HOME HELP FEEDBACK SUBSCRIPTIONS ARCHIVE SEARCH TABLE OF CONTENTS		QUICK SEARCH:   [advanced] Author: Keyword(s): Year:  Vol:  Page:

This Article Abstract Full Text (PDF) Purchase Article View Shopping Cart Alert me when this article is cited Alert me if a correction is posted Citation Map Services Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via HighWire Citing Articles via Google Scholar Google Scholar Articles by Stolzenberg-Solomon, R. Z Articles by Ziegler, R. G Search for Related Content PubMed PubMed Citation Articles by Stolzenberg-Solomon, R. Z Articles by Ziegler, R. G Agricola Articles by Stolzenberg-Solomon, R. Z Articles by Ziegler, R. G

Folate intake, alcohol use, and postmenopausal breast cancer risk in the Prostate, Lung, Colorectal, and Ovarian Cancer Screening Trial^1,2,3

¹ From the Nutritional Epidemiology Branch (RZS-S, S-CC, and MFL) and the Epidemiology and Biostatistics Program (RNH and RGZ), Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Rockville, MD; the Breast and Gynecologic Cancer Research Group, Division of Cancer Prevention, National Institutes of Health, Rockville, MD (KAJ); the Henry Ford Health Sciences Center, Detroit, MI (CJ); and the University of Utah Health Sciences Center, Salt Lake City, UT (SSB)

² Supported by the Intramural Research Program of the Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Department of Health and Human Services.

³ Address reprint requests to RZ Stolzenberg-Solomon, 6120 Executive Boulevard, Suite 320, Rockville, MD 20852. E-mail: rs221z{at}nih.gov.

	ABSTRACT

TOP ABSTRACT INTRODUCTION SUBJECTS AND METHODS RESULTS DISCUSSION REFERENCES

 
Background: Several epidemiologic studies suggest that higher folate intakes are associated with lower breast cancer risk, particularly in women with moderate alcohol consumption.

Objective: We investigated the association between dietary folate, alcohol consumption, and postmenopausal breast cancer in women from the Prostate, Lung, Colorectal, and Ovarian Cancer Screening Trial cohort.

Design: Dietary data were collected at study enrollment between 1993 and 2001. Folate content was assigned on the basis of prefortification (ie, pre-1998) databases. Of the 25 400 women participants with a baseline age of 55–74 y and with complete dietary and multivitamin information, 691 developed breast cancer between September 1993 and May 2003. We used Cox proportional hazard models with age as the underlying time metric to generate hazard ratios (HRs) and 95% CIs.

Results: The adjusted HRs were 1.19 (95% CI: 1.01, 1.41; P for trend = 0.04) for women reporting supplemental folic acid intake 400 µg/d compared with subjects reporting no supplemental intake. Comparison of the highest with the lowest quintile gave adjusted HRs of 1.04 (95% CI: 0.83, 1.31; P for trend = 0.56) and 1.32 (95% CI: 1.04, 1.68; P for trend = 0.03) for food and total folate intake, respectively. Alcohol consumption was positively associated with breast cancer risk (highest compared with lowest quintile: HR = 1.37; 95% CI: 1.08, 1.76; P for trend = 0.02); the risk was greatest in women with lower total folate intake.

Conclusions: Our results do not support the hypothesis that high folate intake reduces breast cancer risk; instead, they suggest that a high intake, generally attributable to supplemental folic acid, may increase the risk in postmenopausal women. However, our results confirm previous studies showing positive associations between moderate alcohol consumption and breast cancer.

Key Words: Folate • alcohol • breast cancer • prospective study • cohort • epidemiology • diet

	INTRODUCTION

TOP ABSTRACT INTRODUCTION SUBJECTS AND METHODS RESULTS DISCUSSION REFERENCES

 
Over the past 10 y, evidence has been mounting that folate inadequacy may be an important risk factor for cancer (1). Low folate intakes and status have been positively associated with several cancers, including colorectal, cervical, lung, esophageal, and pancreas, and the evidence is most compelling for colorectal cancer (1). In addition, some but not all retrospective and prospective studies suggest that high folate intake or circulating folate concentrations may be associated with a lower risk for postmenopausal breast cancer, particularly in women with moderate or high alcohol consumption (2-21). Alcohol use has been consistently associated with increased breast cancer risk (22, 23). Although increases in sex hormones have been proposed to explain the association of alcohol and breast cancer (24), chronically high alcohol consumption, such as that of alcoholics, is also associated with inadequate folate status (25).

The 2 most commonly hypothesized, but yet unproven, mechanisms by which folate inadequacy may contribute to carcinogenesis are 1) DNA hypomethylation and subsequent protooncogene activation and 2) misincorporation of uracil during DNA synthesis, which leads to DNA instability (1). Methionine, in the form S-adenosylmethionine, is the principal methyl donor for >100 biologic methylation reactions, including DNA methylation. S-adenosylhomocysteine, the product of these reactions, is hydrolyzed to homocysteine in a reversible reaction with equilibrium dynamics that favor synthesis of S-adenosylhomocysteine. High S-adenosylhomocysteine concentrations inhibit methyltransferases and thus methylation reactions (26). Folate and vitamin B-12 are coenzymes needed to regenerate methionine from homocysteine. Deficiencies in one-carbon related nutrients, particularly folate, may lead to lower cellular S-adenosylmethionine, diminished or altered DNA methylation (eg, DNA hypomethylation), and accumulation of S-adenosylhomocysteine and homocysteine. Thus, both higher homocysteine concentrations and less methionine regeneration may lead to DNA hypomethylation, which may increase the susceptibility of genes to mutations or alter gene expression, each of which has been hypothesized to increase cancer risk. Although there is evidence to support an influence of folate deficiency on global methylation, the influence of folate on gene-specific methylation is not yet understood (27). Folate, in the form 10-formyl tetrahydrofolate, is also required to synthesize purines for DNA synthesis, whereas folate in the form 5,10-methylenetetrahydrofolate is required to convert deoxyuridylate into deoxythymidylate. Therefore, folate inadequacy may increase cancer susceptibility through greater misincorporation of uracil for thymine in DNA and impaired DNA excision repair, both of which lead to DNA strand breaks and chromosome damage (1). The purpose of the current study was to better understand the association between folate intake (food folate, the natural polyglutamate forms in foods, synthetic folic acid supplements, and total folate), alcohol consumption, the interaction of these factors, and postmenopausal breast cancer in a prospective analysis of women participating in the screening arm of the Prostate, Lung, Colorectal, and Ovarian (PLCO) Cancer Screening Trial.

