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动脉粥样硬化中的血管生成:证据不断积累,不再只是推测。

Angiogenesis in atherosclerosis: gathering evidence beyond speculation.

作者信息

Moulton Karen S

机构信息

Vascular Biology Program, Department of Surgery, Children's Hospital, Karp Family Research Building 11.212, 1 Blackfan Circle, Boston, MA 02115, USA.

出版信息

Curr Opin Lipidol. 2006 Oct;17(5):548-55. doi: 10.1097/01.mol.0000245261.71129.f0.

Abstract

PURPOSE OF REVIEW

The present review summarizes evidence for several functions of neovascularization in plaque growth that sustain perfusion beyond limits of diffusion from the artery lumen and outer adventitial vasa vasorum, deposit proatherogenic plasma molecules, recruit immune cells and progenitors, and promote intraplaque hemorrhage. Recent approvals of antiangiogenesis drugs for clinical use in cancer and macular degeneration improve the feasibility of testing whether such agents inhibit plaque angiogenesis and incidental atherosclerosis.

RECENT FINDINGS

Improvements in large and small animal models of atherosclerosis and knowledge of the molecular regulation of angiogenesis in development and disease have advanced understanding of plaque angiogenesis. Genetic modifications of angiogenesis molecules in mouse strains susceptible to atherosclerosis provide experimental means to identify native molecules that regulate plaque angiogenesis. Studies of plaque angiogenesis are aided by micro-computed tomography techniques that image vasa vasorum anatomy in relation to the atheroma.

SUMMARY

Greater knowledge of plaque angiogenesis regulation is needed to design treatments that target the most critical regulatory pathways. Evolutions in angiogenesis inhibitor treatments for cancer and other diseases call for a need to understand the distinct cardiovascular profiles of different agents to rationally combine agents for optimal selectivity and efficacy in the intended vascular bed.

摘要

综述目的

本综述总结了新生血管形成在斑块生长中的多种作用的证据,这些作用包括维持超过动脉管腔和外膜血管滋养管扩散极限的灌注、沉积促动脉粥样硬化血浆分子、募集免疫细胞和祖细胞以及促进斑块内出血。近期抗血管生成药物在癌症和黄斑变性临床应用中的获批,提高了测试此类药物是否抑制斑块血管生成和偶发性动脉粥样硬化的可行性。

最新发现

动脉粥样硬化大、小动物模型的改进以及对发育和疾病中血管生成分子调控的认识,推动了对斑块血管生成的理解。对易患动脉粥样硬化小鼠品系中血管生成分子的基因改造,为鉴定调节斑块血管生成的天然分子提供了实验手段。微计算机断层扫描技术有助于研究斑块血管生成,该技术可对与动脉粥样瘤相关的血管滋养管解剖结构进行成像。

总结

需要更深入了解斑块血管生成调控,以设计针对最关键调控途径的治疗方法。癌症和其他疾病的血管生成抑制剂治疗的进展,要求了解不同药物独特的心血管特征,以便合理联合用药,在目标血管床中实现最佳选择性和疗效。

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