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关于伊拉地平在中风方面的实验研究。

Experimental studies with isradipine in stroke.

作者信息

Sauter A, Rudin M

机构信息

Preclinical Research, Sandoz Pharma Ltd, Basle, Switzerland.

出版信息

Drugs. 1990;40 Suppl 2:44-51. doi: 10.2165/00003495-199000402-00012.

Abstract

The effects of isradipine in a rat model of embolic stroke [permanent occlusion of the left middle cerebral artery (MCA)] are reviewed. Isradipine, when present or given up to 4 hours after the onset of stroke, reduces the infarct size, determined by magnetic resonance imaging (MRI) 24 hours, and by histology 5 days, after MCA occlusion. These cytoprotective effects seem to be permanent and are paralleled by an improvement in the neurological deficit. Isradipine has proved to be the most potent and effective calcium antagonist for reducing the infarct size compared with other representatives of this class of drugs such as nimodipine, nicardipine and flunarizine. Isradipine is cytoprotective after a stroke when used as an antihypertensive: at doses which normalise high blood pressure in spontaneously hypertensive rats, isradipine reduces by more than 60% the infarct size caused by a subsequent stroke. Since the lowering of blood pressure, e.g. by a calcium antagonist that does not cross the blood-brain barrier, is ineffective in reducing the infarct size, normalisation of blood pressure alone cannot account for the reductions in infarct size observed with isradipine. The antihypertensive drug isradipine seems rather to offer the additional benefit of attenuating the consequences of an eventual stroke. If clinically confirmed, this will be of considerable therapeutic importance. Evidence is presented that isradipine has at least 2 mechanisms within the brain that might be responsible for cytoprotection in stroke.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

综述了伊拉地平在大鼠栓塞性脑卒中模型(永久性闭塞左侧大脑中动脉)中的作用。在脑卒中发作时或发作后4小时内给予伊拉地平,可减小梗死灶大小,这一效果在大脑中动脉闭塞后24小时通过磁共振成像(MRI)测定,5天后通过组织学测定。这些细胞保护作用似乎是永久性的,同时神经功能缺损也有所改善。与尼莫地平、尼卡地平和氟桂利嗪等这类药物的其他代表药物相比,伊拉地平已被证明是最有效且最具效力的可减小梗死灶大小的钙拮抗剂。伊拉地平作为抗高血压药物在脑卒中后具有细胞保护作用:在能使自发性高血压大鼠血压正常化的剂量下,伊拉地平可使随后脑卒中所致的梗死灶大小减小60%以上。由于单纯降低血压(例如通过一种不能透过血脑屏障的钙拮抗剂)在减小梗死灶大小方面无效,因此单纯血压正常化无法解释伊拉地平所观察到的梗死灶大小减小情况。抗高血压药物伊拉地平似乎还具有减轻最终脑卒中后果的额外益处。如果得到临床证实,这将具有相当大的治疗重要性。有证据表明伊拉地平在脑内至少有2种机制可能负责脑卒中时的细胞保护作用。(摘要截短于250字)

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