Hostname: page-component-586b7cd67f-rcrh6 Total loading time: 0 Render date: 2024-11-28T15:18:32.050Z Has data issue: false hasContentIssue false

Risk of endometrial cancer in relation to individual nutrients from diet and supplements

Published online by Cambridge University Press:  14 July 2011

Rita K Biel*
Affiliation:
Division of Cancer Care, Department of Population Health Research, Alberta Health Services, 1331 – 29 St. N.W., Calgary, Alberta T2N 4N2, Canada
Ilona Csizmadi
Affiliation:
Division of Cancer Care, Department of Population Health Research, Alberta Health Services, 1331 – 29 St. N.W., Calgary, Alberta T2N 4N2, Canada Department of Community Health Sciences, Faculty of Medicine, University of Calgary, Calgary, Alberta, Canada Department of Oncology, Faculty of Medicine, University of Calgary, Calgary, Alberta, Canada
Linda S Cook
Affiliation:
Division of Cancer Care, Department of Population Health Research, Alberta Health Services, 1331 – 29 St. N.W., Calgary, Alberta T2N 4N2, Canada Department of Community Health Sciences, Faculty of Medicine, University of Calgary, Calgary, Alberta, Canada Department of Internal Medicine, NM Health Sciences Center, University of New Mexico, Albuquerque, NM, USA
Kerry S Courneya
Affiliation:
Faculty of Physical Education and Recreation, E488 Van Vliet Centre, University of Alberta, Edmonton, Alberta, Canada
Anthony M Magliocco
Affiliation:
Division of Cancer Care, Department of Population Health Research, Alberta Health Services, 1331 – 29 St. N.W., Calgary, Alberta T2N 4N2, Canada Department of Oncology, Faculty of Medicine, University of Calgary, Calgary, Alberta, Canada Department of Pathology and Laboratory Medicine, Faculty of Medicine, University of Calgary, Calgary, Alberta, Canada
Christine M Friedenreich
Affiliation:
Division of Cancer Care, Department of Population Health Research, Alberta Health Services, 1331 – 29 St. N.W., Calgary, Alberta T2N 4N2, Canada Department of Community Health Sciences, Faculty of Medicine, University of Calgary, Calgary, Alberta, Canada Department of Oncology, Faculty of Medicine, University of Calgary, Calgary, Alberta, Canada
*
*Corresponding author: Email [email protected]
Rights & Permissions [Opens in a new window]

Abstract

Objective

Intake of nutrients may influence the risk of endometrial cancer (EC). We aimed to estimate the association of intake of individual nutrients from food and from food plus supplements with EC occurrence.

Design

A population-based case–control study conducted in Canada (2002–2006).

Setting

Nutrient intakes from food and supplements were assessed using an FFQ. Logistic regression was used to estimate EC risk within quartile levels of nutrient intakes.

Subjects

Incident EC cases (n 506) were identified from the Alberta Cancer Registry, and population controls were frequency- and age-matched to cases (n 981).

Results

There existed little evidence of an association with EC for the majority of macronutrients and micronutrients examined. We observed a statistically significant increased risk associated with the highest, compared with the lowest, quartile of intake of dietary cholesterol (multivariable-adjusted OR = 1·51, 95 % CI 1·08, 2·11; P for trend = 0·02). Age-adjusted risk at the highest level of intake was significantly reduced for Ca from food sources (OR = 0·73, 95 % CI 0·54, 0·99) but was attenuated in the multivariable model (OR = 0·82, 95 % CI 0·59, 1·13). When intake from supplements was included in Ca intake, risk was significantly reduced by 28 % with higher Ca (multivariable-adjusted OR = 0·72, 95 % CI 0·51, 0·99, P for trend = 0·04). We also observed unexpected increased risks at limited levels of intakes of dietary soluble fibre, vitamin C, thiamin, vitamin B6 and lutein/zeaxanthin, with no evidence for linear trend.

Conclusions

The results of our study suggest a positive association between dietary cholesterol and EC risk and an inverse association with Ca intake from food sources and from food plus supplements.

Type
Research paper
Copyright
Copyright © The Authors 2011

Endometrial cancer (EC) ranks as the fourth most common cancer among women in Canada, with an estimated 4500 women newly diagnosed and 790 estimated deaths from this cancer in 2010(1). Obesity and oestrogen-only menopausal hormone therapy (HT) expose women to higher levels of oestrogen and are well-established risk factors for EC(Reference Kaaks, Lukanova and Kurzer2). Diet may also mediate endogenous oestrogen levels, promoting endometrial carcinogenesis(Reference Kaaks, Lukanova and Kurzer2). A 2007 review concluded that the evidence for an association between diet and EC was ‘limited’, but ‘suggestive’ for a decrease in risk with consumption of non-starchy vegetables, particularly cruciferous vegetables, and for an increase in risk with consumption of red meat, providing rationale for further study of diet in EC aetiology(3). A conclusive link with macro- and micronutrients has not been established. Micronutrient intake from food alone may not fully reflect an individual's overall biological micronutrient dose, as vitamins and minerals are also widely consumed as supplements. The prevalence of vitamin/mineral supplement use in Canada was recently estimated to be 47 % among women, and a higher 60 % among women aged ≥51 years(Reference Vatanparast, Adolphe and Whiting4). Hence, misclassification among exposure levels has likely impacted the observed dietary associations with EC, contributing to inconsistent findings among studies. Few studies have accounted for these additional nutrient sources through adjustment, through addition to diet or by restriction to non-users of supplements. Only two studies have examined EC risk in association with micronutrient intake from food and supplements combined, examining a limited number of micronutrients(Reference Jain, Howe and Rohan5, Reference Jain, Rohan and Howe6). To address this gap, we collected information on a wide range of micronutrients from food and supplements through a case–control study of EC.

Methods

Study population

A population-based case–control study of EC risk was conducted in Alberta, Canada, and details of this study have been reported(Reference Friedenreich, Cook and Magliocco7). As part of the present study, information was collected on past-year dietary intake. All participants provided signed informed consent, and ethical approval was obtained from the Alberta Cancer Board and from the University of Calgary. Cases, identified from the Alberta Cancer Registry, comprised women aged 30–79 years with incident, primary-site EC diagnosed in Alberta between 12 September 2002 and 15 February 2006. Controls comprised ≥30-year-old Alberta residents recruited through random digit dialling and frequency-matched to cases 2:1 on the basis of age (±5 years)(Reference Waksberg8). All participants completed in-person interviews and a self-administered diet history questionnaire (DHQ). The participation rate was 67·9 % (n 549) for cases and 52·2 % (n 1036) for controls. We excluded eleven women because of unsatisfactory interviews, forty-seven women because they did not complete a DHQ and forty women because they reported total daily energy intake values <2510 kJ (600 kcal)/d (n 33) and >20 920 kJ (5000 kcal)/d (n 7). Thus, 506 cases and 981 controls were included in the present analysis.