	SUBJECTS AND METHODS

TOP ABSTRACT INTRODUCTION SUBJECTS AND METHODS RESULTS DISCUSSION REFERENCES

 
Study design and population
Subjects in this study were women randomly assigned to the intervention arm of the PLCO Cancer Screening Trial, a randomized multicenter trial investigating whether screening for prostate, lung, colorectal, and ovarian cancer can reduce cancer-specific incidence and mortality. Details of the study have been described elsewhere (28). Briefly, women aged 55–74 y were recruited between November 1993 and July 2001 in 10 US centers. Participants with a personal history of 1 of the 4 PLCO cancers, with a recent history of screening procedures for one of the cancers, or with current treatment for any cancer except nonmelanoma skin cancer were excluded from the trial.

Women randomly assigned to the intervention arm underwent periodic cancer screening tests, including chest X-ray, flexible sigmoidoscopy, digital rectal examination, cancer antigen 125 screening, and transvaginal ultrasound. Women randomly assigned to the control arm were instructed to follow their usual medical practice.

Of the 77 376 women enrolled in the PLCO trial, only those in the intervention arm were given the dietary history questionnaire at baseline (n = 38 660 women); of that group, 31 411 (81%) completed the questionnaire. We excluded 6011 of those women for the following reasons: history of any cancer other than nonmelanoma skin cancer (n = 2338); > 8 items missing from the food-frequency questionnaire (n = 319); extreme values for energy intake (lowest or highest 1% of the distribution, n = 544); and missing data on multivitamin use (n = 2810). The current analysis included the remaining 25 400 women. Given the age of the women at randomization (55–74 y), we estimated that <0.3% of them may have been premenopausal at baseline, and we not exclude any women on the basis of menopausal status.

Each eligible participant provided written informed consent. The study was approved by the institutional review boards of the National Cancer Institute and each of the participating centers.

Breast cancer case ascertainment
Participants were sent an annual health survey questionnaire and were asked whether they had been diagnosed by a health care provider as having cancer and, if so, what was the type of cancer. Incident breast cancer cases were identified by self-report in the annual mail-in survey, state cancer registries, death certificates, physician reports, and (for deceased persons) reports from the next of kin. Medical record abstracts containing pathology reports were sought for confirmation of breast cancer diagnosis. Between September 1993 and June 2003, 691 incident breast cancer cases were identified. Five hundred cases (72.4%) were confirmed though medical review, of which 96 were in situ cancers. Analyses that excluded nonconfirmed and in situ cancers did not noticeably differ from those using all of the cases; therefore, we included all ascertained cases in our analysis to increase the statistical power.

Assessment of diet, vitamin supplement and alcohol use, and other baseline characteristics
At randomization, all study subjects were asked to complete a self-administered baseline questionnaire that included questions on demographic factors, medical history, and health-related behaviors. In addition, all participants randomly assigned to the PLCO Trial intervention arm were given the PLCO food-frequency questionnaire (FFQ), which was designed to be self-administered and to characterize usual dietary intake over the past 12 mo (http://www.cancer.gov/prevention/plco/DQX.pdf). With the use of a grid format, frequency of consumption was asked for 137 food items; in addition, usual portion size (small, medium, or large) was queried for 77 items. For beer, wine, and spirits, both frequency and portion size were assessed. Descriptive data for calculating nutrients and food groups were derived from the two 24-h recalls administered in the 1994–1996 Continuing Survey of Food Intake by Individuals (CSFII; 29), a nationally representative survey from the US Department of Agriculture that was conducted during the period when the FFQ was being used. In particular, the cutoffs between small and medium and between medium and large intakes correspond to the 25th and 75th percentiles for portion sizes reported by participants aged 51 y in the 1994–1996 CSFII (29). The choice of food items, the wording, and the assumptions for estimating nutrients and food groups for the PLCO FFQ incorporated elements of both cognitive (30, 31) and database (29) research. Supplemental vitamin and mineral use was assessed for 12 types of supplements by asking for the name of each supplement ever taken since age 25 y, the years of use, and the number of pills and whether the supplement was taken currently, 2 y ago, or 5 y ago. Supplemental folic acid use and dose were derived from recent use (current or 2 y ago) of 4 multivitamins: One-a-Day (100% RDA; Bayer Corp, Pittsburgh, PA), a therapeutic or high-dose type (>100% RDA; eg, Theragran; Bristol-Myers Squibb, New York, NY), Stresstabs (B-complex + vitamin C; Inverness Medical Inc, Waltham, MA), and B-complex. The B-complex multivitamin was assigned a 200-µg folic acid dose, whereas the other multivitamins were assigned a 400-µg folic acid dose.

Statistical analysis
The follow-up period for each participant was from the date of randomization until diagnosis of breast cancer, death, or last completed annual health survey. The analysis reported here included follow-up to June 2003 (median follow-up time: 4.94 y; maximum: 9.33 y), which represents 127 261 person-years of observation.

Analyses were performed separately for folate from foods, supplements, and foods and supplements combined (total) and for the natural folate in foods. The folate species occurring naturally in foods such as green vegetables and oranges are polyglutamates. Also found in food is folic acid, a synthetic folate used to fortify breakfast cereal and grain products. In 1998, in an effort to reduce the incidence of neural tube defects, the FDA instituted in the United States mandatory folic acid fortification of grains at 140 µg folic acid/100 g grain products (32). Therefore, our analyses examined both prefortification and postfortification values for food and total folate. Nutrients were analyzed both as continuous and categorical variables. Continuous variables were categorized on the basis of distribution in our cohort. Trend tests across categorical variables were analyzed by calculating a score variable based on the median values of each category. Spearman correlations were calculated to assess the correspondence between study variables in the cohort. Because most dietary variables were correlated with total energy, nutrient and food variables were energy-adjusted by using the residual method (33). The use of alcohol, supplemental folic acid, and multivitamins was not highly correlated with energy intake, and energy did not change risk estimates when included in these models; therefore, values for alcohol, supplemental folic acid, and multivitamin use were not energy-adjusted.

