Single-cell transcriptomics reveals a mechanosensitive injury signaling pathway in early diabetic nephropathy

Author:

Liu ShuyaORCID,Zhao YuORCID,Lu ShunORCID,Zhang Tianran,Lindenmeyer Maja T.,Nair Viji,Gies Sydney E.,Wu Guochao,Nelson Robert G.,Czogalla Jan,Aypek Hande,Zielinski Stephanie,Liao Zhouning,Schaper Melanie,Fermin Damian,Cohen Clemens D.,Delic Denis,Krebs Christian F.,Grahammer Florian,Wiech Thorsten,Kretzler Matthias,Meyer-Schwesinger Catherine,Bonn Stefan,Huber Tobias B.

Abstract

AbstractDiabetic nephropathy (DN) is the leading cause of end-stage renal disease and histopathologic glomerular lesions are among the earliest structural alterations of DN. However, the signaling pathways that initiate these glomerular alterations are incompletely understood. To delineate the cellular and molecular basis for DN initiation, we performed single-cell and bulk RNA sequencing of renal cells from type 2 diabetes mice (BTBRob/ob) at the early stage of DN. Analysis of differentially expressed genes revealed glucose-independent responses in glomerular cell types. The gene regulatory network upstream of glomerular cell programs suggested the activation of mechanosensitive transcriptional pathway MRTF-SRF predominantly taking place in mesangial cells. Importantly, activation of MRTF-SRF transcriptional pathway was also identified in DN glomeruli in independent patient cohort datasets. Furthermore, ex vivo kidney perfusion suggested that the regulation of MRTF-SRF is a common mechanism in response to glomerular hyperfiltration. Overall, our study presents a comprehensive single-cell transcriptomic landscape of early DN, highlighting mechanosensitive signaling pathways as novel targets of diabetic glomerulopathy.

Publisher

Cold Spring Harbor Laboratory

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