Data collection

In-person interviews were conducted and anthropometric measurements were taken. Participants self-reported their past-year dietary intake using a Canadian version of the National Cancer Institute's (NCI) DHQ(9) following their interview. The cognitively tested DHQ queries frequency and portion size intakes of 124 individual food items. A subset of questions ascertains seasonal food intake, special foods and use or addition of fat. The original US version was validated against biomarkers of energy expenditure and protein intake(Reference Subar, Kipnis and Troiano10Reference Thompson, Subar and Brown12). Because of differences in nutrient fortification(Reference Barr, Kwan and Janelle13), the Canadian DHQ nutrient database was previously modified for use in Canada(Reference Csizmadi, Kahle and Ullman14). The ‘Diet*Calc’ Analysis Program version 1·4·3 (National Cancer Institute, Bethesda, MD, USA) was used to derive nutrient intake variables.

Twenty-seven nutrients were examined in total. Macronutrients included total energy (kJ (kcal)), protein (g), total fat (g), saturated fat (g), monounsaturated fat (g), polyunsaturated fat (g), discretionary fat (g), cholesterol (mg), carbohydrate (g), dietary fibre NDSR (Nutrition Data Systems for Research; g), insoluble fibre (g) and soluble fibre (g). We examined food and supplement intakes, expressed as daily intakes, of twelve individual micronutrients including vitamin A (retinol equivalents), β-carotene (μg), vitamin C (mg), vitamin D (μg), vitamin E (mg α-tocopherol equivalents), folate (μg dietary folate equivalents (DFE)), thiamin (B1; mg), riboflavin (B2; mg), niacin (mg), vitamin B6 (mg), vitamin B12 (μg) and Ca (mg). Methionine (g) and additional phytochemicals lycopene (μg) and lutein/zeaxanthin (μg) were examined from food sources only. Total folate intake, expressed as DFE, was estimated by accounting for the greater bioavailability of synthetic folic acid compared with naturally occurring food folate(15). Synthetic folic acid was multiplied by 1·7 before this amount was added to naturally occurring food folate to derive total DFE from food or from food and supplements(15, Reference Maruti, Ulrich and White16).

Statistical analyses

Nutrients were natural log transformed and adjusted for total energy using the residual method(Reference Willett, Howe and Kushi17). Unconditional logistic regression analysis was used to estimate OR and 95 % CI for the risk of EC within nutrient intake quartiles according to the distribution among controls in age-adjusted and multivariable-adjusted models. If an association with EC was detected, possible effect modification was assessed by stratifying these models by BMI (<25·0 v. ≥25·0 kg/m2), waist circumference (<88 v. ≥88 cm) and menopausal status (pre/perimenopausal v. postmenopausal) and by examining the interaction terms between nutrient intake exposure levels and these effect modifiers in logistic models. A stratified analysis by HT use was also undertaken to examine postmenopausal women not taking HT compared with those taking only oestrogen plus progesterone (E + P) HT. The following factors were considered as confounders because of their known or suspected associations with both EC risk and diet: age (years), total energy intake (kJ (kcal)/d; as per the residuals-adjusted model, except in the case of modelling total energy intake as an exposure), age at menarche (years), BMI (<25·0 v. 25·0–29·9, ≥30·0 kg/m2), parity (0 v. 1–2, more than two pregnancies at ≥20 weeks’ gestation), education (lower than high school v. high school or higher), hypertension history (ever v. never), history of type 2 diabetes (ever v. never), hormone contraceptive use (never v. ever), HT use combined with menopausal status (post/perimenopausal/no HT v. post/perimenopausal + oestrogen; post/perimenopausal + E + P; post/perimenopausal + other menopausal hormones; premenopausal), lifetime alcohol consumption (0 drinks v. <1 drink, ≥1 drink/d) and smoking (smoker, ex-smoker or current smoker). All covariates were first individually assessed.

Age and total energy intake were included in all models. Nutrient-specific supplement use (yes v. no) was included in all micronutrient diet models, except for lycopene, lutein/zeaxanthin and methionine. Covariates were deleted from saturated models using a backward elimination procedure(Reference Kleinbaum and Kupper18), with the exception of biologically important covariates. A significant change in effect was defined as >10 % difference in the point estimate from the saturated model OR. Fully adjusted models included age, total energy intake, age at menarche, BMI, parity, education, hypertension history, hormone contraception use and HT use combined with menopausal status. Model fit was assessed using the Hosmer–Lemeshow goodness-of-fit test(Reference Hosmer and Lemeshow19). Tests for linear trend were conducted for all models of categorized data, with an ordinal-score variable treated as a continuous variable and all P values reported as two-sided. All statistical analyses were performed using the STATA statistical software package version 10·0 (StataCorp LP, College Station, TX, USA)(Reference Levi, Franceschi and Negri51).

Results

Our study population consisted primarily of Caucasian (96 %), postmenopausal (74 %) women, 28–79 years of age, who were married or had been married previously (96 %; Table 1). Risk increased with being overweight or obese (BMI ≥ 25·0 kg/m2v. BMI < 25·0 kg/m2), having a waist circumference ≥88 cm, having a younger age at menarche and having a history of hypertension or type 2 diabetes. Risk was reduced for women who were more educated, parous, past-year dietary supplement users, ever hormone contraception users or post- or perimenopausal and users of E + P HT (Table 1). Women were generally physically inactive and low alcohol consumers; half of them were never smokers (Table 1). The daily nutrient intakes reported by cases and controls are presented in Table 2. The prevalence of use of any multivitamin or any nutrient-only-type supplement was 84 % for cases and 88 % for controls. Vitamin C was the most prevalent supplemental nutrient, taken by 69 % of cases and 74 % of controls.

Table 1 Characteristics of endometrial cancer cases and controls and age-adjusted OR for risk of endometrial cancer with non-dietary risk factors, Alberta, Canada, 2002–2006 (n 1487)

HT, hormone therapy; E, oestrogen; E + P, oestrogen + progesterone; MET, metabolic equivalents.

*Height and weight self-reported for five cases and five controls, not reported by one control.

†Not reported for four cases and nine controls.

‡Not reported for two cases.

§HT use not reported for one case and six controls.

∥Menopausal status not reported in one case and one control.

¶Not reported in two controls; OR compared with never.

**Not reported in three controls; OR compared with never.

††Not reported in one control.

‡‡Lifetime total alcohol consumption (minimum of six drinks per year) assessed at the time of interview. Participants reported the number of drinks of beer (1 can/glass/bottle = 12 oz/360 ml), wine (1 glass = 5 oz/140 ml) or liquor (1·5 oz/45 ml) consumed per week for each pattern of drinking. Responses were used to estimate alcohol consumption in grams of ethanol per year, and this estimate was converted to number of drinks per day.

Table 2 Daily nutrient intakes reported on the DHQ by cases and controls

DHQ, diet history questionnaire; NDSR, Nutrition Data Systems for Research; RE, retinol equivalents; ATE, α-tocopherol equivalents.

*Cases: 1608·6 kJ (627·8 kcal); controls: 1597·1 kJ (626·3 kcal).

