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丙戊酸中的神经嵴细胞运动性

Neural crest cell motility in valproic acid.

作者信息

Fuller Leah C, Cornelius Shannon K, Murphy Charles W, Wiens Darrell J

机构信息

Department of Biology, University of Northern Iowa, Cedar Falls, IA 50614, USA.

出版信息

Reprod Toxicol. 2002 Nov-Dec;16(6):825-39. doi: 10.1016/s0890-6238(02)00059-x.

Abstract

Neural crest cells (NCCs) exit the dorsal neural tube and migrate to sites where they form diverse tissues. Valproic acid (VPA) is an anticonvulsant drug that induces neural tube and related defects. Altered NCC migration and proliferation have been proposed as mechanisms of teratogenicity. We cultured neural tube segments from chick embryos in 0.75-3.0mM VPA. We used image analysis, proliferation assays, and fluorescence localization to investigate NCCs during VPA exposure. VPA inhibited attachment of explants and the number that produced migrating cells. VPA markedly decreased the proportion of cells migrating individually, promoting migration as epithelial sheets. VPA at 3mM decreased cellular spreading. Area and perimeter change per minute were reduced, but migration velocity was not. VPA at 2mM reduced proliferation 11% and 3mM arrested proliferation. Immunostaining of VPA-exposed explants revealed N-cadherin-positive cell boundaries within sheets, but independent NCCs did not stain. F-actin staining was reduced in independent NCCs. The data support a VPA mechanism involving interference with epithelial-mesenchymal transition.

摘要

神经嵴细胞(NCCs)离开背侧神经管并迁移至形成多种组织的部位。丙戊酸(VPA)是一种诱导神经管及相关缺陷的抗惊厥药物。NCC迁移和增殖的改变已被认为是致畸性的机制。我们将鸡胚神经管节段培养于0.75 - 3.0 mM的VPA中。我们使用图像分析、增殖测定和荧光定位来研究VPA暴露期间的NCCs。VPA抑制外植体的附着以及产生迁移细胞的数量。VPA显著降低单个迁移细胞的比例,促进细胞作为上皮片层迁移。3 mM的VPA降低细胞铺展。每分钟的面积和周长变化减少,但迁移速度未受影响。2 mM的VPA使增殖降低11%,3 mM时则使增殖停滞。对暴露于VPA的外植体进行免疫染色显示,片层内有N - 钙黏蛋白阳性的细胞边界,但独立的NCCs未染色。独立NCCs中的F - 肌动蛋白染色减少。这些数据支持VPA的一种涉及干扰上皮 - 间充质转化的机制。

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