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DUSP1 recuses diabetic nephropathy via repressing JNK-Mff-mitochondrial fission pathways
Authors:Junqin Sheng  Hongyan Li  Qin Dai  Chang Lu  Min Xu  Jisheng Zhang  Jianxun Feng
Institution:1. Department of Nephrology, Xuhui District Central Hospital of Shanghai, Shanghai, China

Junqin Sheng and Hongyan Li contributed equally to this work.;2. Department of Nephrology, Huadu District People’s Hospital, Southern Medical University, Guangzhou, China

Junqin Sheng and Hongyan Li contributed equally to this work.;3. Department of Nephrology, Xuhui District Central Hospital of Shanghai, Shanghai, China

Abstract:Excessive mitochondrial fission has been identified as the pathogenesis of diabetic nephropathy (DN), although the upstream regulatory signal for mitochondrial fission activation in the setting of DN remains unknown. In the current study, we found that dual-specificity protein phosphatase-1 (DUSP1) was actually downregulated by chronic hyperglycemia stimulus. Lower DUSP1 expression was associated with glucose metabolism disorder, renal dysfunction, kidney hypertrophy, renal fibrosis, and glomerular apoptosis. At the molecular level, defective DUSP1 expression activated JNK pathway, and the latter selectively opened mitochondrial fission by modulating mitochondrial fission factor (Mff) phosphorylation. Excessive Mff-related mitochondrial fission evoked mitochondrial oxidative stress, promoted mPTP opening, exacerbated proapoptotic protein leakage into the cytoplasm, and finally initiated mitochondria-dependent cellular apoptosis in the setting of diabetes. However, overexpression of DUSP1 interrupted Mff-related mitochondrial fission, reducing hyperglycemia-mediated mitochondrial damage and thus improving renal function. Overall, we have shown that DUSP1 functions as a novel malefactor in diabetic renal damage that mediates via modifying Mff-related mitochondrial fission. Thus, finding strategies to regulate the balance of the DUSP1-JNK-Mff signaling pathway and mitochondrial homeostasis may be a therapeutic target for treating diabetic nephropathy in clinical practice.
Keywords:diabetic renal damage  DUSP1  Mff  mitochondrial fission
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