Affiliation of authors: Obstetrics and Gynecology Epidemiology Center, Brigham and Women's Hospital, and Harvard Medical School (KBM); Departments of Epidemiology (KBM, WCW, EG) and Nutrition (WCW, EG), Harvard School of Public Health, Boston; Channing Laboratory, Department of Medicine, Brigham and Women's Hospital, and Harvard Medical School, Boston (KBM, WCW, CSF, EG); Department of Adult Oncology, Dana-Farber Cancer Institute, Boston, MA (CSF)
Correspondence to: Karin B. Michels, ScD, Obstetrics and Gynecology Epidemiology Center, Brigham and Women's Hospital, 221 Longwood Ave., Boston, MA 02115 (e-mail: kmichels{at}rics.bwh.harvard.edu).
![]() |
ABSTRACT |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
![]() |
INTRODUCTION |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
A meta-analysis of coffee consumption and colorectal cancer risk revealed that conflicting results have been obtained in casecontrol and cohort studies (3). The combined results of 12 casecontrol studies suggested that coffee consumption is associated with a reduced risk of colorectal cancer (odds ratio for high versus low consumption = 0.72; 95% confidence interval [CI] = 0.61 to 0.84). By contrast, the combined results of five prospective cohort studies revealed no association between coffee consumption and colorectal cancer risk, but the number of cases in each study was small (relative risk = 0.97; 95% CI = 0.73 to 1.29).
The constituents of coffee might have genotoxic, mutagenic, or antimutagenic properties, any of which could influence colorectal cancer risk. For example, caffeine has been reported to inhibit chemical carcinogenesis and UVB light-induced carcinogenesis in animal models (46). Conversely, caffeine has also been found to be mutagenic (79). Coffee consumption has also been speculated to decrease the risk for colorectal cancer because it increases large bowel motility in the rectosigmoid region, which might decrease contact between bowel contents and colon epithelia and thus decrease mucosal damage (10). Coffee may also prevent mucosal damage by reducing the excretion of bile acid and sterols into the bowel (11). Furthermore, caffeine has been reported to lower insulin sensitivity (12), and hyperinsulinemia has been hypothesized to increase risk of colon cancer (13). Another caffeinated beverage, black tea, has been suggested to have anticarcinogenic properties due to its flavonoids, which have antioxidative effects (14).
Given the widespread consumption of coffee worldwide and the high incidence of colorectal cancer in industrialized countries and in South America, where coffee consumption is particularly high, any substantial association between the two could have considerable public health implications. We examined the relations between the consumption of caffeinated and decaffeinated coffee, the consumption of tea with caffeine, and total caffeine intake and the incidences of colon and rectal cancers among participants in the Nurses' Health Study (NHS) and the Health Professionals' Follow-up Study (HPFS). To our knowledge, these are the largest prospective studies considering this issue.
![]() |
SUBJECTS AND METHODS |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
The NHS was initiated in 1976, when 121 700 female registered nurses aged 3055 years completed a self-administered questionnaire that provided information on demographics, lifestyle, and medical history. The HPFS comprises 51 529 male health professionals, including dentists, veterinarians, pharmacists, optometrists, osteopaths, and podiatrists, who were 4075 years of age at enrollment in 1986. Participants in both cohorts have been followed through mailed self-administered biennial questionnaires that have updated information on lifestyle factors and disease.
The study populations for the present analyses consisted of all women who were free of cancer, Crohn's disease, and ulcerative colitis in 1980 and who had completed the 1980 food frequency questionnaire and reported having a total caloric intake of between 500 and 3500 calories per day (N = 87 794 women) and all men who were free of cancer in 1986 and who had completed the 1986 food frequency questionnaire and reported having a total caloric intake of between 800 and 4200 calories per day (N = 46 099 men). A greater proportion of HPFS participants than of NHS participants completed the food frequency questionnaire (100% versus 96%) because the food frequency questions were part of the enrollment questionnaire for HPFS, whereas diet was first assessed in the NHS 4 years after study initiation.
This study and the NHS were approved by the Institutional Review Board (IRB) of the Brigham and Women's Hospital (Boston, MA); the HPFS was approved by the IRB of Harvard School of Public Health (Boston, MA).
