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Tristetraprolin regulation of MyoD mRNA stability commits quiescent adult muscle stem cells to myogenesis.

机译：Tristetraprolin对MyoD mRNA稳定性的调节使静止的成年肌肉干细胞发生肌生成。

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In animals, tissue maintenance, plasticity and repair rely on adult stem cells which have been identified in nearly all tissues. Many adult stem cells are typically quiescent and only activate when required for maintenance and repair of adult tissues. Within hours of activation skeletal muscle stem cells called satellite cells begin to express MyoD, a muscle-specific transcription factor that functions as a master regulator, committing satellite cells to myogenesis. The earliest detectable event in satellite cells following muscle injury is phosphorylation of p38alpha/beta MAPKs, which is required for MyoD induction and cell-cycle entry. Loss of Syndecan-4, a component of the satellite cell niche disrupts p38alpha/beta MAPK activation and severely delays MyoD induction. We performed a microarray gene chip experiment to identify genes expressed during satellite cell activation. We identified differentially expressed genes by subtracting genes changing in Sdc4-/- satellite cells from those changing in WT satellite cells following 12h of muscle injury. Unexpectedly, we observed that 70% of RNA-binding proteins (RNA-BPs) decreased in activated satellite cells. Expression levels of the Tristetraprolin (TTP) family of RNA-BPs declined dramatically as satellite cells activated. The TTP family is known to direct mRNA decay and we identified the 3'UTR of MyoD as a direct TTP target. Furthermore, p38alpha/beta MAPK signaling inhibits TTP-mediated mRNA decay in satellite cells. HuR, an RNA-BP that is induced during satellite cell activation is known to stabilize MyoD mRNA. The coordinate inhibition of TTP and induction of HuR may together function as a feed-forward loop to commit satellite cells to myogenesis by rapid induction of MyoD. A similar feed-forward circuit could operate in other stem cell systems, implicating that post-transcriptional regulation of mRNA could play a major role in regulating adult stem cells to maintain and repair adult tissues.

机译：在动物中，组织的维持，可塑性和修复依赖于几乎在所有组织中均已鉴定的成体干细胞。许多成人干细胞通常处于静止状态，仅在需要维护和修复成人组织时才激活。在激活后的几小时内，称为卫星细胞的骨骼肌干细胞开始表达MyoD，这是一种肌肉特异性转录因子，起着主要调节器的作用，使卫星细胞参与肌发生。肌肉损伤后卫星细胞中最早可检测到的事件是p38alpha / beta MAPKs的磷酸化，这是MyoD诱导和细胞周期进入所必需的。 Syndecan-4（卫星细胞小生境的一个组成部分）的丢失会破坏p38alpha / beta MAPK激活并严重延迟MyoD的诱导。我们进行了微阵列基因芯片实验，以鉴定在卫星细胞激活过程中表达的基因。通过从肌肉损伤12小时后WT卫星细胞中变化的基因中减去Sdc4-/-卫星细胞中变化的基因，我们鉴定出差异表达的基因。出乎意料的是，我们观察到70％的RNA结合蛋白（RNA-BPs）在活化的卫星细胞中减少。随着卫星细胞的活化，Tristetraprolin（TTP）RNA-BPs家族的表达水平急剧下降。已知TTP家族指导mRNA衰变，我们将MyoD的3'UTR确定为直接TTP靶标。此外，p38alpha / beta MAPK信号传导抑制卫星细胞中TTP介导的mRNA衰变。 HuR是一种在卫星细胞激活过程中诱导的RNA-BP，可稳定MyoD mRNA。 TTP的协调抑制和HuR的诱导可能一起起前馈回路的作用，通过快速诱导MyoD使卫星细胞发生肌发生。类似的前馈电路也可以在其他干细胞系统中运行，这意味着转录后调节mRNA可能在调节成体干细胞以维持和修复成体组织中起主要作用。

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作者
Hausburg, Melissa Ann.;
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作者单位

University of Colorado at Boulder.;

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授予单位 University of Colorado at Boulder.;
学科 Molecular biology.;Health sciences.
学位 Ph.D.
年度 2010
页码 154 p.
总页数 154
原文格式 PDF
正文语种 eng
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专利

1. The 2′-5′ Oligoadenylate/RNase L/RNase L Inhibitor Pathway Regulates Both MyoD mRNA Stability and Muscle Cell Differentiation [J] . C. Bisbal, M. Silhol, H. Laubenthal, Molecular and Cellular Biology . 2000,第14期

机译：2'-5'寡腺苷酸/ RNase L / RNase L抑制剂途径调节MyoD mRNA稳定性和肌肉细胞分化
2. Isoeugenol destabilizes IL-8 mRNA expression in THP-1 cells through induction of the negative regulator of mRNA stability tristetraprolin [J] . GalbiatiV., CarneA., MitjansM., Archives of Toxicology . 2012,第2期

机译：异丁香酚通过诱导mRNA稳定性tristetraprolin负调节剂破坏THP-1细胞中IL-8 mRNA的表达
3. Isoeugenol destabilizes IL-8 mRNA expression in THP-1 cells through induction of the negative regulator of mRNA stability tristetraprolin [J] . Valentina Galbiati, Alice Carne, Montserrat Mitjans, Archives of Toxicology . 2012,第2期

机译：异丁香酚通过诱导mRNA稳定性tristetraprolin负调节剂来破坏THP-1细胞中IL-8 mRNA的表达
4. Regulation of the stability of m2-cholinergic receptor mRNA in CHO-m2 cells by ZDY101 [C] . The First China-Japan-Korea conference of nuclear medicine . 2002

机译：ZDY101调节CHO-m2细胞中m2-胆碱能受体mRNA的稳定性
5. Skeletal Muscle Satellite Cells Have a MyoD-Positive Developmental Origin and Activated MyoD-Positive Satellite Cells Maintain Their Self-renewal Capacity during Adult Muscle Regeneration. [D] . Kanisicak, Onur. 2011

机译：骨骼肌卫星细胞具有MyoD阳性发育起源，而活化的MyoD阳性卫星细胞在成年肌肉再生过程中保持其自我更新能力。
6. The 2′-5′ Oligoadenylate/RNase L/RNase L Inhibitor Pathway Regulates Both MyoD mRNA Stability and Muscle Cell Differentiation [O] . C. Bisbal, M. Silhol, H. Laubenthal, 1993

机译：2'-5'寡腺苷酸/ RNase L / RNase L抑制剂通路调节MyoD mRNA稳定性和肌肉细胞分化
7. Tristetraprolin Regulation of MyoD mRNA Stability Commits Quiescent Adult Muscle Stem Cells to Myogenesis [O] . Hausburg Melissa Ann 2010

机译：Tristetraprolin对MyoD mRNA稳定性的调节使静止的成年肌肉干细胞新生。
8. Regulation of Estrogen Receptor mRNA Stability in Human Breast Cancer Cells [R] . DiPippo, V. A. 1998

机译：人乳腺癌细胞雌激素受体mRNa稳定性的调节

Tristetraprolin regulation of MyoD mRNA stability commits quiescent adult muscle stem cells to myogenesis.

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