Urinary semaphorin 3A correlates with diabetic proteinuria and mediates diabetic nephropathy and associated inflammation in mice
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- 作者:Riyaz Mohamed (1)
Punithavathi Ranganathan (1)
Calpurnia Jayakumar (1)
Ferdau L. Nauta (2)
Ron T. Gansevoort (2)
Neal L. Weintraub (1)
Michael Brands (3)
Ganesan Ramesh (1) - 关键词:Biomarker ; Sema3A ; Diabetic nephropathy ; Albuminuria
- 刊名:Journal of Molecular Medicine
- 出版年:2014
- 出版时间:December 2014
- 年:2014
- 卷:92
- 期:12
- 页码:1245-1256
- 全文大小:3,372 KB
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Michael Brands (3)
Ganesan Ramesh (1)
1. Department of Medicine, Vascular Biology Center, Georgia Regents University, CB-3702, 1459 Laney-Walker Blvd, Augusta, GA, 30912, USA
2. Department of Nephrology, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands
3. Department of Physiology, Georgia Regents University, Augusta, GA, 30912, USA - ISSN:1432-1440
文摘
Semaphorin 3A (sema3A) was recently identified as an early diagnostic biomarker of acute kidney injury. However, its role as a biomarker and/or mediator of chronic kidney disease (CKD) related to diabetic nephropathy is unknown. We examined the expression of sema3A in diabetic animal models and in humans and tested whether sema3A plays a pathogenic role in the development of diabetic nephropathy. The expression of sema3A was localized to podocytes and epithelial cells in distal tubules and collecting ducts in control animals, and its expression was increased following the induction of diabetes. Quantification of sema3A urinary excretion in three different diabetic mouse models showed that excretion was increased as early as 2?weeks after the induction of diabetes and increased over time, in conjunction with the development of nephropathy. Consistent with the mouse data, increased sema3A urinary excretion was detected in diabetic patients with albuminuria, particularly in those with macroalbuminuria. Genetic ablation of sema3A or pharmacological inhibition with a novel sema3A inhibitory peptide was protected against diabetes-induced albuminuria, kidney fibrosis, inflammation, oxidative stress, and renal dysfunction. We conclude that sema3A is both a biomarker and a mediator of diabetic kidney disease and could be a promising therapeutic target in diabetic nephropathy. Key messages Diabetes induced sema3A excretion in urine. Increased semaphorin 3A was associated with severity of albuminuria. Seme3A-mediated diabetes induced glomerulosclerosis. Peptide-based inhibition of semaphorin3A suppressed diabetic nephropathy.