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成人体咬肌卫星细胞的不均一性及其向心肌细胞分化的潜能。

Heterogeneity of adult masseter muscle satellite cells with cardiomyocyte differentiation potential.

机构信息

Department of Pathology and Laboratory Medicine, University of Cincinnati College of Medicine, Cincinnati, OH, USA.

Department of Anesthesiology, University of Cincinnati College of Medicine, Cincinnati, OH, USA.

出版信息

Exp Cell Res. 2018 Oct 1;371(1):20-30. doi: 10.1016/j.yexcr.2018.05.028. Epub 2018 May 26.

Abstract

Although resident cardiac stem cells have been reported, regeneration of functional cardiomyocytes (CMs) remains a challenge. The present study identifies an alternative progenitor source for CM regeneration without the need for genetic manipulation or invasive heart biopsy procedures. Unlike limb skeletal muscles, masseter muscles (MM) in the mouse head are developed from Nkx2-5 mesodermal progenitors. Adult masseter muscle satellite cells (MMSCs) display heterogeneity in developmental origin and cell phenotypes. The heterogeneous MMSCs that can be characterized by cell sorting based on stem cell antigen-1 (Sca1) show different lineage potential. While cardiogenic potential is preserved in Sca1 MMSCs as shown by expression of cardiac progenitor genes (including Nkx2-5), skeletal myogenic capacity is maintained in Sca1 MMSCs with Pax7 expression. Sca1 MMSC-derived beating cells express cardiac genes and exhibit CM-like morphology. Electrophysiological properties of MMSC-derived CMs are demonstrated by calcium transients and action potentials. These findings show that MMSCs could serve as a novel cell source for cardiomyocyte replacement.

摘要

尽管已有报道称存在驻留心脏干细胞,但功能性心肌细胞(CM)的再生仍然是一个挑战。本研究确定了一种替代祖细胞来源,用于 CM 再生,而无需遗传操作或侵入性心脏活检程序。与肢体骨骼肌不同,小鼠头部的咬肌(MM)是由 Nkx2-5 中胚层祖细胞发育而来。成年咬肌卫星细胞(MMSC)在发育起源和细胞表型上具有异质性。基于干细胞抗原-1(Sca1)的细胞分选可以对异质性 MMSC 进行特征描述,显示出不同的谱系潜能。虽然 Sca1 MMSC 中保留了心脏祖细胞基因(包括 Nkx2-5)表达的心脏发生潜能,但具有 Pax7 表达的 Sca1 MMSC 保持了骨骼肌生成能力。Sca1 MMSC 衍生的搏动细胞表达心脏基因,并表现出 CM 样形态。通过钙瞬变和动作电位证明了 MMSC 衍生的 CM 的电生理特性。这些发现表明,MMSC 可以作为心肌细胞替代的新型细胞来源。

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