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人类和果蝇 Wif-1 分泌因子的 WIF 结构域赋予其对 Wnt 或 Hedgehog 的特异性。

The WIF domain of the human and Drosophila Wif-1 secreted factors confers specificity for Wnt or Hedgehog.

机构信息

Centro de Biología Molecular Severo Ochoa, Universidad Autónoma de Madrid, Cantoblanco, E-28049 Madrid, Spain.

出版信息

Development. 2012 Oct;139(20):3849-58. doi: 10.1242/dev.080028. Epub 2012 Sep 5.

DOI:10.1242/dev.080028
PMID:22951645
Abstract

The Hedgehog (Hh) and Wnt signaling pathways are crucial for development as well as for adult stem cell maintenance in all organisms from Drosophila to humans. Aberrant activation of these pathways has been implicated in many types of human cancer. During evolution, organisms have developed numerous ways to fine-tune Wnt and Hh signaling. One way is through extracellular modulators that directly interact with Wnt or Hh, such as the Wnt inhibitory factor (Wif-1) family of secreted factors. Interestingly, Wif-1 family members have divergent functions in the Wnt and Hh pathways in different organisms. Whereas vertebrate Wif-1 blocks Wnt signaling, Drosophila Wif-1 [Shifted (Shf)] regulates only Hh distribution and spreading through the extracellular matrix. Here, we investigate which parts of the Shf and human Wif-1 (WIF1) proteins are responsible for functional divergence. We analyze the behavior of domain-swap (the Drosophila and human WIF domain and EGF repeats) chimeric constructs during wing development. We demonstrate that the WIF domain confers the specificity for Hh or Wg morphogen. The EGF repeats are important for the interaction of Wif-1 proteins with the extracellular matrix; Drosophila EGF repeats preferentially interact with the glypican Dally-like (Dlp) when the WIF domain belongs to human WIF1 and with Dally when the WIF domain comes from Shf. These results are important both from the evolutionary perspective and for understanding the mechanisms of morphogen distribution in a morphogenetic field.

摘要

刺猬 (Hh) 和 Wnt 信号通路对于从果蝇到人类的所有生物体的发育以及成体干细胞的维持都至关重要。这些途径的异常激活与许多类型的人类癌症有关。在进化过程中,生物体已经开发出许多微调 Wnt 和 Hh 信号的方法。一种方法是通过直接与 Wnt 或 Hh 相互作用的细胞外调节剂,例如 Wnt 抑制因子 (Wif-1) 家族分泌因子。有趣的是,Wif-1 家族成员在不同生物体的 Wnt 和 Hh 途径中具有不同的功能。虽然脊椎动物 Wif-1 阻断 Wnt 信号,但果蝇 Wif-1 [Shifted (Shf)] 仅通过细胞外基质调节 Hh 的分布和扩散。在这里,我们研究了 Shf 和人类 Wif-1 (WIF1) 蛋白的哪些部分负责功能分化。我们分析了在翅膀发育过程中域交换 (果蝇和人类 WIF 结构域和 EGF 重复) 嵌合构建体的行为。我们证明 WIF 结构域赋予了对 Hh 或 Wg 形态发生素的特异性。EGF 重复对于 Wif-1 蛋白与细胞外基质的相互作用很重要;当 WIF 结构域属于人类 WIF1 时,果蝇 EGF 重复优先与糖蛋白 Dally-like (Dlp) 相互作用,而当 WIF 结构域来自 Shf 时,与 Dally 相互作用。这些结果无论是从进化的角度还是从理解形态发生素在形态发生场中的分布机制的角度来看都很重要。

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