胚胎发育肢体中的细胞死亡。

Scanning microscopy Pub Date : 1995-06-01
J M Hurle, M A Ros, V Garcia-Martinez, D Macias, Y Gañan
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引用次数: 0

摘要

在羊膜脊椎动物中,肢芽的形态和结构的发育伴随着大量中胚层细胞死亡的精确模式,具有凋亡的形态学特征。这些细胞死亡区域似乎消除了仅在肢体发育的有限时间内所需的未分化细胞。在突变物种或实验条件下,当细胞死亡模式被改变时,肢体的骨骼和形态异常就会发生。大多数证据表明,局部触发机制的发生解释了细胞死亡区域的建立和随后细胞死亡基因的激活。细胞外基质的改变和邻近组织对生长因子的贡献的减少似乎是触发细胞死亡程序的最可能的潜在候选因素。关于发育肢体中细胞死亡的遗传基础的信息非常少。在其他细胞死亡系统中发现了越来越多的细胞死亡基因,如p-53和ced-3/ICE和ced-9/ bcl-2基因家族,其中只有bcl-2基因在肢体发育过程中得到了详细的研究,但所获得的信息相互矛盾。Bcl-2在发育肢体的细胞死亡区域不表达,但在Bcl-2基因破坏的小鼠中发育正常肢体。显然,阐明细胞死亡基因的作用是今后肢体发育过程中细胞死亡研究的主要任务。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cell death in the embryonic developing limb.

In amniote vertebrates, the development of form and structure of the limb bud is accompanied by precise patterns of massive mesodermal cell death with morphological features of apoptosis. These areas of cell death appear to eliminate undifferentiated cells which are required only for a limited time period of limb development. Predictable skeletal and morphological anomalies of the limb occur when the pattern of cell death is modified in mutant species or under experimental conditions. Most evidence points to the occurrence of local triggering mechanisms to account for the establishment of the areas of cell death and the subsequent activation of cell death genes. Modifications of the extracellular matrix and diminution in the contribution of growth factors by neighbouring tissues appear as the most likely potential candidates for triggering the cell death program. Information on the genetical basis of cell death in the developing limb is very scarce. Among the increasing number of cell death genes identified in other cell death systems, such as p-53 and the ced-3/ICE and ced-9/ bcl-2 gene families, only bcl-2 has been studied in detail during limb development and yet, the information obtained is contradictory. Bcl-2 is not expressed in the areas of cell death of the developing limb, but normal limbs develop in mice with disruption of the bcl-2 gene. Obviously, the clarification of the role of the cell death genes constitute a major task in future studies of cell death in the developing limb.

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