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核苷酸结合位点附近表面环区的序列变异调节软体动物肌球蛋白的ATP转换速率。

Sequence variations in the surface loop near the nucleotide binding site modulate the ATP turnover rates of molluscan myosins.

作者信息

Perreault-Micale C L, Kalabokis V N, Nyitray L, Szent-Györgyi A G

机构信息

Department of Biology, Brandeis University, Waltham, MA 02254-9110, USA.

出版信息

J Muscle Res Cell Motil. 1996 Oct;17(5):543-53. doi: 10.1007/BF00124354.

DOI:10.1007/BF00124354
PMID:8906622
Abstract

The muscle and species-specific differences in enzymatic activity between Placopecten and Argopecten striated and catch muscle myosins are attributable to the myosin heavy chain. To identify sequences that may modulate these differences, we cloned and sequenced the cDNA encoding the myosin heavy chains of Placopecten striated and catch muscle. Deduced protein sequences indicate two similar isoforms in catch and striated myosins (97% identical); variations arise by differential RNA splicing of five alternative exons from a single myosin heavy chain gene. The first encodes the phosphate-binding loop; the second, part of the ATP binding site; the third, part of the actin binding site; the fourth, the hinge in the rod; and the fifth, a tailpiece found only in the catch muscle myosin heavy chain. Both Placopecten myosin heavy chains are 96% identical to Argopecten myosin heavy chaina isoforms. Because subfragment-1 ATPase activities reflect the differences observed in the parent myosins, the motor domain is responsible for the variations in ATPase activities. In addition, data show that differences are due to Vmax and not actin affinity. The sequences of all four myosin heavy chain motor domains diverge only in the flexible surface loop near the nucleotide binding pocket. Thus, the different ATPase activities of four molluscan muscle myosins are likely due to myosin heavy chain sequence variations within the flexible surface loop that forms part of the ATP binding pocket of the motor domain.

摘要

扇贝和海湾扇贝横纹肌与抓肌肌球蛋白之间酶活性的肌肉和物种特异性差异归因于肌球蛋白重链。为了鉴定可能调节这些差异的序列,我们克隆并测序了编码扇贝横纹肌和抓肌肌球蛋白重链的cDNA。推导的蛋白质序列表明抓肌和横纹肌肌球蛋白中有两种相似的同工型(97%相同);差异源于单个肌球蛋白重链基因的五个可变外显子的不同RNA剪接。第一个可变外显子编码磷酸结合环;第二个编码ATP结合位点的一部分;第三个编码肌动蛋白结合位点的一部分;第四个编码杆状结构中的铰链区;第五个编码仅在抓肌肌球蛋白重链中发现的尾段。两种扇贝肌球蛋白重链与海湾扇贝肌球蛋白重链同工型的同源性均为96%。由于亚片段-1 ATP酶活性反映了在亲本肌球蛋白中观察到的差异,因此运动结构域是ATP酶活性变化的原因。此外,数据表明差异是由于最大反应速度(Vmax)而非肌动蛋白亲和力。所有四种肌球蛋白重链运动结构域的序列仅在核苷酸结合口袋附近的柔性表面环处存在差异。因此,四种软体动物肌肉肌球蛋白不同的ATP酶活性可能是由于运动结构域ATP结合口袋一部分的柔性表面环内的肌球蛋白重链序列变化所致。

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Structure of the regulatory domain of scallop myosin at 2.8 A resolution.分辨率为2.8埃的扇贝肌球蛋白调节结构域的结构。
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