Ascertainment of Cases and Follow-Up
On each biennial questionnaire, we asked participants in each cohort whether they had been diagnosed during the previous 2 years with cancer of the colon or rectum. Deaths were reported to us primarily through family members; we also used the National Death Index and the U.S. Postal Service to identify deaths among participants who did not respond to a mailed questionnaire. We estimate that more than 98% of deaths were ascertained (15).
When a participant (or the next of kin, for decedents) reported a diagnosis of cancer, we sought permission to obtain the relevant medical records and pathology reports. Study physicians blinded to all questionnaire data reviewed the medical records and extracted information from them on the histologic type, anatomic location, and stage of the cancer. We included only invasive adenocarcinoma in this analysis; cases of carcinomas in situ were not considered.
For this analysis, participants were followed through 1998 (with a cutoff date of June 1, 1998, for the NHS and January 31, 1998, for the HPFS). Follow-up rates for the cohorts were calculated as the proportion of the number of person-years actually followed out of the total possible number of person-years followed. The follow-up rates for the populations studied in this analysis were 98.5% for the NHS population and 97.0% for HPFS population.
Dietary Assessment
Dietary intake data were collected repeatedly from members of both cohorts with the use of a validated self-administered semiquantitative food frequency questionnaire (16,17). Among participants in the NHS, diet was assessed in 1980, 1984, 1986, 1990, and 1994; among participants in the HPFS, diet was assessed in 1986, 1990, and 1994.
In the NHS, the food frequency questionnaire used for the 1980 dietary assessment consisted of 61 food items and included questions about consumption of coffee with caffeine (in cups), tea with caffeine (in cups), cola or other caffeinated sodas (in glasses), and chocolate (in 1-ounce servings). The 1984 food frequency questionnaire was expanded to include a question about the consumption of decaffeinated coffee (in cups); the unit for sodas was changed to "glass, bottle, or can" and the unit for chocolate was changed to "bars or pieces." The questionnaires used in 1986, 1990, and 1994 were similar to the 1984 questionnaire. In the HPFS, the 1986, 1990, and 1994 food frequency questionnaires were similar to the expanded NHS questionnaires. The expanded questionnaires used in both cohorts provided nine mutually exclusive response possibilities to describe the participant's frequency of intake of a particular item: never or less than once per month; 13 times per month; 1 time per week; 24 times per week; 56 times per week; 1 time per day; 23 times per day; 45 times per day; 6 or more times per day. Participants were asked to report their average intake of one cup of the respective beverages or one serving of any food over the preceding year. We then converted the responses for individual beverages to an average daily intake for each participant.
We used information obtained from U.S. Department of Agriculture food-composition sources (18) to calculate caffeine intake. The caffeine contents used for these calculations were 137 mg caffeine per cup of coffee, 47 mg caffeine per cup of tea, 46 mg caffeine per can or bottle of cola beverage, and 7 mg caffeine per serving of chocolate.
The reproducibility and validity of the food frequency questionnaire for both women and men have been reported previously (16,17). The validity of the questionnaires with respect to individual food items has been documented by comparing the responses of 173 women from the NHS and 127 men from the HPFS to two food frequency questionnaires that were administered approximately 12 months apart and multiple 7-day diet records obtained during the 1-year interval (19,20). Correlation coefficients for the average consumption for coffee and tea as assessed by the food frequency questionnaires and the diet records, correcting for within-person weekly variation in diet, were 0.78 and 0.93, respectively, in the NHS (19) and 0.93 and 0.77, respectively, in the HPFS (20).
Statistical Analysis
Daily consumption of coffee, tea, and caffeine was calculated from the frequencies that were pre-specified on the food frequency questionnaire. Categories of frequency of coffee and tea consumption were created, and the lowest intake category was chosen as referent group. Caffeine intake was calculated from the responses to questions about consumption of coffee with caffeine, tea with caffeine, carbonated beverages with caffeine, and chocolate and was used in the analysis as an energy-adjusted residual. Residuals were obtained by regressing log-transformed caffeine on log total energy and determining the antilog of the resulting residual value (18). The caffeine residual, which retains the units of intake (in milligrams) when the antilog is used, was divided into quintiles on the basis of the distributions of caffeine intakes among women and among men.
