LRP6 细胞质尾部的稳定元件在 DIX 依赖性聚合后赋予有效的信号转导。
Stability elements in the LRP6 cytoplasmic tail confer efficient signalling upon DIX-dependent polymerization.
机构信息
MRC Laboratory of Molecular Biology, Hills Road, Cambridge CB2 0QH, UK.
出版信息
J Cell Sci. 2010 May 1;123(Pt 9):1588-99. doi: 10.1242/jcs.067546. Epub 2010 Apr 13.
Wnt/beta-catenin signalling controls cell fates in development, tissue homeostasis and cancer. Wnt binding to Frizzled receptors triggers recruitment of Dishevelled to the plasma membrane and formation of a signalosome containing the LRP5/6 co-receptor, whose cytoplasmic tail (ctail) thus becomes phosphorylated at multiple PPP(S/T)Px(S/T) motifs. These then directly inhibit GSK3beta, which results in beta-catenin accumulation and signalling. Here, we revisit previous epistasis experiments, and show that Dishevelled signals through LRP5/6 in human cells and Drosophila embryos. To recapitulate this signalling event, and to define its functional elements, we fused the Dishevelled DIX domain to the LRP6 ctail, which forms cytoplasmic signalosomes with potent signalling activity mediated by its PPP(S/T)Px(S/T) motifs. Their phosphorylation and activity depends critically on DIX-mediated polymerization, and on multiple stability elements in the LRP6 ctail, including the T1479 epitope upstream of the membrane-proximal PPP(S/T)Px(S/T) motif. Thus, stable polymerization emerges as a key principle underlying the function of Dishevelled-dependent signalosomes.
Wnt/β-catenin 信号通路控制着细胞在发育、组织稳态和癌症中的命运。Wnt 与 Frizzled 受体结合,触发 Dishevelled 向质膜募集,并形成含有 LRP5/6 共受体的信号体,其细胞质尾巴(ctail)因此在多个 PPP(S/T)Px(S/T)基序处被磷酸化。这些基序随后直接抑制 GSK3β,导致β-catenin 积累和信号转导。在这里,我们重新审视了以前的遗传互补实验,并表明 Dishevelled 在人类细胞和果蝇胚胎中通过 LRP5/6 信号传递。为了重现这一信号事件,并定义其功能元件,我们将 Dishevelled 的 DIX 结构域融合到 LRP6 的 ctail 上,形成具有强大信号活性的细胞质信号体,其活性由 PPP(S/T)Px(S/T)基序介导。它们的磷酸化和活性取决于 DIX 介导的聚合,以及 LRP6 ctail 中的多个稳定性元件,包括位于膜近端 PPP(S/T)Px(S/T)基序上游的 T1479 表位。因此,稳定的聚合成为 Dishevelled 依赖性信号体功能的关键原则。
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