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肌原纤维组装中的支架蛋白和分子伴侣:为横纹肌赋予横纹

Scaffolds and chaperones in myofibril assembly: putting the striations in striated muscle.

作者信息

Crawford Garland L, Horowits Robert

机构信息

Department of Chemistry and Biochemistry, Bloomsburg University, Bloomsburg, PA, USA.

出版信息

Biophys Rev. 2011 Mar 1;3(1):25-32. doi: 10.1007/s12551-011-0043-x.

Abstract

Sarcomere assembly in striated muscles has long been described as a series of steps leading to assembly of individual proteins into thick filaments, thin filaments and Z-lines. Decades of previous work focused on the order in which various structural proteins adopted the striated organization typical of mature myofibrils. These studies led to the view that actin and α-actinin assemble into premyofibril structures separately from myosin filaments, and that these structures are then assembled into myofibrils with centered myosin filaments and actin filaments anchored at the Z-lines. More recent studies have shown that particular scaffolding proteins and chaperone proteins are required for individual steps in assembly. Here, we review the evidence that N-RAP, a LIM domain and nebulin repeat protein, scaffolds assembly of actin and α-actinin into I-Z-I structures in the first steps of assembly; that the heat shock chaperone proteins Hsp90 & Hsc70 cooperate with UNC-45 to direct the folding of muscle myosin and its assembly into thick filaments; and that the kelch repeat protein Krp1 promotes lateral fusion of premyofibril structures to form mature striated myofibrils. The evidence shows that myofibril assembly is a complex process that requires the action of particular catalysts and scaffolds at individual steps. The scaffolds and chaperones required for assembly are potential regulators of myofibrillogenesis, and abnormal function of these proteins caused by mutation or pathological processes could in principle contribute to diseases of cardiac and skeletal muscles.

摘要

长期以来,横纹肌中的肌节组装一直被描述为一系列步骤,这些步骤导致单个蛋白质组装成粗肌丝、细肌丝和Z线。此前数十年的研究聚焦于各种结构蛋白形成成熟肌原纤维典型横纹组织的顺序。这些研究得出的观点是,肌动蛋白和α - 辅肌动蛋白与肌球蛋白丝分别组装成前肌原纤维结构,然后这些结构组装成肌原纤维,其中肌球蛋白丝位于中心,肌动蛋白丝锚定在Z线。最近的研究表明,组装过程中的各个步骤需要特定的支架蛋白和伴侣蛋白。在这里,我们回顾相关证据:N - RAP(一种含LIM结构域和伴肌动蛋白重复序列的蛋白)在组装的第一步将肌动蛋白和α - 辅肌动蛋白支架组装成I - Z - I结构;热休克伴侣蛋白Hsp90和Hsc70与UNC - 45协同作用,指导肌肉肌球蛋白的折叠及其组装成粗肌丝;kelch重复蛋白Krp1促进前肌原纤维结构的横向融合以形成成熟的横纹肌原纤维。证据表明,肌原纤维组装是一个复杂的过程,在各个步骤都需要特定催化剂和支架的作用。组装所需的支架蛋白和伴侣蛋白是肌原纤维生成的潜在调节因子,由突变或病理过程导致的这些蛋白质功能异常原则上可能导致心脏和骨骼肌疾病。

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