experienced surgical team to minimize risk of pneumothorax, hemothorax, hematuria, aneurysms, venous or nerve damage, and microbial contamination. Evaluation of catheter tip location and site care is critically important.
  • Short-term support can be provided via Cordis or Swan Ganz catheters; long-term support can be provided via Hickman or Broviac catheters.

Peripheral venous catheters

  • A short canula is placed in the arm (either the percutaneous subclavian vein in adults or the arteriovenous fistulas are used as access sites).
  • Catheters must be located in peripheral vessels with high blood flow to facilitate rapid dilution of the formula; access may be alternated to avoid thrombophlebitis.
  • Peripherally inserted central catheters (PICC lines) are used for long-term support; the tip of the catheter must be placed in a central vein such as the superior or inferior vena cava to decrease risk of infection and thrombosis.

Solutions

Parenteral nutrition formulas are tailored to individual clinical status and nutritional needs. The formulas contain a combination of amino acids, dextrose, lipids, vitamins, minerals and trace elements, fluids, electrolytes, and, possibly, additives such as insulin, heparin, and antacids.

Solutions running through peripherally placed lines must be altered by reducing the percentage of calories from carbohydrates (hypertonic) and increasing the percentage from lipids (isotonic). Peripheral solutions with a final dextrose concentration lower than 10% and an osmolarity lower than 900 mOsm/kg are generally well tolerated.[27] The mandatory alteration in macronutrients can present problems with delivery of recommended calories/nutrients.

Central infusions are not limited by osmolarity because they use a large vein; this feature makes central venous access a good choice for severely stressed, hypermetabolic individuals and/or individuals requiring a fluids restriction.[27]

Many drugs and compounds are not compatible with parenteral solutions and should not be added to the solutions or even run through parenteral solution-designated lines to avoid the chance of interaction or precipitation. Pharmacists should be consulted in the preparation of parenteral nutrition solutions and before any additional medications or compounds are added.

Complications

Incompatibility with drugs is just one of a number of possible complications associated with parenteral nutrition administration. Complications can be categorized as mechanical (vein thrombosis, pneumothorax, and catheter tip misplacement) or metabolic (hyperglycemia/hypoglycemia, hypokalemia, and elevated liver function tests).[27] Because of the precision that is required to order, administer, and maintain this type of support, trained and experienced medical personnel should be involved. Many facilities have dedicated nutritional support multidisciplinary teams.

Transition to Home

Cancer is one of the most common diagnoses among home parenteral nutrition recipients. The following criteria should be used when assessing the appropriateness of discharge to home on parenteral feeds. The individual must meet the following conditions:[27]

  • Be medically and emotionally stable.
  • Have a relatively long life expectancy (>6 months).
  • Be educated and able to perform the requisite tasks to maintain a sterile access site in a safe and clean environment.
  • Have a long-term access in place and be stable on the formula before being discharged.
  • Have a medical follow-up and support system in place for questions and complications.

Tapering off parenteral nutritional support requires coordination between the medical staff and the patient. Because parenteral support is given continuously, the taper involves a gradual reduction in rate and time. Parenteral nutritional support cannot be abruptly discontinued.

When transitioning to enteral feeds, parenteral support can be decreased to 50% when enteral feeds reach 33% to 50% of the goal rate; it can be discontinued when enteral feeds reach 75% of goal and are tolerated.[27]

When transitioning to oral nutrition, parenteral solutions can be decreased to 50% when the patient is tolerating a full liquid diet or beyond and can be discontinued once solid foods are tolerated in addition to the consumption of adequate fluids.[27]

Both enteral and parenteral nutritional support can be safe and effectively used to help reverse the effects of malnutrition in individuals with cancer. However, nutritional support, particularly parenteral support, is still controversial when used as routine adjuvant therapy to anticancer therapies or when there is an absence of efficacious cancer treatment.[31] Every measure should be employed to sustain an individual and improve his or her condition through oral intake before consideration is given to nutritional support.

Nutritional Suggestions for Symptom Management

Side effects of cancer treatments vary from patient to patient, depending on the type, length, and dose of treatments as well as the type of cancer being treated. This section offers practical suggestions for managing the common symptoms affecting nutrition intake.

Recommendations during treatment may focus on eating foods that are high in energy, protein, and micronutrients to help maintain nutritional status. This may be especially true for individuals with early satiety, anorexia, and alteration in taste, xerostomia, mucositis, nausea, or diarrhea. Under most of these circumstances, eating frequently and including high-energy and high-protein snacks may help overall intake.[25]

Anorexia

Loss of appetite or poor appetite is one of the most common problems that occurs with cancer and its treatment.[32] The cause of anorexia may be multifactorial. Treatment modality, the cancer itself, and psychosocial factors may all play a role in appetite.[32] Eating frequent meals and snacks that are easy to prepare may be helpful. Liquid supplements may improve total energy intake and body function [33] and may work well when eating solids is difficult. Other liquids that contain energy may also help, such as juices, soups, milk, shakes, and fruit smoothies. Eating in a calm, comfortable environment and exercising regularly may also improve appetite.[32]

Suggestions for appetite improvement include the following:[34,35,36]

  • Plan a daily menu in advance.
  • Eat small, frequent, high-calorie meals (every 2 hours).
  • Arrange for help in preparing meals.
  • Add extra protein and calories to food.
  • Prepare and store small portions of favorite foods.
  • Consume one third of daily protein and calorie requirements at breakfast.
  • Snack between meals.
  • Seek foods that appeal to the sense of smell.
  • Be creative with desserts.
  • Experiment with different foods.
  • Perform frequent mouth care to relieve symptoms and decrease aftertastes.

What types of foods are usually recommended?

  • Cheese and crackers.
  • Muffins.
  • Puddings.
  • Nutritional supplements.
  • Milkshakes.
  • Yogurt.
  • Ice cream.
  • Powdered milk added to foods such as pudding, milkshakes, or any recipe using milk.
  • Finger foods (handy for snacking) such as deviled eggs, cream cheese or peanut butter on crackers or celery, or deviled ham on crackers.
  • Chocolate.

See the National Cancer Institute (NCI) Web site [32] for recipes such as Lactose-Free Double Chocolate Pudding Recipe to Help with Lactose Intolerance, Banana Milkshake Recipe to Help with Appetite Loss, and Fruit and Cream Recipe to Help with a Sore Mouth. For a free copy of this booklet, call the Cancer Information Service at 1-800-4-CANCER (1-800-422-6237).

Alterations of taste and smell

Alterations in taste can be related to unknown effects of cancer, radiation treatment, dental problems, mucositis and infection (thrush), or medications. Cancer patients undergoing chemotherapy frequently report changes in their sense of taste, specifically a bitter taste sensation during administration of the cytotoxic drugs.[37] One study measured the taste thresholds among cancer patients under chemotherapy compared with controls.[38] In this study, 62% of patients complained of taste disorders associated with the chemotherapy medications. Taste dysfunction can result in food avoidance, inducing weight loss and anorexia, all of which can have significant consequences on patients' quality of life. Simply changing the types of foods eaten as well as adding additional spices or flavorings to foods may help. Citrus may be tolerated well if no mouth sores or mucositis is present. Rinsing the mouth before eating may help improve the taste of food.[32]

While undergoing cancer therapy, patients may experience taste changes or develop sudden dislikes for certain foods. Their sense of taste may return partially or completely, but it may be a year after therapy ends before their sense of taste is normal again. A randomized clinical trial found that zinc sulfate during treatment may be helpful in expediting the return of taste after head and neck irradiation.[39][Level of evidence: I]

Suggestions for helping cancer patients manage taste changes include the following:

  • Eat small, frequent meals and healthy snacks.
  • Be flexible. Eat meals when hungry rather than at set mealtimes.
  • Use plastic utensils if foods taste metallic.
  • Try favorite foods.
  • Plan to eat with family and friends.
  • Have others prepare the meal.
  • Try new foods when feeling best.
  • Substitute poultry, fish, eggs, and cheese for red meat.
  • A vegetarian or Chinese cookbook can provide useful nonmeat, high-protein recipes.
  • Use sugar-free lemon drops, gum, or mints when experiencing a metallic or bitter taste in the mouth.
  • Add spices and sauces to foods.
  • Eat meat with something sweet, such as cranberry sauce, jelly, or applesauce.

