The p38α/β MAPK functions as a molecular switch to activate the quiescent satellite cell

Author:

Jones Nathan C.1,Tyner Kristina J.2,Nibarger Lisa2,Stanley Heather M.2,Cornelison Dawn D.W.2,Fedorov Yuri V.3,Olwin Bradley B.2

Affiliation:

1. Bayer Corporation, Research Triangle Park, NC 27709

2. Department of Molecular, Cellular, and Developmental Biology, University of Colorado at Boulder, Boulder, CO 80309

3. Dharmacon Research, Lafayette, CO 80026

Abstract

Somatic stem cells cycle slowly or remain quiescent until required for tissue repair and maintenance. Upon muscle injury, stem cells that lie between the muscle fiber and basal lamina (satellite cells) are activated, proliferate, and eventually differentiate to repair the damaged muscle. Satellite cells in healthy muscle are quiescent, do not express MyoD family transcription factors or cell cycle regulatory genes and are insulated from the surrounding environment. Here, we report that the p38α/β family of mitogen-activated protein kinases (MAPKs) reversibly regulates the quiescent state of the skeletal muscle satellite cell. Inhibition of p38α/β MAPKs (a) promotes exit from the cell cycle, (b) prevents differentiation, and (c) insulates the cell from most external stimuli allowing the satellite cell to maintain a quiescent state. Activation of satellite cells and p38α/β MAPKs occurs concomitantly, providing further support that these MAPKs function as a molecular switch for satellite cell activation.

Publisher

Rockefeller University Press

Subject

Cell Biology

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