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体外对内皮素-3产生反应的神经嵴细胞群体包括多能细胞。

The neural crest population responding to endothelin-3 in vitro includes multipotent cells.

作者信息

Stone J G, Spirling L I, Richardson M K

机构信息

Department of Anatomy and Developmental Biology, St George's Hospital Medical School, London, UK.

出版信息

J Cell Sci. 1997 Jul;110 ( Pt 14):1673-82. doi: 10.1242/jcs.110.14.1673.

Abstract

The peptide endothelin 3 (EDN3) is essential for normal neural crest development in vivo, and is a potent mitogen for quail truncal crest cells in vitro. It is not known which subpopulations of crest cells are targets for this response, although it has been suggested that EDN3 is selective for melanoblasts. In the absence of cell markers for different precursor types in the quail crest, we have characterised EDN3-responsive cell types using in vitro colony assay and clonal analysis. Colonies were analysed for the presence of Schwann cells, melanocytes, adrenergic cells or sensory-like cells. We provide for the first time a description of the temporal pattern of lineage segregation in neural crest cultures. In the absence of exogenous EDN3, crest cells proliferate and then differentiate. Colony assay indicates that in these differentiated cultures few undifferentiated precursors remain and there is a low replating efficiency. By contrast, in the presence of 100 ng/ml EDN3 differentiation is inhibited and most of the cells maintain the ability to give rise to mixed colonies and clones containing neural crest derivatives. A high replating efficiency is maintained. In secondary culture there was a progressive decline in the number of cell types per colony in control medium. This loss of developmental potential was not seen when exogenous EDN3 was present. Cell type analysis suggests two novel cellular targets for EDN3 under these conditions. Contrary to expectations, one is a multipotent precursor whose descendants include melanocytes, adrenergic cells and sensory-like cells; the other can give rise to melanocytes and Schwann cells. Our data do not support previous claims that the action of EDN3 in neural crest culture is selective for cells in the melanocyte lineage.

摘要

肽内皮素3(EDN3)对于体内正常的神经嵴发育至关重要,并且在体外是鹌鹑躯干嵴细胞的一种强效促有丝分裂原。尽管有人提出EDN3对黑素母细胞具有选择性,但尚不清楚嵴细胞的哪些亚群是这种反应的靶标。在鹌鹑嵴中缺乏针对不同前体类型的细胞标记物的情况下,我们使用体外集落测定和克隆分析来表征对EDN3有反应的细胞类型。分析集落中是否存在雪旺细胞、黑素细胞、肾上腺素能细胞或感觉样细胞。我们首次描述了神经嵴培养物中谱系分离的时间模式。在没有外源性EDN3的情况下,嵴细胞增殖然后分化。集落测定表明,在这些分化的培养物中,几乎没有未分化的前体残留,并且再接种效率很低。相比之下,在存在100 ng/ml EDN3的情况下,分化受到抑制,大多数细胞保持产生含有神经嵴衍生物的混合集落和克隆的能力。维持了高再接种效率。在传代培养中,对照培养基中每个集落的细胞类型数量逐渐下降。当存在外源性EDN3时,未观察到这种发育潜能的丧失。细胞类型分析表明在这些条件下EDN3有两个新的细胞靶标。与预期相反,一个是多能前体,其后代包括黑素细胞、肾上腺素能细胞和感觉样细胞;另一个可以产生黑素细胞和雪旺细胞。我们的数据不支持先前关于EDN3在神经嵴培养中的作用对黑素细胞谱系中的细胞具有选择性的说法。

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