Xerostomia

Xerostomia (dry mouth) is most commonly caused by radiation therapy that is directed at the head and neck.[35] A number of medications may also induce xerostomia. Dry mouth may affect speech, taste sensation, ability to swallow, and use of oral prostheses. There is also an increased risk of cavities and periodontal disease because less saliva is produced to cleanse the teeth and gums.

A primary method of coping with xerostomia is to drink plenty of liquids (25–30 mL/kg per day) and eat moist foods with extra sauces, gravies, butter, or margarine.[25,36,40] In addition, hard candy, frozen desserts such as frozen grapes, chewing gum, flavored ice pops, and ice chips may be helpful.[32] Oral care is very important to help prevent infections. Irradiation to the head and neck of a patient who has permanent dry mouth symptoms may result in reduced intake of energy, iron, zinc, selenium, and other key nutrients.[41][Level of evidence: II] Special efforts should be made to help tailor meals and snacks for individuals with xerostomia.

Suggestions for lessening or alleviating dry mouth include the following:[36]

  • Perform oral hygiene at least 4 times per day (after each meal and before bedtime). (Refer to the Routine Oral Hygiene Care section of the PDQ summary on Oral Complications of Chemotherapy and Head/Neck Radiation for more information.)
  • Brush and rinse dentures after each meal.
  • Keep water handy at all times to moisten the mouth.
  • Avoid rinses containing alcohol.
  • Consume very sweet or tart foods and beverages, which may stimulate saliva.
  • Drink fruit nectar instead of juice.
  • Use a straw to drink liquids.

(Refer to the PDQ summary on Oral Complications of Chemotherapy and Head/Neck Radiation for more information on xerostomia.)

Mucositis/stomatitis

Stomatitis, or a sore mouth, can occur when cells inside the mouth, which grow and divide rapidly, are damaged by treatment such as bone marrow transplantation, chemotherapy, and radiation therapy. These treatments may also affect rapidly dividing cells in the bone marrow, which may make patients more susceptible to infection and bleeding in their mouth. By carefully choosing foods and by taking good care of their mouths, patients can usually make eating easier.[42,43,44] Individuals who have mucositis, mouth sores, or tender gums should eat foods that are soft, easy to chew and swallow, and nonirritating.[32] Some conditions may require processing foods in a blender. Irritants may include acidic, spicy, salty, and coarse-textured foods. A pilot study found that oral glutamine swishes might be helpful in reducing the duration and severity of mucositis.[45][Level of evidence: I] Glutamine may also reduce the duration and severity of stomatitis during cytotoxic chemotherapy.[45,46][Level of evidence: I]

Suggestions for people with cancer who are experiencing stomatitis include the following:

  • Eat soft foods that are easy to chew and swallow, including bananas and other soft fruits; applesauce; peach, pear, and apricot nectars; watermelon; cottage cheese; mashed potatoes; macaroni and cheese; custards; puddings; gelatin; milkshakes; scrambled eggs; oatmeal or other cooked cereals; pureed or mashed vegetables such as peas and carrots; and pureed meats.
  • Avoid foods that irritate the mouth, including citrus fruits and juices such as orange, grapefruit, or tangerine; spicy or salty foods; and rough, coarse, or dry foods, including raw vegetables, granola, toast, and crackers.
  • Cook foods until soft and tender.
  • Cut foods into small pieces.
  • Use a straw to drink liquids. Eat foods cold or at room temperature; hot and warm foods can irritate a tender mouth.
  • Practice good mouth care, which is very important because of the absence of the antimicrobial effects of saliva.
  • Increase the fluid content of foods by adding gravy, broth, or sauces.
  • Supplement meals with high-calorie, high-protein drinks.
  • Numb the mouth with ice chips or flavored ice pops.

(Refer to the PDQ summary on Oral Complications of Chemotherapy and Head/Neck Radiation for more information on mucositis.)

Nausea

Nausea can affect the amount and types of food eaten during treatment. Eating before treatment is important, as well as finding foods that do not trigger nausea. Frequent triggers for nausea include spicy foods, greasy foods, or foods that have strong odors.[32] Once again, frequent eating, and slowly sipping on fluids throughout the day may help.

Additional eating suggestions include the following:[19]

  • Eat dry foods such as crackers, breadsticks, or toast, throughout the day.
  • Sit up or recline with a raised head for 1 hour after eating.
  • Eat bland, soft, easy-to-digest foods rather than heavy meals.
  • Avoid eating in a room that has cooking odors or is overly warm; keep the living space comfortable but well ventilated.
  • Rinse out the mouth before and after eating.
  • Suck on hard candies such as peppermints or lemon drops if the mouth has a bad taste.

(Refer to the PDQ summary on Nausea and Vomiting for further information.)

Diarrhea

Radiation, chemotherapy, gastrointestinal surgery, or emotional distress can result in diarrhea. Avoiding hyponatremia, hypokalemia, and dehydration during episodes of diarrhea requires the intake of additional oral fluids and electrolytes. Broth, soups, sports drinks, bananas, and canned fruits may be helpful for the replenishment of electrolytes. Diarrhea may worsen with greasy foods, hot or cold liquids, or caffeine.[32] In the presence of radiation enteritis, fibrous foods—especially dried beans and cruciferous vegetables—may contribute to frequent stools.[47] Meal planning should be individualized to meet nutritional needs and tolerances. Oral glutamine may also help prevent intestinal toxicity from fluorouracil.[48][Level of evidence: I]

Additional suggestions include the following:[19]

  • Drink plenty of fluids through the day; room-temperature fluids may be better tolerated.
  • Limit milk to 2 cups or eliminate milk and milk products until the source of the problem is determined.
  • Limit gas-forming foods and beverages such as soda, cruciferous vegetables, legumes and lentils, and chewing gum.
  • Limit the use of sugar-free candies or gum made with sugar alcohol (sorbitol).
  • Drink at least 1 cup of liquid after each loose bowel movement. (Refer to the Impaction section of the PDQ summary on Gastrointestinal Complications for more information.)

(Refer to the PDQ summary on Gastrointestinal Complications for more information on diarrhea.)

Neutropenia

People with cancer may have a low white blood cell count for a variety of reasons, some of which include radiation therapy, chemotherapy, or the cancer itself. Patients who have a low white blood cell count are at an increased risk for developing an infection.[49] Suggestions for helping people prevent infections related to neutropenia include the following:

  • Check expiration dates on food and do not buy or use if the food is out of date.
  • Do not buy or use food in cans that are swollen, dented, or damaged.
  • Thaw foods in the refrigerator or microwave—never thaw foods at room temperature.
  • Cook foods immediately after thawing.
  • Refrigerate all leftovers within 2 hours of cooking and eat them within 24 hours.
  • Keep hot foods hot and cold foods cold.
  • Avoid old, moldy, or damaged fruits and vegetables.
  • Avoid tofu in open bins or containers.
  • Cook all meat, poultry, and fish thoroughly; avoid raw eggs or raw fish.
  • Buy individually packaged foods, which are better than larger portions that result in leftovers.
  • Use caution when eating out—avoid salad bars and buffets.
  • Limit exposure to large groups of people and people who have infections.
  • Wash hands frequently to prevent the spread of bacteria.

This list may be modified after chemotherapy or when blood count returns to normal.

