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人类动脉粥样硬化中的新生血管形成。

Neovascularization in human atherosclerosis.

作者信息

Moreno P R, Purushothaman K R, Zias E, Sanz J, Fuster V

机构信息

The Zena and Michael A. Wiener Cardiovascular Institute, and The Marie-Josee and Henry R. Kravis Cardiovascular Health Center, The Mount Sinai School of Medicine, New York, NY 10029, USA.

出版信息

Curr Mol Med. 2006 Aug;6(5):457-77. doi: 10.2174/156652406778018635.

Abstract

In the absence of disease, microvessels provide vessel wall nutrients to the tunica media, while the intima is fed by oxygen diffusion from the lumen. As disease evolves and the tunica intima thickens, oxygen diffusion is impaired, and microvessels become the major source for nutrients to the vessel wall. Microvessels serve as a port of entry for inflammatory cells, from the systemic circulation to the nascent atherosclerotic lesion. As disease progress, microvessels also play a role in intraplaque hemorrhage, lipid core expansion, and plaque rupture. In addition, microvessels are also involved in stent restenosis, and plaque regression. Therefore, microvessels are a pivotal component of atherosclerosis, and proper patient risk-stratification in the near future may include the detection of increased neovascularization in atherosclerotic lesions. This review divided in two parts summarizes the current understanding of atherosclerosis neovascularization, starting with the normal anatomy and physiology and progressing to more advanced stages of the disease. We will review the structure and function of vasa vasorum in health and disease, the mechanisms responsible for the angiogenic process, the role of the immune system, including inflammation and Toll-like receptors, and the pathology of microvessels in early atherosclerotic plaques. Furthermore, the review addresses the advanced stages of atherosclerosis, summarizing the progressive role for microvessels during disease progression, red blood cell extravasation, lipid core expansion, plaque rupture, healing, repair, restenosis, and disease regression, offering the clinician a state-of-the-art, "bench to bedside" approach to neovascularization in human atherosclerosis.

摘要

在无疾病状态下,微血管为中膜提供血管壁营养物质,而内膜则通过从管腔扩散的氧气获取营养。随着疾病进展,内膜增厚,氧气扩散受损,微血管成为血管壁营养物质的主要来源。微血管是炎症细胞从体循环进入新生动脉粥样硬化病变的入口。随着疾病进展,微血管还在斑块内出血、脂质核心扩大和斑块破裂中起作用。此外,微血管还参与支架再狭窄和斑块消退。因此,微血管是动脉粥样硬化的关键组成部分,在不久的将来,合适的患者风险分层可能包括检测动脉粥样硬化病变中新生血管形成增加。这篇综述分为两部分,总结了目前对动脉粥样硬化新生血管形成的认识,从正常解剖学和生理学开始,进而探讨疾病的更高级阶段。我们将回顾健康和疾病状态下血管滋养管的结构和功能、血管生成过程的机制、免疫系统的作用,包括炎症和Toll样受体,以及早期动脉粥样硬化斑块中微血管的病理学。此外,该综述还涉及动脉粥样硬化的晚期阶段,总结了微血管在疾病进展、红细胞外渗、脂质核心扩大、斑块破裂、愈合、修复、再狭窄和疾病消退过程中的渐进作用,为临床医生提供了一种从基础到临床的人类动脉粥样硬化新生血管形成的前沿方法。

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