A. Aravamudhan scite author profile

A. Aravamudhan

3Publications

84Citation Statements Received

48Citation Statements Given

How they've been cited

113

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Affiliations

Winneshiek Medical Center, Brigham and Women's Hospital, Mayo Clinic

Publications

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Paracrine Wnt1 Drives Interstitial Fibrosis without Inflammation by Tubulointerstitial Cross-Talk

et al. 2016

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AKI with incomplete epithelial repair is a major contributor to CKD characterized by tubulointerstitial fibrosis. Injury-induced epithelial secretion of profibrotic factors is hypothesized to underlie this link, but the identity of these factors and whether epithelial injury is required remain undefined. We previously showed that activation of the canonical Wnt signaling pathway in interstitial pericytes cell autonomously drives myofibroblast activation in vivo. Here, we show that inhibition of canonical Wnt signaling also substantially prevented TGFbdependent myofibroblast activation in vitro. To investigate whether Wnt ligand derived from proximal tubule is sufficient for renal fibrogenesis, we generated a novel mouse strain with inducible proximal tubule Wnt1 secretion. Adult mice were treated with vehicle or tamoxifen and euthanized at 12 or 24 weeks postinjection. Compared with vehicle-treated controls, kidneys with tamoxifen-induced Wnt1 expression from proximal tubules displayed interstitial myofibroblast activation and proliferation and increased matrix protein production. PDGF receptor b-positive myofibroblasts isolated from these kidneys exhibited increased canonical Wnt target gene expression compared with controls. Notably, fibrotic kidneys had no evidence of inflammatory cytokine expression, leukocyte infiltration, or epithelial injury, despite the close histologic correlation of each with CKD. These results provide the first example of noninflammatory renal fibrosis. The fact that epithelialderived Wnt ligand is sufficient to drive interstitial fibrosis provides strong support for the maladaptive repair hypothesis in the AKI to CKD transition.

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Vascular Dysfunction in Aged Mice Contributes to Persistent Lung Fibrosis Through the Impairment of the NO/sGC/cGMP Pathway

Caporarello

Meridew

Haresi

et al. 2020

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Vascular Rarefaction and Loss of Endothelial Identity Accompanies Persistent Fibrosis in Bleomycin-injured Aged Mice

Caporarello

Aravamudhan

Meridew

et al. 2019

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A. Aravamudhan

Paracrine Wnt1 Drives Interstitial Fibrosis without Inflammation by Tubulointerstitial Cross-Talk

Vascular Dysfunction in Aged Mice Contributes to Persistent Lung Fibrosis Through the Impairment of the NO/sGC/cGMP Pathway

Vascular Rarefaction and Loss of Endothelial Identity Accompanies Persistent Fibrosis in Bleomycin-injured Aged Mice

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