Hydration and dehydration

Adequate hydration is critically important for health maintenance. There are several common scenarios found in cancer treatment that may lead to altered hydration status and electrolyte imbalance. Hydration status can become compromised with prolonged disease or treatment-related diarrhea and/or episodes of nausea and vomiting.[50] Acute and chronic pain can also adversely affect the appetite and hence the desire to eat and drink. Fatigue, an all-too-common complaint of people with cancer, can be one of the first signs of dehydration.[51] Once the underlying cause for altered hydration is appropriately managed, some suggestions to promote adequate hydration include the following:[32,52,53]

  • Drink 8 to 12 cups of liquids a day; take a water bottle whenever leaving home. It is important to drink even if not thirsty, as the thirst sensation is not a good indicator of fluid needs.
  • Add food to the diet that contains a significant portion of fluid, such as soup, flavored ice pops, flavored ices, and gelatins.
  • Limit consumption of caffeine-containing products, including colas and other caffeinated sodas, coffee, and tea (both hot and cold); these foods may not be as nourishing as noncaffeinated beverages.
  • Drink most liquids after and/or between meals to increase overall consumption of both liquids and solids.
  • Use antiemetics for relief from nausea and vomiting; antiemetic use can be very helpful and may prevent hospital admissions from dehydration. The classes of available antiemetics include anticholinergics, phenothiazines, antihistamines, butyrophenones, benzamides, and serotonin receptor antagonists. Of note, all of these antiemetics have side effects that many individuals would consider less problematic than nausea and vomiting.

Constipation

Constipation is defined as fewer than three bowel movements per week.[54] It is a very common problem among individuals with cancer and may result from lack of adequate fluids or dehydration, lack of fiber in the diet, physical inactivity or immobility, anticancer therapies such as chemotherapy, and medications used in the treatment of side effects of anticancer therapy such as antiemetics and opioids.[54,55][Level of evidence: I] In addition, commonly used pharmacologic agents such as minerals (calcium, iron), nonsteroidal anti-inflammatory drugs, and antihypertensives can cause constipation.[54]

An effective bowel regimen should be in place before the problem of constipation occurs. Preventive measures should be common practice, and special attention should be paid to the possibility of constipation as a side effect of certain therapies. Suggestions include the following:[52,54]

  • Eat more fiber-containing foods on a regular basis. The recommended fiber intake is 25 to 35 grams per day. Fiber should be gradually added to the diet, and adequate fluids must be consumed at the same time (see list below).
  • Drink 8 to 10 cups of fluid each day; beverages such as water, prune juice and warm juices, decaffeinated teas, and lemonade can be particularly helpful.
  • Take walks and exercise regularly (proper footwear is important).

If prevention does not work and constipation is a problem, the application of a three-pronged approach for treatment is suggested: diet (fiber and fluids), physical activity, and over-the-counter or prescription medication. The use of biofeedback or surgery may also be considered.[56]

Suggestions are as follows:[15,52,54,56,57]

  • Continue to eat high-fiber foods and drink adequate fluids. Try adding wheat bran to the diet; begin with 2 heaping tbsp each day for 3 days, then increase by 1 tbsp each day until constipation is relieved. DO NOT EXCEED 6 TBSP PER DAY.
  • Maintain physical activity.
  • Include over-the-counter treatments if necessary. This refers to bulk-forming products (e.g., psyllium, methylcellulose [Citrucel], psyllium hydrophilic mucilloid [Metamucil (if adequate hydration is tolerated), Fiberall], calcium polycarbophil [FiberCon, Fiber-Lax]); stimulants (e.g., bisacodyl [Dulcolax] tablets or suppositories, glycerin suppositories, and calcium salts of sennosides [Senokot]); stool softeners (e.g., docusate sodium [Colace] and docusate calcium [Surfak]); and osmotics (e.g., milk of magnesia, lactulose, and magnesium sulfate/Epsom salts). Cottonseed and aerosol enemas can also help relieve the problem. Lubricants such as mineral oil would be included in this group but are NOT recommended because of the potential for binding and preventing absorption of essential nutrients.

Good sources of fiber include the following:[19,52]

  • 4+ grams per ½ cup cooked serving.
    • Legumes.*
      • Kidney beans.
      • Navy beans.
      • Garbanzo beans.
      • Lima beans.
      • Split peas.
      • Pinto beans.
      • Lentils.
  • 4+ grams per designated unit.
    • Corn (½ cup).
    • Pears with skin (medium piece of fruit).
    • Popcorn (3 cups popped).
  • 4+ grams per 1 oz serving.
    • Whole-grain cereals (cold).
    • Bran cereals (cold).
  • 4+ grams per 1/3 cup serving, dry.
    • Oatmeal.
    • Oat bran.
    • Grits.
  • 2+ grams per ½ cup cooked or 1 cup raw serving.
    • Asparagus.
    • Green beans.
    • Broccoli.*
    • Cabbage.*
    • Carrots.
    • Cauliflower.
    • Greens.
    • Onions.
    • Peas.
    • Spinach.
    • Squash.
    • Green peppers.
    • Celery.
    • Canned tomatoes.
  • 2+ grams per ½ cup serving or medium piece of fruit.
    • Apples with the skin.
    • Bananas.
    • Oranges.
    • Strawberries.
    • Peaches.
    • Blueberries.
  • 2 grams per slice or designated serving size.
    • Whole wheat bread.
    • Whole grain bagel.
    • Pita (½ portion).
    • Whole-grain crackers.

*These food items may cause gas; products containing alpha-galactosidase enzyme may be helpful.

References:

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46. Anderson PM, Schroeder G, Skubitz KM: Oral glutamine reduces the duration and severity of stomatitis after cytotoxic cancer chemotherapy. Cancer 83 (7): 1433-9, 1998.
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57. Schiller LR: Review article: the therapy of constipation. Aliment Pharmacol Ther 15 (6): 749-63, 2001.

Other Nutrition Issues

Nutrition in Advanced Cancer

Advanced cancer is often associated with cachexia.[1,2,3,4] Individuals diagnosed with cancer may develop new, or worsening, nutrition-related side effects as cancer becomes more advanced. The most prevalent symptoms in this population are the following:[1,2,3]

  • Weight loss.
  • Early satiety.
  • Bloating.
  • Anorexia.
  • Constipation.
  • Xerostomia.
  • Taste changes.
  • Nausea.
  • Vomiting.
  • Dysphagia.

As defined by the World Health Organization, palliative care is an approach that improves the quality of life of patients and their families facing the problems associated with life-threatening illness, through the prevention and relief of suffering by means of early identification and impeccable assessment and treatment of pain and other problems, physical, psychosocial, and spiritual. The goal of palliative care is to give relief of symptoms that are bothersome to the patient. Although some of the symptoms listed above can be effectively treated, anorexia, though common, is a symptom that is often not noted as problematic for most terminally ill patients but is distressing to most family members; this distress may vary according to cultural factors. Several studies have demonstrated that terminally ill patients lack hunger, and of those who did experience hunger, the symptom was relieved with small amounts of oral intake.[5]

Decreased intake, especially of solid foods, is common as death becomes imminent. Individuals usually prefer and tolerate soft-moist foods and refreshing liquids (full and clear liquids). Those who have increased difficulty swallowing have less incidence of aspiration with thick liquids than with thin liquids.

Dietary restriction is not usually necessary, as intake of prohibited foods (e.g., sweets in the diabetic patient) is insufficient to be of concern.[6] As always, food should continue to be treated and viewed as a source of enjoyment and pleasure. Eating should not just be about calories, protein, and other macronutrient and micronutrient needs.

Diet restrictions are sometimes appropriate, however.[6,7] For example, people with pancreatic cancer, gynecologic cancer, abdominal carcinomatosis, pelvic masses, or retroperitoneal lymph node masses may have bowel obstruction less frequently when adhering to a prophylactic soft diet (i.e., no raw fruits and vegetables, no nuts, no skins, no seeds). Any restriction should be considered in terms of quality of life and the patient's wishes.

