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首页> 外文期刊>Biophysical Journal >Different head environments in tarantula thick filaments support a cooperative activation process
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Different head environments in tarantula thick filaments support a cooperative activation process

机译:狼蛛粗丝中的不同头部环境支持协同激活过程

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摘要

Myosin filaments from many muscles are activated by phosphorylation of their regulatory light chains (RLCs). Structural analysis of relaxed tarantula thick filaments shows that the RLCs of the interacting free and blocked myosin heads are in different environments. This and other data suggested a phosphorylation mechanism in which Ser-35 of the free head is exposed and constitutively phosphorylated by protein kinase C, whereas the blocked head is hidden and unphosphorylated; on activation, myosin light chain kinase phosphorylates the monophosphorylated free head followed by the unphosphorylated blocked head, both at Ser-45. Our goal was to test this model of phosphorylation. Mass spectrometry of quickly frozen, intact muscles showed that only Ser-35 was phosphorylated in the relaxed state. The location of this constitutively phosphorylated Ser-35 was analyzed by immunofluorescence, using antibodies specific for unphosphorylated or phosphorylated Ser-35. In the relaxed state, myofibrils were labeled by anti-pSer-35 but not by anti-Ser-35, whereas in rigor, labeling was similar with both. This suggests that only pSer-35 is exposed in the relaxed state, while in rigor, Ser-35 is also exposed. In the interacting-head motif of relaxed filaments, only the free head RLCs are exposed, suggesting that the constitutive pSer-35 is on the free heads, consistent with the proposed mechanism.
机译:来自许多肌肉的肌球蛋白丝通过其调节轻链(RLC)的磷酸化而被激活。松弛的狼蛛粗细丝的结构分析表明,相互作用的游离和封闭的肌球蛋白头的RLC处于不同的环境中。该数据和其他数据表明了一种磷酸化机制,其中游离头的Ser-35被蛋白激酶C暴露并组成性地磷酸化,而被封闭的头被隐藏且未被磷酸化。激活后,肌球蛋白轻链激酶磷酸化单磷酸化的游离头部,然后磷酸化未磷酸化的封闭头部,两者均在Ser-45处。我们的目标是测试这种磷酸化模型。快速冷冻的完整肌肉的质谱显示,只有Ser-35在松弛状态下被磷酸化。使用对未磷酸化或磷酸化的Ser-35特异的抗体,通过免疫荧光分析该组成性磷酸化的Ser-35的位置。在松弛状态下,肌原纤维被抗pSer-35标记,但没有被抗Ser-35标记,而在严格的条件下,两者的标记相似。这表明在松弛状态下仅暴露pSer-35,而在严格条件下也暴露Ser-35。在松弛长丝的相互作用头基序中,仅自由头的RLC暴露,这表明本构pSer-35位于自由头上,与提出的机制一致。

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