| Literature DB >> 31825843 |
Jiagui Song1, Tianzhuo Wang1, Xiaochun Chi1, Xiaofan Wei1, Sidi Xu1, Miao Yu1, Huiying He2, Ji Ma1, Xueying Li1, Juan Du1, Xiaoran Sun1, Yunling Wang3, Jun Zhan4, Hongquan Zhang5.
Abstract
The Hippo signaling pathway plays a key role in development and cancer progression. However, molecules that intrinsically inhibit this pathway are less well known. Here, we report that the focal adhesion molecule Kindlin-2 inhibits Hippo signaling by interacting with and degrading MOB1 and promoting the interaction between MOB1 and the E3 ligase praja2. Kindlin-2 thus inhibits the phosphorylation of LATS1 and YAP and promotes YAP translocation into the nucleus, where it activates downstream Hippo target gene transcription. Kindlin-2 depletion activates Hippo/YAP signaling and alleviates renal fibrosis in Kindlin-2 knockout mice with unilateral ureteral occlusion (UUO). Moreover, Kindlin-2 levels are negatively correlated with MOB1 and phosphorylated (p) YAP in samples from patients with renal fibrosis. Altogether, these results demonstrate that Kindlin-2 inhibits Hippo signaling through degradation of MOB1. A specific long-lasting siRNA against Kindlin-2 effectively alleviated UUO-induced renal fibrosis and could be a potential therapy for renal fibrosis.Entities:
Keywords: Hippo signaling; Kindlin-2; MOB1; YAP; praja2; renal fibrosis; siRNA; unilateral ureteral occlusion
Year: 2019 PMID: 31825843 DOI: 10.1016/j.celrep.2019.11.035
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423