Generalized linear models were used to estimate the means, standard errors, and P for trend within and across the total folate quintiles for the continuous population characteristic variables in Table 1. For the categorical variables, we show frequency proportions, and we used the Cochran-Armitage test to calculate the P for trend. Cox proportional hazard models with age as the underlying time metric were used to generate hazard ratios (HRs) and 95% CIs. Entry time was defined as a subject's age in days at randomization, and exit time was defined as a subject's age in days at cancer diagnosis or censoring. Our multivariable best-fit models were developed separately for each folate variable and alcohol use by entering covariates individually into the model. Variables were included in the model if they were associated with both the disease and exposure and if they either changed the risk estimate by 10% or increased the precision of the risk estimate by narrowing the range of the CI. Variables examined as potential confounders included dietary intakes of energy; vitamins A, B-6, C, D, and E and carotenoids from foods, supplements, and both sources; and protein, fat, carbohydrate, and fiber; alcohol and multivitamin use (ever or never); height (median quintiles or data missing); current body mass index [(BMI; in kg/m²) median quintiles or data missing]; physical activity (<4 h/wk, 4 h/wk, or data missing); age at menarche (<12, 12–13, or 14 y); age at menopause (<40, 40–49, 50–54, or 55 y); age at first birth and number of live births (nulliparous; <20 y and 1, 2, or 3 births; 20–29 y and 1, 2, or 3 births; and 30 y and 1, 2, or 3 births); oral contraceptive use (no, yes, or data missing); hormone replacement therapy (HRT) use (never; former; current and 1–5 y, >5–10 y, or >10 y; unknown; or data missing); mammography history (no, once, more than once, or unknown); history of benign breast disease (no, yes, or data missing): family history of breast cancer (no, yes, or data missing); smoking history (never, quit >10 y ago and smoked 20 cigarettes/d, quit >10 y ago and smoked >20 cigarettes/d, smoked in past 10 y and smoked 20 cigarettes/d, smoked in past 10 y and smoked >20 cigarettes/d, or data missing); and education (11 y, completed high school, some college or vocational training, or college graduate or postgraduate). Nutrients were entered into the models as their score quintile trend variable, and other variables were entered as continuous or categorical. In addition to the variables in the best-fit model, the full multivariable models included putative risk factors for breast cancer (ie, education, energy intake, HRT use, oral contraceptive use, mammography history, history of benign breast disease, family history of breast cancer, age at menarche, age at menopause, and age at first birth and number of live births), although they were not necessarily confounders.

We examined the effect of folic acid fortification of grain by testing whether the calendar year modified the association of folate and breast cancer (binary variable: <1998 and 1998; continuous calendar year from 1993 to 2003) and by ascertaining the association between postfortification food and total folate intakes and breast cancer in those who continued to be part of the cohort (n = 25 152) after 1997. Effect modification of the folate and breast cancer association by alcohol use, BMI, and HRT use and effect modification of the alcohol and breast cancer association by BMI, total folate intake, and HRT use were tested by using cross-product terms in the multivariable model and by comparing estimates of the stratum-specific HRs. Effect modification of the folate and alcohol variables by time during follow-up was also evaluated by using cross-product terms of the binary time variable (eg, <3 and 3 y of follow-up). We used SAS software (version 8.2; SAS Institute, Cary, NC) for these analyses. All tests were 2-sided.

	RESULTS

TOP ABSTRACT INTRODUCTION SUBJECTS AND METHODS RESULTS DISCUSSION REFERENCES

 
Women in our cohort reported a wide range of total folate intake, averaging 263 mg/d in the lowest quintile and 1154 mg/d in the highest quintile, according to the prefortification food composition data (Table 1). Total folate came primarily from food in the 2 lowest quintiles, supplements in the highest quintile, and both sources in the third and fourth quintiles. Of the women in the lowest quintile, 60% had used multivitamins, whereas >97% of the women in the top 3 quintiles had used multivitamins. Statistically significant trends across increasing quintiles of total folate intake were seen for all breast cancer risk factors except family history. Specifically, with increasing total folate intake, women were older, had lower BMIs and greater height, were more physically active and more educated, were younger at menarche and older at menopause, were more likely to report fewer live births, and were more likely to have a history of benign breast disease, oral contraceptive use, HRT use, and more than one mammography; they also less often reported age > 30 y at first birth (P for trend < 0.05). In addition, women in the highest quintile of total folate intake tended to consume more energy, protein, carbohydrate, fiber, carotenoids, and vitamins A, C, and E and less fat and alcohol than did women in the other quintiles.

The breast cancer HRs and 95% CIs for dietary folate from foods, supplements, total folate from foods and supplements, multivitamin use, and alcohol consumption are shown in Table 2. Given the age of women in our cohort, we show only results using the prefortification folate values, because most of our population's exposure occurred before fortification in 1998. We report the results from the best-fit multivariable models because they did not differ substantially from the models that adjusted for all putative breast cancer risk factors. Folate from foods alone and natural folate were not significantly associated with postmenopausal breast cancer. Women consuming 400 µg supplemental folic acid/d had a 19% greater risk (95% CI: 1.01, 1.41; P for trend = 0.04) of postmenopausal breast cancer than did women not taking supplemental folic acid. Those in the highest quintile of total folate had a 32% greater risk (95% CI: 1.04, 1.68; P for trend = 0.03) than did those in the lowest quintile. A 5-knot spline was used to model a nonlinear relation between energy-adjusted total folate and breast cancer risk. The test for nonlinearity did not reach statistical significance (chi-square test: 3.18, P > 0.05), which implies the relation is nearly linear. There was no significant interaction of these associations by calendar year. In addition, in women who remained in the cohort after 1997 and thus were exposed to and using postfortification folic acid concentrations (n = 25 152; 592 incident breast cancers), food folate was not positively associated with breast cancer (highest compared with lowest quintile: HR = 0.87; 95% CI: 0.68, 1.12; P for trend = 0.46), whereas total folate was positively but marginally not significantly associated (highest compared with lowest quintile: HR = 1.29; 95% CI: 0.99, 1.68; P for trend = 0.22).

