Finding disease variants in Mendelian disorders by using sequence data: methods and applications.

[kabuki syndrome]

Many sequencing studies are now underway to identify the genetic causes for both Mendelian and complex traits . Via exome-sequencing , genes harboring variants implicated in several Mendelian traits have already been identified . The underlying methodology in these studies is a multistep algorithm based on filtering variants identified in a small number of affected individuals and depends on whether they are novel (not yet seen in public resources such as dbSNP ), shared among affected individuals , and other external functional information on the variants . Although intuitive , these filter-based methods are nonoptimal and do not provide any measure of statistical uncertainty . We describe here a formal statistical approach that has several distinct advantages : (1 ) it provides fast computation of approximate p values for individual genes , (2 ) it adjusts for the background variation in each gene , (3 ) it allows for incorporation of functional or linkage-based information , and (4 ) it accommodates designs based on both affected relative pairs and unrelated affected individuals . We show via simulations that the proposed approach can be used in conjunction with the existing filter-based methods to achieve a substantially better ranking of a gene relevant for disease when compared to currently used filter-based approaches , this is especially so in the presence of disease locus heterogeneity . We revisit recent studies on three Mendelian diseases and show that the proposed approach results in the implicated gene being ranked first in all studies , and approximate p values of 10 (-6 ) for the Miller Syndrome gene , 1 .0 × 10 (-4 ) for the Freeman-Sheldon Syndrome gene , and 3 .5 × 10 (-5 ) for the Kabuki Syndrome gene .