AUTHOR=Liang Xiujie , Potenza Duilio Michele , Brenna Andrea , Ma Yiqiong , Ren Zhilong , Cheng Xin , Ming Xiu-Fen , Yang Zhihong 

TITLE=Hypoxia Induces Renal Epithelial Injury and Activates Fibrotic Signaling Through Up-Regulation of Arginase-II

JOURNAL=Frontiers in Physiology

VOLUME=12

YEAR=2021

URL=https://www.frontiersin.org/journals/physiology/articles/10.3389/fphys.2021.773719

DOI=10.3389/fphys.2021.773719

ISSN=1664-042X

ABSTRACT=<p>The ureohydrolase, type-II arginase (Arg-II), is a mitochondrial enzyme metabolizing L-arginine into urea and L-ornithine and is highly expressed in renal proximal tubular cells (PTC) and upregulated by renal ischemia. Recent studies reported contradictory results on the role of Arg-II in renal injury. The aim of our study is to investigate the function of Arg-II in renal epithelial cell damage under hypoxic conditions. Human renal epithelial cell line HK2 was cultured under hypoxic conditions for 12–48 h. Moreover, <italic>ex vivo</italic> experiments with isolated kidneys from wild-type (WT) and genetic Arg-II deficient mice (<italic>Arg-II<sup>–/–</sup></italic>) were conducted under normoxic and hypoxic conditions. The results show that hypoxia upregulates Arg-II expression in HK2 cells, which is inhibited by silencing both hypoxia-inducible factors (HIFs) HIF1α and HIF2α. Treatment of the cells with dimethyloxaloylglycine (DMOG) to stabilize HIFα also enhances Arg-II. Interestingly, hypoxia or DMOG upregulates transforming growth factor β1 (TGFβ1) levels and <italic>collagens I</italic>α<italic>1</italic>, which is prevented by <italic>Arg-II</italic> silencing, while TGFβ1-induced <italic>collagen I</italic>α<italic>1</italic> expression is not affected by <italic>Arg-II</italic> silencing. Inhibition of mitochondrial complex-I by rotenone abolishes hypoxia-induced reactive oxygen species (mtROS) and TGFβ1 elevation in the cells. <italic>Ex vivo</italic> experiments show elevated Arg-II and TGFβ1 expression and the injury marker NGAL in the WT mouse kidneys under hypoxic conditions, which is prevented in the <italic>Arg-II<sup>–/–</sup></italic> mice. Taking together, the results demonstrate that hypoxia activates renal epithelial HIFs-Arg-II-mtROS-TGFβ1-cascade, participating in hypoxia-associated renal injury and fibrosis.</p>