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混合谱系白血病 1 抑制通过增加活跃启动子处的 H3K4 单甲基化来增强牛胚胎干细胞的分化潜能。

Mixed-Lineage Leukemia 1 Inhibition Enhances the Differentiation Potential of Bovine Embryonic Stem Cells by Increasing H3K4 Mono-Methylation at Active Promoters.

机构信息

State Key Laboratory of Reproductive Regulation and Breeding of Grassland Livestocks, Inner Mongolia University, Hohhot 010070, China.

出版信息

Int J Mol Sci. 2023 Jul 25;24(15):11901. doi: 10.3390/ijms241511901.

Abstract

Mixed-lineage leukemia 1 (MLL1) introduces 1-, 2- and 3-methylation into histone H3K4 through the evolutionarily conserved set domain. In this study, bovine embryonic stem cells (bESCs, known as bESCs-F7) were established from in vitro-fertilized (IVF) embryos via Wnt signaling inhibition; however, their contribution to the endoderm in vivo is limited. To improve the quality of bESCs, MM-102, an inhibitor of MLL1, was applied to the culture. The results showed that MLL1 inhibition along with GSK3 and MAP2K inhibition (3i) at the embryonic stage did not affect bESCs' establishment and pluripotency. MLL1 inhibition improved the pluripotency and differentiation potential of bESCs via the up-regulation of stem cell signaling pathways such as PI3K-Akt and WNT. MLL1 inhibition decreased H3K4me1 modification at the promoters and altered the distribution of DNA methylation in bESCs. In summary, MLL1 inhibition gives bESCs better pluripotency, and its application may provide high-quality pluripotent stem cells for domestic animals.

摘要

混合谱系白血病 1(MLL1)通过进化上保守的 SET 结构域将 1、2 和 3 个甲基化引入组蛋白 H3K4。在这项研究中,通过 Wnt 信号抑制,从体外受精 (IVF) 胚胎中建立了牛胚胎干细胞 (bESC,称为 bESCs-F7);然而,它们在体内对内胚层的贡献是有限的。为了提高 bESC 的质量,应用了 MLL1 抑制剂 MM-102。结果表明,胚胎期抑制 MLL1 以及 GSK3 和 MAP2K 抑制 (3i) 并不影响 bESC 的建立和多能性。通过上调干细胞信号通路(如 PI3K-Akt 和 WNT),MLL1 抑制可提高 bESC 的多能性和分化潜能。MLL1 抑制降低了启动子处的 H3K4me1 修饰,并改变了 bESC 中 DNA 甲基化的分布。总之,MLL1 抑制赋予 bESC 更好的多能性,其应用可为家畜提供高质量的多能干细胞。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ca3f/10418322/d512b18c93ce/ijms-24-11901-g001.jpg

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