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The role of Kalirin9 in p75/nogo receptor-mediated RhoA activation in cerebellar granule neurons.


ABSTRACT: p75 and the Nogo receptor form a signaling unit for myelin inhibitory molecules, with p75 being responsible for RhoA activation. Because p75 lacks the GDP/GTP exchange factor domain, it has remained unclear how p75 activates RhoA. Here, we report that Kalirin9, a dual RhoGEF, binds p75 directly and regulates p75-Nogo receptor-dependent RhoA activation and neurite inhibition in response to myelin-associated glycoprotein. The region of p75 that Kalirin9 binds includes its mastoparan-like fifth helix, which was shown to recruit RhoGDI-RhoA. As predicted from the presence of a shared binding site, we found that Kalirin9 competes with RhoGDI for p75 binding in a dose-dependent manner in vitro. In line with these data, myelin-associated glycoprotein addition to cerebellar granule neurons resulted in a reduction in the association of Kalirin9 with p75, and a simultaneous increase in the binding of RhoGDI to p75. These results reveal a mechanism by which the fifth helix of p75 regulates RhoA activation.

SUBMITTER: Harrington AW 

PROVIDER: S-EPMC2529002 | biostudies-literature | 2008 Sep

REPOSITORIES: biostudies-literature

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The role of Kalirin9 in p75/nogo receptor-mediated RhoA activation in cerebellar granule neurons.

Harrington Anthony W AW   Li Qi Ming QM   Tep Chhavy C   Park Jong Bae JB   He Zhigang Z   Yoon Sung Ok SO  

The Journal of biological chemistry 20080714 36


p75 and the Nogo receptor form a signaling unit for myelin inhibitory molecules, with p75 being responsible for RhoA activation. Because p75 lacks the GDP/GTP exchange factor domain, it has remained unclear how p75 activates RhoA. Here, we report that Kalirin9, a dual RhoGEF, binds p75 directly and regulates p75-Nogo receptor-dependent RhoA activation and neurite inhibition in response to myelin-associated glycoprotein. The region of p75 that Kalirin9 binds includes its mastoparan-like fifth hel  ...[more]

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