Evaluation of the symmetric model for myosin-linked regulation: effect of site-directed mutations in the regulatory light chain on scallop myosin.

Colegrave M; Patel H; Offer G; Chantler PD

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Evaluation of the symmetric model for myosin-linked regulation: effect of site-directed mutations in the regulatory light chain on scallop myosin.

机译：肌球蛋白连锁调控对称模型的评估：扇贝肌球蛋白调控轻链中的定点突变的影响。

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Regulatory myosins are controlled through mechanisms intrinsic to their structures and can alternate between activated and inhibited states. However, the structural difference between these two states is unclear. Scallop (Pecten maximus) striated adductor myosin is activated directly by calcium. It has been proposed that the two heads of scallop myosin are symmetrically arranged and interact through their regulatory light chains [Offer and Knight (1996) J. Mol. Biol. 256, 407-416], the interface being strengthened in the inhibited state. By contrast, vertebrate smooth-muscle myosin is activated by phosphorylation. Its structure in the inhibited state has been determined from two-dimensional crystalline arrays [Wendt, Taylor, Trybus and Taylor (2001) Proc. Natl. Acad. Sci. U.S.A. 98, 4361-4366] and is asymmetric, requiring no interaction between regulatory light chains. Using site-directed mutagenesis of the scallop regulatory light chain, we have tested the symmetric model for scallop adductor muscle myosin. Specifically, we have made myosin hybrid molecules from scallop (P. maximus) myosin, in which the normal regulatory light chains have been replaced by expressed light chains containing mutations in three residues proposed to participate in the interaction between regulatory light chains. The mutations were R126A (Arg126-->Ala), K130A and E131A; made singly, in pairs or all three together, these mutations were designed to eliminate hydrogen bonding or salt linkages between heads, which are key features of this model. Functional assays to address the competence of these hybrid myosins to bind calcium specifically, to exhibit a calcium-regulated myofibrillar Mg-ATPase and to display calcium-dependent actin sliding were performed. We conclude that the symmetrical model does not describe the inhibited state of scallop regulatory myosin and that an asymmetric structure is a plausible alternative.

机译：调节性肌球蛋白通过其结构固有的机制来控制，并且可以在激活状态和抑制状态之间交替。但是，这两种状态之间的结构差异尚不清楚。扇贝（最大花粉）条纹的内收肌球蛋白由钙直接激活。已经提出，扇贝肌球蛋白的两个头部对称地排列并通过它们的调节性轻链相互作用[Offer和Knight（1996）J.Mol.Biol.215：403-10。生物学256，407-416]，界面在禁止状态下得到加强。相反，脊椎动物的平滑肌肌球蛋白通过磷酸化被激活。从二维晶体阵列已经确定了其处于抑制状态的结构[Wendt，Taylor，Trybus和Taylor（2001）Proc.Natl.Acad.Sci.USA 90：5873-5877。 Natl。学院科学[U.S.A. 98，4361-4366]，并且是不对称的，不需要调节轻链之间的相互作用。使用扇贝调节性轻链的定点诱变，我们测试了扇贝内收肌肌肉肌球蛋白的对称模型。具体而言，我们从扇贝（P. maximus）肌球蛋白中制备了肌球蛋白杂交分子，其中正常的调控轻链已被表达的轻链所取代，该轻链包含三个残基中的突变，提议参与调控轻链之间的相互作用。突变为R126A（Arg126-> Ala），K130A和E131A;这些突变被成对，成对或全部三个一起完成，旨在消除头部之间的氢键或盐键，这是该模型的关键特征。进行功能测定以解决这些杂化肌球蛋白与钙的特异性结合，表现出钙调节的肌原纤维Mg-ATPase以及显示钙依赖性肌动蛋白滑动的能力。我们得出的结论是，对称模型没有描述扇贝调节性肌球蛋白的抑制状态，并且不对称结构是一个合理的选择。

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《The Biochemical Journal 》 |2003年第1期| 共8页
作者
Colegrave M; Patel H; Offer G; Chantler PD;
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正文语种 eng
中图分类生物化学 ;
关键词
Myosins; Scallop; NOS; regulatory; Light; Models; 光;

机译：Myosins;Scallop;NOS;regulatory;Light;Models;光;

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1. Evaluation of the symmetric model for myosin-linked regulation: effect of site-directed mutations in the regulatory light chain on scallop myosin. [J] . Colegrave M, Patel H, Offer G, The Biochemical Journal . 2003 ,第Pta1期

机译：肌球蛋白连锁调控对称模型的评估：扇贝肌球蛋白调控轻链中的定点突变的影响。
2. Evaluation of the symmetric model for myosin-linked regulation: effect of site-directed mutations in the regulatory light chain on scallop myosin [J] . Gerald OFFER, Hitesh PATEL, Melanie COLEGRAVE, The biochemical journal . 2003 ,第1期

机译：肌球蛋白相关调控对称模型的评估：扇贝肌球蛋白调控轻链中的定点突变
3. Evaluation of the symmetric model for myosin-linked regulation: effect of site-directed mutations in the regulatory light chain on scallop myosin [J] . Colegrave M, Patel H, Offer G, The Biochemical Journal . 2003 ,第0期

机译：肌球蛋白连锁调控对称模型的评估：扇贝肌球蛋白调控轻链中的定点突变
4. SOMATIC MUTATIONS CREATE POTENTIAL N-GLYCOSYLATION SITES IN THE IMMUNOGLOBULIN LIGHT CHAIN VARIABLE REGIONS IN PRIMARY AMYLOIDOSIS [C] . T. Prokaeva, B Spencer, G Doros, International Symposium on Amyloidosis . 2008

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6. Evaluation of the symmetric model for myosin-linked regulation: effect of site-directed mutations in the regulatory light chain on scallop myosin. [O] . Melanie Colegrave, Hitesh Patel, Gerald Offer, 2003

机译：肌球蛋白相关调控对称模型的评估：扇贝肌球蛋白调控轻链中的定点突变的影响。
7. Evaluation of the symmetric model for myosin-linked regulation: effect of site-directed mutations in the regulatory light chain on scallop myosin. [O] . Colegrave, Melanie, Patel, Hitesh, Offer, Gerald, 2003

机译：肌球蛋白相关调控对称模型的评估：扇贝肌球蛋白调控轻链中的定点突变的影响。
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Evaluation of the symmetric model for myosin-linked regulation: effect of site-directed mutations in the regulatory light chain on scallop myosin.

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