I-Band Titin in Cardiac Muscle Is a Three-Element Molecular Spring and Is Critical for Maintaining Thin Filament Structure

提丁 肌节 肌原纤维 免疫电镜 基因亚型 默默林 心肌 蛋白质丝 肌动蛋白 生物物理学 星云素 肌丝 生物 心肌细胞 解剖 结晶学 化学 细胞生物学 生物化学 遗传学 抗体 基因
作者
Wolfgang A. Linke,Diane E. Rudy,Thomas Centner,Mathias Gautel,Christian Witt,Siegfried Labeit,Carol C. Gregorio
出处
期刊:Journal of Cell Biology [Rockefeller University Press]
卷期号:146 (3): 631-644 被引量:235
标识
DOI:10.1083/jcb.146.3.631
摘要

In cardiac muscle, the giant protein titin exists in different length isoforms expressed in the molecule's I-band region. Both isoforms, termed N2-A and N2-B, comprise stretches of Ig-like modules separated by the PEVK domain. Central I-band titin also contains isoform-specific Ig-motifs and nonmodular sequences, notably a longer insertion in N2-B. We investigated the elastic behavior of the I-band isoforms by using single-myofibril mechanics, immunofluorescence microscopy, and immunoelectron microscopy of rabbit cardiac sarcomeres stained with sequence-assigned antibodies. Moreover, we overexpressed constructs from the N2-B region in chick cardiac cells to search for possible structural properties of this cardiac-specific segment. We found that cardiac titin contains three distinct elastic elements: poly-Ig regions, the PEVK domain, and the N2-B sequence insertion, which extends ∼60 nm at high physiological stretch. Recruitment of all three elements allows cardiac titin to extend fully reversibly at physiological sarcomere lengths, without the need to unfold Ig domains. Overexpressing the entire N2-B region or its NH2 terminus in cardiac myocytes greatly disrupted thin filament, but not thick filament structure. Our results strongly suggest that the NH2-terminal N2-B domains are necessary to stabilize thin filament integrity. N2-B–titin emerges as a unique region critical for both reversible extensibility and structural maintenance of cardiac myofibrils.

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