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Regulation of Satellite Cells During Skeletal Muscle repair and Regeneration.

机译:骨骼肌修复和再生过程中卫星细胞的调节。

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摘要

Postnatal skeletal muscle repair is dependent on the tight regulation of an adult stem cell population known as satellite cells. In response to injury, these quiescent cells are activated, proliferate and express skeletal muscle-specific genes. The majority of satellite cells will fuse to damaged fibers or form new muscle fibers, while a subset will return to a quiescent state, where they are available for future rounds of repair. Robust muscle repair is dependent on the signals that regulate the mutually exclusive decisions of differentiation and self-renewal. A likely candidate for regulating this process is NUMB, an inhibitor of Notch signaling pathway that has been shown to asymmetrically localize in daughter cells undergoing cell fate decisions. In order to study the role of this protein in muscle repair, an inducible knockout of Numb was made in mice. Numb deficient muscle had a defective repair response to acute induced damage as characterized by smaller myofibers, increased collagen deposition and infiltration of fibrotic cells. Satellite cells isolated from Numb-deficient mice show decreased proliferation rates. Subsequent analyses of gene expression demonstrated that these cells had an aberrantly up-regulated Myostatin (Mstn), an inhibitor of myoblast proliferation. Further, this defect could be rescued with Mstn specific siRNAs. These data indicate that NUMB is necessary for postnatal muscle repair and early proliferative expansion of satellite cells. We used an evolutionary compatible to examine processes controlling satellite cell fate decisions, primary satellite cell lines were generated from Anolis carolinensis . This green anole lizard is evolutionarily the closet animal to mammals that forms de novo muscle tissue while undergoing tail regeneration. The mechanism of regeneration in anoles and the sources of stem cells for skeletal muscle, cartilage and nerves are poorly understood. Thus, satellite cells were isolated from A. carolinensis and analyzed for their plasticity. Anole satellite cells show increased plasticity as compared to mouse as determined by expression of key markers specific for bone and cartilage without administration of exogenous morphogens. These novel data suggest that satellite cells might contribute to more than muscle in tail regeneration of A. carolinensis.
机译:出生后骨骼肌的修复取决于对成体干细胞群体(称为卫星细胞)的严格调控。响应损伤,这些静止细胞被激活,增殖并表达骨骼肌特异性基因。大多数卫星细胞将融合到受损的纤维上或形成新的肌肉纤维,而一部分将恢复到静止状态,以备将来的修复之用。健壮的肌肉修复取决于调节分化和自我更新的互斥决策的信号。调节该过程的可能候选药物是NUMB,它是Notch信号通路的抑制剂,已被证明不对称地位于经历细胞命运决定的子代细胞中。为了研究该蛋白在肌肉修复中的作用,在小鼠中诱导了Numb的诱导敲除。麻木不足的肌肉对急性诱发的损伤的修复反应有缺陷,其特征是肌纤维较小,胶原蛋白沉积增加和纤维化细胞浸润。从Numb缺陷小鼠分离的卫星细胞显示出降低的增殖速率。随后的基因表达分析表明,这些细胞具有异常上调的肌生长抑制素(Mstn),一种成肌细胞增殖的抑制剂。此外,可以使用Mstn特异性siRNA挽救该缺陷。这些数据表明,NUMB对于产后肌肉修复和卫星细胞的早期增殖性扩张是必需的。我们使用了进化兼容技术来检查控制卫星细胞命运决定的过程,主要的卫星细胞系是由Anolis carolinensis产生的。这种绿色的蜥蜴在进化上是哺乳动物的壁橱动物,在经历尾巴再生时会形成新的肌肉组织。对于骨骼肌,软骨和神经的肛门再生机制和干细胞来源知之甚少。因此,从卡氏农杆菌分离了卫星细胞并对其可塑性进行了分析。与小鼠相比,Anole卫星细胞显示出增加的可塑性,这是通过对骨和软骨特异的关键标志物的表达而确定的,而无需给予外源性形态发生剂。这些新的数据表明,卫星细胞可能在肌肉中对A. carolinensis的尾巴再生起更多的作用。

著录项

  • 作者

    George, Rajani M.;

  • 作者单位

    Arizona State University.;

  • 授予单位 Arizona State University.;
  • 学科 Biology Molecular.;Biology Cell.
  • 学位 Ph.D.
  • 年度 2012
  • 页码 95 p.
  • 总页数 95
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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