在发育过程中,Pax3/Pax7标记了一群新的原始生肌细胞。
Pax3/Pax7 mark a novel population of primitive myogenic cells during development.
作者信息
Kassar-Duchossoy Lina, Giacone Ellen, Gayraud-Morel Barbara, Jory Aurélie, Gomès Danielle, Tajbakhsh Shahragim
机构信息
Department of Developmental Biology, Pasteur Institute, Centre Nationale de la Recherche Scientifique Unité de Recherche Associeé 2578, 75724 Paris, Cedex 15, France.
出版信息
Genes Dev. 2005 Jun 15;19(12):1426-31. doi: 10.1101/gad.345505.
Abstract
Skeletal muscle serves as a paradigm for the acquisition of cell fate, yet the relationship between primitive cell populations and emerging myoblasts has remained elusive. We identify a novel population of resident Pax3+/Pax7+, muscle marker-negative cells throughout development. Using mouse mutants that uncouple myogenic progression, we show that these Pax+ cells give rise to muscle progenitors. In the absence of skeletal muscle, they apoptose after down-regulation of Pax7. Furthermore, they mark the emergence of satellite cells during fetal development, and do not require Pax3 function. These findings identify critical cell populations during lineage restriction, and provide a framework for defining myogenic cell states for therapeutic studies.
摘要
骨骼肌是细胞命运获得的一个范例,然而原始细胞群体与新出现的成肌细胞之间的关系一直难以捉摸。我们在整个发育过程中鉴定出了一群新的常驻Pax3+/Pax7+、肌肉标志物阴性的细胞。利用使成肌进程解偶联的小鼠突变体,我们发现这些Pax+细胞可产生肌肉祖细胞。在没有骨骼肌的情况下,它们在Pax7下调后发生凋亡。此外,它们标志着胎儿发育过程中卫星细胞的出现,并且不需要Pax3发挥功能。这些发现确定了谱系限制过程中的关键细胞群体,并为定义用于治疗研究的成肌细胞状态提供了一个框架。
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