Department of Neurosurgery, Mount Sinai Medical School, New York, New York 10029, USA.
J Cereb Blood Flow Metab. 2010 Apr;30(4):808-15. doi: 10.1038/jcbfm.2009.244. Epub 2009 Nov 18.
The mechanisms responsible for vascular autoregulation in the brain during changes in mean arterial blood pressure are ambiguous. Potentially, adenosine, a purine nucleoside and potent vasodilator, may be involved as earlier studies have documented an increase in brain adenosine concentrations with cerebral ischemia and hypotension. Consequently, we tested the hypothesis that adenosine is involved in vasodilatation during hypotension within the autoregulatory range (>50 mm Hg) by exposing adenosine 2a receptor (A2aR) knockout and wild type (WT) mice to short (2 to 5 mins) periods of hypotension. We found that autoregulation was significantly (P<0.05) impaired by 29% in A2a knockout mice as compared with WT animals. Furthermore, the A2R antagonist (A2a>A2b:10-85>1), ZM-241385, in a dose (1, 5, 10 mg/kg, intraperitoneally)-related manner, attenuated autoregulation in WT mice. In knockout mice treated with ZM-2413585 (5 and 10 mg/kg), autoregulation was further impaired indicating that A2b receptors also participated in cerebral vasodilatation. Treatment with dipyridamole (1.0 mg/kg) that increases extracellular concentrations of adenosine improved autoregulation in the A2aR knockout mice. We would conclude that adenosine through both A2a and A2b receptors is involved in physiologic vascular regulation during hypotension even within the autoregulatory range.
在平均动脉血压变化时,负责脑血管自动调节的机制尚不清楚。潜在地,腺苷可能参与其中,因为早期的研究已经记录到脑缺血和低血压时脑腺苷浓度增加。因此,我们通过使腺苷 2a 受体 (A2aR) 敲除和野生型 (WT) 小鼠短暂(2 至 5 分钟)低血压来测试腺苷参与自动调节范围内(>50mmHg)低血压时血管舒张的假说。我们发现,与 WT 动物相比,A2a 敲除小鼠的自动调节明显(P<0.05)受损 29%。此外,A2R 拮抗剂(A2a>A2b:10-85>1),ZM-241385,以剂量(1、5、10mg/kg,腹膜内)相关的方式,减弱了 WT 小鼠的自动调节。在接受 ZM-2413585(5 和 10mg/kg)治疗的敲除小鼠中,自动调节进一步受损,表明 A2b 受体也参与脑血管舒张。用增加细胞外腺苷浓度的双嘧达莫(1.0mg/kg)治疗可改善 A2aR 敲除小鼠的自动调节。我们的结论是,即使在自动调节范围内,腺苷通过 A2a 和 A2b 受体参与低血压时的生理血管调节。
