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Gli3(Xt)和成纤维蛋白(ld)参与极化区域的定位以及后肢芽身份的控制。

Gli3 (Xt) and formin (ld) participate in the positioning of the polarising region and control of posterior limb-bud identity.

作者信息

Zúñiga A, Zeller R

机构信息

EMBL, Meyerhofstrasse 1, D-69117 Heidelberg, Germany.

出版信息

Development. 1999 Jan;126(1):13-21. doi: 10.1242/dev.126.1.13.

DOI:10.1242/dev.126.1.13
PMID:9834182
Abstract

During initiation of limb-bud outgrowth in vertebrate embryos, the polarising region (limb-bud organizer) is established upon activation of the Sonic Hedgehog (SHH) signaling molecule at the posterior limb-bud margin. Another hallmark of establishing anteroposterior limb-bud identities is the colinear activation of HoxD genes located at the 5' end of the cluster (5'HoxD genes). The unique and shared functions of Gli3 and formin in these determinative events were genetically analyzed using single and double homozygous Extra-toes (Xt; disrupting Gli3) and limb deformity (ld; disrupting formin) mouse embryos. Analysis of the limb skeletal phenotypes reveals genetic interaction of the two genes. In addition to loss of digit identity and varying degrees of polydactyly, proximal skeletal elements are severely shortened in Xt;ld double homozygous limbs. The underlying molecular defects affect both establishment of the polarising region and posterior limb-bud identity. In particular, the synergism between Gli3- and formin-mediated mesenchyme-AER interactions positions the SHH signaling center at the posterior limb-bud margin. The present study shows that establishment and positioning of the polarising region is regulated both by restriction of Shh through Gli3 and its positive feedback regulation through formin. Concurrently, Gli3 functions independently of formin during initial posterior nesting of 5'HoxD domains, whereas their subsequent distal restriction and anterior expansion depends on genetic interaction of Gli3 and formin.

摘要

在脊椎动物胚胎肢体芽开始生长的过程中,极化区域(肢体芽组织者)在 Sonic Hedgehog(SHH)信号分子于后肢芽边缘被激活时得以确立。确定前后肢芽身份的另一个标志是位于基因簇 5' 端的 HoxD 基因(5'HoxD 基因)的共线性激活。利用单基因和双基因纯合的多趾(Xt;破坏 Gli3)和肢体畸形(ld;破坏formin)小鼠胚胎,对 Gli3 和 formin 在这些决定性事件中的独特及共同功能进行了遗传学分析。对肢体骨骼表型的分析揭示了这两个基因的遗传相互作用。除了指(趾)身份丧失和不同程度的多指(趾)畸形外,在 Xt;ld 双基因纯合肢体中,近端骨骼元件严重缩短。潜在的分子缺陷影响极化区域的建立和后肢芽身份。特别是,Gli3 和 formin 介导的间充质 - 顶外胚层嵴(AER)相互作用之间的协同作用将 SHH 信号中心定位在后肢芽边缘。本研究表明,极化区域的建立和定位既受 Gli3 对 Shh 的限制调节,也受 formin 对其的正反馈调节。同时,在 5'HoxD 结构域最初的后嵌套过程中,Gli3 的功能独立于 formin,而它们随后的远端限制和前端扩展则依赖于 Gli3 和 formin 的遗传相互作用。

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