Wnt 信号抑制的结构基础:Dickkopf 通过与 LRP5/6 结合。
Structural basis of Wnt signaling inhibition by Dickkopf binding to LRP5/6.
机构信息
Department of Structural Biology, Stanford University School of Medicine, Stanford, CA 94305, USA.
出版信息
Dev Cell. 2011 Nov 15;21(5):862-73. doi: 10.1016/j.devcel.2011.09.003. Epub 2011 Oct 13.
Abstract
LDL receptor-related proteins 5 and 6 (LRP5/6) are coreceptors for Wnt growth factors, and also bind Dkk proteins, secreted inhibitors of Wnt signaling. The LRP5/6 ectodomain contains four β-propeller/EGF-like domain repeats. The first two repeats, LRP6(1-2), bind to several Wnt variants, whereas LRP6(3-4) binds other Wnts. We present the crystal structure of the Dkk1 C-terminal domain bound to LRP6(3-4), and show that the Dkk1 N-terminal domain binds to LRP6(1-2), demonstrating that a single Dkk1 molecule can bind to both portions of the LRP6 ectodomain and thereby inhibit different Wnts. Small-angle X-ray scattering analysis of LRP6(1-4) bound to a noninhibitory antibody fragment or to full-length Dkk1 shows that in both cases the ectodomain adopts a curved conformation that places the first three repeats at a similar height relative to the membrane. Thus, Wnts bound to either portion of the LRP6 ectodomain likely bear a similar spatial relationship to Frizzled coreceptors.
摘要
低密度脂蛋白受体相关蛋白 5 和 6(LRP5/6)是 Wnt 生长因子的核心受体,也与 Wnt 信号的分泌抑制剂 Dkk 蛋白结合。LRP5/6 的细胞外结构域包含四个β-螺旋桨/EGF 样结构域重复序列。前两个重复序列,LRP6(1-2),与几种 Wnt 变体结合,而 LRP6(3-4)与其他 Wnts 结合。我们展示了 Dkk1 C 端结构域与 LRP6(3-4)结合的晶体结构,并表明 Dkk1 N 端结构域与 LRP6(1-2)结合,证明单个 Dkk1 分子可以与 LRP6 细胞外结构域的两部分结合,从而抑制不同的 Wnt。与非抑制性抗体片段或全长 Dkk1 结合的 LRP6(1-4)的小角度 X 射线散射分析表明,在这两种情况下,细胞外结构域都采用弯曲构象,使前三个重复序列相对于膜处于相似的高度。因此,与 LRP6 细胞外结构域的任何一部分结合的 Wnt 可能与 Frizzled 核心受体具有相似的空间关系。
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