Can Lessons Learned from Genome-Wide Research be Applied to Nutrition-Wide and Exposure-Wide Evidence?

Human genomics and human nutrition are two very large domains of epidemiological investigation, but their overlap has remained relatively limited to date. Most studies that address genetic risk factors ignore nutritional and other related exposures, and vice versa. Both domains have not only a history of exciting discoveries, but also a tenuous, if not poor, replication record (Ioannidis, 2005a; Ioannidis et al., 2001). For nutritional and lifestyle epidemiology, randomized trials have failed to confirm a large number of associations proposed by observational data (Ioannidis, 2005b). For genetic epidemiology, a major transformation in the last few years has suggested that most candidate gene associations proposed in the past were likely false-positives (Manolio et al., 2008; McCarthy et al., 2008). The new transformation of genetic epidemiology has led to a new mode of discovery and validation of associations based on shear massive testing (large-scale studies on large-scale massive-testing platforms) (McCarthy et al., 2008). The list of successfully discovered gene variants that regulate the risk for common diseases continues to grow on a weekly basis (Manolio et al., 2008). It is worthwhile to examine whether some of the lessons of this recent transformation can also be extended to human nutritional and lifestyle epidemiology. There are clear differences between the genomics and nutrition fields. A major difference is that massive measurement platforms are not yet available for nutritional and lifestyle exposures, at least on the large scale available for genomic markers. Nevertheless massive-scale biochemical measurements and massive collection of electronic information (e.g., through mobile telephones or the Internet) may get closer to achieving the high-throughput paradigm that is currently prevalent in genomics. The correlation pattern between nutritional/lifestyle variables is far denser than the correlation pattern of genomic markers; however, disequilibrium is also considerable in some areas of the genome linkage and poses similar problems in the attribution of causality. In general, markers that arise from genome-wide association studies are only correlates of risk, and may be far from the real causative culprit. Human genome epidemiology has also made major progress by being able to cut down dramatically in measurement error by imposing very strict quality-control standards. The use of rigorous standards also should be feasible in other areas of epidemiological investigation. The need for longitudinal measurements and the unavoidable missing information may be different from genomic epidemiology; however, genomic markers also need to be further validated in longitudinal studies, rather than only the case-control designs that have been relatively successful for genetic epidemiology so far (Wellcome Trust Case Control Consortium, 2007). Firm documentation of gene-environment interactions will require examination in very large cohorts and biobanks (Elliott et al., 2008). Thus, a new paradigm of extremely large cohorts and coalitions thereof is due to appear. Repeated measurements are also essential for nutritional epidemiology, as opposed to the genotypic information that is standard and fixed at birth. Genomic epidemiology has been more eager to adopt explicit consideration of multiplicity issues, which has led to a more uniform adoption of rigorous standards for what is considered appropriately replicated and credible as an association. Similar improvements must also be made in nutritional epidemiology in which traditional significance levels without any correction are