In the women in our analysis who reported never taking multivitamins (n = 3706), folate from foods and natural folate intake were not associated with breast cancer (Table 3). When the major sources of food folate before 1998 were considered, breast cancer risk increased with the intake of highly fortified cereals: intakes of 100% RDA generated a significant trend (4th compared with the lowest quintile; HR = 1.69; 95% CI: 0.92, 3.10; P for trend = 0.03), whereas orange juice and fiber-rich fortified cereals showed no association. The fortified-cereal model, when adjusted for energy without using the residual method, also showed a strong positive association with breast cancer when nonconsumers were compared with consumers of >0 to < 1 g/d and consumers of 1 g/d (HR = 1.25; 95% CI: 0.74, 2.11 and 1.87; 95% CI: 1.13, 3.11, respectively; P for trend = 0.02). The associations between any of the folate, alcohol, or high folate food variables and breast cancer were not modified by follow-up time (<3 and >3 y follow-up after baseline).

Table 4

	DISCUSSION

TOP ABSTRACT INTRODUCTION SUBJECTS AND METHODS RESULTS DISCUSSION REFERENCES

The strengths of our study include its prospective design, in which diet and other exposures are assessed before the diagnosis of disease, which eliminates recall bias and reverse causation. Our questionnaire likely is comparable to other FFQs in that we relied on nationally representative dietary data to assign the database values used to calculate nutrient estimates from foods reported on the FFQ (29).

Several retrospective and prospective epidemiologic studies support the hypothesis that folate may play a role in postmenopausal breast cancer, but not all study results are consistent (2-21). We reviewed the results of cohort studies because their design is most similar to the current study. The Nurses' Health Study (NHS) has observed a significant inverse association between total folate intake and postmenopausal breast cancer (>600 ug/d compared with 150–299 µg/d total folate intake: RR = 0.86; 95% CI: 0.76, 0.98; P for trend = 0.02) that was limited to the highest category of folate, which included intakes that could be achieved only by taking vitamin supplements (2). The NHS and the Canadian National Breast Screening study both showed stronger protective folate associations in women who reported alcohol consumption of 1 drink (or 15 g)/d (2, 4). In addition, a nested case-control study in the NHS that measured plasma folate showed associations (>14.0 compared with < 4.6 ng/mL: OR = 0.73; 95% CI: 0.50, 1.07; P for trend = 0.06) and interactions with alcohol consumption similar to those observed in the dietary studies; however, no association was observed with plasma homocysteine, a functional biomarker for folate status (3). The Iowa Women's Health Study showed that greater folate intake attenuated the risk of breast cancer in women with a family history of breast cancer but only in those who did not drink alcohol, whereas no association was observed for folate intake in women who did not have a family history of breast cancer (34). In contrast, the American Cancer Society's Cancer Prevention Study did not observe main effects for total dietary folate (>603.7 compared with < 209 µg total folate intake/d: RR = 1.10; 95% CI: 0.94, 1.29) or interactions with alcohol use (8); nor did a nested case-control study of the Washington County CLUE 1 and CLUE 2 cohorts that measured serum folate (lowest compared with highest quintile of serum folate: RR = 0.66; 95% CI: 0.17, 2.60; P for trend = 0.79) (9). Finally, there was no association between dietary folate and breast cancer (RR = 1.01; 95% CI: 0.93, 1.10; P for trend = 0.79) in the Melborne Collaborative Cohort (17).

There are several differences between our study and these earlier prospective studies. The postmenopausal women from the PLCO Trial have considerably higher total folate intake (median intake: 660 µg/d) than do other cohorts (300–350 µg/d; 2, 4, 5, 8), particularly from folic acid, the more biologically available form. Therefore, our population may have not had sufficiently low folate range to allow the observation of protective associations if they exist. The cohorts in which significant protective folate associations were observed (2-4) began in the 1980s with baseline measures and a greater proportion of follow-up occurring before public awareness of the potential health benefits of folate intake, and they had a longer duration of follow-up. Finally, many studies did not control for socioeconomic status or education, both of which are important potential confounders for postmenopausal breast cancer (2-4) that attenuated risk estimates in our analysis.

The positive association between alcohol consumption and breast cancer as modified by folate intake in the current study is consistent with findings from other studies. A meta-analysis of 53 studies examining the association between alcohol consumption and breast cancer showed that, compared with nondrinkers, women consuming 35–44 g alcohol/d (2–3 drinks) had a 32% greater risk for breast cancer, and those consuming 45 g alcohol/d (>3 drinks) had a 46% greater risk, both of which were significant (22). The biological mechanism that may be the most important explanation of the alcohol and breast cancer association—namely, an increase in sex hormone concentrations—is fairly well established and further supported by randomized controlled alcohol feeding trials (24, 35). The NHS (2), Iowa Women's Health Study (5), and the Melborne Collaborative Cohort (17) also showed stronger positive associations with increasing alcohol consumption in women who had low folate intake. Additional analyses within the Iowa Women's Study and the NHS showed that significant positive associations with low folate intake and high alcohol consumption were observed only for estrogen receptor–negative tumors (7, 36). The biological mechanisms that may explain the interactions between alcohol and folate and breast cancer risk, as well as the association with estrogen receptor–negative status, remain unclear.

