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秀丽隐杆线虫的teneurin蛋白ten-1是性腺和咽部基底膜完整性所必需的,并且与整合素ina-1和肌营养不良聚糖dgn-1发挥冗余作用。

Caenorhabditis elegans teneurin, ten-1, is required for gonadal and pharyngeal basement membrane integrity and acts redundantly with integrin ina-1 and dystroglycan dgn-1.

作者信息

Trzebiatowska Agnieszka, Topf Ulrike, Sauder Ursula, Drabikowski Krzysztof, Chiquet-Ehrismann Ruth

机构信息

Friedrich Miescher Institute for Biomedical Research, Novartis Research Foundation, CH-4058 Basel, Switzerland.

出版信息

Mol Biol Cell. 2008 Sep;19(9):3898-908. doi: 10.1091/mbc.e08-01-0028. Epub 2008 Jul 16.

Abstract

The Caenorhabditis elegans teneurin ortholog, ten-1, plays an important role in gonad and pharynx development. We found that lack of TEN-1 does not affect germline proliferation but leads to local basement membrane deficiency and early gonad disruption. Teneurin is expressed in the somatic precursor cells of the gonad that appear to be crucial for gonad epithelialization and basement membrane integrity. Ten-1 null mutants also arrest as L1 larvae with malformed pharynges and disorganized pharyngeal basement membranes. The pleiotropic phenotype of ten-1 mutant worms is similar to defects found in basement membrane receptor mutants ina-1 and dgn-1 as well as in the mutants of the extracellular matrix component laminin, epi-1. We show that the ten-1 mutation is synthetic lethal with mutations of genes encoding basement membrane components and receptors due to pharyngeal or hypodermal defects. This indicates that TEN-1 could act redundantly with integrin INA-1, dystroglycan DGN-1, and laminin EPI-1 in C. elegans development. Moreover, ten-1 deletion sensitizes worms to loss of nidogen nid-1 causing a pharynx unattached phenotype in ten-1;nid-1 double mutants. We conclude that TEN-1 is important for basement membrane maintenance and/or adhesion in particular organs and affects the function of somatic gonad precursor cells.

摘要

秀丽隐杆线虫的teneurin直系同源基因ten-1在性腺和咽部发育中起重要作用。我们发现缺乏TEN-1不会影响生殖系增殖,但会导致局部基底膜缺陷和早期性腺破坏。Teneurin在性腺的体细胞前体细胞中表达,这些细胞似乎对性腺上皮形成和基底膜完整性至关重要。ten-1基因敲除突变体也会停滞在L1幼虫阶段,咽部畸形且咽基底膜紊乱。ten-1突变蠕虫的多效性表型类似于基底膜受体突变体ina-1和dgn-1以及细胞外基质成分层粘连蛋白epi-1突变体中的缺陷。我们表明,由于咽部或皮下组织缺陷,ten-1突变与编码基底膜成分和受体的基因突变是合成致死的。这表明在秀丽隐杆线虫发育过程中,TEN-1可能与整合素INA-1、肌营养不良聚糖DGN-1和层粘连蛋白EPI-1发挥冗余作用。此外,ten-1缺失使蠕虫对巢蛋白nid-1的缺失敏感,导致ten-1;nid-1双突变体出现咽部不附着的表型。我们得出结论,TEN-1对特定器官的基底膜维持和/或黏附很重要,并影响体细胞性腺前体细胞的功能。

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