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秀丽隐杆线虫的肌肉细胞迁移由α-整合素INA-1、Eph受体VAB-1和一种新型肽酶同源物MNP-1介导。

Muscle cell migrations of C. elegans are mediated by the alpha-integrin INA-1, Eph receptor VAB-1, and a novel peptidase homologue MNP-1.

作者信息

Tucker Morgan, Han Min

机构信息

Department of Molecular, Cellular and Developmental Biology, Howard Hughes Medical Institute, Campus Box 0347, University of Colorado, Boulder, CO 80303, USA.

出版信息

Dev Biol. 2008 Jun 15;318(2):215-23. doi: 10.1016/j.ydbio.2008.02.062. Epub 2008 Mar 20.

Abstract

Cell migration is a fundamental process occurring during embryonic development and tissue morphogenesis. In the nematode Caenorhabditis elegans, morphogenesis of the body-wall musculature involves short-range migrations of 81 embryonic muscle cells from the lateral surface of the embryo towards the dorsal and ventral midlines. This study shows that mutations in ina-1 (alpha-integrin), as well as vab-1 (Eph receptor), and vab-2 (ephrin), display defects in embryonic muscle cell migration. Furthermore, an RNAi-based enhancer screen in an ina-1 weak loss-of-function background identified mnp-1 (matrix non-peptidase homologue-1) as a previously uncharacterized gene required for promoting proper migration of the embryonic muscle cells. mnp-1 encodes a membrane associated metalloproteinase homologue that is predicted to be catalytically inactive. Our data suggest that MNP-1 is expressed in migrating muscle cells and localizes to the plasma membrane with the non-peptidase domain exposed to the extra-cellular environment. Double-mutant analysis between mnp-1(RNAi), ina-1, and vab-1 mutations; as well as tissue specific rescue experiments; indicated that each of these gene products function predominantly independent of each other and from different cell types to affect muscle cell migration. Together these results suggest complex interactions between the adjacent epidermal, neuronal, and muscle cells are required to promote proper muscle cell migration during embryogenesis.

摘要

细胞迁移是胚胎发育和组织形态发生过程中发生的一个基本过程。在线虫秀丽隐杆线虫中,体壁肌肉组织的形态发生涉及81个胚胎肌肉细胞从胚胎侧面朝着背中线和腹中线的短距离迁移。本研究表明,ina-1(α-整合素)、vab-1(Eph受体)和vab-2(ephrin)的突变在胚胎肌肉细胞迁移中表现出缺陷。此外,在ina-1功能部分丧失的背景下基于RNA干扰的增强子筛选鉴定出mnp-1(基质非肽酶同源物-1)是促进胚胎肌肉细胞正常迁移所需的一个此前未被表征的基因。mnp-1编码一种膜相关金属蛋白酶同源物,预计其无催化活性。我们的数据表明,MNP-1在迁移的肌肉细胞中表达,并定位于质膜,其非肽酶结构域暴露于细胞外环境。mnp-1(RNA干扰)、ina-1和vab-1突变之间的双突变分析,以及组织特异性拯救实验表明,这些基因产物中的每一个主要独立发挥作用,且来自不同细胞类型,以影响肌肉细胞迁移。这些结果共同表明,相邻的表皮细胞、神经元细胞和肌肉细胞之间需要复杂的相互作用,以促进胚胎发育过程中肌肉细胞的正常迁移。

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