Uncovering the Mechanism of Protein Sulfination in Regulating Atherosclerotic Plaque Calcification via Fluorescence Imaging

IF 6.7 1区 化学 Q1 CHEMISTRY, ANALYTICAL
Wen Gao*, Yinkao Zhou, Guanghan Li*, Shengyue Zhang, Xiaoqing Huang and Bo Tang*, 
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引用次数: 0

Abstract

Atherosclerotic plaque calcification is an oxidative-stress-dependent process involved in the onset of plaque disruption and subsequent atherothrombotic events. Excessive reactive oxygen species (ROS) production determines the structural modification of protein cysteine sulfhydryl (Cys-SH), leading to the alteration of protein functions and redox signaling outputs. Although these redox-centered signaling pathways have been found to play important roles in plaque calcification, the extent of protein Cys-SH modifications and the regulatory regions of specific proteins remains unclear. This is due to the lack of tools that can visually distinguish and characterize the oxidation products of different Cys-SH proteins, especially protein sulfination (Cys-SO2H). Herein, we present a novel “turn-on” fluorescent probe (Z-1) for the in situ visualization of Cys-SO2H modifications and investigate its effects on the initiation of vascular smooth muscle cell (VSMC) calcification. In vitro and in vivo imaging with Z-1, cigarette smoking-induced VSMC calcification, display a significant increase in protein Cys-SO2H levels. Protein spectrum analysis reveals that Cys-SO2H modification occurred at the sulfhydryl active sites of the Kelch-like ECH-associated protein (Keap1). These oxidative modifications are desired to dysregulate the ROS/Keap1/nuclear factor-E2-related factor 2 (Nrf2) antioxidant signaling pathway and accelerate the calcification process. Furthermore, elevated levels of Cys-SO2H observed in serum samples from patients with acute myocardial infarction and cerebral infarction give clinical evidence of the relevance of protein Cys-SO2H modification in pathological calcification.

Abstract Image

荧光成像揭示蛋白质亚硫酸化调控动脉粥样硬化斑块钙化的机制
动脉粥样硬化斑块钙化是一个氧化应激依赖的过程,涉及斑块破裂和随后的动脉粥样硬化血栓事件的发生。过多的活性氧(ROS)的产生决定了蛋白质半胱氨酸巯基(Cys-SH)的结构修饰,导致蛋白质功能和氧化还原信号输出的改变。尽管已经发现这些以氧化还原为中心的信号通路在斑块钙化中起重要作用,但蛋白质Cys-SH修饰的程度和特定蛋白质的调控区域仍不清楚。这是由于缺乏能够直观区分和表征不同Cys-SH蛋白氧化产物的工具,特别是蛋白质亚硫化(Cys-SO2H)。在此,我们提出了一种新的“开启”荧光探针(Z-1),用于原位可视化Cys-SO2H修饰,并研究其对血管平滑肌细胞(VSMC)钙化起始的影响。在Z-1的体外和体内成像中,吸烟引起的VSMC钙化,显示Cys-SO2H蛋白水平显著升高。蛋白谱分析表明,Cys-SO2H修饰发生在kelch样ECH-associated Protein (Keap1)的巯基活性位点。这些氧化修饰可能导致ROS/Keap1/核因子e2相关因子2 (Nrf2)抗氧化信号通路失调,加速钙化过程。此外,在急性心肌梗死和脑梗死患者血清样本中观察到的Cys-SO2H水平升高,为Cys-SO2H蛋白修饰与病理性钙化的相关性提供了临床证据。
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来源期刊
Analytical Chemistry
Analytical Chemistry 化学-分析化学
CiteScore
12.10
自引率
12.20%
发文量
1949
审稿时长
1.4 months
期刊介绍: Analytical Chemistry, a peer-reviewed research journal, focuses on disseminating new and original knowledge across all branches of analytical chemistry. Fundamental articles may explore general principles of chemical measurement science and need not directly address existing or potential analytical methodology. They can be entirely theoretical or report experimental results. Contributions may cover various phases of analytical operations, including sampling, bioanalysis, electrochemistry, mass spectrometry, microscale and nanoscale systems, environmental analysis, separations, spectroscopy, chemical reactions and selectivity, instrumentation, imaging, surface analysis, and data processing. Papers discussing known analytical methods should present a significant, original application of the method, a notable improvement, or results on an important analyte.
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