Litcius/Paper detail

LPS-Induced Acute Kidney Injury Is Mediated by Nox4-SH3YL1

Jung-Yeon Yoo, Dae Ryong, Borim Kim, Eun Jung An, Sae Rom Lee, Jin Joo, Young Sun Kang, Jung Yeon Ghee, Jee‐Young Han, Yun Soo Bae

2020Cell Reports106 citationsDOIOpen Access PDF

Abstract

Cytosolic proteins are required for regulation of NADPH (nicotinamide adenine dinucleotide phosphate) oxidase (Nox) isozymes. Here we show that Src homology 3 (SH3) domain-containing YSC84-like 1 (SH3YL1), as a Nox4 cytosolic regulator, mediates lipopolysaccharide (LPS)-induced H2O2 generation, leading to acute kidney injury. The SH3YL1, Ysc84p/Lsb4p, Lsb3p, and plant FYVE proteins (SYLF) region and SH3 domain of SH3YL1 contribute to formation of a complex with Nox4-p22phox. Interaction of p22phox with SH3YL1 is triggered by LPS, and the complex induces H2O2 generation and pro-inflammatory cytokine expression in mouse tubular epithelial cells. After LPS injection, SH3YL1 knockout mice show lower levels of acute kidney injury biomarkers, decreased secretion of pro-inflammatory cytokines, decreased infiltration of macrophages, and reduced tubular damage compared with wild-type (WT) mice. The results strongly suggest that SH3YL1 is involved in renal failure in LPS-induced acute kidney injury (AKI) mice. We demonstrate that formation of a ternary complex of p22phox-SH3YL1-Nox4, leading to H2O2 generation, induces severe renal failure in the LPS-induced AKI model.

Topics & Concepts

NOX4Acute kidney injuryKidneyMedicineBiologyCell biologyInternal medicineNADPH oxidaseReactive oxygen speciesNeutrophil, Myeloperoxidase and Oxidative MechanismsAdvanced Glycation End Products researchNitric Oxide and Endothelin Effects