†Estimated among users of given supplement; multivitamin or nutrient-only-type source.

Macronutrients

We did not find an association with EC for the majority of macronutrients examined, including total energy intake, protein, total fat, saturated fat, carbohydrate and total dietary fibre (Table 3). We observed a 51–59 % elevation in risk in the highest quartile of intake of dietary cholesterol, with a statistically significant increasing trend in both age-adjusted and multivariable-adjusted models (OR = 1·59, 95 % CI 1·17, 2·16, P for trend = 0·01; OR = 1·51, 95 % CI 1·08, 2·11, P for trend = 0·02, respectively). BMI modified the association at the highest levels of cholesterol intake and EC (P for interaction = 0·01 and 0·00). We observed an 80–211 % statistically significant elevation in risk at the highest level of cholesterol intake for women whose BMI was defined as overweight or obese (BMI ≥ 25·0 kg/m2; OR = 2·11, 95 % CI 1·44, 3·10) but not for normal-weight women (BMI < 25·0 kg/m2; Table 4). A similar pattern of significantly increased risk was observed with waist circumference ≥88 cm (OR = 2·07, 95 % CI 1·32, 3·25; results not shown). We found no statistical interaction between cholesterol intake and menopausal status. However, when models were stratified, risks remained statistically significantly elevated among postmenopausal women in the highest quartile of cholesterol intake (OR = 1·51, 95 % CI 1·04, 2·20, P for trend = 0·04). The association with cholesterol was also strengthened among postmenopausal women who were non-users of HT (OR = 1·79, 95 % CI 1·06, 3·00, P for trend = 0·02) at the highest level of intake when it was examined in models assessing no HT and E + P HT use.

Table 3 Age- and multivariable-adjusted OR and 95 % CI for risk of endometrial cancer with daily intakes of individual macronutrients

NDSR, Nutrition Data Systems for Research.

*Adjusted for age (years) and total energy intake (kcal/d; except in the case of total energy intake).

†Additionally adjusted for age at menarche (years), BMI (<25·0 v. 25·0–29·9, ≥30·0 kg/m2), parity (0 v. 1–2, >2 pregnancies at ≥20 weeks’ gestation), educational level (below high school v. high school or above), hypertension history (ever v. never), hormone contraceptive use (never v. ever), hormone therapy use combined with menopausal status (post/perimenopausal/no hormone therapy v. post/perimenopausal + oestrogen, post/perimenopausal + oestrogen + progesterone, post/perimenopausal + other menopausal hormones and premenopausal), alcohol consumption (0 v. <1 drink, ≥1 drink/d).

‡Quartile cut-off points in kcal: 1166·5, 1489·0, 1882·2 and 4617·2, respectively.

Table 4 Multivariable-adjusted OR and 95 % CI for risk of endometrial cancer with cholesterol intake (mg) stratified by menopausal status (n 1485), BMI (n 1486) and HT use (n 876)

HT, hormone therapy; E + P, oestrogen + progesterone.

*Adjusted for age (years) and total energy intake (kJ (kcal)), age at menarche (years), BMI (<25·0 v. 25·0–29·9, ≥30·0 kg/m2), parity (0 v. 1–2, >2 pregnancies at ≥20 weeks’ gestation), educational level (below high school v. high school or above), hypertension history (ever v. never), hormone contraceptive use (never v. ever), alcohol consumption (0 drink v. <1 drink, ≥1 drink/d).

†If further adjusted for use of HT (lowest to highest quartile of cholesterol intake): OR = 1·14 (95 % CI 0·78, 1·67), 1·16 (95 % CI 0·78, 1·72) and 1·48 (95 % CI 1·02, 2·16).

Micronutrients

We did not observe an association with EC for most micronutrients (Table 5). A reduced risk was detected for dietary intake of riboflavin (multivariable-adjusted OR = 0·66, 95 % CI 0·47, 0·92) in the second, compared with the lowest, quartile of intake, but risk was unchanged for the remaining intake levels and there was no evidence for linear trend. Risk was reduced in the highest quartile of vitamin E intake from food and supplements in the age-adjusted model (OR = 0·66, 95 % CI 0·48, 0·91, P for trend = 0·01) but was attenuated in the multivariable-adjusted model (OR = 0·74, 95 % CI 0·52, 1·04, P for trend = 0·13). Age-adjusted risk accounting for supplement use at the highest level of intake was significantly reduced for Ca from food sources (OR = 0·73, 95 % CI 0·54, 0·99, P for trend = 0·07) but was attenuated in the multivariable-adjusted model (OR = 0·82, 95 % CI 0·59, 1·13, P for trend = 0·28). The strongest association observed was for total combined Ca intake (from both food and supplements), in which we observed a statistically significant 28–40 % reduced risk associated with the highest exposure level (multivariable-adjusted OR = 0·72, 95 % CI 0·51, 0·99, P for trend = 0·04). In an analysis of Ca intake from food, restricted to supplement non-users (n 196 cases, n 300 controls), using quartile cut-off points among non-supplement-using controls we found a statistically significant reduced risk for EC (OR = 0·52, 95 % CI, 0·30, 0·93, P for trend = 0·07). We observed unexpected increased risks at limited levels of intake of dietary soluble fibre, vitamin C, thiamin, vitamin B6 and lutein/zeaxanthin and vitamin B12 from food plus supplements (Table 5). There was no evidence for linear trend being associated with these increased risks, except for vitamin B6 (P for trend = 0·05).

Table 5 Multivariable-adjusted OR and 95 % CI for risk of endometrial cancer with daily intakes of individual micronutrients from diet alone and diet with supplements

RE, retinol equivalents; ATE, α-tocopherol equivalents; DFE, dietary folate equivalents; N/A, not applicable.

*Diet-only models adjusted for age (years), total energy intake (kJ (kcal)/d), nutrient-specific supplement use (no v. yes, except for lycopene, lutein/zeaxanthin and methionine), age at menarche (years), BMI (<25·0 v. 25·0–29·9, ≥30·0 kg/m2), parity (0 v. 1–2, >2 pregnancies at ≥20 weeks’ gestation), educational level (below high school v. high school or above), hypertension history (ever v. never), hormone contraceptive use (never v. ever), hormone therapy use combined with menopausal status (post/perimenopausal/no hormone therapy v. post/perimenopausal + oestrogen, post/perimenopausal + oestrogen + progesterone, post/perimenopausal + other menopausal hormones and premenopausal) and alcohol consumption (0 drink v. <1 drink, ≥1 drink/d).

†Diet and supplement models adjusted for the same covariates as diet-only models, except for nutrient-specific supplement use.

