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中枢神经系统神经母细胞增殖抑制因子ana的突变导致幼虫嗅觉行为缺陷。

Mutation of the central nervous system neuroblast proliferation repressor ana leads to defects in larval olfactory behavior.

作者信息

Park Y, Caldwell M C, Datta S

机构信息

Department of Biochemistry and Biophysics and Center for Advanced Invertebrate Molecular Sciences, Texas A&M University, College Station 77843-2128, USA.

出版信息

J Neurobiol. 1997 Aug;33(2):199-211.

PMID:9240375
Abstract

In the developing nervous system, interactions between glia and immature neurons or neuroblasts regulate axon pathfinding, migration, and cell division, and therefore affect structure and function. Glial control of neuroblast cell division has been documented by studies of the anachronism (ana) gene of Drosophila melanogaster. ana encodes a glycoprotein which, in the developing larval central nervous system, is secreted by glia that neighbor regulated neuroblasts. Mutations in ana lead to premature neuroblast proliferation in the larval brain. Examination of lacZ expression from an ana enhancer trap line as well as detection of the ana protein show that ana is also expressed in the larval antennal-maxillary complex (AMC) at all larval stages. As previously reported for the central nervous system, ana expression in the AMC appears to be confined to glial cells. Larval olfactory system function in ana mutants was assayed in a behavioral paradigm. When tested with the three different chemoattractants, third instar ana9 mutant larvae showed diminished olfactory response compared to controls. Examination of a second ana allele revealed aberrant olfactory response to ethyl acetate, demonstrating that more than one mutation in ana can give rise to abnormal larval olfactory behavior. Assays of early first instar ana9 mutant larvae revealed defective olfactory behavior, implying that the olfactory phenotype stems from early larval AMC and/or embryonic origins. This is consistent with proliferation analysis in the early larval AMC region which uncovered a significantly higher number of S-phase cells in ana9 mutants.

摘要

在发育中的神经系统中,神经胶质细胞与未成熟神经元或神经母细胞之间的相互作用调节轴突导向、迁移和细胞分裂,进而影响结构和功能。果蝇“时代错误”(ana)基因的研究记录了神经胶质细胞对神经母细胞分裂的控制。ana编码一种糖蛋白,在发育中的幼虫中枢神经系统中,它由邻近受调控神经母细胞的神经胶质细胞分泌。ana突变会导致幼虫大脑中神经母细胞过早增殖。对ana增强子捕获系的lacZ表达检测以及ana蛋白的检测表明,ana在幼虫的所有发育阶段也在触角 - 上颌复合体(AMC)中表达。如先前关于中枢神经系统的报道,ana在AMC中的表达似乎局限于神经胶质细胞。通过行为范式检测了ana突变体幼虫的嗅觉系统功能。在用三种不同的化学引诱剂进行测试时,三龄ana9突变体幼虫与对照相比嗅觉反应减弱。对第二个ana等位基因的检测揭示了对乙酸乙酯的异常嗅觉反应,表明ana中的多个突变都可导致幼虫嗅觉行为异常。对一龄早期ana9突变体幼虫的检测显示出嗅觉行为缺陷,这意味着嗅觉表型源于幼虫早期的AMC和/或胚胎起源。这与幼虫早期AMC区域的增殖分析结果一致,该分析发现ana9突变体中S期细胞数量显著增加。

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