DBT is a metabolic switch for maintenance of proteostasis under proteasomal impairment

Author:

Hwang Ran-Der12,Lu Yu-Ning12,Tang Qing12,Periz Goran12,Park Giho12,Li Xiangning12,Xiang Qiwang12,Liu Yang12,Zhang Tao12,Wang Jiou12ORCID

Affiliation:

1. Department of Biochemistry and Molecular Biology, Bloomberg School of Public Health,

2. Department of Neuroscience, School of Medicine, Johns Hopkins University

Abstract

Proteotoxic stress impairs cellular homeostasis and underlies the pathogenesis of many neurodegenerative diseases, including amyotrophic lateral sclerosis (ALS). The proteasomal and autophagic degradation of proteins are two major pathways for protein quality control in the cell. Here, we report a genome-wide CRISPR screen uncovering a major regulator of cytotoxicity resulting from the inhibition of the proteasome. Dihydrolipoamide branched chain transacylase E2 (DBT) was found to be a robust suppressor, the loss of which protects against proteasome inhibition-associated cell death through promoting clearance of ubiquitinated proteins. Loss of DBT altered the metabolic and energetic status of the cell and resulted in activation of autophagy in an AMP-activated protein kinase (AMPK)-dependent mechanism in the presence of proteasomal inhibition. Loss of DBT protected against proteotoxicity induced by ALS-linked mutant TDP-43 in Drosophila and mammalian neurons. DBT is upregulated in the tissues from ALS patients. These results demonstrate that DBT is a master switch in the metabolic control of protein quality control with implications in neurodegenerative diseases.

Publisher

eLife Sciences Publications, Ltd

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