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肌钙蛋白复合体的结构。肌钙蛋白I与肌钙蛋白C硫醇突变体光交联的意义。

Structure of the troponin complex. Implications of photocross-linking of troponin I to troponin C thiol mutants.

作者信息

Kobayashi T, Tao T, Gergely J, Collins J H

机构信息

Department of Biological Chemistry, University of Maryland School of Medicine, Baltimore, Maryland.

出版信息

J Biol Chem. 1994 Feb 25;269(8):5725-9.

PMID:8119911
Abstract

Ca2+ regulation of vertebrate-striated muscle contraction is initiated by conformational changes in the Ca(2+)-binding protein troponin C (TnC) and subsequent changes in the interaction of TnC with the inhibitory protein TnI. We have constructed mutants of rabbit skeletal muscle TnC in which natural Cys-98 was replaced by Leu, and a single Cys residue was introduced at position 12 (TnC12) or 89 (TnC89). Cys residues of mutant TnCs were derivatized with 4-maleimidobenzophenone and photocross-linked to TnI in binary TnC.TnI complexes. After digestion with CNBr or proteases, cross-linked peptides were purified and sequenced. TnC12 cross-linked at or near TnI Met-134 in a region known to be sensitive not only to occupancy of the regulatory Ca(2+)-binding sites of TnC but also to the contractile state of the thin filament. TnC89 cross-linked to TnI(108-113) in the inhibitory region. Taken together with earlier findings, these results indicate that in the TnC.TnI complex, both domains of TnC, as well as the linker region between them, make contact with the inhibitory region of TnI. Our data also indicate that the N- and C-terminal domains of TnC interact with opposite ends of the TnI inhibitory region.

摘要

脊椎动物横纹肌收缩的Ca2+调节是由Ca(2+)结合蛋白肌钙蛋白C(TnC)的构象变化以及随后TnC与抑制蛋白TnI相互作用的变化引发的。我们构建了兔骨骼肌TnC的突变体,其中天然的半胱氨酸-98被亮氨酸取代,并在第12位(TnC12)或第89位(TnC89)引入了单个半胱氨酸残基。突变体TnC的半胱氨酸残基用4-马来酰亚胺基二苯甲酮衍生化,并在二元TnC.TnI复合物中与TnI进行光交联。用溴化氰或蛋白酶消化后,纯化并测序交联的肽段。TnC12在TnI甲硫氨酸-134处或其附近交联,该区域不仅对TnC调节性Ca(2+)结合位点的占据敏感,而且对细肌丝的收缩状态敏感。TnC89在抑制区域与TnI(108 - 113)交联。结合早期的研究结果,这些结果表明,在TnC.TnI复合物中,TnC的两个结构域以及它们之间的连接区都与TnI的抑制区域接触。我们的数据还表明,TnC的N端和C端结构域与TnI抑制区域的两端相互作用。

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