Decisions regarding nutritional support should be made with the following considerations:

  • Will quality of life be improved?
  • Do the potential benefits outweigh the risks/costs?
  • Is there an advance directive?
  • What are the wishes and needs of the family?

The benefit of home parenteral nutrition in patients with advanced cancer is often debated, and evidence-based data regarding its use are lacking. For patients who still have good quality of life but also have mechanical or physiologic barriers to achieving adequate nourishment and hydration orally (e.g., head and neck cancer), prolonged survival may be achieved with the use of enteral or parenteral nutrition.[5] In a qualitative study, 13 patients and 11 family members perceived some benefits with home parenteral nutrition.[8] The most salient positive feature of home parenteral nutrition was a sense of relief and security that nutritional needs were met. In this study, patients were also able to take oral nutrition, and the administration of total parenteral nutrition was often described as a complement to the patients' oral intake. This contradicts the traditional indication for TPN, i.e., that its use be reserved for times when nourishment via the gastrointestinal tract is not possible. Patients in this study also had regular visits by home health care providers, which could have had a positive impact on their physical, social, and psychological well-being.

Although most patients with advanced cancer will not benefit from artificial nutrition, for someone who still has good quality of life but also has mechanical or physiologic barriers to achieving adequate nourishment and hydration orally (e.g., head and neck cancer), prolonged survival can be achieved with the use of enteral or parenteral nutrition.[5]

All people with cancer and their caregivers have the right to make informed decisions. The healthcare team, with guidance from the registered dietitian, should inform patients and their caregivers about the pros and cons of using nutritional support in advanced disease. Despite the lack of proven benefit, artificial nutrition at the end of life will remain a sensitive topic for some patients and families.[5] In most cases, the cons outweigh the pros. The following is a list of the pros and cons of using nutritional support in advanced disease:[6,7,9]

Pros and Cons of Enteral Nutritional Support

  • Pros:
    • May improve alertness.
    • May provide comfort to the family.
    • May decrease nausea.
    • May decrease hopelessness and fears of abandonment.
  • Cons:
    • May increase secretions.
    • Diarrhea/constipation.
    • May increase nausea.
    • Surgery with gastrostomy or jejunostomy.
    • Risk of aspiration or pneumonia.
    • Risk of infection.
    • Greater burden on caregiver.

Drug-nutrient Interactions

Individuals being treated for cancer may require the use of a series of curative or supportive drugs throughout their care; they may also receive advice on the use of dietary supplements, or they may self-diagnose and self-prescribe the use of dietary supplements. Drug-nutrient interactions or dietary supplement-drug-nutrient interactions can occur and can compromise the safety and efficacy of the anticancer treatment plan. A review of antineoplastic drugs listed in various references revealed the interactions listed in Table 2.[10]

Table 2. Antineoplastic Drug-Nutrient Interactions

Trade Name Generic Name Food Interactions
MAOI = monoamine oxidase inhibitor.
Targretin bexarotene Grapefruit juice may increase drug concentration and toxicities.
Folex methotrexate Alcohol may increase hepatotoxicity.
Rheumatrex
Mithracin plicamycin Supplements containing calcium and vitamin D may decrease effect.
Matulane procarbazine This chemotherapy is a mildMAOI; a low-tyramine diet should be followed.
Temodar temozolomide Food may decrease drug rate and absorption.

Nutrition and Survivorship

Survivors of cancer represent a population at risk for many nutrition-related morbidities, suggesting that programs aimed at lifestyle modification could be clinically applicable and beneficial.[11] Research among survivors has focused on stages of and barriers to behavioral change and has included multidisciplinary lifestyle interventions. Lifestyle behaviors that are part of a multidisciplinary approach that includes dietary guidance, exercise, and stress management are more likely to result in success over the long term.

Lifestyle behaviors in adult and pediatric survivors of cancer

A number of surveys evaluating lifestyle practices among survivors of adult and childhood cancer have been published. One of the first studies explored lifestyle habits among 978 individuals who had been diagnosed with breast or prostate cancer.[12] Forty-seven percent of breast cancer survivors and 35% of prostate cancer survivors reported consuming the recommended daily number of servings of fruits and vegetables. Whites were more inclined to eat the recommended number of fruits and vegetables than were African Americans (P = .006). Sixty-nine percent of participants followed a low-fat diet.[12]

In a second prospective cohort study, variations in dietary patterns among 1,901 women with early-stage breast cancer were evaluated for effect on breast cancer recurrence and survival.[13] Women aged 18 to 79 years who were diagnosed with breast cancer within the previous 11 to 39 months were surveyed. Dietary intake was assessed by using the Fred Hutchinson Cancer Research Center Food Questionnaire and by inquiring about dietary intake over the previous year. Healthy dietary patterns were defined by intake of foods typical of a cancer prevention diet and included assessing consumption of cruciferous vegetables, fruits, legumes, onions, and lean meats.[13]

A statistically significant relationship was observed in women who were more physically active (P < .0001) and who gained less weight 1 year before diagnosis (P = .04).[13] Unhealthier dietary patterns that included consumption of red meat, processed meat, creamy soups, butter, refined grains, and sweets were more likely followed by women who:

  • Had a higher body mass index (BMI) at enrollment (P < .0001).
  • Had a history of smoking (P = .04).
  • Gained more weight the year before diagnosis (P = .0002).

Decreased risk of overall death (P trend = .05) and death from noncancer causes (P trend = .02) was observed among women who followed healthier dietary habits. No relationship between dietary patterns and death from breast cancer or recurrence of breast cancer was observed.[13]

Finally, a smaller study explored the effects of dietary habits and exercise patterns on cancer-related late effects, social support, and stressful events in long-term survivors of breast cancer.[14] Of the 227 women surveyed:

  • 58% reported making healthy lifestyle changes after their diagnosis of cancer.
  • 32% reported increased exercise.
  • 44% reported decreasing fat intake.
  • 42% reported increasing fiber intake.
  • 43% reported increasing their intake of fruits and vegetables.

Survivors who adopted an exercise regimen reported decreased fatigue (P = .03). Women who increased their fruit and vegetable intake also reported decreased fatigue (P = .08). No significant effect on symptoms of depression, anxiety about breast cancer, sexual satisfaction, or body satisfaction was reported. Survivors who had a social support system were more inclined to adopt an exercise regimen (P = .06).[14]

Few studies have explored lifestyle habits among survivors of childhood cancer. One survey (N = 380) reported the following:[15]

  • 79% of survivors of childhood cancer did not meet the guidelines for fruit and vegetable consumption.
  • 84% obtained more than 30% of their calories from fat.
  • 48% were meeting exercise guidelines.

A subsequent survey of 144 survivors of childhood cancer explored barriers to consuming healthy foods.[16] Barriers to adopting healthier lifestyle habits included the following:

  • Being too tired (57%).
  • Being too busy (53%).
  • Not belonging to a gym (48%).
  • The visual appeal of fattier foods (58%).
  • The typical consumption of high-fat foods in social situations (50%).
  • Lack of knowledge about choosing healthier options (a major barrier).

A survey conducted of 72 survivors of childhood cancer found similar results.[17] In this survey, none of the participants reported adhering to cancer prevention guidelines.

The results of the surveys described above suggest that survivors of cancer are not adhering to cancer prevention guidelines and are engaging in lifestyle behaviors that may further increase their risk of late effects. Survivors who engage in at-risk lifestyle behaviors are likely to accelerate the progression of some late effects. Given the increased vulnerability to disease among survivors of cancer, this group uniquely represents a high-risk population for whom intervention strategies can be optimally applied and tested. Interventions that educate survivors about modifying risky lifestyle behaviors and that promote self-efficacy may be effective strategies for lowering the risk of late effects.

