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Review
. 2014 Jul;82(7):1113-27.
doi: 10.1002/prot.24560. Epub 2014 Apr 10.

Molecular physiology of the tensin brotherhood of integrin adaptor proteins

Affiliations
Review

Molecular physiology of the tensin brotherhood of integrin adaptor proteins

Donald T Haynie. Proteins. 2014 Jul.

Abstract

Numerous proteins have been identified as constituents of the adhesome, the totality of molecular components in the supramolecular assemblies known as focal adhesions, fibrillar adhesions and other kinds of adhesive contact. The transmembrane receptor proteins called integrins are pivotal adhesome members, providing a physical link between the extracellular matrix (ECM) and the actin cytoskeleton. Tensins are ever more widely investigated intracellular adhesome constituents. Involved in cell attachment and migration, cytoskeleton reorganization, signal transduction and other processes relevant to cancer research, tensins have recently been linked to functional properties of deleted in liver cancer 1 (DLC1) and a mitogen-activated protein kinases (MAPK), to cell migration in breast cancer, and to metastasis suppression in the kidney. Tensins are close relatives of phosphatase homolog/tensin homolog (PTEN), an extensively studied tumor suppressor. Such findings are recasting the earlier vision of tensin (TNS) as an actin-filament (F-actin) capping protein in a different light. This critical review aims to summarize current knowledge on tensins and thus to highlight key points concerning the expression, structure, function, and evolution of the various members of the TNS brotherhood. Insight is sought by comparisons with homologous proteins. Some historical points are added for perspective.

Keywords: C2 domain; PTB domain; PTEN; PTP domain; SH2 domain; actin; adhesome; cytoskeleton; deleted in liver cancer 1; domain; integrin; migration; module; phosphorylation; signal transduction.

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