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肌球蛋白轻链亚型的自上而下蛋白质组学确定了人类心脏中腔室特异性表达。

Top-down Proteomics of Myosin Light Chain Isoforms Define Chamber-Specific Expression in the Human Heart.

作者信息

Bayne Elizabeth F, Rossler Kalina J, Gregorich Zachery R, Aballo Timothy J, Roberts David S, Chapman Emily A, Guo Wei, Ralphe John Carter, Kamp Timothy J, Ge Ying

出版信息

bioRxiv. 2023 Feb 26:2023.01.26.525767. doi: 10.1101/2023.01.26.525767.

DOI:10.1101/2023.01.26.525767
PMID:36747670
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9900887/
Abstract

Myosin functions as the "molecular motor" of the sarcomere and generates the contractile force necessary for cardiac muscle contraction. Myosin light chains 1 and 2 (MLC-1 and -2) play important functional roles in regulating the structure of the hexameric myosin molecule. Each of these light chains has an "atrial" and "ventricular" isoform, so called because they are believed to exhibit chamber-restricted expression in the heart. However, recently the chamber-specific expression of MLC isoforms in the human heart has been questioned. Herein, we analyzed the expression of MLC-1 and -2 atrial and ventricular isoforms in each of the four cardiac chambers in adult non-failing donor hearts using top-down mass spectrometry (MS)-based proteomics. Strikingly, we detected an isoform thought to be ventricular, MLC-2v, in the atria and confirmed the protein sequence using tandem MS (MS/MS). For the first time, a putative deamidation post-translation modification (PTM) located on MLC-2v in atrial tissue was localized to amino acid N13. MLC-1v and MLC-2a were the only MLC isoforms exhibiting chamber-restricted expression patterns across all donor hearts. Importantly, our results unambiguously show that MLC-1v, not MLC-2v, is ventricle-specific in adult human hearts. Overall, top-down proteomics allowed us an unbiased analysis of MLC isoform expression throughout the human heart, uncovering previously unexpected isoform expression patterns and PTMs.

摘要

肌球蛋白作为肌节的“分子马达”,产生心肌收缩所需的收缩力。肌球蛋白轻链1和2(MLC-1和-2)在调节六聚体肌球蛋白分子结构中发挥重要功能作用。这些轻链各自都有一个“心房”和“心室”异构体,之所以这样称呼是因为它们被认为在心脏中表现出腔室限制性表达。然而,最近人心脏中MLC异构体的腔室特异性表达受到了质疑。在此,我们使用基于自上而下质谱(MS)的蛋白质组学分析了成年非衰竭供体心脏四个心腔中MLC-1和-2心房和心室异构体的表达。令人惊讶的是,我们在心房中检测到一种被认为是心室型的异构体MLC-2v,并使用串联质谱(MS/MS)确认了其蛋白质序列。首次在心房组织中定位到位于MLC-2v上的一种假定的翻译后脱酰胺修饰(PTM)至氨基酸N13。MLC-1v和MLC-2a是所有供体心脏中仅有的表现出腔室限制性表达模式的MLC异构体。重要的是,我们的结果明确表明,在成年人心脏中,MLC-1v而非MLC-2v是心室特异性的。总体而言,自上而下的蛋白质组学使我们能够对整个人心脏中的MLC异构体表达进行无偏分析,揭示了以前意想不到的异构体表达模式和PTM。