不可存活的人类胚胎植入前作为干细胞研究和潜在治疗的来源。

Mina Alikani, Santiago Munné
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引用次数: 14

摘要

人类胚胎干细胞来源于人类囊胚的内部细胞群。据推测,正常(冷冻/解冻)的人类着床前胚胎在辅助生殖过程中未使用,为干细胞衍生提供了囊胚的主要来源。另外,胚胎是由捐赠的配子产生的,这些配子用于体外受精、囊胚培养和干细胞分离。本文描述了两种先前发表的方法,以及这些方法的背景,这些方法允许使用排除移植和低温保存的不能存活的胚胎作为干细胞的来源。第一种方法的基础是观察到在培养的最初3-5天内分裂异常的胚胎的一些卵裂球在分离状态下可以继续非常有限的发育。当这些卵裂球以嵌合形式聚集时,其中一些卵裂球可以促进正常组织囊胚的形成。这样获得的囊胚提供了从其他不能存活的胚胎到胚胎干细胞的途径。因此,从三体胚胎中获得的囊胚的内细胞团放置在饲养细胞上并再培养7天,随后检查产生的细胞菌落的染色体含量。第二种方法涉及被诊断为特定染色体异常的胚胎,其中许多是与生命不相容的。这些非整倍体中的一些在培养中不妨碍发育到囊胚阶段。这些细胞中有一部分是二体的,培养物显示出表达OCT-4,一种多能细胞的分子标记物。这种明显的三体状态的纠正在一些细胞内的菌落表明胚胎染色体异常与生命不相容可能是人类胚胎干细胞的另一个来源。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Nonviable human pre-implantation embryos as a source of stem cells for research and potential therapy.

Human embryonic stem cells are derived from the inner cell mass of the human blastocyst. Presumably normal (frozen/thawed) human preimplantation embryos that remain unused following assisted reproduction procedures have provided the main source of blastocysts for stem cell derivation. Alternatively, embryos have been generated from gametes donated for the unique purpose of in vitro fertilization, blastocyst culture, and stem cell isolation. This article describes two previously published methods--and the background to those methods--that allow the use of nonviable embryos excluded from transfer and cryopreservation as a source of stem cells. The first method is based on the observation that some blastomeres from embryos with abnormal division during the first 3-5 d in culture can continue very limited development in isolation. When aggregated in a chimaeric form, some of these blastomeres can contribute to the formation of normally organized blastocysts. Blastocysts so obtained provide a route to embryonic stem cells from otherwise nonviable embryos. Thus the inner cell masses of blastocysts obtained from trisomic embryos were placed on feeder cells and cultured for seven additional days, following which the resulting cell colonies were examined for chromosome content. The second method concerns embryos diagnosed with specific chromosome abnormalities many of which are incompatible with life. Some of these aneuploidies do not preclude development to the blastocyst stage in culture. A proportion of these cells were found to be disomic and the cultures were shown to express OCT-4, a molecular marker for pluripotent cells. This apparent correction of the trisomic state in some cells within the colonies suggests that embryos with cromosomal abnormalities incompatible with life may be another source of human embryonic stem cells.

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