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首页> 外文期刊>Journal of Cell Science >ForC, a novel type of formin family protein lacking an FH1 domain, is involved in multicellular development in Dictyostelium discoideum
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ForC, a novel type of formin family protein lacking an FH1 domain, is involved in multicellular development in Dictyostelium discoideum

机译:ForC是一种缺乏FH1结构域的新型formin家族蛋白,参与了盘基网柄菌的多细胞发育

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摘要

Formins are highly conserved regulators of cytoskeletal organization and share three regions of homology: the FH1, FH2 and FH3 domains. Of the nine known formin genes or pseudogenes carried by Dictyostelium, forC is novel in that it lacks an FH1 domain. Mutant Dictyostelium lacking forC (DeltaforC) grew normally during the vegetative phase and, when starved, migrated normally and formed tight aggregates. Subsequently, however, DeltaforC cells made aberrant fruiting bodies with short stalks and sori that remained unlifted. DeltaforC aggregates were also unable to migrate as slugs, suggesting forC is involved in mediating cell movement during multicellular stages of Dictyostelium development. Consistent with this idea, expression of forC was increased significantly in aggregates of wild-type cells. GFP-ForC expressed in DeltaforC cells was localized at the crowns, which are macropinocytotic structures rich in F-actin, suggesting that, like other formin isoforms, ForC functions in close relation with the actin cytoskeleton. Truncation analysis of GFP-ForC revealed that the FH3 domain is required for ForC localization; moreover, localization of a truncated GFP-ForC mutant at the site of contacts between cells on substrates and along the cortex of cells within a multicellular culminant suggests that ForC is involved in the local actin cytoskeletal reorganization mediating cell-cell adhesion. [References: 54]
机译:福尔马林是高度保守的细胞骨架组织调节剂,共有三个同源性区域:FH1,FH2和FH3结构域。 Dictyostelium携带的九种已知的formin基因或假基因中,forC新颖,因为它缺少FH1结构域。缺乏forC的突变型盘基网柄菌(DeltaforC)在营养期正常生长,饥饿时正常迁移并形成紧密的聚集体。然而,随后,DeltaforC细胞产生了异常结实的子实体,茎秆短,果梗短,没有被提起。 DeltaforC聚集体也无法作为团块迁移,表明forC参与了Dictyostelium发育的多细胞阶段中介导的细胞运动。与这个想法一致,在野生型细胞聚集体中,forC的表达显着增加。在DeltaforC细胞中表达的GFP-ForC位于冠状细胞,其冠状细胞是富含F-肌动蛋白的巨细胞结构,表明ForC与其他formin亚型一样,与肌动蛋白细胞骨架密切相关。 GFP-ForC的截断分析表明,FH3结构域是ForC定位所必需的。此外,截短的GFP-ForC突变体在底物上的细胞之间的接触部位以及沿着多细胞菌种内的细胞皮层的接触部位的定位表明,ForC参与了介导细胞间粘附的局部肌动蛋白细胞骨架重组。 [参考:54]

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