Frische Ester W, Pellis-van Berkel Wendy, van Haaften Gijs, Cuppen Edwin, Plasterk Ronald H A, Tijsterman Marcel, Bos Johannes L, Zwartkruis Fried J T
Department of Physiological Chemistry, Centre for Biomedical Genetics, UMC Utrecht, Utrecht, The Netherlands.
EMBO J. 2007 Dec 12;26(24):5083-92. doi: 10.1038/sj.emboj.7601922. Epub 2007 Nov 8.
The small Ras-like GTPase Rap1 has been identified as a regulator of integrin activation and cadherin-mediated cell-cell contacts. Surprisingly, null mutants of RAP-1 in Caenorhabditis elegans are viable and fertile. In a synthetic lethal RNAi screen with C. elegans rap-1 mutants, the Ras-like GTPase ral-1 emerged as one of seven genes specifically required for viability. Depletion of exoc-8 and sec-5, encoding two putative RAL-1 effectors and members of the exocyst complex, also caused lethality of rap-1 mutants, but did not affect wild-type worms. The RAP-1 and the RAL-1/exocyst pathway appear to coordinate hypodermal cell movement and elongation during embryonic development. They mediate their effect in part through targeting the alpha-catenin homologue HMP-1 to the lateral membrane. Genetic interactions show that the RAP-1 and RAL-1/exocyst pathway also act in parallel during larval stages. Together these data provide in vivo evidence for the exocyst complex as a downstream RAL-1 effector in cell migration.
小Ras样GTP酶Rap1已被确定为整合素激活和钙黏蛋白介导的细胞间接触的调节因子。令人惊讶的是,秀丽隐杆线虫中RAP-1的缺失突变体是可存活且可育的。在一项针对秀丽隐杆线虫rap-1突变体的合成致死RNA干扰筛选中,Ras样GTP酶ral-1作为七个存活所特别需要的基因之一出现。编码两种假定的RAL-1效应器和外泌体复合体成员的exoc-8和sec-5的缺失,也导致rap-1突变体的致死性,但不影响野生型线虫。RAP-1和RAL-1/外泌体途径似乎在胚胎发育过程中协调皮下细胞的移动和伸长。它们部分通过将α-连环蛋白同源物HMP-1靶向侧膜来介导其作用。遗传相互作用表明,RAP-1和RAL-1/外泌体途径在幼虫阶段也并行发挥作用。这些数据共同为外泌体复合体作为细胞迁移中RAL-1的下游效应器提供了体内证据。
