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Dietary fat and early-onset prostate cancer risk

Published online by Cambridge University Press:  19 January 2010

Artitaya Lophatananon*
Affiliation:
Division of Epidemiology, University of Nottingham Medical School, Queen's Medical Centre, Nottingham NG7 2UH, UK Ministry of Public Health, Nonthaburi 11000, Thailand
Jane Archer
Affiliation:
Division of Epidemiology, University of Nottingham Medical School, Queen's Medical Centre, Nottingham NG7 2UH, UK
Douglas Easton
Affiliation:
CR-UK Genetic Epidemiology Unit, Strangeways Research Laboratories, Worts Causeway, Cambridge CB1 8RN, UK
Richard Pocock
Affiliation:
Royal Devon and Exeter NHS Foundation Trust, Barrack Road, Exeter Ex2 5DW, UK
David Dearnaley
Affiliation:
The Institute of Cancer Research, 15 Cotswold Road, Sutton, Surrey, SM2 5NG, UK
Michelle Guy
Affiliation:
The Institute of Cancer Research, 15 Cotswold Road, Sutton, Surrey, SM2 5NG, UK
Zsofia Kote-Jarai
Affiliation:
The Institute of Cancer Research, 15 Cotswold Road, Sutton, Surrey, SM2 5NG, UK
Lynne O'Brien
Affiliation:
The Institute of Cancer Research, 15 Cotswold Road, Sutton, Surrey, SM2 5NG, UK
Rosemary A. Wilkinson
Affiliation:
The Institute of Cancer Research, 15 Cotswold Road, Sutton, Surrey, SM2 5NG, UK
Amanda L. Hall
Affiliation:
The Royal Marsden NHS Foundation Trust, Downs Road, Sutton SM2 5PT, UK
Emma Sawyer
Affiliation:
The Institute of Cancer Research, 15 Cotswold Road, Sutton, Surrey, SM2 5NG, UK
Elizabeth Page
Affiliation:
The Institute of Cancer Research, 15 Cotswold Road, Sutton, Surrey, SM2 5NG, UK
Jo-Fen Liu
Affiliation:
Division of Epidemiology, University of Nottingham Medical School, Queen's Medical Centre, Nottingham NG7 2UH, UK
Sandra Barratt
Affiliation:
Division of Epidemiology, University of Nottingham Medical School, Queen's Medical Centre, Nottingham NG7 2UH, UK
Aneela A. Rahman
Affiliation:
Division of Epidemiology, University of Nottingham Medical School, Queen's Medical Centre, Nottingham NG7 2UH, UK
Rosalind Eeles
Affiliation:
Royal Devon and Exeter NHS Foundation Trust, Barrack Road, Exeter Ex2 5DW, UK The Royal Marsden NHS Foundation Trust, Downs Road, Sutton SM2 5PT, UK
Kenneth Muir
Affiliation:
Division of Epidemiology, University of Nottingham Medical School, Queen's Medical Centre, Nottingham NG7 2UH, UK
*
*Corresponding author: Dr Artitaya Lophatananon, fax +44 121 2469 127, email [email protected]
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Abstract

The UK incidence of prostate cancer has been increasing in men aged < 60 years. Migrant studies and global and secular variation in incidence suggest that modifiable factors, including a high-fat diet, may contribute to prostate cancer risk. The aim of the present study was to investigate the role of dietary fat intake and its derivatives on early-onset prostate cancer risk. During 1999–2004, a population-based case–control study with 512 cases and 838 controls was conducted. Cases were diagnosed with prostate cancer when ≤ 60 years. Controls were sourced from UK GP practice registers. A self-administered FFQ collected data on typical past diet. A nutritional database was used to calculate daily fat intake. A positive, statistically significant risk estimate for the highest v. lowest quintile of intake of total fat, SFA, MUFA and PUFA was observed when adjusted for confounding variables: OR 2·53 (95 % CI 1·72, 3·74), OR 2·49 (95 % CI 1·69, 3·66), OR 2·69 (95 % CI 1·82, 3·96) and OR 2·34 (95 % CI 1·59, 3·46), respectively, with all P for trend < 0·001. In conclusion, there was a positive statistically significant association between prostate cancer risk and energy-adjusted intake of total fat and fat subtypes. These results potentially identify a modifiable risk factor for early-onset prostate cancer.

