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Extrinsic regulation of satellite cell specification

机译:卫星小区规范的外部规定

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摘要

Cellular commitment during vertebrate embryogenesis is controlled by an interplay of intrinsic regulators and morphogenetic signals. These mechanisms recruit a subset of cells in the developing organism to become the ancestors of skeletal muscle. Signals that control progression through the myogenic lineage converge on a battery of hierarchically organized transcription factors which modulate the cells to either remain in a primitive state or allow their commitment and differentiation into skeletal muscle fibers. A small population of cells will retain a largely unspecified state throughout development. Such stem cells, in conjunction with more committed myogenic progenitors, form a heterogeneous population that colonizes adult skeletal muscle as satellite cells. The satellite cell pool is responsible for the remarkable regenerative capacity of skeletal muscle. Similar to their counterparts during embryonic development, satellite cells are capable of self-renewal and can give rise to myogenic progeny. Impaired satellite cell homeostasis has been associated with numerous muscular disorders. Due to intense research efforts in the past two decades, the complex biology of muscle stem cells has now revealed some of its secrets and new avenues for the development of therapeutic molecules have emerged. In the present review we focus on the extrinsic mechanisms that control self-renewal, specification and differentiation of satellite cells and their significance for the development of biologic drugs.
机译:脊椎动物胚胎发生过程中的细胞定向受内在调节因子和形态发生信号的相互作用控制。这些机制在发育中的生物体中募集了一部分细胞,成为骨骼肌的祖先。通过成肌谱系控制进展的信号汇聚在一系列有序组织的转录因子上,这些转录因子调节细胞以使其保持原始状态或使其定向并分化为骨骼肌纤维。一小部分细胞将在整个发育过程中保持很大程度上未指定的状态。此类干细胞与更坚定的成肌祖细胞一起形成异质群体,该群体定居在成年骨骼肌中作为卫星细胞。卫星细胞池负责骨骼肌的显着再生能力。类似于胚胎发育过程中的对应物,卫星细胞具有自我更新的能力,并可以引起成肌后代。卫星细胞动态平衡受损与许多肌肉疾病有关。由于过去二十年来的大量研究工作,肌肉干细胞的复杂生物学现已揭示出它的一些秘密,并出现了开发治疗性分子的新途径。在当前的审查中,我们专注于控制卫星细胞自我更新,规范和分化的外在机制及其对生物药物开发的意义。

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