To represent the long-term consumption patterns for individual subjects as accurately as possible and to reduce random within-person variation in beverage consumption, we modeled the incidence of colorectal cancer in relation to the cumulative average intake of coffee, tea, and caffeine from all dietary questionnaires available up to the start of each 2-year follow-up interval (21). Thus, for the female participants we used dietary data from the 1980 questionnaire for analyses of colorectal cancers diagnosed from 1980 through 1984; the average of the dietary data from the 1980 and 1984 questionnaires was used for analyses of colorectal cancers diagnosed from 1984 through 1986; the average of the dietary data from the 1980, 1984, and 1986 questionnaires was used for analyses of colorectal cancers diagnosed from 1986 through 1990; and so forth. Similarly, for the male participants, dietary data from the 1986 questionnaire were used for analyses of colorectal cancers diagnosed from 1986 through 1990; the average of the dietary data from the 1986 and 1990 questionnaires was used for analyses of colorectal cancers diagnosed from 1990 through 1994; and the average of the dietary data from the 1986, 1990, and 1994 questionnaires was used for analyses of colorectal cancers diagnosed from 1994 through 1998. Consumption of decaffeinated coffee among women was first assessed in 1984. Therefore, all analyses pertaining to decaffeinated coffee intake in women used data collected in 1984 through 1998.
We carried out separate analyses for colon and rectal cancers. Cancer incidence rates associated with each category of coffee intake were calculated by dividing the number of new cases of colon or rectal cancer by the number of person-years of follow-up. The number of person-years of follow-up for each participant was calculated from the month we receive the completed 1980 questionnaire (NHS) or the 1986 questionnaire (HPFS) to the date of diagnosis of colon or rectal cancer, the date of death, or the end of follow-up (June 1, 1998, for the NHS and January 31, 1998, for the HPFS), whichever occurred first. Participants who reported that they had been diagnosed with Crohn's disease, ulcerative colitis, or cancers other than nonmelanoma skin cancer were excluded at baseline, and follow-up was censored when these diseases were diagnosed during follow-up.
We used a Cox proportional hazards model to calculate the relative hazard of developing colon or rectal cancer associated with coffee, tea, or caffeine intake (22). The proportional hazards model permits the simultaneous adjustment for multiple potential confounders, including time-dependent covariates. Proportionality of hazards was confirmed by visual examination of associations across intervals of time. Coffee, tea, and caffeine consumption were used as time-dependent variables and were cumulatively updated every 4 years, as described above. Regression models were adjusted for age (in months), family history of colorectal cancer (yes/no), history of sigmoidoscopy or colonoscopy (ever/never), height (in centimeters; continuous variable), body mass index (in kilograms per meter squared; continuous variable), moderate to vigorous physical activity (women: <1 hour/week, 11.9 hours/week, 23.9 hours/week, 46.9 hours/week, 7 hours/week; men: quintiles of metabolic equivalents [working metabolic rate/resting metabolic rate/week]), regular aspirin use (women: never or <1/week, 16/week,
7/week; men: <2/week,
2/week), pack-years of smoking (both sexes: <10 pack-years,
10 pack-years; among women: pack-years of smoking
35 years in the past; among men: pack-years of smoking before age 30 years), ever-use of vitamin supplement (use of multivitamins or vitamins A, C, or E: yes/no), alcohol consumption (none, <10 g/day, 1019.9 g/day, 2029.9 g/day,
30 g/day), total caloric intake (kilocalories; continuous variable), red meat consumption (<1/week, 1/week, 24/week, 56/week,
1/day), and (among women) menopausal status premenopausal, postmenopausal, uncertain menopausal status and postmenopausal hormone use (never, current, past). Covariates were assessed repeatedly and updated throughout the analysis.
Total caloric intake was included in the covariate-adjusted model to control for confounding by total energy intake and to minimize extraneous variation due to general under- or over-reporting of intake of food items on the food frequency questionnaire (23). Body mass index and height were included in the analytic model to capture the relation between body composition and size and colorectal cancer risk (24). Hazard ratios (HRs) for an increase in intake by one serving (e.g., one cup) per day were obtained by using daily consumption as a continuous variable.
Because the two cohorts differed by sex, follow-up time, food frequency questionnaires, and covariates, we performed separate analyses for each cohort and then combined the results by using a fixed-effects model that weighted the two relative risk estimates by the inverse of the standard error (25). Tests of heterogeneity were used to evaluate whether associations differed between women and men; results are shown separately whenever statistically significant heterogeneity was observed.