Type
Full Papers
Copyright
Copyright © The Authors 2010

Prostate cancer is a substantial cause of morbidity and mortality in westernised countries including the UK. In 2005, more than 34 000 men were diagnosed with prostate cancer(1). Early-onset prostate cancer (age of diagnosis under 60) accounts for about 10 % of the cases, but these subjects are more likely to have positive family history and are associated with a more aggressive disease course. Incidence in these younger men has increased between 1975 and 2005, yet the aetiology remains unclear. The gene–environment interactions in Prostate Cancer study were set up to investigate the role of genetics, as well as modifiable risk factors including high-fat diet, in the development of early-onset prostate cancer and their potential interactions.

Fat intake has been the focus of dietary studies and prostate cancer risk more than any other dietary components. Fat is the most energy-dense dietary constituent. It yields approximately 37·65 J/g (9 calories/g) on complete oxidation. Chemically, fat is composed of a glycerine backbone with three fatty acids attached. The different fatty acids make one fat different from another. These fatty acids can be divided into three sub groups, SFA, MUFA and PUFA (n-6 and n-3 fatty acids). Their biological properties vary by the degree of saturation and the length of the carbon chain(Reference Kolonel2). It has been suggested that 40 % of total energy intake in a traditional Western diet is derived from fat(Reference Pandian, Eremin and McClinton3). The relationship between dietary fat intake and prostate cancer has been proposed through the high correlation between per capita fat consumption and the large international difference in prostate cancer rates(Reference Gann4, Reference Kolonel5). The early epidemiological evidence on fat and prostate cancer was consistent and suggested a possible causal association(Reference Kolonel, Nomura and Cooney6). These studies, however, did not necessarily assess an independent effect of dietary fat and subsequent prostate cancer risk. Since fat is highly correlated with energy intake, energy adjustment is therefore recommended. Later studies allow for energy adjustment and the findings across different types of epidemiological study become mixed. Cohort studies identified weak, positive, non-significant or null associations between prostate cancer risk and total fat intake. Evidence from case–control studies is more consistent with the majority observing positive associations particularly in advanced cases (OR for the highest compared with the lowest category of total fat intake varied from 1·08 to 3·64)(Reference Pandian, Eremin and McClinton3, Reference Andersson, Wolk and Bergstrom7Reference West, Slattery and Robison18). Very few studies, however, investigated dietary fat and early onset of prostate cancer. A study of a relatively young cohort was among those that observed a weak, positive and non-significant association (mean age at prostate cancer diagnosis of 60 years, range 47–67 years)(Reference Veierod, Laake and Thelle19). Null or weak positive non-significant associations were observed for the five analyses of cases aged < 70 years(Reference Kristal, Cohen and Qu13, Reference West, Slattery and Robison18, Reference Bidoli, Talamini and Bosetti20Reference Hodge, English and McCredie22).

In the present study, we investigate the independent effect of dietary fat intake in relation to early-onset prostate cancer. Dietary fat presented here refers to total fat, saturated and unsaturated fat (both MUFA and PUFA).

Materials and methods

Study participants and data collection

The gene–environment interactions in Prostate Cancer study is a multicentre, population-based case–control study conducted during 1999–2004. The present study was conducted according to the guidelines laid down in the Declaration of Helsinki, and all procedures involving human subjects/patients were approved by the Trent Multi-Centre Research Ethics Committee (MREC/99/4/013(Mar)). Written informed consent was obtained from all participants. Cases were men clinically diagnosed with prostate cancer at age less than or equal to 60 years. Cases were recruited through two approaches; firstly, consultants notified cases to the UK Genetic Prostate Cancer Study and secondly, the British Association of Urological Surgeons (BAUS) Section of Oncology database. Controls were randomly selected from the population list at GP practices where each case was registered. Controls were selected and matched by age to the case ( ± 5 years). The study identified 512 cases and 838 population frequency age-matched controls.

