AI Article Synopsis

  • The study highlights a new role for RhoGDI1, traditionally seen as a passive regulator of Rho proteins, showing it acts as a chaperone to prevent degradation of Rho GTPases.
  • It reveals that limited RhoGDI1 creates a balance that can influence the levels and activities of different Rho proteins, emphasizing interconnected regulation among them.
  • The findings suggest a need to rethink previous research on Rho proteins, particularly how manipulating Rho levels might impact other Rho proteins and possibly extend to other GTPases within the Ras superfamily.

Article Abstract

Regulation of the Rho switch has been typically centered on their main regulators, RhoGEFs and RhoGAPs. On the side, RhoGDI proteins have been considered mostly as passive regulators devoid of catalytic activity simply holding Rho proteins in the cytosol. In the May issue of Nature Cell Biology,1 we describe a novel evolutionary conserved function for RhoGDI1 as a chaperoning protein which prevents degradation of prenylated Rho GTPases. The limited amount of RhoGDI1 in cells generates a competitive balance between GTPases in order to prevent their degradation. Therefore, this creates a crosstalk regulatory mechanism of Rho proteins, whereby the level of one Rho protein can affect both the level and activity of the others. For example, overexpression of a single GTPase will promote the degradation and inactivation of all endogenous Rho proteins bound to GDI. These results suggest that some of the conclusions drawn from studies that manipulate Rho protein levels may need to be reevaluated. Here, we discuss some of the consequences of this mechanism on the regulation of Rho proteins, the dissociation of Rho-RhoGDI complexes by GDF and whether this regulation might be extended to other GTPases of the Ras superfamily.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3109479PMC
http://dx.doi.org/10.4161/sgtp.1.1.12990DOI Listing

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