Design and Rationale for the Study of Changes in Iron and Atherosclerosis Risk in Perimenopause.

Georgeta Mihai, Xin He, Xiaolan Zhang, Beth McCarthy, Tam Tran, Michael Pennell, Jessica Blank, Orlando P Simonetti, Rebecca D Jackson, Subha V Raman
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引用次数: 11

Abstract

This study seeks to investigate changes in iron homeostasis and carotid arteries in women at risk of atherosclerosis, addressing a relatively unexplored hypothesis explaining why women have a 5-10 year lag in initial atherosclerotic events. Recent evidence points to hepcidin, the key regulator of macrophage iron uptake and release, as a potential mediator of risk. Furthermore, iron catalyzes the generation of free radicals that oxidize cholesterol stimulating atheroma formation. Magnetic resonance imaging (MRI) is ideally suited to study iron because of iron's local effects on magnetic susceptibility that can be quantified using a relaxation parameter called T2* ('T2-star'), as well as the ability to noninvasively characterize and quantify atherosclerotic plaque with MRI. This work outlines the rationale and study design to provide critical evidence related to the iron hypothesis, such that novel diagnostics and therapeutics to attenuate risk may be derived from a better understanding of iron's role in atherosclerosis.

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围绝经期铁元素变化与动脉粥样硬化风险研究的设计和基本原理。
本研究旨在调查有动脉粥样硬化风险的女性的铁稳态和颈动脉的变化,解决一个相对未被探索的假设,解释为什么女性在初始动脉粥样硬化事件中有5-10年的滞后。最近的证据表明,巨噬细胞铁摄取和释放的关键调节因子hepcidin是一种潜在的风险调节因子。此外,铁催化自由基的产生,氧化胆固醇刺激动脉粥样硬化的形成。磁共振成像(MRI)非常适合研究铁,因为铁对磁化率的局部影响可以通过称为T2* ('T2-star')的松弛参数来量化,并且能够通过MRI无创地表征和量化动脉粥样硬化斑块。这项工作概述了基本原理和研究设计,以提供与铁假说相关的关键证据,例如,新的诊断和治疗方法可以通过更好地了解铁在动脉粥样硬化中的作用来降低风险。
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