The positive association that we observed between breast cancer and total folate intake and supplemental folic acid is biologically plausible, but it should be interpreted with caution. Along with previous experimental and epidemiologic observations, our results suggest that the role of folate in breast cancer development may be more complex than previously appreciated. The 3 rodent studies that have examined the effect of folic acid on breast cancer development suggest that folic acid deficiency decreases chemically induced mammary cancer (37-39). Among participants in a large (n = 2928) trial of folic acid supplementation during pregnancy, women who were randomly assigned to the highest folic acid dose, 5 mg/d, had a 70% greater risk of total cancer (n = 112), which was significant, and a 2-fold greater risk of breast cancer (n = 31), which was not significant, than did women in the placebo group during follow-up that lasted up to 36 y (40). The folic acid dose used in that trial was considerably higher than that currently prescribed to pregnant women, and the greater risk of cancer could have been due to chance, given that the trial was not powered for a cancer outcome (40). In addition, folic acid deprivation with antifolate chemotherapy such as 5-fluorouracil and methotrexate, which interferes with thymidylate uptake and ultimately DNA synthesis, has been commonly used as an effective treatment for patients with breast cancer (41), and it is possible that very high folic acid intakes could promote the growth of an existing breast neoplasm or cancer (42). Compared with matched noncancerous breast tissue, breast cancer tissue contained higher folate concentrations but was more hypomethylated (27). High folic acid concentrations could contribute to epigenetic changes in gene-regulatory mechanisms, which may result in gene silencing and enhanced cancer development (43), or they could promote the growth of tumors expressing folate receptor (FR-), which is present in 25% of breast cancers (44). However, these mechanisms are speculative, and folate's effect on these molecular processes during breast cancer development is unknown.

In conclusion, our study does not support a simple protective association between dietary folate and breast cancer. Although our results confirm previous positive associations between alcohol consumption and breast cancer, particularly in subjects with lower folate intake, they also suggest that high folate intake, which is generally attributable to folic acid from supplements, may increase the risk of breast cancer in postmenopausal women. Because of the complexity of folate function, it is hypothetically possible that both deficiency and abundance of folate may contribute to breast carcinogenesis at different stages of tumor development or in different neoplastic or tumor phenotypes. It is also possible that our observed positive associations may be due to chance or uncontrolled confounding. The associations could be explained by other components of multivitamins and vitamin-fortified breakfast cereals or by behaviors associated with the intake of these products. In particular, residual confounding from HRT, which is known to increase breast cancer risk, is possible. However, the positive association with the intake of 400 µg supplemental folic acid/d remained when the analysis was limited to women reporting no HRT use (n = 7903; HR = 1.48; 95% CI: 1.06, 2.05; P for trend = 0.02). The positive association with total folate intake that the current study found should be interpreted with great caution, and replication of our findings is important. Further research is needed to confirm our results and to elucidate the mechanisms by which folate modifies the association between alcohol consumption and breast cancer development.

	ACKNOWLEDGMENTS

 
We gratefully acknowledge Barry Graubard of the Biostatistics Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Department of Health and Human Services, for his assistance with statistical analysis.

RZS-S, S-CC, MFL, RGZ, and RNH contributed to study design. RZS-S, S-CC, MFL, RNH, and RGZ contributed to data analysis. RZS-S was responsible for writing and revising the manuscript. S-CC, MFL, KAJ, CJ, SSB, RNH, and RGZ provided substantive editorial comments on manuscript drafts. None of the authors had any personal or financial conflict of interest.

	REFERENCES

TOP ABSTRACT INTRODUCTION SUBJECTS AND METHODS RESULTS DISCUSSION REFERENCES

 