Discussion

In this population-based case–control study that had detailed assessments of food and supplement use, we did not find increased risks associated with most macronutrients, including total fat and saturated fat, but did find an association between decreased risks and some micronutrient intakes. Our findings are not corroborated by previous research, which has generally suggested a relationship between increased EC risks and higher intakes of total fat(Reference Goodman, Hankin and Wilkens20Reference Shu, Zheng and Potischman26), saturated fat(Reference Jain, Howe and Rohan5, Reference Goodman, Hankin and Wilkens20, Reference Littman, Beresford and White22, Reference Potischman, Hoover and Brinton27) and animal fat(Reference Jain, Howe and Rohan5, Reference Goodman, Hankin and Wilkens20, Reference Salazar-Martinez, Lazcano-Ponce and Sanchez-Zamorano25, Reference Shu, Zheng and Potischman26, Reference Barbone, Austin and Partridge28). A meta-analysis reported statistically significant increased risks of 24–72 % for total fat, 28–49 % for saturated fat and 34–78 % for animal fat(Reference Bandera, Kushi and Moore29). Two studies have since found an association between non-statistically significant increased risk and higher total fat intake(Reference Xu, Dai and Xiang30, Reference Yeh, Moysich and Jayaprakash31) and one found no association(Reference Lucenteforte, Talamini and Montella32). Meanwhile, our results are consistent with the Women's Health Initiative Dietary Intervention Trial, a study that aimed to reduce fat intake to <20 % of total energy intake from a baseline of ≥32 % and found no change in EC incidence among postmenopausal women(Reference Prentice, Thomson and Caan33).

The most pronounced finding among the macronutrients was a statistically significant increased risk of 51–59 % at the highest level of cholesterol intake. The association between dietary cholesterol and EC has been assessed in nine previous case–control studies(Reference Goodman, Hankin and Wilkens20, Reference Littman, Beresford and White22Reference Salazar-Martinez, Lazcano-Ponce and Sanchez-Zamorano25, Reference Barbone, Austin and Partridge28, Reference Yeh, Moysich and Jayaprakash31, Reference Lucenteforte, Talamini and Montella32, Reference Tzonou, Lipworth and Kalandidi34) with mixed results: three found statistically significant increased risks(Reference Goodman, Hankin and Wilkens20, Reference Potischman, Swanson and Brinton24, Reference Lucenteforte, Talamini and Montella32), but the remaining six found non-significant reduced risks(Reference McCann, Freudenheim and Marshall23, Reference Salazar-Martinez, Lazcano-Ponce and Sanchez-Zamorano25), no association(Reference Tzonou, Lipworth and Kalandidi34) or non-significant increased risks(Reference Littman, Beresford and White22, Reference Barbone, Austin and Partridge28, Reference Yeh, Moysich and Jayaprakash31). A pooled analysis of six of these studies reported a non-statistically significant increased risk of 35–39 % with higher cholesterol intake(Reference Bandera, Kushi and Moore29). Studies of serum cholesterol have shown similar mixed results(Reference Hiatt and Fireman35Reference Zhang, Liu and Yu41).

Our results are consistent with the increased EC risk observed for dietary cholesterol from pooled estimates. Although most cholesterol is produced by the liver, prolonged intake of dietary saturated fat and cholesterol raises the average serum cholesterol concentration, as well as levels of LDL cholesterol and HDL cholesterol(Reference Ye and Kwiterovich42). Individual serum cholesterol response to intake of dietary cholesterol seems to be dependent on genetic susceptibility(Reference Ye and Kwiterovich42), which may, in part, contribute to mixed results from observational studies. The role of cholesterol in endometrial carcinogenesis is biologically plausible, as cholesterol and oestrogen are physiologically interconnected. Cholesterol is the founding substrate in steroid hormone synthesis(Reference Willnow and Nykjaer43) and can be converted to oestrogen via metabolic pathways; thus, increased levels of cholesterol may influence EC risk by increasing bioavailable oestrogen synthesis. Meanwhile, in postmenopausal women, circulating cholesterol levels are decreased as a result of oestrogen therapy(Reference Barrett-Connor, Slone and Greendale44). Further, oestrogen stimulates LDL receptor activity; hence, premenopausal women have lower LDL cholesterol levels, which increase after menopause(45). During premenopause, oestrogen production occurs in the ovaries and circulating oestrogen levels are tightly regulated; hence, any influence of cholesterol on oestrogen levels may be marginal(Reference Key, Allen and Verkasalo46). Since endogenous oestrogen production after menopause occurs primarily in adipose tissue(Reference Key, Allen and Verkasalo46), the relative influence of cholesterol on oestrogen bioavailability is greater than that before menopause. In addition, the oestrogen in HT users may overwhelm any effect of cholesterol. Our finding of a stronger increased risk with dietary cholesterol among postmenopausal women, particularly those not exposed to HT, and among overweight and obese women, is consistent with this hypothesis and suggests that cholesterol may be more influential after menopause. Alternatively, the highest sources of cholesterol among food groups in our questionnaire were, as expected, red meat (including higher fat beef, veal and pork), eggs, poultry and high-fat dairy. Hence, the increased risk with cholesterol may also reflect intake of animal foods that also increase EC risk(Reference Bandera, Kushi and Moore47).

Numerous observational studies have reported on the influence of dietary micronutrients in EC aetiology(Reference Jain, Howe and Rohan5, Reference Jain, Rohan and Howe6, Reference Goodman, Hankin and Wilkens20, Reference Goodman, Wilkens and Hankin21, Reference McCann, Freudenheim and Marshall23Reference Shu, Zheng and Potischman26, Reference Barbone, Austin and Partridge28, Reference Xu, Dai and Xiang30, Reference Yeh, Moysich and Jayaprakash31, Reference Tzonou, Lipworth and Kalandidi34, Reference Kabat, Miller and Jain48Reference Pelucchi, Dal and Montella53); two were cohort studies(Reference Jain, Rohan and Howe6, Reference Kabat, Miller and Jain48) and the rest were case–control studies. Reduced risks have been observed for dietary intake of vitamin C(Reference Goodman, Hankin and Wilkens20, Reference Goodman, Wilkens and Hankin21, Reference McCann, Freudenheim and Marshall23, Reference Xu, Dai and Xiang30, Reference Levi, Franceschi and Negri51, Reference Negri, La and Franceschi52), β-carotene(Reference Goodman, Hankin and Wilkens20, Reference McCann, Freudenheim and Marshall23, Reference Xu, Dai and Xiang30, Reference Yeh, Moysich and Jayaprakash31, Reference Levi, Franceschi and Negri51Reference Pelucchi, Dal and Montella53) or other carotenoids(Reference Goodman, Hankin and Wilkens20, Reference McCann, Freudenheim and Marshall23, Reference Barbone, Austin and Partridge28, Reference Yeh, Moysich and Jayaprakash31, Reference La Vecchia, Decarli and Fasoli50, Reference Pelucchi, Dal and Montella53), as well as for intakes of vitamin A(Reference Goodman, Hankin and Wilkens20, Reference Goodman, Wilkens and Hankin21, Reference Xu, Dai and Xiang30), folate(Reference McCann, Freudenheim and Marshall23, Reference Yeh, Moysich and Jayaprakash31), Ca(Reference Salazar-Martinez, Lazcano-Ponce and Sanchez-Zamorano25, Reference Tzonou, Lipworth and Kalandidi34), vitamins E(Reference Jain, Howe and Rohan5, Reference Yeh, Moysich and Jayaprakash31), D and B12(Reference Salazar-Martinez, Lazcano-Ponce and Lira-Lira54) and lycopene(Reference Kabat, Miller and Jain48). Pooled analyses suggest a reduced risk with intakes of β-carotene (12 %) and vitamins C (15 %) and E (9 %) from food(Reference Bandera, Gifkins and Moore55). A hospital-based case–control study in Korea examined pre-operative levels of plasma micronutrients and found significantly reduced risks associated with higher concentrations of plasma β-carotene and lycopene (OR = 0·12, 95 % CI 0·03, 0·48 and OR = 0·15, 95 % CI 0·04, 0·61, respectively)(Reference Jeong, Song and Lee56). Overall, the evidence from dietary studies is mixed, which may be explained by misclassification of exposure levels or by confounding by unmeasured supplement use. The benefits of supplements on cancer risk are inconclusive; supplements are currently not recommended for cancer prevention(3). A recent meta-analysis of randomized controlled trials showed no benefit of antioxidant supplementation on cancer risk but found that supplementation with β-carotene can increase cancer risk and mortality among smokers(Reference Bardia, Tleyjeh and Cerhan57). Of the observational studies that have examined any supplement use and EC(Reference Jain, Howe and Rohan5, Reference Jain, Rohan and Howe6, Reference Barbone, Austin and Partridge28, Reference Xu, Dai and Xiang30, Reference Terry, Vainio and Wolk58), one showed a reduced risk with B-only vitamins and a reduced risk with multivitamin use that was further decreased with increasing duration of use(Reference Xu, Dai and Xiang30). Another study found a reduced risk with Ca and an increased risk with Fe supplementation(Reference Terry, Vainio and Wolk58). The Women's Health Initiative concluded that there was no significant association of EC with multivitamin use; however, there was a marginal, but non-significant, increased risk with longer duration of use(Reference Neuhouser, Wassertheil-Smoller and Thomson59).

