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Gene expression profiling discerns molecular pathways elicited by ligand signaling to enhance the specification of embryonic stem cells into skeletal muscle lineage

机译:基因表达谱识别配体信号转导的分子途径以增强胚胎干细胞进入骨骼肌谱系的功能

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摘要

Regulation of lineage specification and differentiation in embryonic stem (ES) cells can be achieved through the activation of endogenous signaling, an avenue for potential application in regenerative medicine. During vertebrate development, retinoic acid (RA) plays an important role in body axis elongation and mesoderm segmentation in that graded exposure to RA provides cells with positional identity and directs commitment to specific tissue lineages. Nevertheless, bexarotene, a clinically approved rexinoid, enhances the specification and differentiation of ES cells into skeletal myocytes more effectively than RA. Thus profiling the transcriptomes of ES cells differentiated with bexarotene or RA permits the identification of different genetic targets and signaling pathways that may contribute to the difference of bexarotene and RA in efficiency of myogenesis. Interestingly, bexarotene induces the early expression of a myogenic progenitor marker, Meox1, while the expression of many RA targets is also enhanced by bexarotene. Several signaling molecules involved in the progression of myogenic specification and commitment are differentially regulated by bexarotene and RA, suggesting that early targets of rexinoid allow the coordinated regulation of molecular events which leads to efficient myogenic differentiation in ES cells.
机译:胚胎干细胞(ES)的谱系规范和分化的调控可通过激活内源性信号传导来实现,内源性信号传导是在再生医学中潜在应用的途径。在脊椎动物发育过程中,视黄酸(RA)在体轴延长和中胚层分割中起着重要作用,因为分级暴露于RA可使细胞具有位置同一性,并直接参与特定的组织谱系。然而,贝沙罗汀(一种临床认可的类维生素A)比RA更有效地增强了ES细胞向骨骼肌细胞的分化和分化。因此,对用贝沙罗汀或RA分化的ES细胞的转录组进行谱分析,可以鉴定出不同的遗传靶标和信号通路,这可能会导致贝沙罗汀和RA在成肌效率方面的差异。有趣的是,贝沙罗汀诱导肌成祖标记物Meox1的早期表达,而许多RA靶标的表达也被贝沙罗汀增强。涉及肌原性规范和承诺的进展的几种信号分子受到贝沙罗汀和RA的差异调节,表明类维生素A的早期靶标可对分子事件进行协调调节,从而导致ES细胞有效的肌原性分化。

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