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RET受体酪氨酸激酶:在神经发育和疾病中的激活、信号传导及意义

The RET receptor tyrosine kinase: activation, signalling and significance in neural development and disease.

作者信息

Mason I

机构信息

Department of Developmental Neurobiology, King's College London, UK.

出版信息

Pharm Acta Helv. 2000 Mar;74(2-3):261-4. doi: 10.1016/s0031-6865(99)00048-5.

Abstract

The RET receptor tyrosine kinase was first identified in a screen for human oncogenes and has subsequently been linked to several human syndromes: Hirschprung's disease, multiple endocrine neoplasia types 2A and 2B and familial thyroid carcinoma. Interestingly, all of the tissues affected by mutations in RET are derived from the neural crest during development. RET transduces a signal following activation by ligands of the glial cell line-derived neurotrophic factor (GDNF) family of neurotrophins which currently comprises GDNF, neuturin (NTN), artemin (ART) and persephin (PSP). To activate RET they form a tripartite complex with RET and a member of a family of four extracellular, GPI-linked alpha receptors (GFR alpha 1-4). Specificity is achieved by each GFR alpha binding only one member of the GDNF family with high affinity. Current evidence indicates that signal transduction by RET activates several second messenger systems including the PLC gamma, Ras, JNK and inositol phosphate pathways. Targeted mutagenesis in transgenic mice has shown that Ret, GFR alpha 1 and GDNF are required for multiple developmental events including development of the enteric nervous system (ENS) affected in Hirschsprung's disease. We describe experiments in chick neural crest cells which provide evidence for the normal function of RET and the basis of the defect in Hirschsprung's disease.

摘要

RET受体酪氨酸激酶最初是在一项人类癌基因筛查中被鉴定出来的,随后它被发现与几种人类综合征有关:先天性巨结肠症、2A和2B型多发性内分泌腺瘤病以及家族性甲状腺癌。有趣的是,所有受RET突变影响的组织在发育过程中都源自神经嵴。RET在被胶质细胞系衍生的神经营养因子(GDNF)家族的神经营养素配体激活后转导信号,该家族目前包括GDNF、神经营养素(NTN)、Artemin(ART)和Persephin(PSP)。为了激活RET,它们与RET以及四种细胞外GPI连接的α受体(GFRα1 - 4)家族的一个成员形成三方复合物。特异性是通过每个GFRα仅以高亲和力结合GDNF家族的一个成员来实现的。目前的证据表明,RET介导的信号转导激活了包括PLCγ、Ras、JNK和肌醇磷酸途径在内的几种第二信使系统。转基因小鼠中的靶向诱变表明,Ret、GFRα1和GDNF是包括先天性巨结肠症所影响的肠神经系统(ENS)发育在内的多个发育事件所必需的。我们描述了在鸡神经嵴细胞中的实验,这些实验为RET的正常功能以及先天性巨结肠症缺陷的基础提供了证据。

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