A self-administered postal questionnaire was used to assess exposure history including occupational history (for social class coding), smoking habit, physical activity, body shape and hair pattern, self-reported first degree family history of prostate cancer and diet. Diet was assessed using an adaptation of the validated semi-quantitative FFQ, developed by the MRC Dunn Nutritional Unit at Cambridge for the UK European Prospective Investigation of Cancer in Nutrition(Reference Bingham, Gill and Welch21, Reference Riboli23). Study subjects were asked to recall what their usual diet was 5 years before prostate cancer diagnosis in the case group or to receiving the questionnaire in the control group. Participants were presented with a list of 130 food items, including foods that are main sources of nutrients in the average British diet(Reference Bingham, Gill and Welch21). They were asked to tick the box indicating how often each food was eaten based on a medium portion size; seven pre-defined frequencies range from ‘never or less than once a month’ to ‘more than once a day’. Daily intake was calculated using the nutritional software to compute each nutrient from a total of 130 foods listed in the questionnaire and vitamin and mineral supplements. Nutrient composition values were from the Ministry of Agriculture, Fisheries and Food composition tables(24).

All statistical analyses were undertaken using SPSS for Windows Version 14. An unconditional logistic regression was carried out to obtain OR and 95 % CI. Energy adjustment was done using the residual method proposed by Willett & Stampfer(Reference Willett, Stampfer and Willet25). Each exposure was categorised into quintiles based on the distribution of energy-adjusted value in controls. Age, one or more first-degree relatives with prostate cancer, and baldness in the fourth decade of life were further adjusted in multivariate models. The prostate cancer family history was adjusted for due to potential genetic predisposition in cases. Baldness was adjusted for based on a statistically significant baseline difference between cases and controls and made a difference to the goodness of fit of the model (see Table 1). To assess the existence of dose–response relationships, tests for linear trend (two-tailed) across increasing quintiles of nutrient intake were performed, modelling categorical nutrient intakes as continuous variables in the multivariate model.

Table 1 Characteristics of study participants

(OR values and 95 % CI)

* Participants were categorised by social class by identifying the longest job held: I, professional; II, managerial and technical occupation; IIIN, non-manual skilled occupation; IIIM, manual skilled occupation; IV, partly skilled occupation; V, unskilled occupation.

Finally, etiologic fractions, related to total fat and fat subtypes, were calculated using the Miettinen formula for multi-category indicator: EF=ΣiCFi×(SMRi−1)/SMRi, where EF is the etiologic fractions, CF is the proportion of cases with the marker of increased risk and SMR is the standardised morbidity ratio in that subcategory(Reference Miettinen26).

Results

Table 1 shows the characteristics of study subjects. The mean age of cases and controls was 55·7 years. There was a strong, highly significant increased risk of prostate cancer in those with at least one first-degree relative (OR 6·09, 95 % CI 3·99, 9·27, P < 0·001). The distribution of cases and controls according to social class was very similar, reflected in there being no significant association between prostate cancer risk and social class. There was no significant association between prostate cancer risk and cigarette smoking. Severe baldness in the fourth decade of life, compared with no/negligible baldness, was associated with a weak, statistically significant increase in risk (OR 1·47, 95 % CI 1·09, 1·98, P = 0·01). Participants' perceived body shape and moderate physical activity at different decades in life were similar for cases and controls and were not associated with risk.

Results from Table 2 showed that the difference in mean average energy intake between cases and controls was highly significant (P < 0·001); mean average daily energy intake in cases was 12 060·42 kJ/d (2882·51 kcal/d), 9·8 % higher than that of controls.

