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神经营养因子-3诱导胎鼠肠道神经嵴衍生细胞在体外发育为神经元或神经胶质细胞。

Neurotrophin-3 induces neural crest-derived cells from fetal rat gut to develop in vitro as neurons or glia.

作者信息

Chalazonitis A, Rothman T P, Chen J, Lamballe F, Barbacid M, Gershon M D

机构信息

Department of Anatomy and Cell Biology, Columbia University, College of Physicians and Surgeons, New York, New York 10032.

出版信息

J Neurosci. 1994 Nov;14(11 Pt 1):6571-84. doi: 10.1523/JNEUROSCI.14-11-06571.1994.

Abstract

The precursor cells that form the enteric nervous system (ENS) are multipotent when they arrive in the gut from the neural crest. Their differentiation thus depends on signals from the enteric microenvironment. Crest-derived cells were isolated from the fetal rat bowel by immunoselection at E14 with NC-1/HNK-1 antibodies and secondary antibodies coupled to magnetic beads. NC-1/HNK-1-immunoreactive cells were enriched approximately 36-fold. The NC-1/HNK-1-selected population and the residual population were plated at equal cell density and maintained in a defined medium for 6-7 d. The total number of cells found in the cultures of the residual cells was three- to fourfold that in cultures of immunoselected cells. Neurotrophin-3 (NT-3), but not nerve growth factor (NGF), brain-derived neurotrophic factor (BDNF), or neurotrophin-4/5 (NT-4/5), was found to increase the proportion of neurons (neurofilament-immunoreactive or neuron-specific enolase-immunoreactive) or glia (S-100-immunoreactive) (from 6.6 +/- 0.9% to 15.2 +/- 1.4%; p < 0.001). This effect was concentration dependent (from 1 to 40 ng/ml) and observed only in the cultures of immunoselected cells. NT-3 also enhanced neurite outgrowth. NT-3 increased neither cell number nor bromodeoxyuridine incorporation and thus was not mitogenic. Exposure of immunoselected cells to NT-3 rapidly and transiently induced the appearance of nuclear Fos immunoreactivity. Transcripts coding for TrkC, the transducing receptor for NT-3, were identified in the fetal rat gut (E14-E16) and in the immunoselected population of cells using reverse transcriptase and the polymerase chain reaction. It is concluded that NT-3 specifically promotes the differentiation of enteric crest-derived cells as neurons or glia and may thus play a role in the development and/or maintenance of the ENS.

摘要

形成肠神经系统(ENS)的前体细胞从神经嵴到达肠道时具有多能性。因此,它们的分化取决于来自肠道微环境的信号。在胚胎第14天,通过用NC-1/HNK-1抗体和偶联磁珠的二抗进行免疫选择,从胎鼠肠道中分离出神经嵴来源的细胞。NC-1/HNK-1免疫反应性细胞富集了约36倍。将NC-1/HNK-1选择的细胞群体和剩余细胞群体以相等的细胞密度接种,并在限定培养基中培养6 - 7天。在剩余细胞培养物中发现的细胞总数是免疫选择细胞培养物中的三到四倍。发现神经营养因子-3(NT-3)可增加神经元(神经丝免疫反应性或神经元特异性烯醇化酶免疫反应性)或神经胶质细胞(S-100免疫反应性)的比例(从6.6±0.9%增加到15.2±1.4%;p<0.001),而神经生长因子(NGF)、脑源性神经营养因子(BDNF)或神经营养因子-4/5(NT-4/5)则无此作用。这种作用呈浓度依赖性(1至40 ng/ml),且仅在免疫选择细胞的培养物中观察到。NT-3还增强了神经突生长。NT-既不增加细胞数量,也不增加溴脱氧尿苷掺入,因此没有促有丝分裂作用。将免疫选择的细胞暴露于NT-3会迅速且短暂地诱导核Fos免疫反应性的出现。使用逆转录酶和聚合酶链反应,在胎鼠肠道(胚胎第14 - 16天)和免疫选择的细胞群体中鉴定出编码NT-3转导受体TrkC的转录本。得出的结论是,NT-3特异性地促进肠神经嵴来源细胞向神经元或神经胶质细胞分化,因此可能在肠神经系统的发育和/或维持中发挥作用。

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