Only two studies have examined the risk of EC in relation to micronutrient intake from food and supplements combined(Reference Jain, Howe and Rohan5, Reference Jain, Rohan and Howe6). Jain et al.(Reference Jain, Howe and Rohan5, Reference Jain, Rohan and Howe6) found no association with vitamin C intake in a case–cohort analysis(Reference Jain, Rohan and Howe6) and found a significant reduced risk with vitamin E (OR = 0·61, 95 % CI 0·43, 0·88) in a case–control study that examined vitamins C, E and A and β-carotene from food plus supplements(Reference Jain, Howe and Rohan5).

We found a statistically significant 28–38 % reduction in EC risk with Ca intake when dietary and supplemental sources were combined. Dietary Ca intake has been assessed in four previous hospital-based case–control studies(Reference Salazar-Martinez, Lazcano-Ponce and Sanchez-Zamorano25, Reference Barbone, Austin and Partridge28, Reference Tzonou, Lipworth and Kalandidi34, Reference Negri, La and Franceschi52), and supplemental Ca has been assessed in one hospital-based(Reference Barbone, Austin and Partridge28) and one population-based case–control study(Reference Terry, Vainio and Wolk58). Dietary Ca reduced EC risk by 52–61 % in two studies(Reference Salazar-Martinez, Lazcano-Ponce and Sanchez-Zamorano25, Reference Tzonou, Lipworth and Kalandidi34) and Ca supplements reduced risk by 50 %, which became 70 % among women whose dairy intake was below the median(Reference Terry, Vainio and Wolk58). The other study reported a non-significant reduced risk with ever use(Reference Barbone, Austin and Partridge28). Because of a lack of intervention and cohort studies of Ca intake, and because of high heterogeneity between estimates, a review of these studies concluded that evidence to date is too sparse and inconclusive(Reference McCullough, Bandera and Moore60). Our study supports the hypothesis that Ca from food and from supplementation lowers EC risk. The strengthened reductions in risk that we observed in our analysis restricted to non-users of supplemental Ca suggest that dietary Ca is important in EC risk reduction, which may reflect better dietary Ca absorption. Dietary Ca, especially from dairy foods, is important in energy metabolism and can help maintain a healthy body weight(Reference Major, Chaput and Ledoux61). Greater weight and fat loss have been observed in randomized trials for groups with high-dairy supplementation(Reference Zemel, Thompson and Milstead62Reference Eagan, Lyle and Gunther65). These findings are still inconclusive, however, as a review of randomized controlled trials of Ca supplementation and body weight revealed no association(Reference Trowman, Dumville and Hahn66). Ca supplementation may be beneficial only in populations with low baseline Ca intake(Reference Gibson, Ferrucci and Tangrea67). For cancer prevention, Ca may act through vitamin D, a nutrient with anti-neoplastic potential, as it is highly correlated and metabolically tied to vitamin D. Vitamin D plays a role in cellular growth and differentiation through vitamin D receptors that are present in endometrial tissue(Reference Vigano, Lattuada and Mangioni68, Reference Vienonen, Miettinen and Blauer69). Our analysis did not reveal an association with dietary intake of vitamin D; however, circulating serum levels of 25-hydroxyvitamin D may be more relevant in cancer prevention since a substantial portion of vitamin D is derived from the sun. A recent nested case–control study of 830 cases and 992 controls from seven cohorts, however, found no association between circulating 25-hydroxyvitamin D and EC(Reference Zeleniuch-Jacquotte, Gallicchio and Hartmuller70).

We observed a reduced risk within the second quartile of riboflavin intake in our study, suggesting that riboflavin may play a role in EC risk reduction. Riboflavin is being investigated in cancer aetiology because of its role in folate metabolism(Reference Powers71). Minimum adult requirements are between 0·5 and 0·8 mg/d and urinary excretion increases at intakes of 1·1–1·6 mg/d(45). Since risk was not reduced at higher levels in our study, our results would be consistent with riboflavin bioavailability, suggesting that adequate levels may provide benefit. We observed unexpected increased risks with dietary soluble fibre, vitamin C, thiamin, vitamin B6 and lutein/zeaxanthin and with combined vitamin B12 intakes. Detection of risks at limited levels of intake for these nutrients, an absence of linear trend and the presence of multiple comparisons suggest that these may be chance findings. Our results for vitamins B6 and B12 might be reflective of meat intake, as higher intake of meat, particularly of red meat, has been associated with an increased risk for EC(Reference Bandera, Kushi and Moore47). Adjustment for meat intake attenuated these associations only marginally, but there could be residual confounding. The increased risk we observed for vitamin C from diet is in contrast to the results from other studies(Reference Goodman, Hankin and Wilkens20, Reference Goodman, Wilkens and Hankin21, Reference McCann, Freudenheim and Marshall23, Reference Xu, Dai and Xiang30, Reference Levi, Franceschi and Negri51, Reference Negri, La and Franceschi52) and could suggest something about foods high in vitamin C. A hypothesis suggesting that grapefruit intake, through inhibition of the cytochrome P450 3A4 enzyme system, can affect oestrogen metabolism, leading to higher levels of circulating oestrogen and increased breast cancer risk, was examined in the Multiethnic Cohort Study(Reference Monroe, Murphy and Kolonel72). We were unable to examine grapefruit intake with respect to the observed association with vitamin C because it was not assessed separately from intake of other citrus fruits in our questionnaire.