Intervention trials among survivors of cancer

The growing population of survivors has fueled awareness about the unique needs for effective lifestyle intervention programs specifically designed for survivors of cancer. As highlighted by the literature, most survivors of cancer are not following cancer prevention guidelines. A number of trials have aimed to modify lifestyle behaviors, with the goal of minimizing the risk of developing late effects or decreasing the odds of recurrence. A summary of select intervention studies is presented below.

Breast cancer

The association between increased fat intake and increased breast cancer recurrence coupled with an increase in the survivor population among breast cancer patients led to the development of two National Cancer Institute–funded trials evaluating dietary patterns and the effects of dietary intake of fat on breast cancer recurrence.

The Women's Intervention Nutrition Study (WINS) (N = 2,437) was the first large-scale trial that explored the effects of dietary intervention on survival, relapse, or recurrence in women with breast cancer.[18] The primary outcome measure of this trial was the effect of a low-fat diet on relapse-free survival among women who were within 1 year of diagnosis with breast cancer. In this study, subjects were counseled to reduce fat intake to 15% of total energy intake while maintaining a nutritionally balanced diet. Exercise was not a component of the intervention.

WINS participants maintained a favorable response rate at year 1: 86% for the intervention group and 91% for the control group. However, at year 5 the response rate decreased to 39% for the intervention group and 44% for the control group. A significant reduction in weight loss was observed at months 12, 24, 36, 48, and 60, compared to baseline (P < .0001).[18]

The study did not find that adoption of a low-fat diet had an effect on overall survival, relapse, or recurrence. An exploratory analysis revealed a beneficial effect among women with estrogen receptor–negative breast cancer. In this group, adherence to a low-fat diet increased relapse-free survival in the intervention group, compared with controls (P < .034).[18] WINS was limited by its sole reliance on self-reported data and by most patients being white and having advanced degrees, thereby limiting the generalizability of the study.

The Women's Healthy Eating and Living (WHEL) Study (N = 3,088) explored the effect of a dietary intervention promoting daily consumption of five vegetable servings plus 16 oz of vegetable juice, three fruit servings, and 30 g of fiber, with fat comprising 15% to 20% of energy intake.[19] The primary outcome measures were cancer recurrence or new primary breast cancer and death from any cause.

The intervention arm included a series of telephone counseling sessions combined with 12 cooking classes held during the first year of the study, along with monthly newsletters tailored to the individuals. The control arm received education about the "5-A-Day" diet, attended an average of one of four cooking classes in the first year, and received 24 newsletters tailored to them. Objective data were also collected in this study. Plasma concentration of nutrients was obtained at 12, 48, and 72 months. Participants were monitored for 7 years, with response rates at 77.9% in the intervention arm and 86.2% in the control arm at 72 months.[19]

Participants in the intervention arm of the WHEL Study significantly increased their vegetable consumption, from 3.9 servings per day at baseline to 5.8 servings per day at 72 months. Fruit intake went from 3.5 to 3.4 servings per day. The control arm reported decreased intake of fruits, from 3.4 to 2.6 servings per day, and of vegetables, from 3.8 to 3.6 servings per day. No significant effect on dietary fat intake as a percentage of total calories or fiber was observed in the intervention group.[19] In concordance with WINS, no effect on overall survival or cancer recurrence was observed. A nested case-control analysis revealed that women who were hot flash negative at recruitment experienced a significantly decreased risk of cancer recurrence (P = .002).[20]

While both WINS and the WHEL Study found that nutrition education can produce sustained dietary change among survivors of cancer, neither trial found significant effects on primary study outcomes. It is important to recognize that these studies evaluated slightly different questions.[21] WINS focused more on the effects of a low-fat diet based on data correlating breast cancer with fat and circulating estrogen levels, while the WHEL Study evaluated a comprehensive diet change that included fruits, vegetables, decreased fat, and increased fiber.

These studies demonstrate that distance medicine–based nutrition education is effective at instituting change. However, the clinical benefit of these studies remains to be seen. WINS and the WHEL Study differ slightly in the following ways:

  • The WHEL Study recruited women from a wider age range (18 to 70 years vs. 48 to 79 years for WINS) and included more women with larger tumor burden and increased nodal activity.
  • The WHEL Study excluded women with cancers that recurred within the first 2 years of diagnosis, whereas women recruited to WINS were undergoing conventional therapy while also adopting dietary changes.
  • The WHEL Study recruited women within 4 years of diagnosis, whereas WINS recruited women within 1 year of diagnosis.

As highlighted by the author, the WHEL Study undersampled individuals who experienced recurrence within 4 years of diagnosis.[21]

WINS and the WHEL Study are limited in their generalizability because most participants were white and had higher levels of formal education. It is unknown whether the nutrition education interventions would be effective in ethnically diverse populations, low-income households, or individuals with low levels of education.

Only one study has explored the effects of a diet-plus-spirituality education intervention in a nonwhite population of survivors of breast cancer.[22] The investigators hypothesized that the addition of a spiritual component would provide further support to dietary change. Participants were obese (BMI 30–45) African American women aged 18 to 70 years who had been diagnosed with breast cancer in the 10 years before recruitment. Individualized dietary counseling was provided by a registered dietician for 18 months. Counseling sessions were provided in person at baseline, 6 months, and 12 months, with interim telephone counseling. Participants also received coupons for free attendance at Weight Watchers meetings between visits to the registered dietician.[22]

Participant dietary and exercise goals included the following:

  • Decrease fat to 20% to 25% of calories.
  • Maintain protein at 20% of calories.
  • Choose whole grains for at least half of their daily grain intake.
  • Eat at least six to eight servings of fruits and vegetables daily.
  • Exercise for at least 30 minutes per day, at least 5 days per week.

Spiritual counseling focused on issues relevant to weight loss and was conducted by telephone weekly for 3 months, biweekly for 3 months, and then monthly. Objective assessments were collected at baseline, 6 months, 12 months, and 18 months. Thirty-one subjects were recruited to the study; however, five subjects did not meet the 6-month benchmark. At month 6, 24 subjects were randomly assigned to receive dietician-led counseling with or without spiritual counseling. Of the 24 women, 11 subjects in each arm completed the study.

No significant differences in weight loss were observed between the two groups. The spirituality group reported a larger increase in fruit consumption (2.5 servings per day) than did the dietician-only group (1.1 servings per day) and improved quality of life.[22]

Endometrial cancer

One small study has investigated a lifestyle modification program that included nutrition and exercise education for 45 obese or overweight women with endometrial cancer.[23] Participants were randomly assigned to a 6-month intervention or usual care. The intervention group met weekly for 6 weeks, biweekly for 1 month, and then monthly thereafter.

The study's primary endpoint was weight change. Secondary endpoints were leisure activity and nutrition analysis, as measured by 3-day food records. Overall attrition to the study was 16%: 10% in the usual care group, compared with 22% in the intervention group. At 12 months, the intervention group had lost 3.5 kg, compared with a 1.4-kg gain in the usual care group (P = .018). Leisure scores increased for the intervention group, compared with the control group (P = .002).[23]

Although these results may be encouraging, this study is limited by the small sample and high drop-out rate in the intervention group. The high attrition rate in the intervention group calls into question the feasibility of this intervention in a larger setting.

Breast and prostate cancer

In another large study (N = 543), FRESH START explored the effects of nutrition education coupled with exercise intervention in individuals with prostate cancer or breast cancer.[24] FRESH START recruited individuals who were within 9 months of the diagnosis of breast or prostate cancer. The 10-month intervention trial included tailored printed education materials targeting behaviors to:

  • Consume five or more servings of fruits and vegetables per day.
  • Reduce total fat intake to 30% of total caloric intake.
  • Increase exercise to at least 150 minutes per week.

The primary outcome measure was the percentage of patients who achieved goal behavior in at least two of the three behavioral domains.

