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The mode and molecular mechanisms of the migration of presumptive PGC in the endoderm cell mass of Xenopus embryos

机译:推测性PGC在非洲爪蟾胚胎内胚层细胞团中迁移的模式和分子机制

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摘要

We investigated the mode of migration of presumptive primordial germ cells (pPGC) in the endoderm cell mass of Xenopus embryos at stages 7-40. The molecules underlying the migration were also studied cytochemically and immunocytologically. By examining the relative positions of pPGC and somatic cells derived from the single, fluorescein-dextran lysine (FDL)-injected, germ plasm-bearing cells of stage 6 embryos, pPGC in embryos at stages 7-23 and those at stages later than 24 were assumed to passively and actively migrate in the endoderm cell mass, respectively. This assumption was supported by the observation that F-actin, essential for active cell migration, was recognized on pPGC of the latter stages, but never on those of the former ones. In addition, the molecule like CXC chemokine receptor 4 (CXCR4) found on directionally migrating PGC in mouse and zebrafish, probably Xenopus CXCR4 (xCXCR4), was detected on pPGC only at latter stages. Accordingly, F-actin and xCXCR4, and probably beta1-integrin and collagen type IV, which are indispensable for the formation of F-actin, are thought to be involved in the active migration of pPGC in the endoderm cell mass.
机译:我们调查了非洲爪蟾胚胎内胚层细胞团中第7-40阶段推测性原始生殖细胞(pPGC)的迁移模式。还对迁移的基础分子进行了细胞化学和免疫细胞学研究。通过检查pPGC和体细胞的相对位置,这些体细胞来自单个荧光素-葡聚糖-赖氨酸(FDL)注射的6期胚胎的带有种质的细胞,pPGC在7-23期和24以后的胚胎中假定它们分别在内胚层细胞团中被动和主动迁移。这一假设得到以下观察结果的支持:对于活跃细胞迁移至关重要的F-肌动蛋白在后一阶段的pPGC上被识别,而在前一阶段则未被识别。此外,在小鼠和斑马鱼的定向迁移PGC中发现的类似CXC趋化因子受体4(CXCR4)的分子,可能是非洲爪蟾CXCR4(xCXCR4),仅在后期才在pPGC上被检测到。因此,认为F-肌动蛋白和xCXCR4以及可能的β1-整合素和IV型胶原蛋白对于形成F-肌动蛋白是必不可少的,它们参与了内胚层细胞团中pPGC的主动迁移。

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