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Actomyosin Contractility and Microtubules Drive Apical Constriction in Xenopus Bottle Cells

机译:肌动球蛋白的收缩力和微管驱动非洲爪蟾瓶细胞的根尖收缩。

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摘要

Cell shape changes are critical for morphogenetic events such as gastrulation, neurulation, and organogenesis. However, the cell biology driving cell shape changes is poorly understood, especially in vertebrates. The beginning of Xenopus laevis gastrulation is marked by the apical constriction of bottle cells in the dorsal marginal zone, which bends the tissue and creates a crevice at the blastopore lip. We found that bottle cells contribute significantly to gastrulation, as their shape change can generate the force required for initial blastopore formation. As actin and myosin are often implicated in contraction, we examined their localization and function in bottle cells. F-actin and activated myosin accumulate apically in bottle cells, and actin and myosin inhibitors either prevent or severely perturb bottle cell formation, showing that actomyosin contractility is required for apical constriction. Microtubules were localized in apicobasally directed arrays in bottle cells, emanating from the apical surface. Surprisingly, apical constriction was inhibited in the presence of nocodazole but not taxol, suggesting that intact, but not dynamic, microtubules are required for apical constriction. Our results indicate that actomyosin contractility is required for bottle cell morphogenesis and further suggest a novel and unpredicted role for microtubules during apical constriction.
机译:细胞形态的变化对于形态发生事件(例如胃形成,神经形成和器官发生)至关重要。但是,驱动细胞形状变化的细胞生物学了解甚少,尤其是在脊椎动物中。非洲爪蟾胃化的开始以背边缘区的瓶状细胞的顶缩为标志,该弯曲使组织弯曲并在胚孔唇上产生缝隙。我们发现瓶形细胞对胃化有重要作用,因为它们的形状变化会产生初始胚孔形成所需的力。由于肌动蛋白和肌球蛋白通常与收缩有关,因此我们检查了它们在瓶状细胞中的定位和功能。 F-肌动蛋白和活化的肌球蛋白在顶端细胞中积累,肌动蛋白和肌球蛋白抑制剂阻止或严重干扰了瓶细胞的形成,表明肌动球蛋白的收缩是顶端收缩所必需的。将微管定位在瓶顶细胞的顶突定向阵列中,从顶表面发出。出乎意料的是,在存在诺考达唑而不是紫杉醇的情况下抑制了根尖收缩,这表明对于根尖收缩需要完整但不是动态的微管。我们的结果表明,肌动球蛋白的收缩是瓶细胞形态发生所必需的,并且进一步提示了在根尖收缩期间微管的新的和不可预测的作用。

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