After 1 year, a significant difference between the two arms in goal behaviors was observed, with 34% of subjects adopting two or more behaviors in FRESH START (P < .001) and 18% of subjects in the attention-control arm adopting change. Improvement in diet and exercise resulted in a significant loss of weight.[24] This study did not explore the effects of dietary change on cancer recurrence or overall mortality.

FRESH START was one of the first studies to document significant improvements in fruit and vegetable consumption through a distance medicine–based educational program. One of the strengths of FRESH START was that it was a tailored intervention program; such interventions may be particularly effective at reaching a geographically scattered population, as the rate of attrition in this study was quite low.

As seen in the other behavioral studies described in this section, FRESH START was limited in that most survivors were white and had more years of formal education. It is unknown whether these types of lifestyle interventions would be effective in other patient populations.

Mixed cancer

The Reach out to ENhancE Wellness (RENEW) trial was a distance medicine–based nutrition and exercise intervention program that consisted of a personally tailored workbook and a series of quarterly newsletters, along with a program of telephone counseling and automated prompts (15 sessions and 8 prompts over the 12-month period).[25] Eligible participants were survivors of breast, prostate, or colorectal cancer for 5 years or longer, had BMIs between 25 and 39.9, and were at least 65 years old.

The primary outcome measure was change in functional status between baseline and 12 months. The goals of intervention included having subjects:

  • Engage in 15 minutes of strength training every other day.
  • Engage in 30 minutes of endurance exercises every day.
  • Consume at least seven servings (for women) or nine servings (for men) of fruits and vegetables every day.
  • Limit consumption of saturated fat to less than 10% of total energy intake.
  • Attain a 10% weight loss during the 12-month period.

At 12 months, significant differences in the change scores between the intervention and control groups were observed for the following outcomes:[25]

  • Strength training (P < .001).
  • Duration of endurance training (P = .003).
  • Strength training frequency (P < .001).
  • Daily number of servings of fruits and vegetables (P < .001).
  • Daily intake of saturated fat (P < .001).

At 12 months, more participants in the intervention group met the recommendations for the following outcomes:

  • Strength training (P < 0.001).
  • Endurance exercise (P = .07).
  • Fruit and vegetable servings (P < .001).
  • Saturated fat guidelines (P = .001).

As with most of the studies described in this section, the RENEW trial was limited in its generalizability. The population was primarily white and had at least some college education. Significant differences were also observed in respondents compared with nonrespondents:

  • Participants were younger.
  • There were more women than men.
  • There were fewer cases of colorectal cancer.
  • Time at recruitment was closer to diagnosis.

As in WINS, all outcome assessments were based on self-report; no objective measures were collected in RENEW.

Childhood cancer

The only intervention aimed at survivors of childhood cancer has been a small pilot study of 13 children aged 4 to 10 years who were in the maintenance phase of therapy for acute lymphoblastic leukemia.[26] This study explored the feasibility of a 12-month home-based nutrition and exercise intervention program. Children were randomly assigned to the intervention group or the control group. The primary objectives of the program were to increase physical activity and to improve dietary patterns.

A physical activity pyramid for youth and the U.S. Department of Agriculture (USDA) Food Guide Pyramid provided the foundation for exercise and nutrition recommendations. The control group received standard recommendations to eat a well-balanced diet and perform activity as tolerated (essentially, standard of care).

Three-day activity records and 2-day food records were completed on a monthly basis by parents. Objective measures of progress were obtained through fitness tests conducted at baseline and at 3, 6, 9, and 12 months. Anthropometric measures and BMIs were obtained at baseline and every 3 months.

No significant differences were observed at 3, 6, and 12 months in any of the nutrition-related parameters. Improvements in physical activity and cardiovascular fitness were observed in the intervention group, compared with controls. Activity levels were higher for the intervention group than for controls (P = .05); however, improvements in fitness assessments did not differ between groups at 6 or 12 months.[26]

Recommendations for patients/clinical applications

Special attention and research should be focused on nutrition and lifestyle behaviors among survivors of cancer, who are at increased risk of many nutrition-related and lifestyle-related late effects.

The studies described in this section provide clear evidence that distance medicine–based lifestyle education programs that include nutrition counseling with or without exercise counseling are effective at promoting behavioral change among survivors of cancer. On the basis of two large studies of survivors of breast cancer, it seems prudent to recommend a low-fat, healthy diet to survivors who have estrogen receptor–negative breast cancer or who are symptomatic at diagnosis.

On the basis of available evidence, the effect of a low-fat diet or healthy diet on recurrence of breast cancer among women diagnosed with other stages of breast cancer is not conclusive. However, although diet may not prevent breast cancer recurrence, the data do not refute the importance of a healthy diet for minimizing the development of nutrition-related late effects such as obesity, heart disease, and metabolic syndrome. When counseling survivors of breast cancer, nutrition educators should highlight the global benefits and importance of a healthy diet. As more survivors enter ongoing research protocols, future studies may reveal that dietary change may play a more prominent role in preventing late effects when compared with preventing recurrence or second malignancies.

Guidelines for Healthy Eating

Health agencies and disease prevention organizations have developed diet and lifestyle guidelines for the public. These recommendations have been created for healthy individuals and are not based on the unique needs of survivors of cancers. More information about these guidelines may be found at U.S. Department of Agriculture's (USDA's) MyPlate and in the USDA and U.S. Department of Health and Human Services Dietary Guidelines for Americans, 2010.[27]

Cancer Prevention Dietary Guidelines

The American Cancer Society (ACS) Guidelines on Nutrition and Physical Activity for Cancer Prevention,[28] first published in 1996, provide more detailed dietary advice with a focus on cancer prevention. These guidelines, updated in 2006, are consistent in principle with those recommended by the U.S. Department of Agriculture (USDA) and other organizations.

The ACS guidelines form the beginning of a report that contains the most up-to-date information available on nutrition issues linked to neoplastic diseases. Included are in-depth answers on how different foods, food preparation methods, portion sizes, variety, and overall calories can reduce or increase the risk of specific cancers. These guidelines provide sound advice regarding healthy eating for cancer prevention for all individuals, including cancer survivors.[29]

The ACS guidelines include the following:

  • Choose most of the foods you eat from plant sources. Consume at least five servings of fruit and vegetables daily, as well as whole-grain products such as cereals, breads, and pasta plus beans several times daily.
  • Limit your intake of high-fat foods, particularly from animal sources. This is accomplished by choosing foods low in fat and by cutting back on meat consumption.
  • Be physically active: achieve and maintain a healthy weight. Be at least moderately active for 30 minutes on most days of the week. Stay within a healthy weight range.
  • Limit consumption of alcoholic beverages, if you drink at all.

The American Institute for Cancer Research (AICR) published a report in 1997 [30] that included an expert scientist panel review and evaluation of more than 4,500 studies on diet and cancer. The AICR Diet and Health Guidelines for Cancer Prevention were developed from these recommendations, which were updated in 2007.[31] The AICR also maintains a Web site that provides information on recipes with a focus on cancer prevention.[32] The AICR and ACS guidelines are similar.

The AICR guidelines include the following:

  • Choose a diet rich in a variety of plant-based foods.
  • Eat plenty of vegetables and fruits.
  • Maintain a healthy weight and be physically active.
  • Drink alcohol in moderation, if at all.
  • Select foods low in fat and salt.
  • Prepare and store food safely.
  • Do not use tobacco in any form.

Soy

The use of soy foods in breast cancer survivors has led to significant research in this area. Several studies suggest soy consumption may reduce breast cancer risk and improve survival; however, the estrogenic effects of isoflavones naturally found in soy products have led to controversy among health professionals over the use of soy by breast cancer patients, especially those with estrogen receptor–positive tumors.

