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背唇成熟和原肠胚早期延伸依赖于 Wnt11 家族配体。

Dorsal lip maturation and initial archenteron extension depend on Wnt11 family ligands.

机构信息

Department of Systems Biology, Harvard Medical School, Boston, MA, 02115, USA.

Department of Systems Biology, Harvard Medical School, Boston, MA, 02115, USA.

出版信息

Dev Biol. 2023 Jan;493:67-79. doi: 10.1016/j.ydbio.2022.10.013. Epub 2022 Nov 2.

Abstract

Wnt11 family proteins are ligands that activate a type of Dishevelled-mediated, non-canonical Wnt signaling pathway. Loss of function causes defects in gastrulation and/or anterior-posterior axis extension in all vertebrates. Non-mammalian vertebrate genomes encode two Wnt11 family proteins whose distinct functions have been unclear. We knocked down Wnt11b and Wnt11, separately and together, in Xenopus laevis. Single morphants exhibited very similar phenotypes of delayed blastopore closure, but they had different phenotypes during the tailbud period. In response to their very similar gastrulation phenotypes, we chose to characterize dual morphants. Using dark field illuminated time-lapse imaging and kymograph analysis, we identified a failure of dorsal blastopore lip maturation that correlated with slower blastopore closure and failure to internalize the endoderm at the dorsal blastopore lip. We connected these externally visible phenotypes to cellular events in the internal tissues by imaging intact fixed embryos stained for anillin and microtubules. We found that the initial extension of the archenteron is correlated with blastopore lip maturation, and archenteron extension is dramatically disrupted by decreased Wnt11 family signaling. We were aided in our interpretation of the immunofluorescence by the novel, membrane proximal location of the cleavage furrow protein anillin in the epithelium of the blastopore lip and early archenteron.

摘要

Wnt11 家族蛋白是一类配体,可激活 Dishevelled 介导的非经典 Wnt 信号通路。功能丧失会导致所有脊椎动物的原肠胚形成和/或前后轴延伸缺陷。非哺乳动物脊椎动物基因组编码两种 Wnt11 家族蛋白,其功能尚不清楚。我们分别和同时敲低了非洲爪蟾的 Wnt11b 和 Wnt11。单个突变体表现出非常相似的胚孔晚期闭合延迟表型,但在尾芽期具有不同的表型。鉴于它们非常相似的原肠胚形成表型,我们选择了双突变体进行研究。通过暗场照明延时成像和动图分析,我们发现背唇成熟失败,这与胚孔晚期闭合较慢和背唇内胚层内化失败有关。我们通过对完整固定胚胎进行肌动蛋白和微管染色的成像,将这些外部可见的表型与内部组织中的细胞事件联系起来。我们发现,原肠的最初延伸与胚孔唇的成熟有关,而 Wnt11 家族信号的减少会严重破坏原肠的延伸。我们通过对胚孔唇和早期原肠上皮中分裂沟蛋白肌动蛋白的新颖的、靠近膜的位置的免疫荧光进行解释。

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