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芽体外翻过程中顶端和基部上皮肌动蛋白丝的动态变化。

Apical and basal epitheliomuscular F-actin dynamics during bud evagination.

作者信息

Aufschnaiter Roland, Wedlich-Söldner Roland, Zhang Xiaoming, Hobmayer Bert

机构信息

Department for Evolutionary Developmental Biology, Institute of Zoology and Centre for Molecular Biosciences, University of Innsbruck, Technikerstr. 25, A-6020 Innsbruck, Austria.

Max-Planck-Institute of Biochemistry, Research Group Cellular Dynamics and Cell Patterning, Am Klopferspitz 18, D-82152 Planegg, Martinsried, Germany.

出版信息

Biol Open. 2017 Aug 15;6(8):1137-1148. doi: 10.1242/bio.022723.

Abstract

Bending of 2D cell sheets is a fundamental morphogenetic mechanism during animal development and reproduction. A critical player driving cell shape during tissue bending is the actin cytoskeleton. Much of our current knowledge about actin dynamics in whole organisms stems from studies of embryonic development in bilaterian model organisms. Here, we have analyzed actin-based processes during asexual bud evagination in the simple metazoan We created transgenic strains stably expressing the actin marker Lifeact-GFP in either ectodermal or endodermal epitheliomuscular cells. We then combined live imaging with conventional phalloidin staining to directly follow actin reorganization. Bending of the epithelial double layer is initiated by a group of epitheliomuscular cells in the endodermal layer. These cells shorten their apical-basal axis and arrange their basal muscle processes in a circular configuration. We propose that this rearrangement generates the initial forces to bend the endoderm towards the ectoderm. Convergent tissue movement in both epithelial layers towards the centre of evagination then leads to elongation and extension of the bud along its new body axis. Tissue movement into the bud is associated with lateral intercalation of epithelial cells, remodelling of apical septate junctions, and rearrangement of basal muscle processes. The work presented here extends the analysis of morphogenetic mechanisms beyond embryonic tissues of model bilaterians.

摘要

二维细胞片层的弯曲是动物发育和繁殖过程中的一种基本形态发生机制。在组织弯曲过程中驱动细胞形状变化的一个关键因素是肌动蛋白细胞骨架。我们目前对整个生物体中肌动蛋白动力学的许多了解都源于对两侧对称模式生物胚胎发育的研究。在这里,我们分析了简单后生动物无性芽外翻过程中基于肌动蛋白的过程。我们创建了转基因品系,使其在外胚层或内胚层上皮肌肉细胞中稳定表达肌动蛋白标记Lifeact-GFP。然后,我们将实时成像与传统的鬼笔环肽染色相结合,以直接跟踪肌动蛋白的重组。上皮双层的弯曲由内胚层中的一组上皮肌肉细胞启动。这些细胞缩短其顶-基轴,并将其基底肌肉突起排列成圆形。我们认为这种重排产生了使内胚层向外胚层弯曲的初始力。然后,两个上皮层朝着外翻中心的汇聚组织运动导致芽沿着其新的身体轴伸长和延伸。组织向芽内的运动与上皮细胞的侧向插入、顶端隔膜连接的重塑以及基底肌肉突起的重排有关。本文所展示的工作将形态发生机制的分析扩展到了两侧对称模式生物的胚胎组织之外。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3552/5576072/d7d315809e05/biolopen-6-022723-g1.jpg

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