Research on genistein and daidzein, the two main isoflavones in soy, has shown that these phytochemicals may bind to estrogen receptors and decrease the plasma estrogen levels in women, thus acting in a preventive manner.[33] Animal studies, however, have found that genistein inhibited the efficacy of tamoxifen, a drug used to block the body's circulating estrogen.[34]

One study [35] reviewed the relevant literature and found no convincing data to support the claim that soy is protective against breast cancer or that soy is harmful for women with a history of, or at high risk for, breast cancer. A follow-up study using data collected from a large cohort of breast cancer patients as part of the Shanghai Breast Cancer Study also concluded that soy foods do not have an adverse effect on breast cancer survival.[36]

Researchers from these studies concluded that soy foods, as part of a healthy diet and in moderate amounts, are safe to consume; however, there is not enough evidence to recommend that breast cancer patients begin to consume soy specifically to prevent the occurrence of a secondary tumor and enhance survival.[33] Adding soy to the diet after a diagnosis of breast cancer has not been shown to be protective against recurrences. Likewise, the consumption of concentrated, isolated isoflavone supplements in the form of powders or pills has not shown effects consistent with breast cancer risk reduction and is not recommended.[35,37]

As more research is conducted on the biological mechanisms relating to soy isoflavone intake, scientists may clarify the optimal exposure, duration, and timing of intake. Recommendations for the inclusion of soy in the diets of breast cancer survivors should be based on all available (and the most current) evidence.[38]

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3. Fearon KC, Barber MD, Moses AG: The cancer cachexia syndrome. Surg Oncol Clin N Am 10 (1): 109-26, 2001.
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7. Piazza-Barnett R, Matarese LE: Enteral nutrition in adult medical/surgical oncology. In: McCallum PD, Polisena CG, eds.: The Clinical Guide to Oncology Nutrition. Chicago, Ill: The American Dietetic Association, 2000, pp 106-18.
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10. Hodgson B, Kizior RJ: Saunders Nursing Drug Handbook 2002. Philadelphia, Pa: WB Saunders, 2002.
11. Robien K, Demark-Wahnefried W, Rock CL: Evidence-based nutrition guidelines for cancer survivors: current guidelines, knowledge gaps, and future research directions. J Am Diet Assoc 111 (3): 368-75, 2011.
12. Demark-Wahnefried W, Peterson B, McBride C, et al.: Current health behaviors and readiness to pursue life-style changes among men and women diagnosed with early stage prostate and breast carcinomas. Cancer 88 (3): 674-84, 2000.
13. Kwan ML, Weltzien E, Kushi LH, et al.: Dietary patterns and breast cancer recurrence and survival among women with early-stage breast cancer. J Clin Oncol 27 (6): 919-26, 2009.
14. Alfano CM, Day JM, Katz ML, et al.: Exercise and dietary change after diagnosis and cancer-related symptoms in long-term survivors of breast cancer: CALGB 79804. Psychooncology 18 (2): 128-33, 2009.
15. Demark-Wahnefried W, Werner C, Clipp EC, et al.: Survivors of childhood cancer and their guardians. Cancer 103 (10): 2171-80, 2005.
16. Arroyave WD, Clipp EC, Miller PE, et al.: Childhood cancer survivors' perceived barriers to improving exercise and dietary behaviors. Oncol Nurs Forum 35 (1): 121-30, 2008.
17. Robien K, Ness KK, Klesges LM, et al.: Poor adherence to dietary guidelines among adult survivors of childhood acute lymphoblastic leukemia. J Pediatr Hematol Oncol 30 (11): 815-22, 2008.
18. Chlebowski RT, Blackburn GL, Thomson CA, et al.: Dietary fat reduction and breast cancer outcome: interim efficacy results from the Women's Intervention Nutrition Study. J Natl Cancer Inst 98 (24): 1767-76, 2006.
19. Pierce JP, Natarajan L, Caan BJ, et al.: Influence of a diet very high in vegetables, fruit, and fiber and low in fat on prognosis following treatment for breast cancer: the Women's Healthy Eating and Living (WHEL) randomized trial. JAMA 298 (3): 289-98, 2007.
20. Gold EB, Pierce JP, Natarajan L, et al.: Dietary pattern influences breast cancer prognosis in women without hot flashes: the women's healthy eating and living trial. J Clin Oncol 27 (3): 352-9, 2009.
21. Pierce JP: Diet and breast cancer prognosis: making sense of the Women's Healthy Eating and Living and Women's Intervention Nutrition Study trials. Curr Opin Obstet Gynecol 21 (1): 86-91, 2009.
22. Djuric Z, Mirasolo J, Kimbrough L, et al.: A pilot trial of spirituality counseling for weight loss maintenance in African American breast cancer survivors. J Natl Med Assoc 101 (6): 552-64, 2009.
23. von Gruenigen VE, Courneya KS, Gibbons HE, et al.: Feasibility and effectiveness of a lifestyle intervention program in obese endometrial cancer patients: a randomized trial. Gynecol Oncol 109 (1): 19-26, 2008.
24. Demark-Wahnefried W, Clipp EC, Lipkus IM, et al.: Main outcomes of the FRESH START trial: a sequentially tailored, diet and exercise mailed print intervention among breast and prostate cancer survivors. J Clin Oncol 25 (19): 2709-18, 2007.
25. Morey MC, Snyder DC, Sloane R, et al.: Effects of home-based diet and exercise on functional outcomes among older, overweight long-term cancer survivors: RENEW: a randomized controlled trial. JAMA 301 (18): 1883-91, 2009.
26. Moyer-Mileur LJ, Ransdell L, Bruggers CS: Fitness of children with standard-risk acute lymphoblastic leukemia during maintenance therapy: response to a home-based exercise and nutrition program. J Pediatr Hematol Oncol 31 (4): 259-66, 2009.
27. U.S. Department of Agriculture., U.S. Department of Health and Human Services.: Dietary Guidelines for Americans, 2010. 7th ed. Washington, DC: U.S. Government Printing Office, 2010. Also available online. Last accessed January 5, 2012.
28. Kushi LH, Byers T, Doyle C, et al.: American Cancer Society Guidelines on Nutrition and Physical Activity for cancer prevention: reducing the risk of cancer with healthy food choices and physical activity. CA Cancer J Clin 56 (5): 254-81; quiz 313-4, 2006 Sep-Oct.
29. Brown J, Byers T, Thompson K, et al.: Nutrition during and after cancer treatment: a guide for informed choices by cancer survivors. CA Cancer J Clin 51 (3): 153-87; quiz 189-92, 2001 May-Jun.
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32. American Institute for Cancer Research.: AICR Brochures. Washington, DC: AICR, 2010. Available online. Last accessed January 5, 2012.
33. Messina M: Soy intake and breast cancer risk: a review of the animal, epidemiologic and clinical data. Oncology Nutrition Connection 11 (4): 1-10, 2003.
34. Ju YH, Doerge DR, Allred KF, et al.: Dietary genistein negates the inhibitory effect of tamoxifen on growth of estrogen-dependent human breast cancer (MCF-7) cells implanted in athymic mice. Cancer Res 62 (9): 2474-7, 2002.
35. Messina MJ, Loprinzi CL: Soy for breast cancer survivors: a critical review of the literature. J Nutr 131 (11 Suppl): 3095S-108S, 2001.
36. Boyapati SM, Shu XO, Ruan ZX, et al.: Soyfood intake and breast cancer survival: a followup of the Shanghai Breast Cancer Study. Breast Cancer Res Treat 92 (1): 11-7, 2005.
37. Touillaud MS, Pillow PC, Jakovljevic J, et al.: Effect of dietary intake of phytoestrogens on estrogen receptor status in premenopausal women with breast cancer. Nutr Cancer 51 (2): 162-9, 2005.
38. Fletcher DM, Hayward MC: Breast cancer. In: Kogut VJ, Luthringer SL, eds.: Nutritional Issues in Cancer Care. Pittsburgh, Pa: Oncology Nursing Society, 2005, pp 15-28.

