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A high-throughput siRNA library screen identifies osteogenic suppressors in human mesenchymal stem cells

机译:高通量siRNA文库筛选可鉴定人间充质干细胞中的成骨抑制因子

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Tissue-specific (or adult) stem/progenitor cells are regarded as the source for normal tissue homeostasis and tissue repair. They also provide tremendous promise for regenerative medicine because of their capacity to proliferate and differentiate into a variety of mature cell types. Human mesenchymal stem cells (hMSCs) can differentiate into osteocytes, adipocytes, chondrocytes, muscle cells, and neurons. However, the molecular mechanisms underlying these differentiation processes are poorly understood. We screened a synthetic siRNA library targeting 5,000 human genes to identify the endogenous repressors of osteogenic specification, which when silenced could initiate differentiation of hMSCs into osteoblasts. This screen yielded 53 candidate suppressors, and 12 of those were further confirmed for their dynamic roles in suppressing osteogenic specification in hMSCs. Furthermore, cAMP was identified to play opposing roles in osteogenesis vs. adipo-genesis. This study provides a basis for further elucidation of the genetic network controlling osteogenesis and, potentially, the molecular rationale for treating bone diseases.
机译:组织特异性(或成年)干/祖细胞被认为是正常组织动态平衡和组织修复的来源。由于它们具有增殖和分化成多种成熟细胞类型的能力,它们还为再生医学提供了巨大的希望。人间充质干细胞(hMSCs)可以分化为骨细胞,脂肪细胞,软骨细胞,肌肉细胞和神经元。但是,这些分化过程的分子机制了解得很少。我们筛选了针对5,000个人类基因的合成siRNA文库,以鉴定成骨规范的内源性阻遏物,如果沉默,则可以启动hMSC分化为成骨细胞。该筛选产生了53种候选抑制子,其中12种在抑制hMSCs成骨特性方面的动态作用被进一步证实。此外,已确定cAMP在成骨和脂肪形成中起相反的作用。该研究为进一步阐明控制成骨的遗传网络以及潜在地治疗骨疾病的分子原理提供了基础。

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