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a dual binding mode for rhogtpases in plexin signalling双绑定模式rhogtpases plexin信号
A Dual Binding Mode for RhoGTPases in Plexin Signalling
Christian H. Bell, A. Radu Aricescu, E. Yvonne Jones*, Christian Siebold*
Division of Structural Biology, Wellcome Trust Centre for Human Genetics, University of Oxford, Oxford, United Kingdom
Abstract
Plexins are cell surface receptors for the semaphorin family of cell guidance cues. The cytoplasmic region comprises a Ras
GTPase-activating protein (GAP) domain and a RhoGTPase binding domain. Concomitant binding of extracellular
semaphorin and intracellular RhoGTPase triggers GAP activity and signal transduction. The mechanism of this intricate
regulation remains elusive. We present two crystal structures of the human Plexin-B1 cytoplasmic region in complex with a
constitutively active RhoGTPase, Rac1. The structure of truncated Plexin-B1-Rac1 complex provides no mechanism for
coupling RhoGTPase and Ras binding sites. On inclusion of the juxtamembrane helix, a trimeric structure of Plexin-B1-Rac1
complexes is stabilised by a second, novel, RhoGTPase binding site adjacent to the Ras site. Site-directed mutagenesis
combined with cellular and biophysical assays demonstrate that this new binding site is essential for signalling. Our findings
are consistent with a model in which extracellular and intracellular plexin clustering events combine into a single signalling
output.
Citation: Bell CH, Aricescu AR, Jones EY, Siebold C (2011) A Dual Binding Mode for RhoGTPases in Plexin Signalling. PLoS Biol 9(8): e1001134. doi:10.1371/
journal.pbio.1001134
Academic Editor: Gregory A. Petsko, Brandeis University, United States of America
Received January 26, 2011; Accepted July 20, 2011; Published August 30, 2011
Copyright: 2011 Bell et al
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