| Literature DB >> 31243340 |
Padmashree Rao1, Min Pang1,2, Xi Qiao1,2, Hong Yu1, Hailong Wang1,2, Ying Yang1,2, Xiaojun Ren1,2, Min Hu1, Titi Chen1, Qi Cao1, Yiping Wang1, Matloob Khushi3,4, Geoff Zhang5, Yuan Min Wang5, Chow Heok P'ng6, Brian Nankivell6, Vincent W Lee1,6, Stephen I Alexander5, Guoping Zheng7, David C Harris1,6.
Abstract
Transforming growth factor β (TGF-β) is the key cytokine involved in causing fibrosis through cross-talk with major profibrotic pathways. However, inhibition of TGF-β to prevent fibrosis would also abrogate its anti-inflammatory and wound-healing effects. β-catenin is a common co-factor in most TGF-β signaling pathways. β-catenin binds to T-cell factor (TCF) to activate profibrotic genes and binds to Forkhead box O (Foxo) to promote cell survival under oxidative stress. Using a proximity ligation assay in human kidney biopsies, we found that β-catenin/Foxo interactions were higher in kidney with little fibrosis, whereas β-catenin/TCF interactions were upregulated in the kidney of patients with fibrosis. We hypothesised that β-catenin/Foxo is protective against kidney fibrosis. We found that Foxo1 protected against rhTGF-β1-induced profibrotic protein expression using a CRISPR/cas9 knockout of Foxo1 or TCF1 in murine kidney tubular epithelial C1.1 cells. Co-administration of TGF-β with a small molecule inhibitor of β-catenin/TCF (ICG-001), protected against kidney fibrosis in unilateral ureteral obstruction. Collectively, our human, animal and in vitro findings suggest β-catenin/Foxo as a therapeutic target in kidney fibrosis.Entities:
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Year: 2019 PMID: 31243340 DOI: 10.1038/s41374-019-0276-z
Source DB: PubMed Journal: Lab Invest ISSN: 0023-6837 Impact factor: 5.662