Department of Molecular and Cellular Physiology, Louisiana State University Health Science Center, 1501 Kings Hwy, Shreveport, LA 71130-3932.
Hypertension. 2010 Dec;56(6):1089-95. doi: 10.1161/HYPERTENSIONAHA.110.158220. Epub 2010 Oct 25.
Hypertension is associated with an increased risk of thrombosis that appears to involve an interaction between the renin-angiotensin system and hemostasis. In this study we determined whether angiotensin II-mediated thrombosis occurs in arterioles and/or venules and assessed the involvement of type 1 (AT₁), type 2 (AT₂), and type 4 (AT₄) angiotensin II receptors, as well as receptors for endothelin 1 and bradykinin 1 and 2 in angiotensin II-enhanced microvascular thrombosis. Thrombus development in mouse cremaster microvessels was quantified after light/dye injury using the time of onset of the thrombus and time to blood flow cessation. Wild-type and AT₁ receptor-deficient mice were implanted with an angiotensin II-loaded ALZET pump for 2 weeks. Angiotensin II administration in both wild-type and ATAT₁ receptor-deficient mice significantly accelerated thrombosis in arterioles. Genetic deficiency and pharmacological antagonism of AT₁ receptors did not alter the thrombosis response to angiotensin II. Isolated murine platelets aggregated in response to low (picomolar) but not high (nanomolar) concentrations of angiotensin II. The platelet aggregation response to angiotensin II depended on AT₁ receptors. Antagonism of AT₂ receptors in vivo significantly prolonged the onset of angiotensin II-enhanced thrombosis, whereas an AT₄ receptor antagonist prolonged the time to flow cessation. Selective antagonism of either endothelin 1 or bradykinin 1 receptors largely prevented both the onset and flow cessation responses to chronic angiotensin II infusion. Our findings indicate that angiotensin II induced hypertension is accompanied by enhanced thrombosis in arterioles, and this response is mediated by a mechanism that involves AT₂, AT₄, bradykinin 1, and endothelin 1 receptor-mediated signaling.
高血压与血栓形成的风险增加有关,这种风险似乎涉及肾素-血管紧张素系统和止血之间的相互作用。在这项研究中,我们确定血管紧张素 II 是否在小动脉和/或小静脉中引起血栓形成,并评估了 1 型(AT₁)、2 型(AT₂)和 4 型(AT₄)血管紧张素 II 受体以及内皮素 1 和缓激肽 1 和 2 受体在血管紧张素 II 增强微血管血栓形成中的作用。在使用血栓形成开始时间和血流停止时间的方法通过光/染料损伤定量测定小鼠提睾肌微血管中的血栓形成发展。将载有血管紧张素 II 的 ALZET 泵植入野生型和 AT₁ 受体缺陷型小鼠体内 2 周。在野生型和 ATAT₁ 受体缺陷型小鼠中,血管紧张素 II 的给予均显著加速了小动脉的血栓形成。AT₁ 受体的遗传缺失和药理学拮抗作用并没有改变对血管紧张素 II 的血栓形成反应。分离的小鼠血小板对低(皮摩尔)而非高(纳摩尔)浓度的血管紧张素 II 聚集。血管紧张素 II 对血小板聚集的反应依赖于 AT₁ 受体。体内 AT₂ 受体拮抗剂显著延长了血管紧张素 II 增强的血栓形成的开始时间,而 AT₄ 受体拮抗剂延长了血流停止的时间。选择性拮抗内皮素 1 或缓激肽 1 受体在很大程度上防止了慢性血管紧张素 II 输注引起的起始和血流停止反应。我们的发现表明,血管紧张素 II 诱导的高血压伴有小动脉血栓形成的增强,这种反应是通过涉及 AT₂、AT₄、缓激肽 1 和内皮素 1 受体介导的信号转导的机制介导的。