Table 2 Daily energy and total fat intake among 512 prostate cancer cases and 838 controls: UK 1999–2004

(Mean values and standard deviations with their mean difference)

Overall, the diet of study subjects contained fat as approximately 30 % of total energy intake. There was no significant difference in mean total fat intake between cases and controls when measured as a percentage of total energy (P < 0·001). The actual total fat intake in cases though was 13 % higher than that of controls. Similar percentage differences were also observed with fat subtypes.

Estimated risks are presented in Table 3. Moderate to strong, statistically significant OR were found for the highest three quintiles v. lowest quintile of total fat intake when adjusted only for age and for age, family history and baldness. For fat subtypes, moderate to strong, statistically significant OR were found for the highest three quintiles of intake v. the lowest when adjusted for age only, when further adjusted for family history and baldness, only the highest two quintiles v. lowest quintile remained significant. OR from the fully adjusted model ranged from 1·57 to 2·69.

Table 3 Risk estimates according to quintile of fat intake and its derivatives; energy-adjusted residual method

(OR values and 95 % CI)

Q, reference quintile.

Values in each quintile were mutually exclusive; cut points are given to two decimal places.

* Model 1, adjusted for age as a continuous variable.

Model 2, adjusted for age as a continuous variable, first-degree relative with prostate cancer and baldness in 40s.

A highly significant trend was observed for increased risk of prostate cancer with increased intake of total fat and its subtypes across quintiles in both models.

Etiologic fractions

Assuming the relationship between fat intake and prostate cancer is causal; etiologic fraction results suggested that on average, about 42 % of prostate cancer cases in the present study could be attributed to increased fat intake (greater than 64·48 g/d).

Discussion

We have conducted a UK nationwide prostate cancer case–control study with 512 early-onset cases and 838 population based controls. A self-administered FFQ was employed to collect typical dietary data. A value based on daily intake was assessed and the estimated risk was calculated based on quintile distribution. The results appear to support the hypothesis that increased total fat, SFA, MUFA and PUFA intakes increase the risk of prostate cancer diagnosed at a young age of 60 years or less. A positive, strong, statistically significant association between total fat and fat subtypes was observed (adjusted OR of the highest compared to the lowest quintile of intake were between 2·34 and 2·69).

Like other diet and cancer case–control studies, the present study could be subject to recall bias particularly in the control group. To evaluate the representativeness of the control group's nutrient intake, comparisons of crude mean intake of controls in the present study were made with The National Diet and Nutrition Survey by Henderson et al. (Reference Henderson, Gregory and Irving27) and that of controls from a UK case–control study of diet and prostate cancer by Key et al. (Reference Key, Silcocks and Davey11).

The National Diet and Nutrition Survey was chosen as the sampling methods attempted to recruit a nationally representative sample and thorough methods were used to establish diet (both interviews and 7-d weighed records). Controls' mean daily intake of total and SFA was virtually the same as that reported in this survey (the survey reported daily intake values of 86·5 and 32·5 g)(Reference Henderson, Gregory and Irving27). However, controls' mean daily energy intake was higher with the survey-reported values of 9719·43 kJ (2323 kcal) in adult men (19–64 years) as compared to 10 878·40 kJ (2600 kcal) in our controls reflecting the lower percentage of energy from fat and fat subtypes in study controls. Department of Health suggested dietary reference values for energy for healthy men were 10 669·20 kJ (2550 kcal)(28). Study controls had similar energy intake but consistently and substantially lower intakes of fat and fat derivatives than controls in the study by Key et al.; intake was 34 % lower for total fat and MUFA and over 50 % lower for SFA. Key et al. (Reference Key, Silcocks and Davey11) acknowledged that the average fat intake in their study was high. We therefore concluded that study controls could include some over-representation of health-conscious controls; however, any recall bias occurred was considered minimal.

