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ced-10 Rac和mig-2具有冗余功能,并与unc-73 trio共同作用,以控制秀丽隐杆线虫中阴门细胞分裂和迁移的方向。

ced-10 Rac and mig-2 function redundantly and act with unc-73 trio to control the orientation of vulval cell divisions and migrations in Caenorhabditis elegans.

作者信息

Kishore Ranjana S, Sundaram Meera V

机构信息

Department of Genetics, University of Pennsylvania School of Medicine, 422 Curie Boulevard, Philadelphia, PA 19104-6100, USA.

出版信息

Dev Biol. 2002 Jan 15;241(2):339-48. doi: 10.1006/dbio.2001.0513.

Abstract

Vulval development in the nematode Caenorhabditis elegans can be divided into a fate specification phase controlled in part by let-60 Ras, and a fate execution phase involving stereotypical patterns of cell division and migration controlled in part by lin-17 Frizzled. Since the small GTPase Rac has been implicated as a downstream target of both Ras and Frizzled and influences cytoskeletal dynamics, we investigated the role of Rac signaling during each phase of vulval development. We show that the Rac gene ced-10 and the Rac-related gene mig-2 are redundantly required for the proper orientation of certain vulval cell divisions, suggesting a role in spindle positioning. ced-10 Rac and mig-2 are also redundantly required for vulval cell migrations and play a minor role in vulval fate specification. Constitutively active and dominant-negative mutant forms of mig-2 cause vulval defects that are very similar to those seen in ced-10;mig-2 double loss-of-function mutants, indicating that they interfere with the functions of both ced-10 Rac and mig-2. Mutations in unc-73 (a Trio-like guanine nucleotide exchange factor) cause similar vulval defects, suggesting that UNC-73 is an exchange factor for both CED-10 and MIG-2. We discuss the similarities and differences between the cellular defects seen in Rac mutants and let-60 Ras or lin-17 Frizzled mutants.

摘要

线虫秀丽隐杆线虫的外阴发育可分为一个部分受let-60 Ras控制的命运指定阶段,以及一个部分受lin-17 Frizzled控制的涉及细胞分裂和迁移的刻板模式的命运执行阶段。由于小GTP酶Rac被认为是Ras和Frizzled的下游靶点,并影响细胞骨架动力学,我们研究了Rac信号在每个外阴发育阶段的作用。我们发现,Rac基因ced-10和Rac相关基因mig-2对于某些外阴细胞分裂的正确定向是冗余必需的,提示其在纺锤体定位中发挥作用。ced-10 Rac和mig-2对于外阴细胞迁移也是冗余必需的,并且在外阴命运指定中发挥次要作用。组成型激活和显性负性突变形式的mig-2导致的外阴缺陷与ced-10;mig-2双功能缺失突变体中所见的缺陷非常相似,表明它们干扰了ced-10 Rac和mig-2的功能。unc-73(一种Trio样鸟嘌呤核苷酸交换因子)的突变导致类似的外阴缺陷,提示UNC-73是CED-10和MIG-2的交换因子。我们讨论了Rac突变体与let-60 Ras或lin-17 Frizzled突变体中所见细胞缺陷的异同。

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