Scribble/YAP/β-catenin 轴的失调在 PKHD1 先天性肝纤维化小鼠模型中维持着纤维炎症反应。
Dysregulation of the Scribble/YAP/β-catenin axis sustains the fibroinflammatory response in a PKHD1 mouse model of congenital hepatic fibrosis.
机构信息
Department of Molecular Medicine (DMM), University of Padova, Padova, Italy.
International Center for Digestive Health (ICDH), University of Milan-Bicocca, Milan, Italy.
出版信息
FASEB J. 2022 Jun;36(6):e22364. doi: 10.1096/fj.202101924R.
Congenital hepatic fibrosis (CHF), a genetic cholangiopathy characterized by fibropolycystic changes in the biliary tree, is caused by mutations in the PKHD1 gene, leading to defective fibrocystin (FPC), changes in planar cell polarity (PCP) and increased β-catenin-dependent chemokine secretion. In this study, we aimed at understanding the role of Scribble (a protein involved in PCP), Yes-associated protein (YAP), and β-catenin in the regulation of the fibroinflammatory phenotype of FPC-defective cholangiocytes. Immunohistochemistry showed that compared with wild type (WT) mice, in FPC-defective (Pkhd1 ) mice nuclear expression of YAP/TAZ in cystic cholangiocytes, significantly increased and correlated with connective tissue growth factor (CTGF) expression and pericystic fibrosis, while Scribble expression on biliary cyst cells was markedly decreased. Cholangiocytes isolated from WT mice showed intense Scribble immunoreactivity at the membrane, but minimal nuclear expression of YAP, which conversely increased, together with CTGF, after small interfering RNA (siRNA) silencing of Scribble. In FPC-defective cholangiocytes, inhibition of YAP nuclear import reduced β-catenin nuclear expression, and CTGF, integrin β6, CXCL1, and CXCL10 mRNA levels, whereas inhibition of β-catenin signaling did not affect nuclear translocation of YAP. Notably, siRNA silencing of Scribble and YAP in WT cholangiocytes mimics the fibroinflammatory changes of FPC-defective cholangiocytes. Conditional deletion of β-catenin in Pkhd1 mice reduced cyst growth, inflammation and fibrosis, without affecting YAP nuclear expression. In conclusion, the defective anchor of Scribble to the membrane facilitates the nuclear translocation of YAP and β-catenin with gain of a fibroinflammatory phenotype. The Scribble/YAP/β-catenin axis is a critical factor in the sequence of events linking the genetic defect to fibrocystic trait of cholangiocytes in CHF.
先天性肝纤维化 (CHF) 是一种遗传性胆管病,其特征为胆管的纤维多囊性改变,由 PKHD1 基因突变引起,导致纤维囊性蛋白 (FPC) 缺陷、平面细胞极性 (PCP) 改变和β-连环蛋白依赖性趋化因子分泌增加。在这项研究中,我们旨在了解 Scribble(参与 PCP 的一种蛋白)、Yes 相关蛋白 (YAP) 和β-连环蛋白在调节 FPC 缺陷胆管细胞的纤维炎症表型中的作用。免疫组织化学显示,与野生型 (WT) 小鼠相比,在 FPC 缺陷型 (Pkhd1) 小鼠的囊性胆管细胞中,YAP/TAZ 的核表达显著增加,并与结缔组织生长因子 (CTGF) 表达和囊周纤维化相关,而胆管囊泡细胞的 Scribble 表达明显减少。从 WT 小鼠分离的胆管细胞在膜上显示出强烈的 Scribble 免疫反应,但 YAP 的核表达很少,在用小干扰 RNA (siRNA) 沉默 Scribble 后,YAP 则与 CTGF 一起增加。在 FPC 缺陷的胆管细胞中,抑制 YAP 核内易位可降低β-连环蛋白核内表达以及 CTGF、整合素 β6、CXCL1 和 CXCL10 mRNA 水平,而抑制β-连环蛋白信号传导不会影响 YAP 的核内易位。值得注意的是,在 WT 胆管细胞中沉默 Scribble 和 YAP 可模拟 FPC 缺陷的胆管细胞的纤维炎症变化。在 Pkhd1 小鼠中条件性敲除β-连环蛋白可减少囊肿生长、炎症和纤维化,而不影响 YAP 的核内表达。总之,Scribble 膜锚定的缺陷促进了 YAP 和β-连环蛋白的核内易位,导致纤维炎症表型。Scribble/YAP/β-连环蛋白轴是将遗传缺陷与 CHF 胆管纤维囊性特征联系起来的关键因素。
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