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Efficient endoderm induction from human pluripotent stem cells by logically directing signals controlling lineage bifurcations

机译:通过逻辑指导控制谱系分支的多能干细胞有效诱导内胚层

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Human pluripotent stem cell (hPSC) differentiation typically yields heterogeneous populations. Knowledge of signals controlling embryonic lineage bifurcations could efficiently yield desired cell types through exclusion of alternate fates. Therefore, we revisited signals driving induction and anterior-posterior patterning of definitive endoderm to generate a coherent roadmap for endoderm differentiation. With striking temporal dynamics, BMP and Wnt initially specified anterior primitive streak (progenitor to endoderm), yet, 24 hr later, suppressed endoderm and induced mesoderm. At lineage bifurcations, cross-repressive signals separated mutually exclusive fates; TGF-β and BMP/MAPK respectively induced pancreas versus liver from endoderm by suppressing the alternate lineage. We systematically blockaded alternate fates throughout multiple consecutive bifurcations, thereby efficiently differentiating multiple hPSC lines exclusively into endoderm and its derivatives. Comprehensive transcriptional and chromatin mapping of highly pure endodermal populations revealed that endodermal enhancers existed in a surprising diversity of "pre-enhancer" states before activation, reflecting the establishment of a permissive chromatin landscape as a prelude to differentiation.
机译:人多能干细胞(hPSC)分化通常产生异质群体。通过排除其他命运,控制胚胎谱系分支的信号知识可以有效产生所需的细胞类型。因此,我们重新审视了驱动定型内胚层的诱导和前后模式的信号,以生成内胚层分化的连贯路线图。随着惊人的时间动态,BMP和Wnt最初指定了前原始条纹(内胚层的祖细胞),然而24小时后,其抑制了内胚层并诱导了中胚层。在谱系分叉处,交叉抑制信号将相互排斥的命运分开。 TGF-β和BMP / MAPK通过抑制交替谱系分别从内胚层诱导胰腺对肝脏。我们系统性地阻断了多个连续分叉过程中的交替命运,从而有效地将多个hPSC系专门区分为内胚层及其衍生物。对高纯度内胚层种群进行全面的转录和染色质图谱分析后发现,内胚层增强剂在激活前以令人惊讶的“增强前”状态存在,反映出允许的染色质景观建立是分化的前奏。

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