Genetic heterogeneity in affective disorders.

Abstract

The extent of genetic heterogeneity in major affective illness was estimated via 3 paradigms of single-major-locus inheritance. In the 1st paradigm bipolar and unipolar disorders were represented at different liability thresholds on a genetic-environmental continuum. The 2nd paradigm incorporated sex-related thresholds into the model, thereby testing the hypothesis that affective illness is a transmitted trait whose phenotypic expression is a function of the individual''s sex. The 3rd paradigm included both clinical polarity and sex effect as threshold phenomena. All 3 paradigms predicted considerable genetic heterogeneity in affective disorders. Bipolar homozygotes were far more common than unipolar homozygotes, although the majority of ill individuals in the first 2 paradigms were heterozygotes. According to the 3rd paradigm bipolar males had the highest proportion of homozygotes amongst the affected population. Significant increases in homozygosity occurred using the dual mating sampling method. Depending on the model paradigm and parameters these increases were 140-25,000% over the random sample method. The implications for biologic and gnetic research in affective disorders were discussed.