Rho protein GTPases and their interactions with NFκB: crossroads of inflammation and matrix biology

Author:

Tong Louis1234,Tergaonkar Vinay5

Affiliation:

1. Singapore National Eye Center, 11 Third Hospital Avenue, Singapore 168751

2. Singapore Eye Research Institute, Singapore

3. Duke-NUS Graduate Medical School, Singapore

4. Yong Loo Lin School of Medicine, National University of Singapore, Singapore

5. Institute of Molecular and Cell Biology, A*Star Institute in Singapore, Singapore

Abstract

The RhoGTPases, with RhoA, Cdc42 and Rac being major members, are a group of key ubiquitous proteins present in all eukaryotic organisms that subserve such important functions as cell migration, adhesion and differentiation. The NFκB (nuclear factor κB) is a family of constitutive and inducible transcription factors that through their diverse target genes, play a major role in processes such as cytokine expression, stress regulation, cell division and transformation. Research over the past decade has uncovered new molecular links between the RhoGTPases and the NFκB pathway, with the RhoGTPases playing a positive or negative regulatory role on NFκB activation depending on the context. The RhoA–NFκB interaction has been shown to be important in cytokine-activated NFκB processes, such as those induced by TNFα (tumour necrosis factor α). On the other hand, Rac is important for activating the NFκB response downstream of integrin activation, such as after phagocytosis. Specific residues of Rac1 are important for triggering NFκB activation, and mutations do obliterate this response. Other upstream triggers of the RhoGTPase–NFκB interactions include the suppressive p120 catenin, with implications for skin inflammation. The networks described here are not only important areas for further research, but are also significant for discovery of targets for translational medicine.

Publisher

Portland Press Ltd.

Subject

Cell Biology,Molecular Biology,Biochemistry,Biophysics

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