血管紧张素诱导高血压期间,血细胞相关血管紧张素II型1受体在缺血性脑卒中的脑微血管反应中的作用

Mutsumi Nagai, Satoshi Terao, Shantel A Vital, Stephen F Rodrigues, Gokhan Yilmaz, D Neil Granger
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引用次数: 22

摘要

背景:血管紧张素II型1受体(AT1R)阻滞剂可降低高血压患者缺血性卒中的发生率,减轻动物模型中的脑炎症和脑损伤。尽管血液细胞(BC)和血管内皮细胞(EC)上的AT1R可以被血管紧张素II (Ang II)激活,从而引发炎症,但在血管紧张素诱导高血压的情况下,BC和EC上表达的AT1R对缺血再灌注(I/R)脑损伤反应的相对贡献尚不清楚。方法:采用野生型(WT)、AT1aR-/-和骨髓嵌合体小鼠(BC+/EC+ (WT→WT)或BC-/EC+ (AT1aR-/-→WT) AT1aR分布,评估BC-和EC相关的AT1R对I/ r诱导的脑炎症和损伤的贡献。在正常血压和angii诱导的高血压小鼠脑缺血后监测小静脉中白细胞和血小板的粘附、血脑屏障(BBB)的通透性和梗死面积。结果:在angii诱导的高血压中,炎症(血细胞粘附)和损伤(血脑屏障通透性、梗死体积)反应被大大夸大。在AT1aR-/-小鼠中,Ang ii增强的反应明显减弱。在AT1aR-/-→WT小鼠中,对血脑屏障通透性和梗死体积也有类似的保护作用,而对白细胞和血小板粘附的保护作用则较少或没有。结论:BC和EC相关的AT1aR均参与Ang ii型高血压缺血性脑卒中的脑损伤反应,EC AT1aR更多地参与血细胞募集反应,BC AT1aR对I/R引起的血脑屏障破坏和组织坏死有显著影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Role of blood cell-associated angiotensin II type 1 receptors in the cerebral microvascular response to ischemic stroke during angiotensin-induced hypertension.

Role of blood cell-associated angiotensin II type 1 receptors in the cerebral microvascular response to ischemic stroke during angiotensin-induced hypertension.

Role of blood cell-associated angiotensin II type 1 receptors in the cerebral microvascular response to ischemic stroke during angiotensin-induced hypertension.

Role of blood cell-associated angiotensin II type 1 receptors in the cerebral microvascular response to ischemic stroke during angiotensin-induced hypertension.

Background: Angiotensin II type 1 receptor (AT1R) blockers lower the incidence of ischemic stroke in hypertensive patients and attenuate brain inflammation and injury in animal models. Although AT1R on both blood cells (BC) and vascular endothelial cells (EC) can be activated by angiotensin II (Ang II) to elicit inflammation, little is known about the relative contributions of AT1R expressed on BC and EC to the brain injury responses to ischemia and reperfusion (I/R) in the setting of angiotensin-induced hypertension.

Methods: The contributions of BC- and EC-associated AT1R to I/R-induced brain inflammation and injury were evaluated using wild type (WT), AT1aR-/-, and bone marrow chimera mice with either a BC+/EC+ (WT→WT) or BC-/EC+ (AT1aR-/-→WT) distribution of AT1aR. The adhesion of leukocytes and platelets in venules, blood brain barrier (BBB) permeability and infarct volume were monitored in postischemic brain of normotensive and Ang II-induced hypertensive mice.

Results: The inflammatory (blood cell adhesion) and injury (BBB permeability, infarct volume) responses were greatly exaggerated in the presence of Ang II-induced hypertension. The Ang II-enhanced responses were significantly blunted in AT1aR-/- mice. A similar level of protection was noted in AT1aR-/- →WT mice for BBB permeability and infarct volume, while less or no protection was evident for leukocyte and platelet adhesion, respectively.

Conclusions: BC- and EC-associated AT1aR are both involved in the brain injury responses to ischemic stroke during Ang II-hypertension, with EC AT1aR contributing more to the blood cell recruitment response and BC AT1aR exerting a significant influence on the BBB disruption and tissue necrosis elicited by I/R.

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