In terms of case and control characteristics, it is important to highlight that all of these cases were diagnosed clinically in younger men presenting with significant disease (not through prostate specific antigen measurement/screening). As for the controls, there is a possibility of low-grade cases being included in the control group, as is the situation with all case–control studies using community-derived controls, but the potential size of this effect is less due to the younger age group on which the present study focuses. We therefore suggest that the above factors are unlikely to have had a significant effect on the results presented.

The positive association between total fat and prostate cancer risk observed is concordant with most case–control studies in the literature review where all stages of prostate cancer were combined. Of these, only three reported a statistically significant increased risk, also of moderate to strong magnitude(Reference Lee, Wang and Hsing29Reference Whittemore, Kolonel and Wu31).

The only UK case–control study identified in the literature review did not specifically look at younger cases and found a non-significant inverse association between prostate cancer risk and high v. low total fat intake (OR 0·85, 95 % CI 0·57, 1·25); the lack of a significant association is thought to be attributable to participants' narrow range of high fat intake(Reference Lagiou, Trichopoulos and Tzonou32).

Increased saturated fat intake is positively associated with early-onset prostate cancer risk. The positive association observed is in keeping with approximately half of the case–control studies regardless of their age group identified in the literature review(Reference Andersson, Wolk and Bergstrom7, Reference Pandian, Eremin and McClinton3, Reference Lee, Wang and Hsing29, Reference Whittemore, Kolonel and Wu31, Reference Lagiou, Trichopoulos and Tzonou32).

Not all of the findings from previous studies supported a MUFA role in prostate cancer aetiology. This inconsistency may be partly related to the food sources of MUFA in different populations (e.g. meat in Western diet and olive oil in Mediterranean diet), as other components in the food sources may confound the effects of MUFA. One analysis of aggressive prostate cancer and another of early-onset prostate cancer observed statistically significant point estimates of lesser magnitude to those in the present study (OR 2·00, 95 % CI 1·03, 3·87) and (OR 1·9, 95 % CI 1·1, 3·4)(Reference Kristal, Cohen and Qu13, Reference Bidoli, Talamini and Bosetti20).

The literature supporting an increased prostate cancer risk with high PUFA intake is inconsistent. One study reported a statistically significant OR with a significant P for trend across quintiles(Reference Tzonou, Signorello and Lagiou33). Conversely, five studies suggested inverse associations(Reference Andersson, Wolk and Bergstrom7, Reference Kristal, Cohen and Qu13, Reference Ramon, Bou and Romea15, Reference Bidoli, Talamini and Bosetti20, Reference Hill, Wynder and Garbaczewski34).

A high fat intake may increase the levels of endogenous androgens(Reference Hill, Wynder and Garbaczewski34). There are different mechanisms proposed depending on the type of fat. Polyunsaturated fat is prone to oxidation, generating lipid radicals and hydroperoxides that cause DNA damage leading to carcinogenesis(Reference Kolonel2). The synthesis of PG and leukotrienes is regulated by fatty acid. PG and leukotrienes affect cell proliferation and metastases(Reference Pandian, Eremin and McClinton3, Reference Ghosh and Myers35). There may be an association between hypercholesterolaemia and prostate cancer(Reference Bravi, Scotti and Bosetti36, Reference Freeman and Solomon37). Additionally, cholesterol is a major substrate for androgen synthesis. This may suggest that dietary fat influences prostate cancer risk though being a major determinant of plasma cholesterol levels. Other forms of fatty acid play a part in protecting against carcinogenesis. Fish oil, which rich in n-3 fatty acids EPA and DHA, may increase the accumulation of lipid peroxidation products in tumour tissue. These products subsequently decrease cell proliferation or increase cell death(Reference Pandian, Eremin and McClinton3).

The consistent results observed in the present study suggest that total fat intake is implicated in young-onset prostate cancer risk; thus, variation in risk estimates would be expected if a specific fat derivative was conferring risk, unless SFA, MUFA and PUFA were so highly collinear that they were not mutually exclusive. Also, early-onset prostate cancer cases are distinct from the case mix used in previous studies. A greater proportion of aggressive phenotypes would be expected to be more strongly associated with risk of prostate cancer due to fat intake. The greater risk seen in the present study could also be explained by the confounding interaction between the genetic component and the exposure. The younger-aged case series have a greater proportion due to genetic predisposition than older cases. The effects of the interaction could either be multiplicative or additive.

