RhoU forms homo-oligomers to regulate cellular responses

Author:

Clayton Natasha S.12ORCID,Hodge Richard G.3ORCID,Infante Elvira3ORCID,Alibhai Dominic45ORCID,Zhou Felix678ORCID,Ridley Anne J.123ORCID

Affiliation:

1. University of Bristol 1 School of Cellular and Molecular Medicine , , Biomedical Sciences Building , , Bristol BS8 1TD , UK

2. University Walk 1 School of Cellular and Molecular Medicine , , Biomedical Sciences Building , , Bristol BS8 1TD , UK

3. Randall Centre for Cell and Molecular Biophysics, King's College London 2 , Guy's Campus, London SE1 1UL , UK

4. Wolfson Bioimaging Facility, University of Bristol 3 , Biomedical Sciences Building , , Bristol BS8 1TD , UK

5. University Walk 3 , Biomedical Sciences Building , , Bristol BS8 1TD , UK

6. Ludwig Institute for Cancer Research 4 , Nuffield Department of Clinical Medicine , , Oxford OX3 7DQ , UK

7. University of Oxford 4 , Nuffield Department of Clinical Medicine , , Oxford OX3 7DQ , UK

8. University of Texas Southwestern Medical Center 5 Lyda Hill Department of Bioinformatics , , Dallas, TX 75390 , USA

Abstract

ABSTRACT RhoU is an atypical member of the Rho family of small G-proteins, which has N- and C-terminal extensions compared to the classic Rho GTPases RhoA, Rac1 and Cdc42, and associates with membranes through C-terminal palmitoylation rather than prenylation. RhoU mRNA expression is upregulated in prostate cancer and is considered a marker for disease progression. Here, we show that RhoU overexpression in prostate cancer cells increases cell migration and invasion. To identify RhoU targets that contribute to its function, we found that RhoU homodimerizes in cells. We map the region involved in this interaction to the C-terminal extension and show that C-terminal palmitoylation is required for self-association. Expression of the isolated C-terminal extension reduces RhoU-induced activation of p21-activated kinases (PAKs), which are known downstream targets for RhoU, and induces cell morphological changes consistent with inhibiting RhoU function. Our results show for the first time that the activity of a Rho family member is stimulated by self-association, and this is important for its activity.

Funder

Cancer Research UK

University of Bristol Cancer Research Fund

University of Bristol

King's Bioscience Institute

Guy's and St Thomas’ Charity

National Institute for Health Research

King's College London

King's College Hospital NHS Foundation Trust

Publisher

The Company of Biologists

Subject

Cell Biology

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