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Both high throughput screening and crystallization are now able to be performed efficiently with robotics, further decreasing the cost and increasing the speed with which PDE selective inhibitors can be discovered. Unfortunately, much less effort has gone into identification of activators of PDEs although much of the same technology could be applied. At the functional level the identification of new PDE enzymes has been greatly aided by developments in molecular biology. In particular the publication of the human and mouse genomes has led to the discovery of new PDE isoforms and the identification of variants of previously known ones. These advances have implicated the involvement of PDEs in many pathological conditions. 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