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Characterization of signaling pathways enabling coordinated morphogenesis of tissues during Drosophila dorsal closure

机译:果蝇背闭合过程中能够协调组织形态发生的信号传导途径的表征

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摘要

Drosophila dorsal closure (DC) is the best-characterized model system for studying wound healing. During DC, a hole in the dorsal epidermis, covered by an epithelium called the amnioserosa (AS), is sealed by migration of the epidermal flanks. Seamless closure is achieved through coordinated morphogenesis of the AS and epidermis, which is facilitated by communication between the two tissues via bidirectional signaling networks. To better understand this crosstalk, three diffusible signals present during DC were analyzed, and their signaling roles were identified: 1.) Folded gastrulation (Fog), which may act as an upstream activator of a JNK pathway in the epidermis; 2.) the TGF-β ligand, Decapentaplegic (Dpp), which regulates production of the steroid hormone, 20- hydroxyecdysone (ecdysone) in the AS; 3.) ecdysone, which interacts with the transcription factor AP-1 to regulate gene transcription in the AS. Signaling via these molecules ultimately regulates myosin contractility necessary for morphogenesis of both tissues during DC.
机译:果蝇背闭合(DC)是研究伤口愈合的最典型模型系统。在DC期间,通过表皮侧翼的迁移将背侧表皮上的一个孔(称为羊膜膜(AS))覆盖。无缝闭合是通过AS和表皮的协同形态发生来实现的,这是通过双向信号网络在两个组织之间进行通信而促进的。为了更好地理解这种串扰,分析了DC期间存在的三个扩散信号,并确定了它们的信号传导作用:1.)折叠胃(Fog),其可能充当表皮JNK通路的上游激活剂; 2.)TGF-β配体Decapentaplegic(Dpp),它调节AS中类固醇激素20-羟基蜕皮激素(蜕皮激素)的产生; 3.)蜕皮激素,其与转录因子AP-1相互作用以调节AS中的基因转录。通过这些分子发出的信号最终调节DC期间两个组织的形态发生所必需的肌球蛋白收缩性。

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    Kim Hae-Yoon;

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  • 年度 2017
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