One might suggest that cases are overeating or over-reporting the amount of food eaten. A post hoc analysis of protein and carbohydrate intake was conducted to investigate the possibility of overeating or over-reporting of all macronutrients by cases. Cases had approximately 10 % higher mean daily intake of protein and carbohydrate, a difference which was highly statistically significant (P < 0·001). This suggested that overeating or over-reporting by cases was plausible. On further multivariate analysis of protein and carbohydrate intakes, moderate to strong, positive, statistically significant OR in the highest v. lowest quintile of intake (when adjusted for age, family history and baldness) were observed. When adjusted for fat intake, the increased risk for protein and carbohydrate was no longer significant. This suggests that the risk conferred by protein and carbohydrate was due to confounding by fat intake and that while cases do eat more macronutrients than controls, it is the over-consumption of fat intake that is particularly associated with prostate cancer risk.

Given that the residual method of energy adjustment should differentiate the effects of food intake overall from those of diet composition(Reference Willett, Stampfer and Willet25), the significant associations observed when adjusted for energy intake may not be caused by excess total nutrient intake or, by implication, excess energy intake of cases.

The positive, statistically significant associations observed indicate that 5 years before diagnosis could be the aetiologically relevant time for exposure to dietary fat, or whatever fat intake is a marker of, in relation to prostate cancer risk. Alternatively, it could show that intake 5 years before diagnosis is highly correlated with the true aetiologically relevant exposure period. Equally, subjects could report their typical diet, which has not changed during the last decade; thus, the findings could reflect the relevant time up to a decade before diagnosis. Considering this time implication together with the aggressive disease in our cases, high fat intake may play a role in both initiation and progression.

Conclusion

The present study observed an association between an early-onset prostate cancer risk and a relatively high intake of total fat and fat derivatives. There was a strong, statistically significant positive risk estimate for high v. low intake of total fat, SFA, MUFA and PUFA; each risk estimate was of similar magnitude (OR between 2·34 and 2·69). A highly significant dose–response relationship was also observed for total fat and fat subtypes (P for trend < 0·001), suggesting an increase in the risk of prostate cancer with increase in fat intake. Etiologic fractions suggest that if these associations are causal, approximately 40 % of early-onset prostate cancer cases could have an aetiology related to their fat intake. This has implications for prevention.

Acknowledgements

The study has no conflicts of interest. The present research was supported by the Prostate Cancer Research Foundation and Cancer Research UK grant C5047/A3354. The authors thank the UK Genetic Prostate Cancer Study Collaborators and the British Association of Urological Surgeons' Section of Oncology for their collaboration on the study. The original authors and their contributions are as follows: A. L. was involved in the conduct of the study, analysed the data and drafted the paper. J. A. was involved in the data quality control and analysed the data. D. E., R. P., D. D., M. G., Z. K.-J. L. O'B., R. A. W., A. L. H., E. S. and E. P. were involved in the development of the protocol, conduct of the study and revision of the paper. J.-F. L., S. B. and A. A. R. were involved in the data management, data collection and updated diet calculation programme. R. E. and K. M. were involved in the development of the protocol, conduct of the study and revision of the paper, and they are the principal investigator and guarantor.

