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USP18 is an essential regulator of muscle cell differentiation and maturation

Medicine and Health

USP18 is an essential regulator of muscle cell differentiation and maturation

C. S. Olie, A. Pinto-fernández, et al.

This groundbreaking study by Cyriel Sebastiaan Olie and colleagues uncovers the pivotal role of ubiquitin-specific protease 18 (USP18) in muscle cell differentiation. It reveals how USP18 influences both the initiation and maintenance of muscle cell formation, independent of its immune response role. Delve into the intricate relationship between gene expression and muscle physiology, as this research opens new avenues for understanding muscle pathologies.

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~3 min • Beginner • English
Abstract
The ubiquitin proteasomal system is a critical regulator of muscle physiology, and impaired UPS is key in many muscle pathologies. Yet, little is known about the function of deubiquitinating enzymes (DUBs) in the muscle cell context. We performed a genetic screen to identify DUBs as potential regulators of muscle cell differentiation. Surprisingly, we observed that the depletion of ubiquitin-specific protease 18 (USP18) affected the differentiation of muscle cells. USP18 depletion first stimulated differentiation initiation. Later, during differentiation, the absence of USP18 expression abrogated myotube maintenance. USP18 enzymatic function typically attenuates the immune response by removing interferon-stimulated gene 15 (ISG15) from protein substrates. However, in muscle cells, we found that USP18, predominantly nuclear, regulates differentiation independent of ISG15 and the ISG response. Exploring the pattern of RNA expression profiles and protein networks whose levels depend on USP18 expression, we found that differentiation initiation was concomitant with reduced expression of the cell-cycle gene network and altered expression of myogenic transcription (co) factors. We show that USP18 depletion altered the calcium channel gene network, resulting in reduced calcium flux in myotubes. Additionally, we show that reduced expression of sarcomeric proteins in the USP18 proteome was consistent with reduced contractile force in an engineered muscle model. Our results revealed nuclear USP18 as a critical regulator of differentiation initiation and maintenance, independent of ISG15 and its role in the ISG response.
Publisher
Cell Death and Disease
Published On
Mar 31, 2023
Authors
Cyriel Sebastiaan Olie, Adán Pinto-Fernández, Andreas Damianou, Iolanda Vendrell, Hailiang Mei, Bianca den Hamer, Erik van der Wal, Jessica C. de Greef, Vered Raz, Benedikt M. Kessler
Tags
ubiquitin proteasomal system
deubiquitinating enzymes
muscle cell differentiation
USP18
myotube maintenance
gene expression
calcium flux
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