Analyses were stratified by current smoking status and by alcoholic beverage consumption (both of which were time-dependent covariates). All tests of statistical significance were two-sided.
![]() |
RESULTS |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
The number of participants who reported drinking decaffeinated coffee increased over time. Among women, 49.3% drank decaffeinated coffee with any regularity in 1984 and 71.5% did so in 1994. Among men, 48.8% drank decaffeinated coffee with any regularity in 1986, whereas 62.5% did so in 1994.
Coffee consumption varied greatly among the participants in each cohort. Although in both cohorts the most frequent category of caffeinated coffee consumption selected was two to three cups per day, considerable numbers of participants reported that they either consumed no coffee or more than five cups per day (Table 1). Higher consumption of caffeinated coffee was associated with a lower mean body mass index among women and with a higher mean body mass index among men. In both cohorts, higher caffeinated coffee consumption was also associated with a lower frequency of sigmoidoscopy, a lower use of vitamin supplements, and higher frequencies of smoking, alcohol consumption, aspirin use, and red meat consumption. Higher consumption of decaffeinated coffee was associated with higher frequencies of sigmoidoscopy, vitamin supplement use, and smoking in both cohorts and with a higher frequency of aspirin use among men. In both cohorts, higher tea consumption was associated with lower alcohol consumption. Patterns for caffeine intake were similar to those for caffeinated coffee consumption (Table 1).
|
Total coffee consumption, which included caffeinated and decaffeinated coffee consumption, was not associated with the incidence of colorectal, colon, or rectal cancer. The covariate-adjusted hazard ratios for colorectal cancer for each additional cup of any coffee consumed were 0.99 (95% confidence interval [CI] = 0.95 to 1.04) among women and 0.98 (95% CI = 0.92 to 1.03) among men.
Results of our analysis of the association between caffeinated coffee consumption and incidence of colorectal cancer are presented in Table 2. Because the hazard ratios adjusted for age only did not differ appreciably from the hazard ratios adjusted for all covariates, we present only the latter in Table 2. We found no significant association between consumption of caffeinated coffee and the incidence of colorectal cancer (Table 2). Among women and men combined, the pooled hazard ratio for colorectal cancer for one additional cup of caffeinated coffee per day was 1.01 (95% CI = 0.97 to 1.04) when we adjusted for age only and 0.99 (95% CI = 0.96 to 1.03) when we adjusted for age, family history of colorectal cancer, history of sigmoidoscopy, height, body mass index, pack-years of smoking, physical activity, aspirin use, vitamin supplement intake, total caloric intake, alcohol consumption, red meat consumption, and, among women, menopausal status and postmenopausal hormone use. Compared with no consumption, consumption of four or more cups of coffee per day was associated with a slight although not statistically significant increase in rectal cancer (pooled HR = 1.55, 95% CI = 0.97 to 2.45). No statistically significant trend of higher rectal cancer incidence emerged with increasing coffee consumption (Ptrend = .31). When we only used coffee consumption reported in 1980 for women and 1986 for men and did not update consumption during follow-up, the results did not differ from the results presented for cumulatively updated coffee consumption (data not shown).
|
|
|
|
|
![]() |
DISCUSSION |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
To our knowledge, this is the largest study on coffee and tea consumption and the incidence of colon and rectal cancer. A meta-analysis of coffee consumption and the risk of colorectal cancer that used the combined data from all prospective studies included 931 cases of colorectal cancer (3); the present study comprised 1433 cases of colorectal cancer. Results of casecontrol studies that have examined this association have suggested that coffee consumption is associated with a decreased risk of colorectal cancer, whereas results of prospective cohort studies have suggested that coffee consumption is not associated with a reduction in colorectal cancer incidence (3,26). Results from casecontrol studies have to be evaluated with caution because these studies are subject to selection bias and to differential misclassification of coffee consumption because participants' recall of coffee consumption from the time before their cancer diagnosis may be influenced by their current coffee consumption and by their disease status. In addition, most of the casecontrol studies were conducted in Europe, where coffee preparation and brewing methods may be different from those used in the United States. Results from only one casecontrol study that was carried out in the United States using hospital-based control subjects suggested that coffee consumption is inversely associated with the risk of colorectal cancer (27).
