USP13 Deficiency Impairs Autophagy and Facilitates Age-related Lung Fibrosis

Idiopathic pulmonary fibrosis (IPF) is an age-related disease. Failure of the proteostasis network with age, including insufficient autophagy, contributes to the pathology of IPF. Mechanisms underlying autophagy disruption in IPF are unclear and may involve regulation of USP (ubiquitin-specific protease) by post-translational modifications. To expand our previous observation of low USP13 expression in IPF, this study evaluated the role of USP13 in age-related lung fibrosis. Here, we demonstrated that Usp13-deficient aged mice exhibited impaired autophagic activity and increased vulnerability to bleomycin-induced fibrosis. Mechanistically, USP13 interacted with and deubiquitinated Beclin 1, and Beclin 1 overexpression abolished the effects of USP13 disruption. In addition, Beclin 1 inhibition resulted in insufficient autophagy and more severe lung fibrosis after bleomycin injury, consistent with the phenotype of aged Usp13-deficient mice. Collectively, we show a protective role of USP13 in age-related pulmonary fibrosis. Aging-mediated USP13 loss impairs autophagic activity and facilitates lung fibrosis through Beclin 1 deubiquitination. Our findings support the notion that age-dependent dysregulation of autophagic regulators enhances vulnerability to lung fibrosis.

Correspondence and requests for reprints should be addressed to Chen Wang, Ph.D., No.9 Dongdan 3rd Alley, Dongcheng District, Beijing 100730, China. E-mail:
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*These authors contributed equally to this study.

Supported by National Natural Science Foundation of China grants 81800067 and 81870056.

Author Contributions: All authors participated in study design, interpretation of the studies, analysis of the data, and review of the manuscript. Y.L. designed and performed the experiments, analyzed and interpreted the data, and drafted the manuscript. Z.L., H.X., B.X., J.H., and M.S. participated in the experiments and analyzed data. J.W., J.G., H.D., and C.W. contributed to the revision of the article. J.G., H.D., and C.W. commented on the manuscript and supervised all aspects of the project and contributed equally to this study.

Data sharing statement: The data for this study will be made available by contacting authors J.G. or H.D. or C.W. upon reasonable request.

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Originally Published in Press as DOI: 10.1165/rcmb.2022-0002OC on September 23, 2022

Author disclosures are available with the text of this article at www.atsjournals.org.

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