SETA/CIN85/Ruk and its binding partner AIP1 associate with diverse cytoskeletal elements, including FAKs, and modulate cell adhesion

doi:10.1242/jcs.00522

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JCS ePress online publication date 27 May 2003
doi: 10.1242/jcs.00522

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Research Article

SETA/CIN85/Ruk and its binding partner AIP1 associate with diverse cytoskeletal elements, including FAKs, and modulate cell adhesion

Mirko H.H. Schmidt, Baihua Chen, Lisa M. Randazzo, and Oliver Bögler^*
^* Author for correspondence (e-mail: oliver{at}bogler.net)

The adaptor protein SETA/CIN85/Ruk is involved in regulatingdiverse signal transduction pathways, including the internalizationof tyrosine kinase receptors via the Cbl ubiquitin ligases,and attenuating PI3K activity by interaction with its regulatorysubunit. Here we present evidence for a new aspect of SETA function,based on the initial observation that it co-localizes with actinin microfilaments and at focal adhesions, and with microtubules.Although there was no evidence for direct molecular interactionsbetween SETA and cytoskeletal proteins, the SETA-interactingprotein AIP1, which is a rat ortholog of the Xenopus src substrateXp95, strongly interacted with structural proteins of the cytoskeleton,including actin and tubulins. Both SETA and AIP1 interactedwith focal adhesion kinase (FAK) and proline rich tyrosine kinase2 (PYK-2), and c-Cbl interacted with PYK-2. AIP1, which interactedmore strongly than either SETA or c-Cbl, required an intactconsensus tyrosine kinase phosphorylation sequence at Y319 tobind to focal adhesion kinases, which suggests that phosphorylationis an important mediator of this complex. SETA, which interactedas a dimer with focal adhesion kinases, promoted the interactionbetween PYK-2 and AIP1. Direct analysis of the impact of theseproteins on cell adhesion, by use of an electrical cell-substrateimpedance sensor (ECIS), showed that SETA promoted cell adhesionwhile AIP1 and c-Cbl reduced it. Furthermore, the ability ofAIP1 and AIP1 mutants to decrease cell adhesion in ECIS analysiscorrelated with their presence in PYK-2 complexes, providinga direct link between AIP1-mediated molecular interactions andcellular behavior. Transfection of AIP1 also reduced the levelof phosphorylation of endogenous PYK-2 and FAK, suggesting thatthis protein may directly regulate focal adhesion kinases, andthereby cell adhesion. These data are the first to implicatethe adaptor protein SETA and its binding partner AIP1 as beinginvolved with the cytoskeleton and in the regulation of celladhesion, and suggest that they may be part of the focal adhesionkinase regulatory complex.

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