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内皮功能作为干预试验的终点:概念、方法及当前数据。

Endothelial function as an end-point in interventional trials: concepts, methods and current data.

作者信息

Lüscher T F, Noll G

机构信息

Cardiology, University Hospital, Zurich, Switzerland.

出版信息

J Hypertens Suppl. 1996 Sep;14(2):S111-9; discussion S119-21. doi: 10.1097/00004872-199609002-00020.

Abstract

UNLABELLED

SURROGATE END-POINTS: Pharmacotherapy of cardiovascular disease has been increasingly validated in large interventional trials to assess its efficacy, safety and costs. As endpoints, morbidity and mortality are evaluated. More recently, surrogate end-points have been included in interventional trials, both to increase our understanding of pathogenic mechanisms and for their potential use as markers of risk in patients.

ENDOTHELIAL FUNCTION

The endothelium lies in a strategic anatomical position between the circulating blood and vascular smooth muscle and hence is a major local mediator of cardiovascular function. Also, endothelial cells are a target for mechanical forces and cardiovascular risk factors in the circulation. Thus, it is not surprising that their function becomes impaired at an early stage in the disease process. The cells are able to produce numerous proteins and mediators. This review focuses on nitric oxide and endothelin-1, which are endothelium-derived relaxing and constrictor factors, respectively. Nitric oxide also prevents platelet adhesion and aggregation and the adhesion of monocytes. Both substances also affect vascular structure in that nitric oxide inhibits while endothelin stimulates vascular smooth muscle proliferation and migration.

MEASUREMENTS OF ENDOTHELIAL FUNCTION

Endothelial function and the effects of nitric oxide and endothelin in particular can be evaluated in the coronary circulation by quantitative coronary angiography and Doppler flow wire, and in the peripheral circulation with plethysmography and new ultrasound/Doppler devices. In these experimental set-ups, lipid-lowering drugs and angiotensin converting enzyme (ACE) inhibitors have been evaluated. Lipid-lowering drugs improve endothelium-dependent vasodilation in the coronary and forearm circulation of patients with hyperlipidemia and atherosclerosis. Similarly, ACE inhibitors improve coronary vasomotion in patients with coronary artery disease and normal lipid levels. In hypertension, ACE inhibitors have failed to improve endothelium-dependent vasodilation, while studies with other drugs are planned.

CONCLUSIONS

Endothelial function can now be assessed precisely in patients in vivo, in both the coronary and the peripheral circulation. Tests can detect early dysfunction in patients with a risk of cardiovascular disease and the possible effects of drugs on endothelial function. Large interventional trials are needed to establish how far endothelial dysfunction can or cannot predict clinical outcome.

摘要

未标注

替代终点:心血管疾病的药物治疗已在大型干预试验中得到越来越多的验证,以评估其疗效、安全性和成本。作为终点,评估发病率和死亡率。最近,替代终点已被纳入干预试验,这既有助于加深我们对致病机制的理解,也因其有可能用作患者风险的标志物。

内皮功能

内皮位于循环血液和血管平滑肌之间的关键解剖位置,因此是心血管功能的主要局部介质。此外,内皮细胞是循环中机械力和心血管危险因素的作用靶点。因此,在疾病过程的早期阶段其功能受损也就不足为奇了。这些细胞能够产生多种蛋白质和介质。本综述重点关注一氧化氮和内皮素 -1,它们分别是内皮衍生的舒张因子和收缩因子。一氧化氮还可防止血小板黏附和聚集以及单核细胞黏附。这两种物质也会影响血管结构,即一氧化氮抑制而内皮素刺激血管平滑肌增殖和迁移。

内皮功能的测量

内皮功能以及一氧化氮和内皮素的作用尤其可通过定量冠状动脉造影和多普勒血流导丝在冠状动脉循环中进行评估,在外周循环中可通过体积描记法和新型超声/多普勒设备进行评估。在这些实验设置中,已对降脂药物和血管紧张素转换酶(ACE)抑制剂进行了评估。降脂药物可改善高脂血症和动脉粥样硬化患者冠状动脉和前臂循环中的内皮依赖性血管舒张。同样,ACE抑制剂可改善冠状动脉疾病且血脂水平正常患者的冠状动脉血管运动。在高血压患者中,ACE抑制剂未能改善内皮依赖性血管舒张,不过正在计划开展其他药物的研究。

结论

现在可以在体内对患者的冠状动脉和外周循环中的内皮功能进行精确评估。检测可以发现有心血管疾病风险患者的早期功能障碍以及药物对内皮功能的可能影响。需要进行大型干预试验来确定内皮功能障碍在多大程度上能够或不能预测临床结果。

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