Mmp14-dependent remodeling of the pericellular–dermal collagen interface governs fibroblast survival

Author:

Sabeh Farideh1ORCID,Li Xiao-Yan1ORCID,Olson Adam W.1ORCID,Botvinick Elliot2ORCID,Kurup Abhishek2ORCID,Gimenez Luis E.3ORCID,Cho Jung-Sun1ORCID,Weiss Stephen J.1ORCID

Affiliation:

1. Life Sciences Institute, University of Michigan 1 Division of Genetic Medicine, Department of Internal Medicine, , Ann Arbor, MI, USA

2. The Henry Samueli School of Engineering, University of California 2 , Irvine, CA, USA

3. Life Sciences Institute, University of Michigan 3 , Ann Arbor, MI, USA

Abstract

Dermal fibroblasts deposit type I collagen, the dominant extracellular matrix molecule found in skin, during early postnatal development. Coincident with this biosynthetic program, fibroblasts proteolytically remodel pericellular collagen fibrils by mobilizing the membrane-anchored matrix metalloproteinase, Mmp14. Unexpectedly, dermal fibroblasts in Mmp14−/− mice commit to a large-scale apoptotic program that leaves skin tissues replete with dying cells. A requirement for Mmp14 in dermal fibroblast survival is recapitulated in vitro when cells are embedded within, but not cultured atop, three-dimensional hydrogels of crosslinked type I collagen. In the absence of Mmp14-dependent pericellular proteolysis, dermal fibroblasts fail to trigger β1 integrin activation and instead actuate a TGF-β1/phospho-JNK stress response that leads to apoptotic cell death in vitro as well as in vivo. Taken together, these studies identify Mmp14 as a requisite cell survival factor that maintains dermal fibroblast viability in postnatal dermal tissues.

Funder

National Institutes of Health

Breast Cancer Research Foundation

Margolies Family Discovery Fund for Cancer Research

Publisher

Rockefeller University Press

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