Although our assessments of associations among non-users of the given supplemental nutrient were limited by sample size, restriction caused the detected association to be attenuated towards the null for thiamin and vitamin B6 and it lost statistical significance for vitamin C. Risk was also attenuated and became non-significant for lutein/zeaxanthin among non-users of any supplements. Meanwhile, the results for dietary Ca were strengthened with restriction to non-users of supplemental Ca. Our results highlight that misclassification on exposure and possible confounding by supplement use are issues in studies of dietary nutrients and disease risk, leading to potentially spurious associations when these additional nutrients are not accounted for. Restriction to non-users of given supplements in the analysis may provide additional insight into detected associations. Future studies should incorporate measures of supplement use in addition to dietary assessment.

The population-based design, large sample size and comprehensive information on a wide range of risk factors are the strengths of our study. We were also able to evaluate the influence of supplement use combined with dietary sources of micronutrients, which has been carried out in only a limited number of previous studies(Reference Jain, Howe and Rohan5, Reference Jain, Rohan and Howe6). Limitations in dietary assessment are recognized, as is the possibility of recall bias because of the retrospective dietary assessment. Any random measurement error associated with reporting past dietary exposures tends to attenuate associations(Reference Kipnis and Freedman73). Nevertheless, we were able to detect statistically significant associations, with evidence for linear trend, for some of these dietary and supplemental exposures; however, our estimates are likely to be conservative. The supplemental exposure variables from our questionnaire summarized exposure from all forms of supplements; hence, we could not evaluate risk for nutrients derived from multivitamins in relation to individual vitamins. Further, the potential for confounding by other nutrients in multivitamins also exists. Another limitation was our low control response rate, which we addressed by comparing our sample to a larger sample of Alberta women from the Canadian Community Health Survey Cycle 2·2 to evaluate possible selection bias. From this comparison we found that the control group was somewhat more educated than the base population but was otherwise similar with regard to age, height, weight and BMI(Reference Friedenreich, Cook and Magliocco7).

In summary, our study is supportive of a positive association between dietary cholesterol and EC risk. Risk was reduced with intake of Ca from food sources and from food plus supplements. Prospective studies of detailed dietary intakes of nutrients from food and supplements and biomarkers of nutritional and metabolic status are needed to confirm the roles of overall diet and specific nutrients in EC risk and provide additional insight into mechanisms that may underlie a true impact.

Acknowledgements

The case–control study of endometrial cancer was conducted at the Tom Baker Cancer Centre in Calgary, Alberta, and was supported by grants from the National Cancer Institute of Canada with funding from the Canadian Cancer Society. C.M.F. was supported by a Career Award from the Canadian Institutes of Health Research; C.M.F. and L.S.C. were supported by career awards from the Alberta Heritage Foundation for Medical Research; and L.S.C. and K.S.C. were supported by Canada Research Chairs. The authors have no conflict of interest to declare. R.K.B. conceptualized the study, performed the analysis and wrote the manuscript; C.M.F. and I.C. provided expertise in nutritional epidemiology; C.M.F., L.S.C., K.S.C. and A.M.M. obtained funding for data collection. All authors reviewed and contributed to drafts of the manuscript.

