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细胞黏合张力的增加控制着果蝇前后体腔边界处的细胞分类。

Increased cell bond tension governs cell sorting at the Drosophila anteroposterior compartment boundary.

机构信息

Max Planck Institute of Molecular Cell Biology and Genetics, Dresden, Germany.

出版信息

Curr Biol. 2009 Dec 1;19(22):1950-5. doi: 10.1016/j.cub.2009.10.021. Epub 2009 Oct 29.

Abstract

Subdividing proliferating tissues into compartments is an evolutionarily conserved strategy of animal development [1-6]. Signals across boundaries between compartments can result in local expression of secreted proteins organizing growth and patterning of tissues [1-6]. Sharp and straight interfaces between compartments are crucial for stabilizing the position of such organizers and therefore for precise implementation of body plans. Maintaining boundaries in proliferating tissues requires mechanisms to counteract cell rearrangements caused by cell division; however, the nature of such mechanisms remains unclear. Here we quantitatively analyzed cell morphology and the response to the laser ablation of cell bonds in the vicinity of the anteroposterior compartment boundary in developing Drosophila wings. We found that mechanical tension is approximately 2.5-fold increased on cell bonds along this compartment boundary as compared to the remaining tissue. Cell bond tension is decreased in the presence of Y-27632 [7], an inhibitor of Rho-kinase whose main effector is Myosin II [8]. Simulations using a vertex model [9] demonstrate that a 2.5-fold increase in local cell bond tension suffices to guide the rearrangement of cells after cell division to maintain compartment boundaries. Our results provide a physical mechanism in which the local increase in Myosin II-dependent cell bond tension directs cell sorting at compartment boundaries.

摘要

将增殖组织划分为隔室是动物发育的一种进化保守策略[1-6]。隔室之间的边界信号可以导致分泌蛋白的局部表达,从而组织生长和模式形成[1-6]。隔室之间的锐利和直线界面对于稳定组织者的位置至关重要,因此对于精确实施身体计划至关重要。在增殖组织中维持边界需要机制来抵消细胞分裂引起的细胞重排;然而,这种机制的性质尚不清楚。在这里,我们定量分析了细胞形态以及对发育中的果蝇翅膀前后隔室边界附近细胞键激光消融的反应。我们发现,与剩余组织相比,沿该隔室边界的细胞键的机械张力大约增加了 2.5 倍。存在 Y-27632[7](Rho-激酶的抑制剂,其主要效应物是肌球蛋白 II[8])时,细胞键张力降低。使用顶点模型[9]的模拟表明,局部细胞键张力增加 2.5 倍足以指导细胞分裂后细胞的重排以维持隔室边界。我们的结果提供了一种物理机制,其中肌球蛋白 II 依赖性细胞键张力的局部增加指导隔室边界处的细胞分选。

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