首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >ROLE OF ESSENTIAL LIGHT CHAIN EF HAND DOMAINS IN CALCIUM BINDING AND REGULATION OF SCALLOP MYOSIN
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ROLE OF ESSENTIAL LIGHT CHAIN EF HAND DOMAINS IN CALCIUM BINDING AND REGULATION OF SCALLOP MYOSIN

机译:基本光链手域在钙结合和扇贝肌球蛋白调控中的作用

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摘要

The specific Ca2+ binding site that triggers contraction of molluscan muscle requires the presence of an essential light chain (ELC) from a Ca2+ binding myosin. Of the four EF hand-like domains in molluscan ELCs, only domain III has an amino acid sequence predicted to be capable of binding Ca2+. In this report, we have used mutant ELCs to locate the Ca2+ binding site in scallop myosin and to probe the role of the ELC in regulation. Point mutations in domain III of scallop ELC have no effect on Ca2+ binding. Interestingly, scallop and rat cardiac ELC chimeras support Ca2+ binding only if domain I is scallop. These results are nevertheless in agreement with structural studies on a proteolytic fragment of scallop myosin, the regulatory domain. Furthermore, Ca2+ sensitivity of the scallop myosin ATPase requires scallop FLC domain I: ELCs containing cardiac domain I convert scallop myosin to an unregulated molecule whose activity is no longer repressed in the absence of Ca2+. Despite its unusual EF hand domain sequence, our data indicate that the unique and required contribution of molluscan ELCs to Ca2+ binding and regulation of molluscan myosins resides exclusively in domain I. [References: 37]
机译:触发软体动物肌肉收缩的特定Ca2 +结合位点需要存在来自Ca2 +结合肌球蛋白的必需轻链(ELC)。在软体动物ELC中的四个EF手状结构域中,只有结构域III的氨基酸序列预计能够结合Ca2 +。在本报告中,我们已使用突变型ELC在扇贝肌球蛋白中定位Ca2 +结合位点,并探讨了ELC在调节中的作用。扇贝ELC结构域III中的点突变对Ca2 +结合没有影响。有趣的是,仅当结构域I是扇贝时,扇贝和大鼠心脏ELC嵌合体才支持Ca2 +结合。然而,这些结果与对扇贝肌球蛋白(调节域)的蛋白水解片段的结构研究一致。此外,扇贝肌球蛋白ATPase的Ca2 +敏感性需要扇贝FLC结构域I:包含心脏结构域I的ELC将扇贝肌球蛋白转变为不受调控的分子,其活性在没有Ca2 +的情况下不再受到抑制。尽管它具有异常的EF手域序列,但我们的数据表明,软体动物ELC对Ca2 +结合和软体动物肌球蛋白的调控的独特而必要的贡献仅存在于域I中。[参考文献:37]

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