Our unanticipated finding of an inverse association between decaffeinated coffee consumption and the incidence of rectal cancer is consistent with a threshold effect rather than a doseresponse relation. Only one other study (28) has examined associations between decaffeinated coffee consumption and the risks of colon and rectal cancer, perhaps because dietary assessment instruments do not always differentiate between caffeinated and decaffeinated coffee. In that casecontrol study, conducted in Italy, the odds ratios associated with decaffeinated coffee consumption were 0.92 (95% CI = 0.72 to 1.18) for colon cancer and 0.88 (95% CI = 0.65 to 1.20) for rectal cancer; however, in that study population only 4% of the case patients and control subjects consumed decaffeinated coffee (28).
Our data suggest that individuals who regularly drink decaffeinated coffee are more health conscious in their behaviors than those who do not drink decaffeinated coffee, in that a higher percentage had undergone sigmoidoscopy screening for colorectal cancer and reported using vitamin supplements. Many individuals who drink decaffeinated coffee may be former caffeinated coffee drinkers who like the taste of coffee but cannot or do not want to drink caffeinated coffee. Thus, residual confounding by healthy lifestyle and chance should be considered as possible explanations for the observed inverse association between decaffeinated coffee consumption and the incidence of colorectal cancer, especially given that we observed no doseresponse relation. However, participants who reported that they regularly consumed decaffeinated coffee were not more physically active, did not drink less alcohol or smoke less, and did not consume less red meat than those who did not drink decaffeinated coffee. Furthermore, although tea drinkers had healthy lifestyle patterns similar to those of decaffeinated coffee drinkers, the incidence rates of colorectal cancer were not lower among those who frequently consumed tea than among those who did not. Few of the participants in our study reported very high consumption of either tea or decaffeinated coffee. The consistency of the inverse association between decaffeinated coffee consumption and rectal cancer incidence across both cohorts and the observation that the association between decaffeinated coffee consumption and the incidence of colon cancer was restricted to cancers in the proximal colon among both women and men lend credibility to our results.
A number of biologic mechanisms could underlie the observed inverse association between decaffeinated coffee consumption and colorectal cancer. Given its constituents, intake of caffeinated coffee could either increase or decrease the incidence of colorectal cancer. Decaffeinated coffee, however, may not contain potentially harmful constituents, such as caffeine, or have the homocysteine-raising effect of coffee (29). It has been reported that both regular and decaffeinated coffee increase rectosigmoid motility (10). However, we previously found that, among the women in our cohort, the self-reported frequency of bowel movements was not associated with colon or rectal cancer risk (30). By contrast, in another study population constipation was associated with an increased risk of colon cancer (31). Among participants in the NHS, we found a U-shaped relation between coffee consumption and bowel movement: modest consumption was associated with a decreased risk of constipation, whereas frequent consumption was associated with increased risk of constipation, possibly because of the dehydrating effect of high coffee intake (32).
Reports on the association between tea consumption and the risk of colorectal cancer have been inconsistent. Tea consumption was associated with an increased incidence of colon cancer but not rectal cancer in a cohort of Finnish men (33). In a Swedish casecontrol study, tea consumption was associated with a reduced risk of rectal cancer for participants who drank two or more cups per day; no association between tea consumption and colon cancer risk was found (34). Frequent tea consumption was associated with a decreased incidence of colon cancer in the National Health and Nutrition Examination Survey I Epidemiologic Follow-up study (35). Other studies (28,36,37) have found no association between self-reported tea consumption and the risk of colorectal cancer.
Data collected in any observational study are measured with error, and nondifferential measurement error has to be considered as a possible explanation for the lack of association we observed for coffee consumption and incidence of colorectal cancer. However, results from our validation study suggest that coffee consumption was reported with good accuracy. Moreover, our findings are largely consistent with previous cohort studies on this topic (3,26). Furthermore, the repeated assessments of food and beverage consumption in these cohorts, the considerable variation in coffee consumption, and the long duration of follow-up minimize the likelihood that any important effects would be missed.
In conclusion, we found that regular consumption of caffeinated coffee or tea or total caffeine intake was not associated with a reduced incidence of colon or rectal cancers. Although consumption of decaffeinated coffee was inversely associated with the incidence of rectal cancer, this association needs to be confirmed in other studies.
