The Cell Adhesion Molecule L1 Is Required for Chain Migration of Neural Crest Cells in the Developing Mouse Gut

IF 25.7 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Richard B. Anderson , Kirsty N. Turner , Alexander G. Nikonenko , John Hemperly , Melitta Schachner , Heather M. Young
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引用次数: 93

Abstract

Background & Aims: During development, the enteric nervous system is derived from neural crest cells that emigrate from the hindbrain, enter the foregut, and colonize the gut. Defects in neural crest migration can result in intestinal aganglionosis. Hirschsprung’s disease (congenital aganglionosis) is a human condition in which enteric neurons are absent from the distal bowel. A number of clinical studies have implicated the cell adhesion molecule L1 in Hirschsprung’s disease. We examined the role of L1 in the migration of neural crest cells through the developing mouse gut. Methods: A variety of in vitro and in vivo assays were used to examine: (1) the effect of L1 blocking antibodies or exogenous soluble L1 protein known to compromise L1 function on the rate of crest cell migration, (2) the effect of blocking L1 activity on the dynamic behavior of crest cells using time-lapse microscopy, and (3) whether the colonization of the gut by crest cells in L1-deficient mice differs from control mice. Results: We show that L1 is expressed by neural crest cells as they colonize the gut. Perturbation studies show that disrupting L1 activity retards neural crest migration and increases the number of solitary neural crest cells. L1-deficient mice show a small but significant reduction in neural crest cell migration at early developmental stages, but the entire gastrointestinal tract is colonized. Conclusions: L1 is important for the migration of neural crest cells through the developing gut and is likely to be involved in the etiology of Hirschsprung’s disease.

细胞粘附分子L1是发育中的小鼠肠道神经嵴细胞链式迁移所必需的
背景,目的:在发育过程中,肠神经系统来源于神经嵴细胞,这些细胞从后脑迁移到前肠,并定植在肠道内。神经嵴迁移缺陷可导致肠神经节病。先天性巨结肠病(先天性神经节病)是一种人类疾病,其中肠远端神经细胞缺失。许多临床研究表明,细胞粘附分子L1与巨结肠病有关。我们研究了L1在神经嵴细胞通过发育中的小鼠肠道迁移中的作用。方法:采用多种体外和体内实验来检验:(1)L1阻断抗体或已知会损害L1功能的外源性可溶性L1蛋白对嵴细胞迁移速度的影响,(2)使用延时显微镜观察L1阻断活性对嵴细胞动态行为的影响,以及(3)L1缺陷小鼠中嵴细胞在肠道中的定植是否与对照小鼠不同。结果:我们发现神经嵴细胞在肠道定植时表达L1。微扰研究表明,破坏L1活性会延缓神经嵴迁移,增加孤神经嵴细胞的数量。l1缺陷小鼠在早期发育阶段显示出神经嵴细胞迁移的小而显著的减少,但整个胃肠道被定植。结论:L1在神经嵴细胞通过发育中的肠道迁移中起重要作用,并可能参与巨结肠病的病因学。
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来源期刊
Gastroenterology
Gastroenterology 医学-胃肠肝病学
CiteScore
45.60
自引率
2.40%
发文量
4366
审稿时长
26 days
期刊介绍: Gastroenterology is the most prominent journal in the field of gastrointestinal disease. It is the flagship journal of the American Gastroenterological Association and delivers authoritative coverage of clinical, translational, and basic studies of all aspects of the digestive system, including the liver and pancreas, as well as nutrition. Some regular features of Gastroenterology include original research studies by leading authorities, comprehensive reviews and perspectives on important topics in adult and pediatric gastroenterology and hepatology. The journal also includes features such as editorials, correspondence, and commentaries, as well as special sections like "Mentoring, Education and Training Corner," "Diversity, Equity and Inclusion in GI," "Gastro Digest," "Gastro Curbside Consult," and "Gastro Grand Rounds." Gastroenterology also provides digital media materials such as videos and "GI Rapid Reel" animations. It is abstracted and indexed in various databases including Scopus, Biological Abstracts, Current Contents, Embase, Nutrition Abstracts, Chemical Abstracts, Current Awareness in Biological Sciences, PubMed/Medline, and the Science Citation Index.
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