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首页> 外文期刊>Journal of hypertension >Effects of losartan on cerebral arteries in stroke-prone spontaneously hypertensive rats.
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Effects of losartan on cerebral arteries in stroke-prone spontaneously hypertensive rats.

机译:氯沙坦对脑卒中脑动脉脑动脉的影响自发性高血压大鼠。

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OBJECTIVE: To investigate in young salt-loaded stroke-prone spontaneously hypertensive rats (SHR-SP) the effects of a long-term administration of the angiotensin II AT1 receptor antagonist losartan [1 mg/kg (L1) and 10 mg/kg (L10) per day, from 5 to 20 weeks of age] on the structural and functional characteristics of the middle cerebral artery. METHODS: Morphological measurements and isometric tension recordings (myograph, contractile responses to potassium chloride and serotonin, relaxant responses to bradykinin and sodium nitroprusside) were performed on isolated vessels from randomly selected control and losartan-treated SHR-SP and age-matched Wistar-Kyoto (WKY) rats killed at ages 6-7, 10-11 and 16-17 weeks. RESULTS: Whereas all control SHR-SP had died within 18 weeks of being born, losartan at both doses afforded full protection against stroke and mortality. Losartan limited malignant hypertension development dose-dependently. Age-related increases in cerebral arterial wall thickness and wall:lumen ratio were not affected (L1) or limited slightly (L10) by losartan. In control SHR-SP, contractile responses of cerebral arteries to agonists decreased with ageing and stroke occurrence and were significantly smaller than those of age-matched WKY rat arteries. Losartan limited the cerebrovascular contractility impairment dose-dependently in SHR-SP but did not affect the WKY rat cerebral artery contractility. In addition, losartan limited the age-related alteration of the endothelium-dependent relaxation of cerebral arteries observed in control SHR-SP dose-dependently. CONCLUSIONS: In SHR-SP, losartan prevented stroke and improved the cerebral artery's smooth muscle and endothelial cell functions, which are altered during ageing and impaired even more dramatically by stroke occurrence.
机译:目的:探讨青少年盐水脑卒中的自发性高血压大鼠(SHR-SP)长期施用血管紧张素II AT1受体拮抗剂氯沙坦的影响[1mg / kg(L1)和10mg / kg( L10)每天,从5至20周龄]在中间脑动脉的结构和功能特征。方法:形态学测量和等距张力记录(Imograph,对氯化钾的收缩反应,对Bradykinin和Bradykinin和Nitroprseide的缓解反应)进行来自随机选择的对照和氯沙坦处理的SHR-SP和Agate-Formated Wistar-Kyoto的血清(WKY)大鼠在6-7岁,10-11和16-17周丧生。结果:虽然所有对照SHR-SP在出生的18周内已在18周内死亡,但氯沙坦两种剂量都充分保护了冲程和死亡率。洛萨兰有限的恶性高血压发育依赖性剂量。年龄相关的脑动脉壁厚和壁的增加:腔比不受影响(L1)或氯沙坦略微有限(L10)。在对照SHR-SP中,脑动脉对激动剂的收缩反应随着衰老和中风发生而降低,并且显着小于年龄匹配的WKY大鼠动脉。洛萨兰限制脑血管收缩性损伤剂量依赖于SHR-SP,但不影响WKY大鼠脑动脉收缩性。此外,氯沙坦限制了依赖于控制Sh-Sp剂量观察到的脑动脉内皮依赖性放松的年龄相关的易变化。结论:在SHR-SP中,氯沙坦预防脑卒中和改善脑动脉的平滑肌和内皮细胞功能,其在老化期间改变并通过中风发生甚至更大地损害。

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