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Anchor cell signaling and vulval precursor cell positioning establish a reproducible spatial context during C. elegans vulval induction

机译:秀丽隐杆线虫外阴诱导过程中,锚细胞信号传导和外阴前体细胞定位建立了可重现的空间环境

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摘要

How cells coordinate their spatial positioning to successfully communicate is poorly understood. Here we address this topic using C. elegans vulval patterning during which hypodermal vulval precursor cells (VPCs) adopt distinct cell fates determined by their relative positions to the gonadal anchor cell (AC). LIN-3/EGF signaling by the AC induces the central VPC, P6.p, to adopt a 1° vulval fate. Exact alignment of AC and VPCs is thus critical for correct fate patterning, yet, as we show here, the initial AC-VPC positioning is both highly variable and asymmetric among individuals, with AC and P6.p only becoming aligned at the early L3 stage. Cell ablations and mutant analysis indicate that VPCs, most prominently 1° cells, move towards the AC. We identify AC-released LIN-3/EGF as a major attractive signal, which therefore plays a dual role in vulval patterning (cell alignment and fate induction). Additionally, compromising Wnt pathway components also induces AC-VPC alignment errors, with loss of posterior Wnt signaling increasing stochastic vulval centering on P5.p. Our results illustrate how intercellular signaling reduces initial spatial variability in cell positioning to generate reproducible interactions across tissues.
机译:人们对细胞如何协调其空间定位以成功交流的了解甚少。在这里,我们使用秀丽隐杆线虫的外阴部模式来解决这个问题,在此期间,皮下外阴部前体细胞(VPC)采用不同的细胞命运,这取决于它们相对于性腺锚定细胞(AC)的相对位置。 AC发出的LIN-3 / EGF信号诱导中央VPC P6.p采用1°外阴命运。因此,AC和VPC的精确对准对于正确的命运模式至关重要,但是,正如我们在此处所示,AC-VPC的初始定位在个体之间高度可变且不对称,AC和P6.p仅在L3早期阶段对准。细胞消融和突变分析表明,VPC(最突出的1°细胞)向AC移动。我们确定交流释放的LIN-3 / EGF为主要诱人信号,因此在外阴模式(细胞排列和命运诱导)中起着双重作用。此外,折衷的Wnt通路成分也会引起AC-VPC对齐错误,后Wnt信号的丢失会增加以P5.p为中心的随机性外阴。我们的结果说明了细胞间信号传导如何降低细胞定位中的初始空间变异性,从而在组织之间产生可再现的相互作用。

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