CDK5 is a major regulator of the tumor suppressor DLC1.
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Abstract | DLC1 is a tumor suppressor protein whose full activity depends on its presence at focal adhesions, its Rho-GTPase activating protein (Rho-GAP) function, and its ability to bind several ligands, including tensin and talin. However, the mechanisms that regulate and coordinate these activities remain poorly understood. Here we identify CDK5, a predominantly cytoplasmic serine/threonine kinase, as an important regulator of DLC1 functions. The CDK5 kinase phosphorylates four serines in DLC1 located N-terminal to the Rho-GAP domain. When not phosphorylated, this N-terminal region functions as an autoinhibitory domain that places DLC1 in a closed, inactive conformation by efficiently binding to the Rho-GAP domain. CDK5 phosphorylation reduces this binding and orchestrates the coordinate activation DLC1, including its localization to focal adhesions, its Rho-GAP activity, and its ability to bind tensin and talin. In cancer, these anti-oncogenic effects of CDK5 can provide selective pressure for the down-regulation of DLC1, which occurs frequently in tumors, and can contribute to the pro-oncogenic activity of CDK5 in lung adenocarcinoma. |
Year of Publication | 2014
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Journal | J Cell Biol
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Volume | 207
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Issue | 5
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Pages | 627-42
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Date Published | 2014 Dec 08
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ISSN | 1540-8140
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URL | |
DOI | 10.1083/jcb.201405105
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PubMed ID | 25452387
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PubMed Central ID | PMC4259810
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Grant list | Intramural NIH HHS / United States
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