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DNA synthesis is required for reprogramming mediated by stem cell fusion

机译:DNA合成是干细胞融合介导的重编程所必需的

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Embryonic stem cells (ESCs) can instruct the conversion of differentiated cells toward pluripotency following cell-to-cell fusion by a mechanism that is rapid but poorly understood. Here, we used centrifugal elutriation to enrich for mouse ESCs at sequential stages of the cell cycle and showed that ESCs in S/G2 phases have an enhanced capacity to dominantly reprogram lymphocytes and fibroblasts in heterokaryon and hybrid assays. Reprogramming success was associated with an ability to induce precocious nucleotide incorporation within the somatic partner nuclei in heterokaryons. BrdU pulse-labeling experiments revealed that virtually all successfully reprogrammed somatic nuclei, identified on the basis of Oct4 re-expression, had undergone DNA synthesis within 24 hr of fusion with ESCs. This was essential for successful reprogramming because drugs that inhibited DNA polymerase activity effectively blocked pluripotent conversion. These data indicate that nucleotide incorporation is an early and critical event in the epigenetic reprogramming of somatic cells in experimental ESC-heterokaryons.
机译:胚胎干细胞(ESC)可以通过快速但了解甚少的机制指示细胞间融合后分化的细胞向多能性转化。在这里,我们使用离心淘析来富集小鼠周期细胞周期中的小鼠胚胎干细胞,并表明S / G2期的胚胎干细胞具有增强的能力,可以在异核和杂交试验中显着地重编程淋巴细胞和成纤维细胞。重新编程的成功与诱导异核体的体细胞伴侣核内早熟核苷酸掺入的能力有关。 BrdU脉冲标记实验表明,实际上所有成功重编程的体细胞核(根据Oct4重新表达确定)都在与ESC融合后24小时内进行了DNA合成。这对于成功进行重新编程至关重要,因为抑制DNA聚合酶活性的药物可有效阻断多能转化。这些数据表明核苷酸掺入是实验性ESC杂核中体细胞表观遗传重编程的早期和关键事件。

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