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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Reduction of cerebral injury in stroke-prone spontaneously hypertensive rats by amlodipine.
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Reduction of cerebral injury in stroke-prone spontaneously hypertensive rats by amlodipine.

机译:氨氯地平减轻中风自发性高血压大鼠的脑损伤。

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Dihydropyridine Ca(2+) channel antagonists, initiated together with high salt intake, prevent the development of hypertension and subsequent cerebral damage in stroke-prone spontaneously hypertensive rats (SHRSP). We hypothesized that the dihydropyridine Ca(2+) channel antagonist amlodipine (approximately 15 mg/kg/day) could also reverse established hypertension and cerebral damage. SHRSP drank 1% NaCl from 8 weeks of age. Cerebral damage (cerebral edema and blood-brain barrier integrity) was investigated with magnetic resonance imaging twice a week. Systolic blood pressure was measured weekly. All rats developed severe hypertension and subsequent cerebral damage (defined as day 0). Untreated controls (n=7) died at day 12 (range: 7-28). Oral treatment with amlodipine (n=7), initiated at day 0, reduced systolic blood pressure, reversed cerebral edema and restored blood-brain barrier integrity. Systolic blood pressure remained low and eventually rats died after 450 days (range: 350-580) showing nephrosis but no recurrence of cerebral damage. In conclusion, established hypertension and cerebral damage are reversed by amlodipine in SHRSP.
机译:Dihydropyridine Ca(2+)通道拮抗剂,与高盐摄入量一起启动,可预防中风倾向性自发性高血压大鼠(SHRSP)的高血压发展和随后的脑损伤。我们假设二氢吡啶Ca(2+)通道拮抗剂氨氯地平(约15 mg / kg /天)也可以逆转既定的高血压和脑损伤。 SHRSP从8周龄开始饮用1%NaCl。每周两次磁共振成像检查脑损伤(脑水肿和血脑屏障完整性)。每周测量收缩压。所有大鼠均出现严重的高血压和随后的脑损伤(定义为第0天)。未经治疗的对照组(n = 7)在第12天死亡(范围:7-28)。从第0天开始口服氨氯地平(n = 7)口服治疗,可降低收缩压,逆转脑水肿并恢复血脑屏障的完整性。收缩压仍然很低,最终大鼠在450天(范围:350-580)后死亡,显示出肾病但没有脑损伤的复发。总之,氨氯地平在SHRSP中可以逆转既定的高血压和脑损伤。

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