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. 2008 Jan 25;283(4):1893-901.
doi: 10.1074/jbc.M706822200. Epub 2007 Nov 19.

ErbB-2 and met reciprocally regulate cellular signaling via plexin-B1

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Free article

ErbB-2 and met reciprocally regulate cellular signaling via plexin-B1

Jakub M Swiercz et al. J Biol Chem. .
Free article

Abstract

Sema4D-induced activation of plexin-B1 has been reported to evoke different and sometimes opposing cellular responses. The mechanisms underlying the versatility of plexin-B1-mediated effects are not clear. Plexin-B1 can associate with the receptor tyrosine kinases ErbB-2 and Met. Here we show that Sema4D-induced activation and inactivation of RhoA require ErbB-2 and Met, respectively. In breast carcinoma cells, Sema4D can have pro- and anti-migratory effects depending on the presence of ErbB-2 and Met, and the exchange of the two receptor tyrosine kinases is sufficient to convert the cellular response to Sema4D from pro- to anti-migratory and vice versa. This work identifies a novel mechanism by which plexin-mediated signaling can be regulated and explains how Sema4D can exert different biological activities through the differential association of its receptor with ErbB-2 and Met.

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