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32细胞期非洲爪蟾胚胎卵裂球的命运

Fates of the blastomeres of the 32-cell-stage Xenopus embryo.

作者信息

Moody S A

出版信息

Dev Biol. 1987 Aug;122(2):300-19. doi: 10.1016/0012-1606(87)90296-x.

Abstract

A detailed fate map of all of the progeny derived from each of the blastomeres of the 32-cell-stage South African clawed frog embryo (Xenopus laevis), which were selected for stereotypic cleavages, is presented. Individual blastomeres were injected with horseradish peroxidase and all of their descendants in the late tailbud embryo (stages 32 to 34) were identified after histochemical processing of serial tissue sections and whole-mount preparations. The progeny of each blastomere were distributed characteristically, both in phenotype and location. Most organs were populated largely by the descendants of particular sets of blastomeres, the progeny of each often being restricted to defined spatial addresses. Thus, the descendants of any one blastomere were distinct and predictable when embryos were preselected for stereotypic cleavages. However, variations among embryos were common and the frequencies with which one may expect organs to contain progeny from any particular blastomere are reported. The differences in the fates of the 16-cell-stage blastomeres and their 32-cell-stage daughter blastomeres are outlined and can be grouped into three general categories. The two daughter cells may give rise to equal numbers of cells in a particular organ, one daughter cell may give rise to many more of the cells in an organ derived from the mother blastomere, or one daughter cell may give rise to all of the progeny in an organ derived from the mother blastomere. Thus, cell fates are segregated during cleavage stages in both symmetric and asymmetric manners, and the lineages exhibit a diversification mode (G. S. Stent, 1985, Philos. Trans R. Soc. London Ser. B 312, 3-19) of cell division.

摘要

本文展示了南非爪蟾胚胎(非洲爪蟾)32细胞期每个卵裂球产生的所有后代的详细命运图谱,这些卵裂球是为典型卵裂而挑选的。对单个卵裂球注射辣根过氧化物酶,并在对连续组织切片和整装标本进行组织化学处理后,识别其在晚期尾芽胚胎(32至34期)中的所有后代。每个卵裂球的后代在表型和位置上均有特征性分布。大多数器官主要由特定卵裂球组产生的后代组成,每组后代通常局限于特定的空间位置。因此,当胚胎被预先选择进行典型卵裂时,任何一个卵裂球的后代都是独特且可预测的。然而,胚胎间差异普遍存在,本文报告了各器官中包含任何特定卵裂球后代的预期频率。概述了16细胞期卵裂球及其32细胞期子卵裂球命运上的差异,这些差异可分为三大类。两个子细胞可能在特定器官中产生等量的细胞,一个子细胞可能在源自母卵裂球的器官中产生更多细胞,或者一个子细胞可能产生源自母卵裂球的器官中的所有后代。因此,细胞命运在卵裂阶段以对称和不对称方式分离,并且谱系呈现出细胞分裂的多样化模式(G. S. 斯滕特,1985年,《伦敦皇家学会哲学学报》B辑312卷,3 - 19页)。

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