The recent systematic review of epidemiological studies of the associations between long-chain (LC) n-3 PUFA and the risk of several cancers highlights the need for additional prospective studies that use valid and unbiased measures of dietary intake(Reference Gerber1). Specifically, it was noted that additional prospective studies using blood biomarker-based assessments of LC n-3 PUFA exposure would minimise the measurement error inherent in all measures based upon dietary recall. We agree with this. The conclusions of the review of the associations between LC n-3 PUFA and prostate cancer risk are based on two case–control and four prospective studies; five out of six of these studies used retrospective dietary assessment using FFQ. Missing from the review, however, are findings from several prospective biomarker studies(Reference Crowe, Allen and Appleby2–Reference Park, Wilkens and Henning4) including the two largest blood biomarker studies published to date on the topic(Reference Crowe, Allen and Appleby2, Reference Brasky, Till and White3). In a small (n cases 376) case–control study nested within the Multiethnic Cohort, no association was reported between LC n-3 PUFA and prostate cancer risk(Reference Park, Wilkens and Henning4). However, in a much larger case–control study (n cases 962) nested within the European Prospective Investigation into Cancer and Nutrition, a 31 % (relative risk (RR) 1·31, 95 % CI 0·96, 1·81) and 39 % (RR 1·39, 95 % CI 1·02, 1·90) increase in prostate cancer risk in the highest compared with the lowest quintile of plasma phospholipid EPA and DHA was seen, respectively(Reference Crowe, Allen and Appleby2). There was a 100 % increased risk (RR 2·00, 95 % CI 1·07, 3·76) of high-grade cancer contrasting the highest to lowest quintiles of EPA(Reference Crowe, Allen and Appleby2). In a case–control study nested within the Prostate Cancer Prevention Trial (n cases 1658), which was a unique study because the presence or absence of prostate cancer was determined by biopsy for all participants, a 150 and 99 % increased risk of high-grade prostate cancer in the highest v. the lowest quartile of serum phospholipid DHA (OR 2·50, 95 % CI 1·34, 4·65) or EPA+DHA (OR 1·99, 95 % CI 1·08, 3·68), respectively, was found, although there was no association for EPA alone(Reference Brasky, Till and White3). Although the findings from the Prostate Cancer Prevention Trial were based on screen-detected cancers, which identifies cases that might never have become clinically relevant, the strength of the associations for high-grade cancer suggests that the findings are indeed clinically relevant.
The addition of these prospective and biomarker-based studies to the studies reviewed recently(Reference Gerber1) would certainly modify the conclusion on whether or not LC n-3 PUFA could reduce the risk of prostate cancer. Indeed, the findings from these biomarker-based studies challenge the generally accepted notion that increasing consumption of foods high in LC n-3 PUFA uniformly reduces chronic disease risk(Reference Moyad5).