Matsumoto Sachiko, Shimabukuro Michio, Fukuda Daiju, Soeki Takeshi, Yamakawa Ken, Masuzaki Hiroaki, Sata Masataka
Department of Cardio-Diabetes Medicine, The University of Tokushima Graduate School of Health Biosciences, 3-18-15 Kuramoto, Tokushima 770-8503, Japan.
Cardiovasc Diabetol. 2014 Jan 31;13:30. doi: 10.1186/1475-2840-13-30.
Azilsartan, an angiotensin II type 1 (AT1) receptor blocker (ARB), has a higher affinity for and slower dissociation from AT1 receptors and shows stronger inverse agonism compared to other ARBs. Possible benefits of azilsartan in diabetic vascular dysfunction have not been established.
We measured vascular reactivity of aortic rings in male KKAy diabetic mice treated with vehicle, 0.005% azilsartan, or 0.005% candesartan cilexetil for 3 weeks. Expression of markers of inflammation and oxidative stress was measured using semiquantitative RT-PCR in the vascular wall, perivascular fat, and skeletal muscle. Phosphorylation of endothelial nitric oxide synthase (eNOS) at Ser1177 and Thr495 was measured using Western blotting, and the ratio of phosphorylation at Ser1177 to phosphorylation at Thr495 was used as a putative indicator of vascular eNOS activity.
(1) Vascular endothelium-dependent relaxation with acetylcholine in KKAy mice was improved by azilsartan treatment compared to candesartan cilexetil; (2) the ratio of Ser1177/Thr495 phosphorylation of eNOS was impaired in KKAy and was effectively restored by azilsartan; (3) anomalies in the expression levels of monocyte chemotactic protein 1 (MCP1), F4/80, NAD(P)H oxidase (Nox) 2, and Nox4 of the aortic wall and in the expression of TNFα in the perivascular fat were strongly attenuated by azilsartan compared to candesartan cilexetil.
These results provide evidence that azilsartan prevents endothelial dysfunction in diabetic mice, more potently than does candesartan cilexetil. Azilsartan's higher affinity for and slower dissociation from AT1 receptors may underlie its efficacy in diabetic vascular dysfunction via a dual effect on uncoupled eNOS and on Nox.
阿齐沙坦是一种血管紧张素II 1型(AT1)受体阻滞剂(ARB),与其他ARB相比,它对AT1受体具有更高的亲和力和更慢的解离速度,并且表现出更强的反向激动作用。阿齐沙坦在糖尿病血管功能障碍方面的潜在益处尚未得到证实。
我们对雄性KKAy糖尿病小鼠进行了为期3周的实验,分别用赋形剂、0.005%阿齐沙坦或0.005%坎地沙坦酯治疗,然后测量主动脉环的血管反应性。使用半定量逆转录聚合酶链反应(RT-PCR)测量血管壁、血管周围脂肪和骨骼肌中炎症和氧化应激标志物的表达。使用蛋白质印迹法测量内皮型一氧化氮合酶(eNOS)在丝氨酸1177和苏氨酸495位点的磷酸化水平,并将丝氨酸1177位点的磷酸化与苏氨酸495位点的磷酸化之比用作血管eNOS活性的推定指标。
(1)与坎地沙坦酯相比,阿齐沙坦治疗可改善KKAy小鼠中乙酰胆碱介导的血管内皮依赖性舒张;(2)KKAy小鼠中eNOS的丝氨酸1177/苏氨酸495磷酸化比值受损,而阿齐沙坦可有效恢复该比值;(3)与坎地沙坦酯相比,阿齐沙坦可显著减轻主动脉壁中单核细胞趋化蛋白1(MCP1)、F4/80、NAD(P)H氧化酶(Nox)2和Nox4的表达异常以及血管周围脂肪中肿瘤坏死因子α(TNFα)的表达异常。
这些结果表明,阿齐沙坦比坎地沙坦酯更有效地预防糖尿病小鼠的内皮功能障碍。阿齐沙坦对AT1受体的更高亲和力和更慢解离速度可能是其通过对解偶联eNOS和Nox的双重作用而在糖尿病血管功能障碍中发挥疗效的基础。
