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Chemical Enhancement in Embryo Development and Stem Cell Derivation from Single Blastomeres

机译:单个卵裂球的胚胎发育和干细胞衍生过程中的化学增强作用

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摘要

Several chemicals targeting the mitogen-activated protein (MAP) kinase signaling pathway, which play an important role in regulating cell growth and differentiation, have shown enhancing effects on the development of the inner cell mass (ICM) and the derivation of ES cells. However, investigation of such chemicals on early embryonic development and the establishment of ES cell lines has not been elucidated. This study was aimed to determine if ACTH, MAP2K1 inhibitor [MAP2K1 (I)], and MAPK14 inhibitor [MAPK14 (I)] could enhance the development of the ICM in preimplantation mouse embryos and blastocyst outgrowths, and the establishment of ES cell lines from blastomeres of early embryos. We have demonstrated that both MAP2K1 (I) and MAPK14 (I) delay early embryo development and inhibit the development of embryos from early blastomeres. On the other hand, ACTH had a positive effect on embryos derived from early blastomeres. As a result, 17 ES cell lines were established. Among these ES cell lines, nine and five ES cell lines were established from single blastomeres of two-cell embryos with and without the supplement of ACTH, respectively. In addition to two-cell isolated blastomeres, three ES cell lines were established from blastomeres of four-cell embryos only with the supplement of ACTH. Our results suggest that ACTH can enhance the derivation of ES cells from single blastomere-derived embryos.
机译:几种靶向有丝分裂原活化蛋白(MAP)激酶信号通路的化学物质在调节细胞生长和分化中起着重要作用,它们显示出对内细胞团(ICM)发育和ES细胞衍生的增强作用。然而,尚未阐明对此类化学物质在早期胚胎发育和ES细胞系建立方面的研究。这项研究旨在确定ACTH,MAP2K1抑制剂[MAP2K1(I)]和MAPK14抑制剂[MAPK14(I)]是否可以增强植入前小鼠胚胎和胚泡生长中ICM的发育,以及建立ES细胞系的方法。早期胚胎的卵裂球。我们已经证明,MAP2K1(I)和MAPK14(I)都延迟了早期胚胎发育并抑制了来自早期卵裂球的胚胎发育。另一方面,ACTH对源自早期卵裂球的胚胎具有积极作用。结果,建立了17个ES细胞系。在这些ES细胞系中,分别从具有和不具有ACTH的两细胞胚胎的单个卵裂球中建立了9个和5个ES细胞系。除了两细胞分离的卵裂球外,仅在添加了ACTH的情况下,由四细胞胚胎的卵裂球建立了三个ES细胞系。我们的结果表明,ACTH可以增强单个卵裂球来源的胚胎中ES细胞的衍生。

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