References

1 Cancer Research UK (2008) UK prostate cancer incidence statistics. http://info.cancerresearchuk.org/cancerstats/types/prostate/index.htm?script=true.Google Scholar
2 Kolonel, LN (2001) Fat, meat, and prostate cancer. Epidemiol Rev 23, 7281.CrossRefGoogle ScholarPubMed
3 Pandian, SS, Eremin, OE, McClinton, S, et al. (1999) Fatty acids and prostate cancer: current status and future challenges. J R Coll Surg Edinb 44, 352361.Google ScholarPubMed
4 Gann, PH (2002) Risk factors for prostate cancer. Rev Urol 4, Suppl. 5, S3S10.Google ScholarPubMed
5 Kolonel, LN (1996) Nutrition and prostate cancer. Cancer Causes Control 7, 8394.CrossRefGoogle ScholarPubMed
6 Kolonel, LN, Nomura, AMY & Cooney, RV (1999) Dietary fat and prostate cancer: current status. J Natl Cancer Inst 91, 414428.CrossRefGoogle ScholarPubMed
7 Andersson, SO, Wolk, A, Bergstrom, R, et al. (1996) Energy, nutrient intake and prostate cancer risk: a population-based case–control study in Sweden. Int J Cancer 68, 716722.3.0.CO;2-6>CrossRefGoogle Scholar
8 Chan, JM, Pietinen, P, Virtanen, M, et al. (2000) Diet and prostate cancer risk in a cohort of smokers, with a specific focus on calcium and phosphorus (Finland). Cancer Causes Control 11, 859867.CrossRefGoogle Scholar
9 Deneo-Pellegrini, H, Stefani, ED, Ronco, A, et al. (1999) Foods, nutrients and prostate cancer: a case–control study in Uruguay. Br J Cancer 80, 591597.CrossRefGoogle ScholarPubMed
10 Hayes, RB, Ziegler, RG, Gridley, G, et al. (1999) Dietary factors and risks for prostate cancer among blacks and whites in the United States. Cancer Epidemiol Biomarkers Prev 8, 2534.Google ScholarPubMed
11 Key, TJ, Silcocks, PB, Davey, GK, et al. (1997) A case–control study of diet and prostate cancer. Br J Cancer 76, 678687.CrossRefGoogle ScholarPubMed
12 Kolonel, LN, Yoshizawa, CN & Hankin, JH (1988) Diet and prostatic cancer: a case–control study in Hawaii. Am J Epidemiol 127, 9991012.CrossRefGoogle ScholarPubMed
13 Kristal, AR, Cohen, JH, Qu, P, et al. (2002) Associations of energy, fat, calcium, and vitamin D with prostate cancer risk. Cancer Epidemiol Biomarkers Prev 11, 719725.Google ScholarPubMed
14 Ohno, Y, Yoshida, O, Oishi, K, et al. (1988) Dietary beta-carotene and cancer of the prostate: a case–control study in Kyoto, Japan. Cancer Res 48, 13311336.Google ScholarPubMed
15 Ramon, JM, Bou, R, Romea, S, et al. (2000) Dietary fat intake and prostate cancer risk: a case–control study in Spain. Cancer Causes Control 11, 679685.CrossRefGoogle Scholar
16 Rohan, TE, Howe, GR, Burch, JD, et al. (1995) Dietary factors and risk of prostate cancer: a case–control study in Ontario, Canada. Cancer Causes Control 6, 145154.CrossRefGoogle ScholarPubMed
17 Turkes, A (2000) Can diet reduce the risk of prostate cancer? In Challenges in Prostate Cancer, pp. 36 [Bowsher, W, editor]. Malden, MA: Blackwell.Google Scholar
18 West, DW, Slattery, ML, Robison, LM, et al. (1991) Adult dietary intake and prostate cancer risk in Utah: a case–control study with special emphasis on aggressive tumors. Cancer Causes Control 2, 8594.CrossRefGoogle ScholarPubMed
19 Veierod, MB, Laake, P & Thelle, DS (1997) Dietary fat intake and risk of prostate cancer: a prospective study of 25708 Norwegian men. Int J Cancer 73, 634638.3.0.CO;2-Y>CrossRefGoogle Scholar
20 Bidoli, E, Talamini, R, Bosetti, C, et al. (2005) Macronutrients, fatty acids, cholesterol and prostate cancer risk. Ann Oncol 16, 152157.CrossRefGoogle ScholarPubMed
