利钠肽清除受体缺失可减轻 TGF-β1 诱导的选择性心房纤维化和心房颤动。
Absence of natriuretic peptide clearance receptor attenuates TGF-β1-induced selective atrial fibrosis and atrial fibrillation.
机构信息
Division of Cardiology, Cardiovascular Research Institute, University of California, San Francisco, 505 Parnassus Avenue, M1182, Box 0124, San Francisco, CA, USA.
出版信息
Cardiovasc Res. 2019 Feb 1;115(2):357-372. doi: 10.1093/cvr/cvy224.
AIMS
TGF-β1 plays an important role in atrial fibrosis and atrial fibrillation (AF); previous studies have shown that the atria are more susceptible to TGF-β1 mediated fibrosis than the ventricles. Natriuretic peptides (NPs) play an important role in cardiac remodelling and fibrosis, but the role of natriuretic peptide clearance (NPR-C) receptor is largely unknown. We investigated the role of NPR-C in modulating TGF-β1 signalling in the atria.
METHODS AND RESULTS
MHC-TGF-β1 transgenic (TGF-β1-Tx) mice, which develop isolated atrial fibrosis and AF, were cross-bred with NPR-C knock-out mice (NPR-C-KO). Transverse aortic constriction (TAC) was performed in wild type (Wt) and NPR-C knockout mice to study. Atrial fibrosis and AF inducibility in a pathophysiologic model. Electrophysiology, molecular, and histologic studies were performed in adult mice. siRNA was used to interrogate the interaction between TGF-β1 and NP signalling pathways in isolated atrial and ventricular fibroblasts/myofibroblasts. NPR-C expression level was 17 ± 5.8-fold higher in the atria compared with the ventricle in Wt mice (P = 0.009). Cross-bred mice demonstrated markedly decreased pSmad2 and collagen expression, atrial fibrosis, and AF compared with TGF-β1-Tx mice with intact NPR-C. There was a marked reduction in atrial fibrosis gene expression and AF inducibility in the NPR-C-KO-TAC mice compared with Wt-TAC. In isolated fibroblasts, knockdown of NPR-C resulted in a marked reduction of pSmad2 (56 ± 4% and 24 ± 14% reduction in atrial and ventricular fibroblasts, respectively) and collagen (76 ± 15% and 35 ± 23% reduction in atrial and ventricular fibroblasts/myofibroblasts, respectively) in response to TGF-β1 stimulation. This effect was reversed by simultaneously knocking down NPR-A but not with simultaneous knock down of PKG-1.
CONCLUSION
The differential response to TGF-β1 stimulated fibrosis between the atria and ventricle are in part mediated by the abundance of NPR-C receptors in the atria.
目的
TGF-β1 在心房纤维化和心房颤动(AF)中起重要作用;先前的研究表明,与心室相比,心房更容易受到 TGF-β1 介导的纤维化影响。利钠肽(NPs)在心腔重塑和纤维化中起重要作用,但 NPR-C 受体的作用在很大程度上尚不清楚。我们研究了 NPR-C 在调节心房中 TGF-β1 信号转导中的作用。
方法和结果
MHC-TGF-β1 转基因(TGF-β1-Tx)小鼠会发展为孤立性心房纤维化和 AF,这些小鼠与 NPR-C 敲除(NPR-C-KO)小鼠进行杂交。在野生型(Wt)和 NPR-C 敲除小鼠中进行了横主动脉缩窄(TAC)以研究在病理生理模型中的心房纤维化和 AF 易感性。在成年小鼠中进行了电生理学、分子和组织学研究。使用 siRNA 来研究 TGF-β1 与 NP 信号通路之间的相互作用在分离的心房和心室成纤维细胞/肌成纤维细胞中。在 Wt 小鼠中,NPR-C 在心房中的表达水平比心室高 17±5.8 倍(P=0.009)。与具有完整 NPR-C 的 TGF-β1-Tx 小鼠相比,杂交小鼠的 pSmad2 和胶原表达、心房纤维化和 AF 明显降低。与 Wt-TAC 相比,NPR-C-KO-TAC 小鼠的心房纤维化基因表达和 AF 易感性明显降低。在分离的成纤维细胞中,NPR-C 的敲低导致 pSmad2 的明显减少(心房和心室成纤维细胞分别减少 56±4%和 24±14%)和胶原的明显减少(心房和心室成纤维细胞/肌成纤维细胞分别减少 76±15%和 35±23%)对 TGF-β1 刺激的反应。同时敲低 NPR-A 可逆转这种作用,但同时敲低 PKG-1 则不行。
结论
心房和心室对 TGF-β1 刺激的纤维化反应不同部分是由心房中 NPR-C 受体的丰度介导的。
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