![]() |
NOTES |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
We are indebted to Ya-Hua Chen, MS, for expert programming assistance. We thank Karen Corsano, Gary Chase, Barbara Egan, and Elizabeth Frost-Hawes for their unfailing assistance in maintaining these cohorts. We are grateful to the participants of the Nurses' Health Study and the Health Professionals' Follow-up Study for providing the relevant information.
![]() |
REFERENCES |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
(1) World Cancer Research Fund/American Institute for Cancer Research. Food, nutrition and prevention of cancer: a global perspective. Washington (DC): American Institute for Cancer Research; 1997. p. 21651.
(2) Ekbom A. Review: Substantial coffee consumption was associated with a lower risk of colorectal cancer in the general population. Gut 1999;44:597.
(3) Giovannucci E. Meta-analysis of coffee consumption and risk of colorectal cancer. Am J Epidemiol 1998;147:104352.[Abstract]
(4) Rothwell K. Dose-related inhibition of chemical carcinogenesis in mouse skin by caffeine. Nature 1974;252:6970.[ISI][Medline]
(5) Lu YP, Lou YR, Xie JG, Xie JG, Peng QY, Liao J, et al. Topical applications of caffeine or ()-epigallocatechin gallate (EGCG) inhibit carcinogenesis and selectively increase apoptosis in UVB-induced skin tumors in mice. Proc Natl Acad Sci U S A 2002;99:1245560.
(6) Lou YR, Lu YP, Xie JG, Huang MT, Conney AH. Effects of oral administration of tea, decaffeinated tea, and caffeine on the formation and growth of tumors in high-risk SKH-1 mice previously treated with ultraviolet B light. Nutr Cancer 1999;33:14653.[CrossRef][ISI][Medline]
(7) Timson J. Caffeine. Mutat Res 1977;47:152.[ISI][Medline]
(8) Levin RE. Influence of caffeine on mutations induced by nitrosoguanidine in Salmonella typhimurium tester strains. Environ Mutagen 1982;4: 68994.[ISI][Medline]
(9) Ivankovic S, Seibel J, Komitowski D, Spiegelhalder B, Preussmann R, Siddiqi M. Caffeine-derived N-nitroso compounds. V. Carcinogenicity of mononitrosocaffeidine and dinitrosocaffeidine in bd-ix rats. Carcinogenesis 1998;19:9337.[Abstract]
(10) Brown SR, Cann PA, Read NW. Effect of coffee on distal colon function. Gut 1990;31;4503.[Abstract]
(11) Jacobsen BK, Thelle DS. Coffee, cholesterol, and colon cancer: is there a link. BMJ Clin Res Ed 1987;294:45.[ISI][Medline]
(12) Keijzers GB, De Galan BE, Tack CJ, Smits P. Caffeine can decrease insulin sensitivity in humans. Diabetes Care 2002;25:3649.
(13) Giovannucci E. Insulin, insulin-like growth factors and colon cancer: a review of the evidence. J Nutr 2001;131:3109S20S.
(14) Trevisanato SI, Kim YI. Tea and health. Nutr Rev 2000;58:110.[ISI][Medline]
(15) Stampfer MJ, Willett WC, Speizer FE, Dysert DC, Lipnick R, Rosner B, et al. Test of the National Death Index. Am J Epidemiol 1984;119:8379.[ISI][Medline]
(16) Willett WC, Sampson L, Stampfer MJ, Rosner B, Bain C, Witschi J, et al. Reproducibility and validity of a semiquantitative food frequency questionnaire. Am J Epidemiol 1985;122:5165.[Abstract]
(17) Rimm EB, Giovannucci EL, Stampfer MJ, Colditz GA, Litin LB, Willett WC. Reproducibility and validity of an expanded self-administered semiquantitative food frequency questionnaire among male health professionals. Am J Epidemiol 1992;135:111426.[Abstract]
(18) Willett WC. Nutritional epidemiology, 2nd ed. New York (NY): Oxford University Press; 1998.
