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XIAP 丝氨酸 180 位的磷酸化控制其在 Wnt 信号通路中的活性。

Phosphorylation of XIAP at threonine 180 controls its activity in Wnt signaling.

机构信息

Program in Cancer Biology, Vanderbilt University, Nashville, TN 37232, USA.

Department of Cell & Developmental Biology, Vanderbilt University, Nashville, TN 37232, USA.

出版信息

J Cell Sci. 2018 May 22;131(10):jcs210575. doi: 10.1242/jcs.210575.

Abstract

X-linked inhibitor of apoptosis (XIAP) plays an important role in preventing apoptotic cell death. XIAP has been shown to participate in signaling pathways, including Wnt signaling. XIAP regulates Wnt signaling by promoting the monoubiquitylation of the co-repressor Groucho/TLE family proteins, decreasing its affinity for the TCF/Lef family of transcription factors and allowing assembly of transcriptionally active β-catenin-TCF/Lef complexes. We now demonstrate that XIAP is phosphorylated by GSK3 at threonine 180, and that an alanine mutant (XIAP) exhibits decreased Wnt activity compared to wild-type XIAP in cultured human cells and in embryos. Although XIAP ubiquitylates TLE3 at wild-type levels , it exhibits a reduced capacity to ubiquitylate and bind TLE3 in human cells. XIAP binds Smac (also known as DIABLO) and inhibits Fas-induced apoptosis to a similar degree to wild-type XIAP. Our studies uncover a new mechanism by which XIAP is specifically directed towards a Wnt signaling function versus its anti-apoptotic function. These findings have implications for development of anti-XIAP therapeutics for human cancers.

摘要

X 连锁凋亡抑制蛋白(XIAP)在防止细胞凋亡方面起着重要作用。已经证明 XIAP 参与信号通路,包括 Wnt 信号通路。XIAP 通过促进共抑制物 Groucho/TLE 家族蛋白的单泛素化来调节 Wnt 信号通路,降低其与 TCF/Lef 家族转录因子的亲和力,并允许转录活性β-连环蛋白-TCF/Lef 复合物的组装。我们现在证明 XIAP 可以被 GSK3 在苏氨酸 180 处磷酸化,并且与野生型 XIAP 相比,在培养的人类细胞和 胚胎中,XIAP 的突变体(XIAP)表现出降低的 Wnt 活性。尽管 XIAP 以野生型水平泛素化 TLE3,但它在人类细胞中表现出降低的泛素化和与 TLE3 结合的能力。XIAP 与 Smac(也称为 DIABLO)结合并抑制 Fas 诱导的凋亡,与野生型 XIAP 相似。我们的研究揭示了 XIAP 被专门导向 Wnt 信号功能而不是其抗凋亡功能的新机制。这些发现对开发针对人类癌症的抗 XIAP 治疗方法具有重要意义。

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