A metazoan-specific C-terminal motif in EXC-4 and Gα-Rho/Rac signaling regulate cell outgrowth during tubulogenesis in C. elegans

Author:

Arena Anthony F.12,Escudero Julianna1ORCID,Shaye Daniel D.13ORCID

Affiliation:

1. University of Illinois at Chicago - College of Medicine 1 Department of Physiology and Biophysics , , Chicago, IL 60612, USA

2. University of Illinois at Chicago - College of Medicine 2 Graduate Education in Biomedical Sciences program , , Chicago, IL 60612, USA

3. University of Illinois at Chicago - College of Medicine 3 Center for Cardiovascular Research , , Chicago, IL 60612, USA

Abstract

ABSTRACT Chloride intracellular channels (CLICs) are conserved proteins for which the cellular and molecular functions remain mysterious. An important insight into CLIC function came from the discovery that Caenorhabditis elegans EXC-4/CLIC regulates morphogenesis of the excretory canal (ExCa) cell, a single-cell tube. Subsequent work showed that mammalian CLICs regulate vascular development and angiogenesis, and human CLIC1 can rescue exc-4 mutants, suggesting conserved function in biological tube formation (tubulogenesis) and maintenance. However, the cell behaviors and signaling pathways regulated by EXC-4/CLICs during tubulogenesis in vivo remain largely unknown. We report a new exc-4 mutation, affecting a C-terminal residue conserved in virtually all metazoan CLICs, that reveals a specific role for EXC-4 in ExCa outgrowth. Cell culture studies suggest a function for CLICs in heterotrimeric G protein (Gα/β/γ)-Rho/Rac signaling, and Rho-family GTPases are common regulators of cell outgrowth. Using our new exc-4 mutant, we describe a previously unknown function for Gα-encoding genes (gpa-12/Gα12/13, gpa-7/Gαi, egl-30/Gαq and gsa-1/Gαs), ced-10/Rac and mig-2/RhoG in EXC-4-mediated ExCa outgrowth. Our results demonstrate that EXC-4/CLICs are primordial players in Gα-Rho/Rac-signaling, a pathway that is crucial for tubulogenesis in C. elegans and in vascular development.

Funder

National Science Foundation

National Heart, Lung, and Blood Institute

National Institute of General Medical Sciences

Howard Hughes Medical Institute

Columbia University

United States Department of Education

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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