References

1.Canadian Cancer Society's Steering Committee (2010) Canadian Cancer Statistics 2010. Toronto: Canadian Cancer Society.Google Scholar
2.Kaaks, R, Lukanova, A & Kurzer, MS (2002) Obesity, endogenous hormones, and endometrial cancer risk: a synthetic review. Cancer Epidemiol Biomarkers Prev 11, 15311543.Google Scholar
3.World Cancer Research Fund/American Institute for Cancer Research (2007) Food, Nutrition, Physical Activity, and the Prevention of Cancer: a Global Perspective. Washington, DC: AICR.Google Scholar
4.Vatanparast, H, Adolphe, JL & Whiting, SJ (2010) Socio-economic status and vitamin/mineral supplement use in Canada. Health Rep 21, issue 4, 1925.Google ScholarPubMed
5.Jain, MG, Howe, GR & Rohan, TE (2000) Nutritional factors and endometrial cancer in Ontario, Canada. Cancer Control 7, 288296.CrossRefGoogle ScholarPubMed
6.Jain, MG, Rohan, TE, Howe, GR et al. (2000) A cohort study of nutritional factors and endometrial cancer. Eur J Epidemiol 16, 899905.CrossRefGoogle ScholarPubMed
7.Friedenreich, CM, Cook, LS, Magliocco, AM et al. (2010) Case–control study of lifetime total physical activity and endometrial cancer risk. Cancer Causes Control 21, 11051116.CrossRefGoogle ScholarPubMed
8.Waksberg, J (1978) Sampling methods for random digit dialing. J Am Stat Soc 73, 4046.CrossRefGoogle Scholar
9.National Cancer Institute (2007) Diet History Questionnaire http://riskfactor.cancer.gov/DHQ/ (accessed June 2007).Google Scholar
10.Subar, AF, Kipnis, V, Troiano, RP et al. (2003) Using intake biomarkers to evaluate the extent of dietary misreporting in a large sample of adults: the OPEN study. Am J Epidemiol 158, 113.CrossRefGoogle Scholar
11.Subar, AF, Thompson, FE, Kipnis, V et al. (2001) Comparative validation of the Block, Willett, and National Cancer Institute food frequency questionnaires: the Eating at America's Table Study. Am J Epidemiol 154, 10891099.CrossRefGoogle Scholar
12.Thompson, FE, Subar, AF, Brown, CC et al. (2002) Cognitive research enhances accuracy of food frequency questionnaire reports: results of an experimental validation study. J Am Diet Assoc 102, 212225.CrossRefGoogle ScholarPubMed
13.Barr, SI, Kwan, S & Janelle, KC (1994) Nutrient analysis using computer programs: comparison of a Canadian and an American database. J Am Diet Assoc 91, 2932.Google Scholar
14.Csizmadi, I, Kahle, L, Ullman, R et al. (2007) Adaptation and evaluation of the National Cancer Institute's Diet History Questionnaire and nutrient database for Canadian populations. Public Health Nutr 10, 8896.CrossRefGoogle ScholarPubMed
15.National Academy of Sciences, Institute of Medicine (1998) Dietary Reference Intakes for Thiamin, Riboflavin, Niacin, Vitamin B6, Folate, Vitamin B12, Pantothenic Acid, Biotin, and Choline. Washington, DC: National Academy Press.Google Scholar
16.Maruti, SS, Ulrich, CM & White, E (2009) Folate and one-carbon metabolism nutrients from supplements and diet in relation to breast cancer risk. Am J Clin Nutr 89, 624633.CrossRefGoogle ScholarPubMed
17.Willett, WC, Howe, GR & Kushi, LH (1997) Adjustment for total energy intake in epidemiologic studies. Am J Clin Nutr 65, 4 Suppl., 1220S1228S.CrossRefGoogle ScholarPubMed
18.Kleinbaum, D & Kupper, L (1978) Applied Regression Analysis and Other Multivariable Methods. Belmont, CA: Wadsworth Publishing Company Inc.Google Scholar
19.Hosmer, DW & Lemeshow, S (1989) Applied Logistic Regression. New York, NY: Wiley.Google Scholar
20.Goodman, MT, Hankin, JH, Wilkens, LR et al. (1997) Diet, body size, physical activity, and the risk of endometrial cancer. Cancer Res 57, 50775085.Google ScholarPubMed
21.Goodman, MT, Wilkens, LR, Hankin, JH et al. (1997) Association of soy and fiber consumption with the risk of endometrial cancer. Am J Epidemiol 146, 294306.CrossRefGoogle ScholarPubMed
22.Littman, AJ, Beresford, SA & White, E (2001) The association of dietary fat and plant foods with endometrial cancer (United States). Cancer Causes Control 12, 691702.CrossRefGoogle ScholarPubMed
23.McCann, SE, Freudenheim, JL, Marshall, JR et al. (2000) Diet in the epidemiology of endometrial cancer in western New York (United States). Cancer Causes Control 11, 965974.CrossRefGoogle ScholarPubMed
24.Potischman, N, Swanson, CA, Brinton, LA et al. (1993) Dietary associations in a case–control study of endometrial cancer. Cancer Causes Control 4, 239250.CrossRefGoogle Scholar
25.Salazar-Martinez, E, Lazcano-Ponce, E, Sanchez-Zamorano, LM et al. (2005) Dietary factors and endometrial cancer risk. Results of a case–control study in Mexico. Int J Gynecol Cancer 15, 938945.CrossRefGoogle ScholarPubMed
26.Shu, XO, Zheng, W, Potischman, N et al. (1993) A population-based case–control study of dietary factors and endometrial cancer in Shanghai, People's Republic of China. Am J Epidemiol 137, 155165.CrossRefGoogle ScholarPubMed
27.Potischman, N, Hoover, RN, Brinton, LA et al. (1996) Case–control study of endogenous steroid hormones and endometrial cancer. J Natl Cancer Inst 88, 11271135.CrossRefGoogle ScholarPubMed
28.Barbone, F, Austin, H & Partridge, EE (1993) Diet and endometrial cancer: a case–control study. Am J Epidemiol 137, 393403.CrossRefGoogle ScholarPubMed
29.Bandera, EV, Kushi, LH, Moore, DF et al. (2007) Dietary lipids and endometrial cancer: the current epidemiologic evidence. Cancer Causes Control 18, 687703.CrossRefGoogle ScholarPubMed
30.Xu, WH, Dai, Q, Xiang, YB et al. (2007) Nutritional factors in relation to endometrial cancer: a report from a population-based case–control study in Shanghai, China. Int J Cancer 120, 17761781.CrossRefGoogle ScholarPubMed
31.Yeh, M, Moysich, KB, Jayaprakash, V et al. (2009) Higher intakes of vegetables and vegetable-related nutrients are associated with lower endometrial cancer risks. J Nutr 139, 317322.CrossRefGoogle ScholarPubMed
32.Lucenteforte, E, Talamini, R, Montella, M et al. (2008) Macronutrients, fatty acids and cholesterol intake and endometrial cancer. Ann Oncol 19, 168172.CrossRefGoogle ScholarPubMed
33.Prentice, RL, Thomson, CA, Caan, B et al. (2007) Low-fat dietary pattern and cancer incidence in the Women's Health Initiative Dietary Modification Randomized Controlled Trial. J Natl Cancer Inst 99, 15341543.CrossRefGoogle ScholarPubMed
34.Tzonou, A, Lipworth, L, Kalandidi, A et al. (1996) Dietary factors and the risk of endometrial cancer: a case–control study in Greece. Br J Cancer 73, 12841290.CrossRefGoogle ScholarPubMed
35.Hiatt, RA & Fireman, BH (1986) Serum cholesterol and the incidence of cancer in a large cohort. J Chronic Dis 39, 861870.CrossRefGoogle ScholarPubMed
36.Kark, JD, Smith, AH & Hames, CG (1980) The relationship of serum cholesterol to the incidence of cancer in Evans County, Georgia. J Chronic Dis 33, 311332.CrossRefGoogle Scholar
37.Lindemann, K, Vatten, LJ, Ellstrom-Engh, M et al. (2009) Serum lipids and endometrial cancer risk: results from the HUNT-II study. Int J Cancer 124, 29382941.CrossRefGoogle ScholarPubMed
38.Swanson, CA, Potischman, N, Barrett, RJ et al. (1994) Endometrial cancer risk in relation to serum lipids and lipoprotein levels. Cancer Epidemiol Biomarkers Prev 3, 575581.Google ScholarPubMed
39.Wallace, RB, Rost, C, Burmeister, LF et al. (1982) Cancer incidence in humans: relationship to plasma lipids and relative weight. J Natl Cancer Inst 68, 915918.Google ScholarPubMed