1. Choi SW, Mason JB. Folate status: effects on pathways of colorectal carcinogenesis. J Nutr 2002; 132: 2413S-8S.[Abstract/Free Full Text]
2. Zhang S, Hunter DJ, Hankinson SE, et al. A prospective study of folate intake and the risk of breast cancer. JAMA 1999; 281: 1632-7.[Abstract/Free Full Text]
3. Zhang SM, Willett WC, Selhub J, et al. Plasma folate, vitamin B6, vitamin B12, homocysteine, and risk of breast cancer. J Natl Cancer Inst 2003; 95: 373-80.[Abstract/Free Full Text]
4. Rohan TE, Jain MG, Howe GR, Miller AB. Dietary folate consumption and breast cancer risk. J Natl Cancer Inst 2000; 92: 266-9.[Free Full Text]
5. Sellers TA, Kushi LH, Cerhan JR, et al. Dietary folate intake, alcohol, and risk of breast cancer in a prospective study of postmenopausal women. Epidemiology 2001; 12: 420-8.[Medline]
6. Sellers TA, Alberts SR, Vierkant RA, et al. High-folate diets and breast cancer survival in a prospective cohort study. Nutr Cancer 2002; 44: 139-44.[Medline]
7. Sellers TA, Vierkant RA, Cerhan JR, et al. Interaction of dietary folate intake, alcohol, and risk of hormone receptor-defined breast cancer in a prospective study of postmenopausal women. Cancer Epidemiol Biomarkers Prev 2002; 11: 1104-7.[Abstract/Free Full Text]
8. Feigelson HS, Jonas CR, Robertson AS, McCullough ML, Thun MJ, Calle EE. Alcohol, folate, methionine, and risk of incident breast cancer in the American Cancer Society Cancer Prevention Study II Nutrition Cohort. Cancer Epidemiol Biomarkers Prev 2003; 12: 161-4.[Abstract/Free Full Text]
9. Wu K, Helzlsouer KJ, Comstock GW, Hoffman SC, Nadeau MR, Selhub J. A prospective study on folate, B12, and pyridoxal 5-phosphate (B6) and breast cancer. Cancer Epidemiol Biomarkers Prev 1999; 8: 209-17.[Abstract/Free Full Text]
10. Graham S, Hellmann R, Marshall J, et al. Nutritional epidemiology of postmenopausal breast cancer in western New York. Am J Epidemiol 1991; 134: 552-66.[Abstract/Free Full Text]
11. Levi F, Pasche C, Lucchini F, La Vecchia C. Dietary intake of selected micronutrients and breast-cancer risk. Int J Cancer 2001; 91: 260-3.[Medline]
12. Negri E, La Vecchia C, Franceschi S. Re: dietary folate consumption and breast cancer risk. J Natl Cancer Inst 2000; 92: 1270-1.[Free Full Text]
13. Chen J, Gammon MD, Chan W, et al. One-carbon metabolism, MTHFR polymorphisms, and risk of breast cancer. Cancer Res 2005; 65: 1606-14.[Abstract/Free Full Text]
14. Shrubsole MJ, Jin F, Dai Q, et al. Dietary folate intake and breast cancer risk: results from the Shanghai Breast Cancer Study. Cancer Res 2001; 61: 7136-41.[Abstract/Free Full Text]
15. Potischman N, Swanson CA, Coates RJ, et al. Intake of food groups and associated micronutrients in relation to risk of early-stage breast cancer. Int J Cancer 1999; 82: 315-21.[Medline]
16. Freudenheim JL, Marshall JR, Vena JE, et al. Premenopausal breast cancer risk and intake of vegetables, fruits, and related nutrients. J Natl Cancer Inst 1996; 88: 340-8.[Abstract/Free Full Text]
17. Baglietto L, English DR, Gertig DM, Hopper JL, Giles GG. Does dietary folate intake modify effect of alcohol consumption on breast cancer risk? Prospective cohort study. BMJ 2005; 331: 807. Epub 2005 Aug 8.[Abstract/Free Full Text]
18. Cho E, Spiegelman D, Hunter DJ, et al. Premenopausal intakes of vitamins A, C, and E, folate, and carotenoids, and risk of breast cancer. Cancer Epidemiol Biomarkers Prev. 2003; 12: 713-20.[Abstract/Free Full Text]
19. Eichholzer M, Luthy J, Moser U, Fowler B. Folate and the risk of colorectal, breast and cervix cancer: the epidemiological evidence. Swiss Med Wkly 2001; 131: 539-49.[Medline]
20. Thorand B, Kohlmeier L, Simonsen N, Croghan C, Thamm M. Intake of fruits, vegetables, folic acid and related nutrients and risk of breast cancer in postmenopausal women. Public Health Nutr 1998; 1: 147-56.[Medline]
21. Zhu K, Davidson NE, Hunter S, et al. Methyl-group dietary intake and risk of breast cancer among African-American women: a case-control study by methylation status of the estrogen receptor alpha genes. Cancer Causes Control 2003; 14: 827-36.[Medline]
22. Hamajima N, Hirose K, Tajima K, et al. Alcohol, tobacco and breast cancer—collaborative reanalysis of individual data from 53 epidemiological studies, including 58,515 women with breast cancer and 95,067 women without the disease. Br J Cancer 2002; 87: 1234-45.[Medline]
23. Smith-Warner SA, Spiegelman D, Yaun SS, et al. Alcohol and breast cancer in women: a pooled analysis of cohort studies. JAMA 1998; 279: 535-40.[Abstract/Free Full Text]
24. Dorgan JF, Baer DJ, Albert PS, et al. Serum hormones and the alcohol-breast cancer association in postmenopausal women. J Natl Cancer Inst 2001; 93: 710-5.[Abstract/Free Full Text]
25. Halsted CH, Villanueva JA, Devlin AM, Chandler CJ. Metabolic interactions of alcohol and folate. J Nutr 2002; 132: 2367S-72S.[Abstract/Free Full Text]
26. Johanning GL, Heimburger DC, Piyathilake CJ. DNA methylation and diet in cancer. J Nutr 2002; 132: 3814S-8S.[Abstract/Free Full Text]
27. Prorok PC, Andriole GL, Bresalier RS, et al. Design of the Prostate, Lung, Colorectal and Ovarian (PLCO) Cancer Screening Trial. Control Clin Trials 2000; 21: 273S-309S.[Medline]
28. Subar AF, Midthune D, Kulldorff M, et al. Evaluation of alternative approaches to assign nutrient values to food groups in food frequency questionnaires. Am J Epidemiol 2000; 152: 279-86.[Abstract/Free Full Text]
29. Subar AF, Thompson FE, Smith AF, et al. Improving food frequency questionnaires: a qualitative approach using cognitive interviewing. J Am Diet Assoc 1995; 95: 781-8.[Medline]
30. Thompson FE, Subar AF, Brown CC, et al. Cognitive research enhances accuracy of food frequency questionnaire reports: results of an experimental validation study. J Am Diet Assoc 2002; 102: 212-25.[Medline]
31. Yetley EA, Rader JI. Modeling the level of fortification and post-fortification assessments: U.S. experience. Nutr Rev 2004; 62: S50-9.[Medline]
32. Willett W, Stampfer MJ. Total energy intake: implications for epidemiologic analyses. Am J Epidemiol 1986; 124: 17-27.[Free Full Text]
33. Sellers TA, Grabrick DM, Vierkant RA, et al. Does folate intake decrease risk of postmenopausal breast cancer among women with a family history? Cancer Causes Control 2004; 15: 113-20.[Medline]
34. Dorgan JF, Reichman ME, Judd JT, et al. The relation of reported alcohol ingestion to plasma levels of estrogens and androgens in premenopausal women (Maryland, United States). Cancer Causes Control 1994; 5: 53-60.[Medline]
35. Zhang SM, Hankinson SE, Hunter DJ, Giovannucci EL, Colditz GA, Willett WC. Folate intake and risk of breast cancer characterized by hormone receptor status. Cancer Epidemiol Biomarkers Prev 2005; 14: 2004-8.[Abstract/Free Full Text]
36. Baggott JE, Vaughn WH, Juliana MM, Eto I, Krumdieck CL, Grubbs CJ. Effects of folate deficiency and supplementation on methylnitrosourea-induced rat mammary tumors. J Natl Cancer Inst 1992; 84: 1740-4.[Abstract/Free Full Text]
37. Kotsopoulos J, Sohn KJ, Martin R, et al. Dietary folate deficiency suppresses N-methyl-N-nitrosourea-induced mammary tumorigenesis in rats. Carcinogenesis 2003; 24: 937-44.[Abstract/Free Full Text]
38. Kotsopoulos J, Medline A, Renlund R, et al. Effects of dietary folate on the development and progression of mammary tumors in rats. Carcinogenesis 2005; 26: 1603-12.[Abstract/Free Full Text]
39. Charles D, Ness AR, Campbell D, Davey SG, Hall MH. Taking folate in pregnancy and risk of maternal breast cancer. BMJ 2004; 329: 1375-6.[Free Full Text]
40. Lehman NL. Future potential of thymidylate synthase inhibitors in cancer therapy. Expert Opin Investig Drugs 2002; 11: 1775-87.[Medline]
41. Sohn KJ, Croxford R, Yates Z, Lucock M, Kim YI. Effect of the methylenetetrahydrofolate reductase C677T polymorphism on chemosensitivity of colon and breast cancer cells to 5-fluorouracil and methotrexate. J Natl Cancer Inst 2004; 96: 134-44.[Abstract/Free Full Text]
42. Kim YI. Will mandatory folic acid fortification prevent or promote cancer? Am J Clin Nutr 2004; 80: 1123-8.[Abstract/Free Full Text]
43. Russell-Jones G, McTavish K, McEwan J, Rice J, Nowotnik D. Vitamin-mediated targeting as a potential mechanism to increase drug uptake by tumors. J Inorg Biochem 2004; 98: 1625-33.[Medline]