Additional Resources

Books

The American Cancer Society's Healthy Eating Cookbook: a Celebration of Food, Friends, and Healthy Living. 3rd ed. Atlanta, Ga: The American Cancer Society, 2005.

Bloch A, Cassileth BR, Holmes MD, Thomson CA, eds.: Eating Well, Staying Well During and After Cancer. Atlanta, GA: American Cancer Society, 2004.

Eldridge B, Hamilton K: Management of Nutrition Impact Symptoms in Cancer and Educational Handouts. Chicago, Ill: The American Dietetic Association, 2004.

Ghosh K, Carson L, and Cohen E: Betty Crocker's Living With Cancer Cookbook: Easy Recipes and Tips Through Treatment and Beyond. New York, NY: Hungry Minds, 2002.

Kogut VJ, Luthringer SL, eds.: Nutritional Issues In Cancer Care. Pittsburgh, Pa: The Oncology Nursing Society, 2005.

McCallum PD, Polisena CG, eds.: The Clinical Guide to Oncology Nutrition. Chicago, Ill: The American Dietetic Association, 2000.

Weihofen DL, Robbins J, Sullivan PA: Easy-To-Swallow, Easy-To-Chew Cookbook: Over 150 Tasty and Nutritious Recipes for People Who Have Difficulty Swallowing. New York, NY: John Wiley & Sons, Inc., 2002.

Wilson JR: I-Can't-Chew Cookbook: Delicious Soft-Diet Recipes for People With Chewing, Swallowing, or Dry-Mouth Disorders. Alameda, Calif: Hunter House Inc., 2003.

Organizations

  • American Botanical Council
    800-373-7105
    abc.herbalgram.org
  • American Cancer Society
    800-227-2345
    www.cancer.org
  • American Dietetic Association
    800-877-1600
    www.eatright.org
  • American Institute for Cancer Research
    800-843-8114
    www.aicr.org
  • American Society for Clinical Oncology
    888-282-2552
    www.asco.org
  • American Society for Parenteral and Enteral Nutrition
    800-727-4567
    www.nutritioncare.org
  • National Cancer Institute
    www.cancer.gov
  • National Center for Complementary and Alternative Medicine (NCCAM)
    888-644-6226 (NCCAM Clearinghouse)
    866-464-3615 (toll-free TTY)
    nccam.nih.gov
  • Office of Dietary Supplements
    301-435-2920
    ods.od.nih.gov
  • Oncology Nursing Society
    866-257-4667
    www.ons.org

Current Clinical Trials

Check NCI's list of cancer clinical trials for U.S. supportive and palliative care trials about malnutrition, nutritional support and nutritional therapy that are now accepting participants. The list of trials can be further narrowed by location, drug, intervention, and other criteria.

General information about clinical trials is also available from the NCI Web site.

Changes to This Summary (11 / 30 / 2011)

The PDQ cancer information summaries are reviewed regularly and updated as new information becomes available. This section describes the latest changes made to this summary as of the date above.

Other Nutrition Issues

Added the new section on Nutrition and Survivorship to replace the section on Survivorship and Prevention of Second Cancers.

The section on Guidelines for Healthy Eating was extensively revised.

The section on Cancer Prevention Dietary Guidelines was renamed from Cancer prevention guidelines.

This summary is written and maintained by the PDQ Supportive and Palliative Care Editorial Board, which is editorially independent of NCI. The summary reflects an independent review of the literature and does not represent a policy statement of NCI or NIH. More information about summary policies and the role of the PDQ Editorial Boards in maintaining the PDQ summaries can be found on the About This PDQ Summary and PDQ NCI's Comprehensive Cancer Database pages.

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About This PDQ Summary

Purpose of This Summary

This PDQ cancer information summary for health professionals provides comprehensive, peer-reviewed, evidence-based information about nutrition before, during, and after cancer treatment. It is intended as a resource to inform and assist clinicians who care for cancer patients. It does not provide formal guidelines or recommendations for making health care decisions.

Reviewers and Updates

This summary is reviewed regularly and updated as necessary by the PDQ Supportive and Palliative Care Editorial Board, which is editorially independent of the National Cancer Institute (NCI). The summary reflects an independent review of the literature and does not represent a policy statement of NCI or the National Institutes of Health (NIH).

Board members review recently published articles each month to determine whether an article should:

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  • be cited with text, or
  • replace or update an existing article that is already cited.

Changes to the summaries are made through a consensus process in which Board members evaluate the strength of the evidence in the published articles and determine how the article should be included in the summary.

The lead reviewers for Nutrition in Cancer Care are:

  • Shalini Dalal, MD (M.D. Anderson Cancer Center)
  • Jean Kristeller, PhD (Indiana State University)
  • Elena J. Ladas, PhD, RD (Columbia University)

Any comments or questions about the summary content should be submitted to Cancer.gov through the Web site's Contact Form. Do not contact the individual Board Members with questions or comments about the summaries. Board members will not respond to individual inquiries.

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Some of the reference citations in this summary are accompanied by a level-of-evidence designation. These designations are intended to help readers assess the strength of the evidence supporting the use of specific interventions or approaches. The PDQ Supportive and Palliative Care Editorial Board uses a formal evidence ranking system in developing its level-of-evidence designations.

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National Cancer Institute: PDQ® Nutrition in Cancer Care. Bethesda, MD: National Cancer Institute. Date last modified <MM/DD/YYYY>. Available at: http://cancer.gov/cancertopics/pdq/supportivecare/nutrition/HealthProfessional. Accessed <MM/DD/YYYY>.

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The information in these summaries should not be used as a basis for insurance reimbursement determinations. More information on insurance coverage is available on Cancer.gov on the Coping with Cancer: Financial, Insurance, and Legal Information page.

Contact Us

More information about contacting us or receiving help with the Cancer.gov Web site can be found on our Contact Us for Help page. Questions can also be submitted to Cancer.gov through the Web site's Contact Form.

Get More Information From NCI

Call 1-800-4-CANCER

For more information, U.S. residents may call the National Cancer Institute's (NCI's) Cancer Information Service toll-free at 1-800-4-CANCER (1-800-422-6237) Monday through Friday from 8:00 a.m. to 8:00 p.m., Eastern Time. A trained Cancer Information Specialist is available to answer your questions.

Chat online

The NCI's LiveHelp® online chat service provides Internet users with the ability to chat online with an Information Specialist. The service is available from 8:00 a.m. to 11:00 p.m. Eastern time, Monday through Friday. Information Specialists can help Internet users find information on NCI Web sites and answer questions about cancer.

Write to us

For more information from the NCI, please write to this address:

NCI Public Inquiries Office
9609 Medical Center Dr.
Room 2E532 MSC 9760
Bethesda, MD 20892-9760

Search the NCI Web site

The NCI Web site provides online access to information on cancer, clinical trials, and other Web sites and organizations that offer support and resources for cancer patients and their families. For a quick search, use the search box in the upper right corner of each Web page. The results for a wide range of search terms will include a list of "Best Bets," editorially chosen Web pages that are most closely related to the search term entered.

There are also many other places to get materials and information about cancer treatment and services. Hospitals in your area may have information about local and regional agencies that have information on finances, getting to and from treatment, receiving care at home, and dealing with problems related to cancer treatment.

Find Publications

The NCI has booklets and other materials for patients, health professionals, and the public. These publications discuss types of cancer, methods of cancer treatment, coping with cancer, and clinical trials. Some publications provide information on tests for cancer, cancer causes and prevention, cancer statistics, and NCI research activities. NCI materials on these and other topics may be ordered online or printed directly from the NCI Publications Locator. These materials can also be ordered by telephone from the Cancer Information Service toll-free at 1-800-4-CANCER (1-800-422-6237).

Last Revised: 2011-11-30

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