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动脉髓过氧化物酶在易损动脉粥样硬化斑块检测与治疗中的应用:旧方法迎来新曙光

Arterial myeloperoxidase in the detection and treatment of vulnerable atherosclerotic plaque: a new dawn for an old light.

作者信息

Nadel James, Jabbour Andrew, Stocker Roland

机构信息

Heart Research Institute, The University of Sydney, 7 Eliza St, Newtown, 2042 Sydney, NSW, Australia.

Cardiology Department, St Vincent's Hospital, Sydney, Australia.

出版信息

Cardiovasc Res. 2023 Mar 17;119(1):112-120. doi: 10.1093/cvr/cvac081.

Abstract

Intracellular myeloperoxidase (MPO) plays a specific role in the innate immune response; however, upon release into the extracellular space in the setting of inflammation, drives oxidative tissue injury. Extracellular MPO has recently been shown to be abundant in unstable atheroma and causally linked to plaque destabilization, erosion, and rupture, identifying it as a potential target for the surveillance and treatment of vulnerable atherosclerosis. Through the compartmentalization of MPO's protective and deleterious effects, extracellular MPO can be selectively detected using non-invasive molecular imaging and targeted by burgeoning pharmacotherapies. Given its causal relationship to plaque destabilization coupled with an ability to preserve its beneficial properties, MPO is potentially a superior translational inflammatory target compared with other immunomodulatory therapies and imaging biomarkers utilized to date. This review explores the role of MPO in plaque destabilization and provides insights into how it can be harnessed in the management of patients with vulnerable atherosclerotic plaque.

摘要

细胞内髓过氧化物酶(MPO)在先天性免疫反应中发挥特定作用;然而,在炎症情况下释放到细胞外空间时,会引发氧化组织损伤。最近研究表明,细胞外MPO在不稳定动脉粥样硬化斑块中含量丰富,且与斑块不稳定、糜烂和破裂存在因果关系,这使其成为监测和治疗易损性动脉粥样硬化的潜在靶点。通过区分MPO的保护作用和有害作用,可以使用非侵入性分子成像选择性检测细胞外MPO,并通过新兴的药物疗法对其进行靶向治疗。鉴于其与斑块不稳定的因果关系以及保留其有益特性的能力,与迄今为止使用的其他免疫调节疗法和成像生物标志物相比,MPO可能是一个更优越的可转化炎症靶点。本综述探讨了MPO在斑块不稳定中的作用,并深入了解如何在易损性动脉粥样硬化斑块患者的管理中利用它。

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