This article has been cited by other articles:

				J. W Miller, M. G Garrod, L. H Allen, M. N Haan, and R. Green Metabolic evidence of vitamin B-12 deficiency, including high homocysteine and methylmalonic acid and low holotranscobalamin, is more pronounced in older adults with elevated plasma folate Am. J. Clinical Nutrition, December 1, 2009; 90(6): 1586 - 1592. [Abstract] [Full Text] [PDF]

				M. Ebbing, K. H. Bonaa, O. Nygard, E. Arnesen, P. M. Ueland, J. E. Nordrehaug, K. Rasmussen, I. Njolstad, H. Refsum, D. W. Nilsen, et al. Cancer Incidence and Mortality After Treatment With Folic Acid and Vitamin B12 JAMA, November 18, 2009; 302(19): 2119 - 2126. [Abstract] [Full Text] [PDF]

				G. M. Lindzon, A. Medline, K.-J. Sohn, F. Depeint, R. Croxford, and Y.-I. Kim Effect of folic acid supplementation on the progression of colorectal aberrant crypt foci Carcinogenesis, September 1, 2009; 30(9): 1536 - 1543. [Abstract] [Full Text] [PDF]

				J. Q. Lew, N. D. Freedman, M. F. Leitzmann, L. A. Brinton, R. N. Hoover, A. R. Hollenbeck, A. Schatzkin, and Y. Park Alcohol and Risk of Breast Cancer by Histologic Type and Hormone Receptor Status in Postmenopausal Women: The NIH-AARP Diet and Health Study Am. J. Epidemiol., August 1, 2009; 170(3): 308 - 317. [Abstract] [Full Text] [PDF]

				Q. Yang, R. M. Bostick, J.M. Friedman, and W. D. Flanders Serum Folate and Cancer Mortality Among U.S. Adults: Findings from the Third National Health and Nutritional Examination Survey Linked Mortality File Cancer Epidemiol. Biomarkers Prev., May 1, 2009; 18(5): 1439 - 1447. [Abstract] [Full Text] [PDF]

				U. Ericson, E. Sonestedt, M. I.L. Ivarsson, B. Gullberg, J. Carlson, H. Olsson, and E. Wirfalt Folate Intake, Methylenetetrahydrofolate Reductase Polymorphisms, and Breast Cancer Risk in Women from the Malmo Diet and Cancer Cohort Cancer Epidemiol. Biomarkers Prev., April 1, 2009; 18(4): 1101 - 1110. [Abstract] [Full Text] [PDF]

				S. R. Cummings, J. A. Tice, S. Bauer, W. S. Browner, J. Cuzick, E. Ziv, V. Vogel, J. Shepherd, C. Vachon, R. Smith-Bindman, et al. Prevention of Breast Cancer in Postmenopausal Women: Approaches to Estimating and Reducing Risk J Natl Cancer Inst, March 18, 2009; 101(6): 384 - 398. [Abstract] [Full Text] [PDF]

				S. S Maruti, C. M Ulrich, and E. White Folate and one-carbon metabolism nutrients from supplements and diet in relation to breast cancer risk Am. J. Clinical Nutrition, February 1, 2009; 89(2): 624 - 633. [Abstract] [Full Text] [PDF]

				R. Green Is it time for vitamin B-12 fortification? What are the questions? Am. J. Clinical Nutrition, February 1, 2009; 89(2): 712S - 716S. [Abstract] [Full Text] [PDF]

				S. C. Larsson, L. Bergkvist, and A. Wolk Folate Intake and Risk of Breast Cancer by Estrogen and Progesterone Receptor Status in a Swedish Cohort Cancer Epidemiol. Biomarkers Prev., December 1, 2008; 17(12): 3444 - 3449. [Abstract] [Full Text] [PDF]

				R. D. Kalmbach, S. F. Choumenkovitch, A. P. Troen, P. F. Jacques, R. D'Agostino, and J. Selhub A 19-Base Pair Deletion Polymorphism in Dihydrofolate Reductase Is Associated with Increased Unmetabolized Folic Acid in Plasma and Decreased Red Blood Cell Folate J. Nutr., December 1, 2008; 138(12): 2323 - 2327. [Abstract] [Full Text] [PDF]

				C. H Halsted Perspectives on obesity and sweeteners, folic acid fortification and vitamin D requirements Fam. Pract., December 1, 2008; 25(suppl_1): i44 - i49. [Abstract] [Full Text] [PDF]

				K. B Michels The promise and challenges of population strategies of prevention Int. J. Epidemiol., October 1, 2008; 37(5): 914 - 916. [Full Text] [PDF]

