| Literature DB >> 32161193 |
Marina Morigi1, Luca Perico1, Daniela Corna1, Monica Locatelli1, Paola Cassis1, Claudia Elisa Carminati1, Silvia Bolognini1, Carlamaria Zoja1, Giuseppe Remuzzi1,2, Ariela Benigni1, Simona Buelli1.
Abstract
Renal activation of the complement system has been described in patients with diabetic nephropathy (DN), although its pathological relevance is still ill-defined. Here, we studied whether glomerular C3a, generated by uncontrolled complement activation, promotes podocyte damage, leading to proteinuria and renal injury in mice with type 2 diabetes. BTBR ob/ob mice exhibited podocyte loss, albuminuria, and glomerular injury accompanied by C3 deposits and increased C3a and C3a receptor (C3aR) levels. Decreased glomerular nephrin and α-actinin4 expression, coupled with integrin-linked kinase induction, were also observed. Treatment of DN mice with a C3aR antagonist enhanced podocyte density and preserved their phenotype, limiting proteinuria and glomerular injury. Mechanistically, ultrastructural and functional mitochondrial alterations, accompanied by downregulation of antioxidant superoxide dismutase 2 (SOD2) and increased protein oxidation, occurred in podocytes and were normalized by C3aR blockade. In cultured podocytes, C3a induced cAMP-dependent mitochondrial fragmentation. Alterations of mitochondrial membrane potential, SOD2 expression, and energetic metabolism were also found in response to C3a. Notably, C3a-induced podocyte motility was inhibited by SS-31, a peptide with mitochondrial protective effects. These data indicate that C3a blockade represents a potentially novel therapeutic strategy in DN for preserving podocyte integrity through the maintenance of mitochondrial functions.Entities:
Keywords: Complement; Diabetes; Mitochondria; Nephrology
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Year: 2020 PMID: 32161193 PMCID: PMC7141402 DOI: 10.1172/jci.insight.131849
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708