Tissue stiffening promotes keratinocyte proliferation via activation of epidermal growth factor signaling

Author:

Kenny Fiona N.1,Drymoussi Zoe1,Delaine-Smith Robin23,Kao Alexander P.2,Laly Ana Catarina13,Knight Martin M.23,Philpott Michael P.1,Connelly John T.13ORCID

Affiliation:

1. Centre for Cell Biology and Cutaneous Research, Barts and the London School of Medicine and Dentistry, Queen Mary University of London, UK

2. School of Engineering and Materials Science, Queen Mary University of London, UK

3. Institute of Bioengineering, Queen Mary University of London, UK

Abstract

Tissue biomechanics regulate a wide range of cellular functions, but the influences on epidermal homeostasis and repair remain unclear. Here, we examined the role of extracellular matrix stiffness on human keratinocyte behavior using elastomeric substrates with defined mechanical properties. Increased matrix stiffness beyond normal physiologic levels promoted keratinocyte proliferation but did not alter the ability to self-renew or terminally differentiate. Activation of epidermal growth factor (EGF) signaling mediated the proliferative response to matrix stiffness and depended on focal adhesion assembly and cytoskeletal tension. Comparison of normal skin with keloid scar tissue further revealed an up-regulation of EGF signaling within the epidermis of stiffened scar tissue. We conclude that matrix stiffness regulates keratinocyte proliferation independently of changes in cell fate and is mediated by EGF signaling. These findings provide mechanistic insights into how keratinocytes sense and respond to their mechanical environment and suggest that matrix biomechanics may play a role in the pathogenesis keloid scar formation.

Funder

British Skin Foundation

European Research Council

Publisher

The Company of Biologists

Subject

Cell Biology

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