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通过免疫筛选从肠道分离出的神经嵴衍生细胞,在层粘连蛋白上培养时会发育出神经元和神经胶质细胞表型。

Neural crest-derived cells isolated from the gut by immunoselection develop neuronal and glial phenotypes when cultured on laminin.

作者信息

Pomeranz H D, Rothman T P, Chalazonitis A, Tennyson V M, Gershon M D

机构信息

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

出版信息

Dev Biol. 1993 Apr;156(2):341-61. doi: 10.1006/dbio.1993.1082.

Abstract

The neural crest-derived cells that colonize the bowel are different from their predecessors in the premigratory crest. A procedure, which utilized the immunoselection of cells with a magnet, was thus devised to obtain crest-derived precursors from developing gut. Primary antibodies against cell surface antigens, NC-1 in chick, quail, and rat, or antibodies to a 110-kDa laminin binding protein (alpha-110) in mouse, were used in conjunction with secondary antibodies coupled to magnetic beads. Immediately after immunoselection with NC-1, almost all of the selected cells were NC-1-immunoreactive. Neurons and glia, identified immunocytochemically with antibodies to specific markers, developed preferentially in cultures of immunoselected cells. Some of the phenotypes expressed by neurons arising in vitro were appropriate for the bowel (serotonin- and vasoactive intestinal peptide-immunoreactive); however, catecholaminergic neurons, which are not present in the enteric nervous system, also differentiated in the cultures. Neuronal development, as well as neurite outgrowth, were promoted by laminin. Cells selected with alpha-110 from the fetal murine bowel preferentially gave rise in vitro to neurons and glia. These data suggest that the population of crest-derived cells that colonizes the gut is multipotent, that development of catecholaminergic neurons in situ is prevented by the intact enteric microenvironment, that laminin is important in the formation of enteric ganglia, and that the 110-kDa laminin binding protein is expressed on the surfaces of the immediate precursors of enteric neurons and glia.

摘要

定植于肠道的神经嵴衍生细胞与其迁移前嵴中的前身不同。因此,设计了一种利用磁体对细胞进行免疫筛选的方法,以从发育中的肠道中获取嵴衍生前体细胞。针对细胞表面抗原(鸡、鹌鹑和大鼠中的NC-1)的一抗,或针对小鼠中一种110 kDa层粘连蛋白结合蛋白(α-110)的抗体,与偶联磁珠的二抗联合使用。在用NC-1进行免疫筛选后,几乎所有选定的细胞均为NC-1免疫反应性细胞。用针对特定标志物的抗体进行免疫细胞化学鉴定的神经元和神经胶质细胞,在免疫筛选细胞的培养物中优先发育。体外产生的神经元所表达的一些表型适合于肠道(血清素和血管活性肠肽免疫反应性);然而,在培养物中也分化出了肠神经系统中不存在的儿茶酚胺能神经元。层粘连蛋白促进神经元发育以及神经突生长。从胎鼠肠道中用α-110筛选的细胞在体外优先产生神经元和神经胶质细胞。这些数据表明,定植于肠道的嵴衍生细胞群体具有多能性,完整的肠道微环境可阻止儿茶酚胺能神经元在原位发育,层粘连蛋白在肠神经节形成中很重要,并且110 kDa层粘连蛋白结合蛋白在肠神经元和神经胶质细胞的直接前体细胞表面表达。

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