40.Williams, RR, Sorlie, PD, Feinleib, M et al. (1981) Cancer incidence by levels of cholesterol. JAMA 245, 247252.CrossRefGoogle ScholarPubMed
41.Zhang, Y, Liu, Z, Yu, X et al. (2010) The association between metabolic abnormality and endometrial cancer: a large case–control study in China. Gynecol Oncol 117, 4146.CrossRefGoogle ScholarPubMed
42.Ye, SQ & Kwiterovich, PO Jr (2000) Influence of genetic polymorphisms on responsiveness to dietary fat and cholesterol. Am J Clin Nutr 72, 5 Suppl., 1275S1284S.CrossRefGoogle ScholarPubMed
43.Willnow, TE & Nykjaer, A (2010) Cellular uptake of steroid carrier proteins – mechanisms and implications. Mol Cell Endocrinol 316, 93102.CrossRefGoogle ScholarPubMed
44.Barrett-Connor, E, Slone, S, Greendale, G et al. (1997) The Postmenopausal Estrogen/Progestin Interventions Study: primary outcomes in adherent women. Maturitas 27, 261274.CrossRefGoogle ScholarPubMed
45.The Nutrition Society (2002) Introduction to Human Nutrition. Oxford, UK: Blackwell Science Ltd.Google Scholar
46.Key, TJ, Allen, NE, Verkasalo, PK et al. (2001) Energy balance and cancer: the role of sex hormones. Proc Nutr Soc 60, 8189.CrossRefGoogle ScholarPubMed
47.Bandera, EV, Kushi, LH, Moore, DF et al. (2007) Consumption of animal foods and endometrial cancer risk: a systematic literature review and meta-analysis. Cancer Causes Control 18, 967988.CrossRefGoogle Scholar
48.Kabat, GC, Miller, AB, Jain, M et al. (2008) Dietary iron and haem iron intake and risk of endometrial cancer: a prospective cohort study. Br J Cancer 98, 194198.CrossRefGoogle ScholarPubMed
49.Kallianpur, AR, Lee, SA, Xu, WH et al. (2010) Dietary iron intake and risk of endometrial cancer: a population-based case–control study in Shanghai, China. Nutr Cancer 62, 4050.CrossRefGoogle ScholarPubMed
50.La Vecchia, C, Decarli, A, Fasoli, M et al. (1986) Nutrition and diet in the etiology of endometrial cancer. Cancer 57, 12481253.3.0.CO;2-V>CrossRefGoogle ScholarPubMed
51.Levi, F, Franceschi, S, Negri, E et al. (1993) Dietary factors and the risk of endometrial cancer. Cancer 71, 35753581.3.0.CO;2-0>CrossRefGoogle ScholarPubMed
52.Negri, E, La, VC, Franceschi, S et al. (1996) Intake of selected micronutrients and the risk of endometrial carcinoma. Cancer 77, 917923.3.0.CO;2-6>CrossRefGoogle ScholarPubMed
53.Pelucchi, C, Dal, ML, Montella, M et al. (2008) Dietary intake of carotenoids and retinol and endometrial cancer risk in an Italian case–control study. Cancer Causes Control 19, 12091215.CrossRefGoogle Scholar
54.Salazar-Martinez, E, Lazcano-Ponce, EC, Lira-Lira, GG et al. (2000) Case–control study of diabetes, obesity, physical activity and risk of endometrial cancer among Mexican women. Cancer Causes Control 11, 707711.CrossRefGoogle ScholarPubMed
55.Bandera, EV, Gifkins, DM, Moore, DF et al. (2009) Antioxidant vitamins and the risk of endometrial cancer: a dose–response meta-analysis. Cancer Causes Control 20, 699711.CrossRefGoogle ScholarPubMed
56.Jeong, NH, Song, ES, Lee, JM et al. (2009) Preoperative levels of plasma micronutrients are related to endometrial cancer risk. Acta Obstet Gynecol Scand 88, 434439.CrossRefGoogle ScholarPubMed
57.Bardia, A, Tleyjeh, IM, Cerhan, JR et al. (2008) Efficacy of antioxidant supplementation in reducing primary cancer incidence and mortality: systematic review and meta-analysis. Mayo Clin Proc 83, 2334.CrossRefGoogle ScholarPubMed
58.Terry, P, Vainio, H, Wolk, A et al. (2002) Dietary factors in relation to endometrial cancer: a nationwide case–control study in Sweden. Nutr Cancer 42, 2532.CrossRefGoogle ScholarPubMed
59.Neuhouser, ML, Wassertheil-Smoller, S, Thomson, C et al. (2009) Multivitamin use and risk of cancer and cardiovascular disease in the Women's Health Initiative cohorts. Arch Intern Med 169, 294304.CrossRefGoogle ScholarPubMed
60.McCullough, ML, Bandera, EV, Moore, DF et al. (2008) Vitamin D and calcium intake in relation to risk of endometrial cancer: a systematic review of the literature. Prev Med 46, 298302.CrossRefGoogle ScholarPubMed
61.Major, GC, Chaput, JP, Ledoux, M et al. (2008) Recent developments in calcium-related obesity research. Obes Rev 9, 428445.CrossRefGoogle ScholarPubMed
62.Zemel, MB, Thompson, W, Milstead, A et al. (2004) Calcium and dairy acceleration of weight and fat loss during energy restriction in obese adults. Obes Res 12, 582590.CrossRefGoogle ScholarPubMed
63.Zemel, MB, Richards, J, Mathis, S et al. (2005) Dairy augmentation of total and central fat loss in obese subjects. Int J Obes (Lond) 29, 391397.CrossRefGoogle ScholarPubMed
64.Zemel, MB, Richards, J, Milstead, A et al. (2005) Effects of calcium and dairy on body composition and weight loss in African-American adults. Obes Res 13, 12181225.CrossRefGoogle ScholarPubMed
65.Eagan, MS, Lyle, RM, Gunther, CW et al. (2006) Effect of 1-year dairy product intervention on fat mass in young women: 6-month follow-up. Obesity (Silver Spring) 14, 22422248.CrossRefGoogle ScholarPubMed
66.Trowman, R, Dumville, JC, Hahn, S et al. (2006) A systematic review of the effects of calcium supplementation on body weight. Br J Nutr 95, 10331038.CrossRefGoogle ScholarPubMed
67.Gibson, TM, Ferrucci, LM, Tangrea, JA et al. (2010) Epidemiological and clinical studies of nutrition. Semin Oncol 37, 282296.CrossRefGoogle ScholarPubMed
68.Vigano, P, Lattuada, D, Mangioni, S et al. (2006) Cycling and early pregnant endometrium as a site of regulated expression of the vitamin D system. J Mol Endocrinol 36, 415424.CrossRefGoogle ScholarPubMed
69.Vienonen, A, Miettinen, S, Blauer, M et al. (2004) Expression of nuclear receptors and cofactors in human endometrium and myometrium. J Soc Gynecol Investig 11, 104112.CrossRefGoogle ScholarPubMed
70.Zeleniuch-Jacquotte, A, Gallicchio, L, Hartmuller, V et al. (2010) Circulating 25-hydroxyvitamin D and risk of endometrial cancer: Cohort Consortium Vitamin D Pooling Project of Rarer Cancers. Am J Epidemiol 172, 3646.CrossRefGoogle ScholarPubMed
71.Powers, HJ (2003) Riboflavin (vitamin B-2) and health. Am J Clin Nutr 77, 13521360.CrossRefGoogle ScholarPubMed
72.Monroe, KR, Murphy, SP, Kolonel, LN et al. (2007) Prospective study of grapefruit intake and risk of breast cancer in postmenopausal women: the Multiethnic Cohort Study. Br J Cancer 97, 440445.CrossRefGoogle ScholarPubMed
73.Kipnis, V & Freedman, LS (2008) Impact of exposure measurement error in nutritional epidemiology. J Natl Cancer Inst 100, 16581659.CrossRefGoogle ScholarPubMed
Figure 0

Table 1 Characteristics of endometrial cancer cases and controls and age-adjusted OR for risk of endometrial cancer with non-dietary risk factors, Alberta, Canada, 2002–2006 (n 1487)

Figure 1

Table 2 Daily nutrient intakes reported on the DHQ by cases and controls

Figure 2

Table 3 Age- and multivariable-adjusted OR and 95 % CI for risk of endometrial cancer with daily intakes of individual macronutrients

Figure 3

Table 4 Multivariable-adjusted OR and 95 % CI for risk of endometrial cancer with cholesterol intake (mg) stratified by menopausal status (n 1485), BMI (n 1486) and HT use (n 876)

Figure 4

Table 5 Multivariable-adjusted OR and 95 % CI for risk of endometrial cancer with daily intakes of individual micronutrients from diet alone and diet with supplements