(19) Salvini S, Hunter DJ, Sampson L, Stampfer MJ, Colditz GA, Rosner B, et al. Food-based validation of a dietary questionnaire: the effects of week-to-week variation in food consumption. Int J Epidemiol 1989;18:85867.[Abstract]
(20) Feskanich D, Rimm EB, Giovannucci EL, Colditz GA, Stampfer MJ, Litin LB, et al. Reproducibility and validity of food intake measurements from a semiquantitative food frequency questionnaire. J Am Diet Assoc 1993;93:7906.[ISI][Medline]
(21) Hu FB, Stampfer MJ, Rimm E, Ascherio A, Rosner BA, Spiegelman D,Willett WC. Dietary fat and coronary heart disease: a comparison of approaches for adjusting for total energy intake and modeling repeated dietary measurements. Am J Epidemiol 1999;149:53140.[Abstract]
(22) Cox DR. Regression models and life tables. J R Stat Soc 1972;32:187220.
(23) Willett WC, Stampfer MJ. Total energy intake: implications for epidemiologic analyses. Am J Epidemiol 1986;124:1727.[Abstract]
(24) Michels KB, Greenland S, Rosner BA. Does body mass index adequately capture the relation of body composition and body size to health outcomes. Am J Epidemiol 1998;147:16772.[Abstract]
(25) Hedges LV, Olkin I. Statistical methods for meta-analysis. New York (NY): Academic Press; 1985.
(26) Terry P, Bergkvist L, Holmberg L, Wolk A. Coffee consumption and risk of colorectal cancer in a population based prospective cohort of Swedish women. Gut 2001;49:8790.
(27) Rosenberg L, Werler MM, Palmer JR, Kaufman DW, Warshauer ME, Stolley PD, et al. The risks of cancers of the colon and rectum in relation to coffee consumption. Am J Epidemiol 1989;130:895903.[Abstract]
(28) Tavani A, Pregnolato A, La Vecchia C, Negri E, Talamini R, Franceschi S. Coffee and tea intake and risk of cancers of the colon and rectum: a study of 3,530 cases and 7,057 controls. Int J Cancer 1997;73:1937.[CrossRef][ISI][Medline]
(29) Verhoef P, Pasman WJ, Van Vliet T, Urgert R, Katan MB. Contribution of caffeine to the homocysteine-raising effect of coffee: a randomized controlled trial in humans. Am J Clin Nutr 2002;76:12448.
(30) Dukas L, Willett WC, Colditz GA, Fuchs CS, Rosner B, Giovannucci EL. Prospective study of bowel movement, laxative use, and risk of colorectal cancer among women. Am J Epidemiol 2000;151:95864.[Abstract]
(31) Kotake K, Koyama Y, Nasu J, Fukutomi T, Yamaguchi N. Relation of family history of cancer and environmental factors to the risk of colorectal cancer: a casecontrol study. Jpn J Clin Oncol 1995;25:195202.[Abstract]
(32) Dukas L, Willett WC, Giovannucci EL. Association between physical activity, fiber intake, and other lifestyle variables and constipation in a study of women. Am J Gastroenterol 2003;98:17906.[CrossRef][ISI][Medline]
(33) Hartman TJ, Tangrea JA, Pietinen P, Malila N, Virtanen M, Taylor PR, et al. Tea and coffee consumption and risk of colon and rectal cancer in middle-aged Finnish men. Nutr Cancer 1998;31:418.[ISI][Medline]
(34) Baron JA, Gerhardsson de Verdier M, Ekbom A. Coffee, tea, tobacco, and cancer of the large bowel. Cancer Epidemiol Biomarkers Prev 1994;3:56570.[Abstract]
(35) Su LJ, Arab L. Tea consumption and the reduced risk of colon cancerresults from a national prospective cohort study. Public Health Nutr 2002;5:41925.[CrossRef][ISI][Medline]
(36) Woolcott CG, King WD, Marrett LD. Coffee and tea consumption and cancers of the bladder, colon and rectum. Eur J Cancer Prev 2002;11: 13745.[CrossRef][ISI][Medline]
(37) Terry P, Wolk A. Tea consumption and the risk of colorectal cancer in Sweden. Nutr Cancer 2001;39:1769.[CrossRef][ISI][Medline]
Manuscript received June 25, 2004; revised November 22, 2004; accepted December 14, 2004.
This article has been cited by other articles in HighWire Press-hosted journals:
Related Memo to the Media
![]() |
||||
|
Oxford University Press Privacy Policy and Legal Statement |