The concerted action of SEPT9 and EPLIN modulates the adhesion and migration of human fibroblasts

Author:

Hecht Matthias1,Alber Nane1,Marhoffer Pia1,Johnsson Nils1ORCID,Gronemeyer Thomas1ORCID

Affiliation:

1. Institute of Molecular Genetics and Cell Biology, James Franck Ring N27, Ulm University

Abstract

Septins are cytoskeletal proteins that participate in cell adhesion, migration, and polarity establishment. The septin subunit SEPT9 directly interacts with the single LIM domain of epithelial protein lost in neoplasm (EPLIN), an actin-bundling protein. Using a human SEPT9 KO fibroblast cell line, we show that cell adhesion and migration are regulated by the interplay between both proteins. The low motility of SEPT9-depleted cells could be partly rescued by increased levels of EPLIN. The normal organization of actin-related filopodia and stress fibers was directly dependent on the expression level of SEPT9 and EPLIN. Increased levels of SEPT9 and EPLIN enhanced the size of focal adhesions in cell protrusions, correlating with stabilization of actin bundles. Conversely, decreased levels had the opposite effect. Our work thus establishes the interaction between SEPT9 and EPLIN as an important link between the septin and the actin cytoskeleton, influencing cell adhesion, motility, and migration.

Publisher

Life Science Alliance, LLC

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