Complex traits, including aging-associated conditions, can be influenced by a multiplicity of genetic and environmental factors. Because each factor is expected to make only a small contribution to trait variability, and this contribution may itself be influenced by interactions with other susceptibility factors, identifying the genetic basis of complex traits is challenging and requires large sample sizes [1]. Isolated founder populations, which have already proven useful in the study of many Mendelian disorders [2], provide an attractive setting for the study of complex traits [3,4] because they typically exhibit greater genetic and environmental homogeneity than more cosmopolitan populations.
