| Literature DB >> 32305173 |
Ruofeng Tang1, Xin Wang2, Junxiang Zhou1, Fengxia Zhang3, Shan Zhao2, Qiwen Gan1, Liyuan Zhao4, Fengyang Wang4, Qian Zhang4, Jie Zhang2, Guodong Wang3, Chonglin Yang5.
Abstract
Arginine catabolism involves enzyme-dependent reactions in both mitochondria and the cytosol, defects in which may lead to hyperargininemia, a devastating developmental disorder. It is largely unknown if defective arginine catabolism has any effects on mitochondria. Here we report that normal arginine catabolism is essential for mitochondrial homeostasis in Caenorhabditiselegans. Mutations of the arginase gene argn-1 lead to abnormal mitochondrial enlargement and reduced adenosine triphosphate (ATP) production in C. elegans hypodermal cells. ARGN-1 localizes to mitochondria and its loss causes arginine accumulation, which disrupts mitochondrial dynamics. Heterologous expression of human ARG1 or ARG2 rescued the mitochondrial defects of argn-1 mutants. Importantly, genetic inactivation of the mitochondrial basic amino acid transporter SLC-25A29 or the mitochondrial glutamate transporter SLC-25A18.1 fully suppressed the mitochondrial defects caused by argn-1 mutations. These findings suggest that mitochondrial damage probably contributes to the pathogenesis of hyperargininemia and provide clues for developing therapeutic treatments for hyperargininemia.Entities:
Keywords: Arginase; Arginine; C. elegans; Hyperargininemia; Mitochondrial homeostasis
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Year: 2020 PMID: 32305173 DOI: 10.1016/j.jgg.2020.02.007
Source DB: PubMed Journal: J Genet Genomics ISSN: 1673-8527 Impact factor: 4.275