				R. D Kalmbach, S. F Choumenkovitch, A. M Troen, R. D'Agostino, P. F Jacques, and J. Selhub Circulating folic acid in plasma: relation to folic acid fortification Am. J. Clinical Nutrition, September 1, 2008; 88(3): 763 - 768. [Abstract] [Full Text] [PDF]

				E. G. Luebeck, S. H. Moolgavkar, A. Y. Liu, A. Boynton, and C. M. Ulrich Does Folic Acid Supplementation Prevent or Promote Colorectal Cancer? Results from Model-Based Predictions Cancer Epidemiol. Biomarkers Prev., June 1, 2008; 17(6): 1360 - 1367. [Abstract] [Full Text] [PDF]

				K. Ishitani, J. Lin, J. E. Manson, J. E. Buring, and S. M. Zhang A Prospective Study of Multivitamin Supplement Use and Risk of Breast Cancer Am. J. Epidemiol., May 15, 2008; 167(10): 1197 - 1206. [Abstract] [Full Text] [PDF]

				J. Lin, I-M. Lee, N. R Cook, J. Selhub, J. E Manson, J. E Buring, and S. M Zhang Plasma folate, vitamin B-6, vitamin B-12, and risk of breast cancer in women Am. J. Clinical Nutrition, March 1, 2008; 87(3): 734 - 743. [Abstract] [Full Text] [PDF]

				A. E Millen, A. F Subar, B. I Graubard, U. Peters, R. B Hayes, J. L Weissfeld, L. A Yokochi, R. G Ziegler, and for the Prostate, Lung, Colorectal, and Ovarian (P Fruit and vegetable intake and prevalence of colorectal adenoma in a cancer screening trial Am. J. Clinical Nutrition, December 1, 2007; 86(6): 1754 - 1764. [Abstract] [Full Text] [PDF]

				M. van den Donk, L. Pellis, J. W. Crott, M. van Engeland, P. Friederich, F. M. Nagengast, J. D. van Bergeijk, S. Y. de Boer, J. B. Mason, F. J. Kok, et al. Folic Acid and Vitamin B-12 Supplementation Does Not Favorably Influence Uracil Incorporation and Promoter Methylation in Rectal Mucosa DNA of Subjects with Previous Colorectal Adenomas J. Nutr., September 1, 2007; 137(9): 2114 - 2120. [Abstract] [Full Text] [PDF]

				R. G. Ziegler and U. Lim One-Carbon Metabolism, Colorectal Carcinogenesis, Chemoprevention with Caution J Natl Cancer Inst, August 15, 2007; 99(16): 1214 - 1215. [Full Text] [PDF]

				C. M Ulrich Folate and cancer prevention: a closer look at a complex picture Am. J. Clinical Nutrition, August 1, 2007; 86(2): 271 - 273. [Full Text] [PDF]

				U. Ericson, E. Sonestedt, B. Gullberg, H. Olsson, and E. Wirfalt High folate intake is associated with lower breast cancer incidence in postmenopausal women in the Malmo Diet and Cancer cohort Am. J. Clinical Nutrition, August 1, 2007; 86(2): 434 - 443. [Abstract] [Full Text] [PDF]

				X. Xu, M. D. Gammon, H. Zhang, J. G. Wetmur, M. Rao, S. L. Teitelbaum, J. A. Britton, A. I. Neugut, R. M. Santella, and J. Chen Polymorphisms of one-carbon-metabolizing genes and risk of breast cancer in a population-based study Carcinogenesis, July 1, 2007; 28(7): 1504 - 1509. [Abstract] [Full Text] [PDF]

				N. J Wald and G. P Oakley Should folic acid fortification be mandatory? Yes BMJ, June 16, 2007; 334(7606): 1252 - 1252. [Full Text] [PDF]

				R. A Hubner, R. D Houlston, and K. R Muir Should folic acid fortification be mandatory? No BMJ, June 16, 2007; 334(7606): 1253 - 1253. [Full Text] [PDF]

				B. F. Cole, J. A. Baron, R. S. Sandler, R. W. Haile, D. J. Ahnen, R. S. Bresalier, G. McKeown-Eyssen, R. W. Summers, R. I. Rothstein, C. A. Burke, et al. Folic Acid for the Prevention of Colorectal Adenomas: A Randomized Clinical Trial JAMA, June 6, 2007; 297(21): 2351 - 2359. [Abstract] [Full Text] [PDF]

				X. Xu, M. D Gammon, J. G Wetmur, M. Rao, M. M Gaudet, S. L Teitelbaum, J. A Britton, A. I Neugut, R. M Santella, and J. Chen A functional 19-base pair deletion polymorphism of dihydrofolate reductase (DHFR) and risk of breast cancer in multivitamin users Am. J. Clinical Nutrition, April 1, 2007; 85(4): 1098 - 1102. [Abstract] [Full Text] [PDF]

				S. C. Larsson, E. Giovannucci, and A. Wolk Folate and Risk of Breast Cancer: A Meta-analysis J Natl Cancer Inst, January 3, 2007; 99(1): 64 - 76. [Abstract] [Full Text] [PDF]

				S. J. Lewis, R. M. Harbord, R. Harris, and G. D. Smith Meta-analyses of Observational and Genetic Association Studies of Folate Intakes or Levels and Breast Cancer Risk. J Natl Cancer Inst, November 15, 2006; 98(22): 1607 - 1622. [Abstract] [Full Text] [PDF]

				Y-I Kim Folate: a magic bullet or a double edged sword for colorectal cancer prevention? Gut, October 1, 2006; 55(10): 1387 - 1389. [Full Text] [PDF]

This Article Abstract Full Text (PDF) Purchase Article View Shopping Cart Alert me when this article is cited Alert me if a correction is posted Citation Map Services Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via HighWire Citing Articles via Google Scholar Google Scholar Articles by Stolzenberg-Solomon, R. Z Articles by Ziegler, R. G Search for Related Content PubMed PubMed Citation Articles by Stolzenberg-Solomon, R. Z Articles by Ziegler, R. G Agricola Articles by Stolzenberg-Solomon, R. Z Articles by Ziegler, R. G