Abstract Cilia are found on most cells of the body and are thought to play important roles in physiology and development. Not surprisingly, it is now understood that a very wide range of human diseases and developmental defects results from defects in ciliary assembly or function [1]. The steadily increasing number of disease genes related to cilia suggests that identification of ciliary proteins is a productive way to identify new candidate disease genes. Recent bioinformatics studies have followed this strategy by using comparative genomics to identify likely ciliary genes found only in organisms that have cilia and flagella. This ingenious approach has turned out to be highly productive, most notably by revealing the identity of the Bardet-Biedl Syndrome BBS5 gene [2]. In a recent Current Biology Dispatch [3], Greg Pazour presented a carefully thought-out analysis of these approaches, and after discussing several potential limitations, concluded that there is an urgent need for proteomic analysis to determine directly which proteins are contained in cilia and flagella.
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