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Structures of the cancer-related Aurora-A,FAK, and EphA2 protein kinases from nanovolume crystallography
Authors:Nowakowski Jacek  Cronin Ciarán N  McRee Duncan E  Knuth Mark W  Nelson Christian G  Pavletich Nikola P  Rogers Joe  Sang Bi-Ching  Scheibe Daniel N  Swanson Ronald V  Thompson Devon A
Affiliation:Syrrx, Inc., 10410 Science Center Drive, San Diego, CA 92121, USA. jacek.nowakoski@syrrx.com
Abstract:Protein kinases are important drug targets in human cancers, inflammation, and metabolic diseases. This report presents the structures of kinase domains for three cancer-associated protein kinases: ephrin receptor A2 (EphA2), focal adhesion kinase (FAK), and Aurora-A. The expression profiles of EphA2, FAK, and Aurora-A in carcinomas suggest that inhibitors of these kinases may have inherent potential as therapeutic agents. The structures were determined from crystals grown in nanovolume droplets, which produced high-resolution diffraction data at 1.7, 1.9, and 2.3 A for FAK, Aurora-A, and EphA2, respectively. The FAK and Aurora-A structures are the first determined within two unique subfamilies of human kinases, and all three structures provide new insights into kinase regulation and the design of selective inhibitors.
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