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Trophoblast cell lineage in cloned mouse embryos

机译:克隆小鼠胚胎中的滋养层细胞谱系

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摘要

Most conceptuses derived by somatic cell nuclear transfer (SCNT) in mice undergo developmental arrest as a result of embryonic or extraembryonic defects. Even when fetuses survive to term, prominent placental overgrowth or placentomegaly is often present, indicating that SCNT affects the development of trophoblast cell lineage. The trophoblast cell lineage is established at the blastocyst stage when the stem cell population of the trophoblast cell lineage resides in the polar trophectoderm. Therefore, it is possible that the developmental arrest and placentomegaly that accompany SCNT are induced by insufficient reprogramming of the donor somatic nucleus to enable the cells to acquire full potency as stem cells of the trophoblast cell lineage. Despite the abnormalities of the extraembryonic tissues of SCNT embryos, trophoblast stem (TS) cell lines have been successfully isolated from SCNT blastocysts and their properties appear to be indistinguishable from those of TS cells derived from native blastocysts. This suggests that SCNT does not affect the emergence and autonomous properties of TS cells. In this review, we discuss specification of cell lineage and the extent of reprogramming of TS cells in SCNT blastocysts.
机译:小鼠中大多数由体细胞核转移(SCNT)衍生的概念都由于胚胎或胚外缺陷而发生发育停滞。即使胎儿存活至足月,也经常出现明显的胎盘过度生长或胎盘肥大,这表明SCNT影响滋养层细胞谱系的发育。当滋养层细胞谱系的干细胞群体位于极地滋养外胚层时,滋养层细胞谱系建立在胚泡期。因此,可能是由于供体体细胞核的重新编程不足而导致伴随SCNT的发育停滞和胎盘增大,从而使细胞能够获得作为滋养层细胞谱系干细胞的全部潜能。尽管SCNT胚胎的胚外组织异常,但已成功地从SCNT囊胚中分离出滋养层干(TS)细胞系,并且其性质似乎与源自天然囊胚的TS细胞没有区别。这表明SCNT不会影响TS细胞的出现和自主性。在这篇综述中,我们讨论了细胞谱系的规范以及SCNT胚泡中TS细胞的重编程程度。

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