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仿生结构钴纳米催化剂通过催化抗氧化抑制主动脉夹层进展。

Biomimetic-Structured Cobalt Nanocatalyst Suppresses Aortic Dissection Progression by Catalytic Antioxidation.

机构信息

Shanghai Institute of Ceramics, Chinese Academy of Sciences, Shanghai 200050, P. R. China.

Department of Vascular Surgery, Zhongshan Hospital, Fudan University, 180 Fenglin Road, Shanghai 200032, China.

出版信息

J Am Chem Soc. 2024 Jun 26;146(25):17201-17210. doi: 10.1021/jacs.4c03344. Epub 2024 Jun 14.

Abstract

As one of the most lethal cardiovascular diseases, aortic dissection (AD) is initiated by overexpression of reactive oxygen species (ROS) in the aorta that damages the vascular structure and finally leads to massive hemorrhage and sudden death. Current drugs used in clinics for AD treatment fail to efficiently scavenge ROS to a large extent, presenting undesirable therapeutic effect. In this work, a nanocatalytic antioxidation concept has been proposed to elevate the therapeutic efficacy of AD by constructing a cobalt nanocatalyst with a biomimetic structure that can scavenge pathological ROS in an efficient and sustainable manner. Theoretical calculations demonstrate that the antioxidation reaction is catalyzed by the redox transition between hydroxocobalt(III) and oxo-hydroxocobalt(V) accompanied by inner-sphere proton-coupled two-electron transfer, forming a nonassociated activation catalytic cycle. The efficient antioxidation action of the biomimetic nanocatalyst in the AD region effectively alleviates oxidative stress, which further modulates the aortic inflammatory microenvironment by promoting phenotype transition of macrophages. Consequently, vascular smooth muscle cells are also protected from inflammation in the meantime, suppressing AD progression. This study provides a nanocatalytic antioxidation approach for the efficient treatment of AD and other cardiovascular diseases.

摘要

作为最致命的心血管疾病之一,主动脉夹层(AD)是由主动脉中活性氧(ROS)的过度表达引发的,它会损害血管结构,最终导致大量出血和突然死亡。目前临床上用于 AD 治疗的药物在很大程度上不能有效地清除 ROS,治疗效果不理想。在这项工作中,提出了一种纳米催化抗氧化概念,通过构建具有仿生结构的钴纳米催化剂来清除病理性 ROS,从而提高 AD 的治疗效果。理论计算表明,抗氧化反应是由羟基金属钴(III)和氧-羟基金属钴(V)之间的氧化还原跃迁催化的,同时伴随着内球质子耦合的两电子转移,形成非缔合活化催化循环。仿生纳米催化剂在 AD 区域的有效抗氧化作用有效缓解了氧化应激,通过促进巨噬细胞表型转化进一步调节主动脉炎症微环境。同时,血管平滑肌细胞也免受炎症的影响,抑制 AD 的进展。本研究为 AD 及其他心血管疾病的有效治疗提供了一种纳米催化抗氧化方法。

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