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首页> 外文期刊>Journal of Muscle Research and Cell Motility >The sarcomeric M-band during development and in disease
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The sarcomeric M-band during development and in disease

机译:发育中和疾病中的肌节M带

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摘要

The C-terminus of connectin/titin at the M-band of the sarcomere interacts with several structural as well as potential signalling proteins. One of these is myomesin, which can also bind to myosin and has been suggested to function as an integral structural linker of the thick filaments into the sarcomere. Recent evidence that myomesin possesses the ability to form antiparallel dimers via its C-terminal domain has prompted us to propose a novel three-dimensional model for the sarcomeric M-band. A splice variant of myomesin, termed EH-myomesin, contains an additional segment that has disordered conformation and functions as an entropic spring. It is expressed in a subset of muscle types that are characterised by a broader operational range and are more resistant to damage caused by eccentric contraction. In addition, it is also re-expressed in dilated cardiomyopathy. DRAL/FHL-2 is another protein that interacts with the M-band portion of connectin/titin and which probably functions as an adaptor for the compartmentalisation of metabolic enzymes. Together these results suggest that the M-band is crucial for sarcomere function and maintenance and that its molecular composition can be adapted to divergent physiological needs in different muscle types, which may help to cope with pathological alterations.
机译:在肌节的M带,连接素/ titin的C-末端与几种结构以及潜在的信号蛋白相互作用。其中之一是肌球蛋白,它也可以与肌球蛋白结合,并被建议作为肌节中粗丝的整体结构连接子。最近的证据表明,肌细胞分裂素具有通过其C末端结构域形成反平行二聚体的能力,这促使我们为肌节M带提出了一个新颖的三维模型。肌球蛋白的剪接变体,称为EH-肌球蛋白,包含一个附加的片段,该片段具有无序的构象并起着熵的作用。它以一组更广泛的操作范围且对偏心收缩引起的损伤更具有抵抗力的肌肉类型的子集表达。另外,它在扩张型心肌病中也重新表达。 DRAL / FHL-2是与connectin / titin的M带部分相互作用的另一种蛋白,可能充当代谢酶区室化的衔接子。这些结果共同表明,M带对肌节功能和维持至关重要,其分子组成可以适应不同肌肉类型的生理需求,这可能有助于应对病理变化。

著录项

  • 来源
    《Journal of Muscle Research and Cell Motility 》 |2005年第8期| 375-379| 共5页
  • 作者单位

    The Randall Division of Cell Molecular Biophysics and the Cardiovascular Division King’s College LondonInstitute of Cell Biology ETH Zurich-Honggerberg;

    Institute of Cell Biology ETH Zurich-Honggerberg;

    Institute of Cell Biology ETH Zurich-Honggerberg;

    The Randall Division of Cell Molecular Biophysics and the Cardiovascular Division King’s College London;

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