21 Bingham, SA, Gill, C, Welch, A, et al. (1997) Validation of dietary assessment methods in the UK arm of EPIC using weighed records, and 24-hour urinary nitrogen and potassium and serum vitamin C and carotenoids as biomarkers. Int J Epidemiol 26, S137S151.CrossRefGoogle ScholarPubMed
22 Hodge, AM, English, DR, McCredie, MR, et al. (2004) Foods, nutrients and prostate cancer. Cancer Causes Control 15, 1120.CrossRefGoogle ScholarPubMed
23 Riboli, E (1992) Nutrition and cancer: background and rationale of the European Prospective Investigation into Cancer and Nutrition (EPIC). Ann Oncol 3, 783791.CrossRefGoogle ScholarPubMed
24 Ministry of Agriculture Fisheries and Foods (1993) Annual Reports of National Food Survey Committee. London: HMSO.Google Scholar
25 Willett, W & Stampfer, M (1998) Implications of total energy intake for epidemiologic analyses. In Nutritional Epidemiology, pp. 273301 [Willet, W, editor]. Oxford: Oxford University Press.CrossRefGoogle Scholar
26 Miettinen, OS (1974) Proportion of disease caused or prevented by a given exposure, trait or intervention. Am J Epidemiol 99, 325332.CrossRefGoogle ScholarPubMed
27 Henderson, L, Gregory, J & Irving, K (2003) The National Diet and Nutrition Survey. London: HMSO.Google Scholar
28 Department of Health (1991) Dietary Reference Values for Food Energy and Nutrients for the United Kingdom. London: HMSO.Google Scholar
29 Lee, MM, Wang, RT, Hsing, AW, et al. (1998) Case–control study of diet and prostate cancer in China. Cancer Causes Control 9, 545552.CrossRefGoogle ScholarPubMed
30 Vlajinac, HD, Marinkovic, JM, Ilic, MD, et al. (1997) Diet and prostate cancer: a case–control study. Eur J Cancer 33, 101107.CrossRefGoogle ScholarPubMed
31 Whittemore, AS, Kolonel, LN, Wu, AH, et al. (1995) Prostate cancer in relation to diet, physical activity, and body size in blacks, whites, and Asians in the United States and Canada. J Natl Cancer Inst 87, 652661.CrossRefGoogle Scholar
32 Lagiou, A, Trichopoulos, D, Tzonou, A, et al. (2001) Are there age-dependent effects of diet on prostate cancer risk? Soz Praventivmed 46, 329334.CrossRefGoogle ScholarPubMed
33 Tzonou, A, Signorello, LB, Lagiou, P, et al. (1999) Diet and cancer of the prostate: a case–control study in Greece. Int J Cancer 80, 704708.3.0.CO;2-Z>CrossRefGoogle ScholarPubMed
34 Hill, P, Wynder, EL, Garbaczewski, L, et al. (1979) Diet and urinary steroids in black and white North American men and black South African men. Cancer Res 39, 51015105.Google ScholarPubMed
35 Ghosh, J & Myers, CE Jr (1998) Arachidonic acid metabolism and cancer of the prostate. Nutrition 14, 4849.Google ScholarPubMed
36 Bravi, F, Scotti, L, Bosetti, C, et al. (2006) Self-reported history of hypercholesterolaemia and gallstones and the risk of prostate cancer. Ann Oncol 17, 10141017.CrossRefGoogle ScholarPubMed
37 Freeman, MR & Solomon, KR (2004) Cholesterol and prostate cancer. J Cell Biochem 91, 5469.CrossRefGoogle ScholarPubMed
Figure 0

Table 1 Characteristics of study participants(OR values and 95 % CI)

Figure 1

Table 2 Daily energy and total fat intake among 512 prostate cancer cases and 838 controls: UK 1999–2004(Mean values and standard deviations with their mean difference)

Figure 2

Table 3 Risk estimates according to quintile of fat intake and its derivatives; energy-adjusted residual method(OR values and 95 % CI)