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(±)-(E)-1-(3-氟-6,11-二氢二苯并[b,e] - 氧杂卓-11-基)-4-(3-苯基-2-丙烯基)-哌嗪二马来酸盐对大鼠蛛网膜下腔出血模型中脑血管痉挛和脑循环障碍的影响

Effect of (+/-)-(E)-1-(3-fluoro-6,11-dihydrodibenz[b,e]-oxepine-11 -yl)-4-(3-phenyl-2-propenyl)-piperazine dimaleate on cerebral vasospasm and impairment of cerebral circulation in subarachnoid hemorrhage model in rats.

作者信息

Honda Y, Minato H, Masuda Y, Fujitani B, Hosoki K

机构信息

Department of Pharmacology I, Dainippon Pharmaceutical, Co, Ltd, Osaka, Japan.

出版信息

Arzneimittelforschung. 1996 Aug;46(8):746-50.

PMID:9125271
Abstract

A subarachnoid hemorrhage (SAH) model in rats was produced by the injection of homologous blood into the cisterna magna. Effects of AJ-3941 ((+/-)-(E)-1-(3-fluoro-6,11 -dihydrodibenz[b,e]-oxepine-11-yl)-4-(3-phenyl-2-propenyl)-p iperazine dimaleate, CAS 143110-70-7) on the development of cerebral vasospasm and the change of regional cerebral blood flow (rCBF) following SAH was investigated in this model. Cerebral vasospasm following SAH showed a biphasic pattern with an early phrase at 10 min and a late phrase on 1 day after blood injection. The physiological parameters (blood pressure, heart rate and blood gas contents) remained stable within the physiological range throughout the course of the experiment. AJ-3941 (0.01 mg/kg i.v. or 0.3 mg/kg p.o.) significantly prevented the development of late phase cerebral vasospasm. Cisternal injection of homologous blood significantly reduced rCBF immediately after the injection and the reduction lasted during the observation period (30 min). Reduction in rCBF after the injection of homologous blood was prevented by AJ-3941 (0.01 mg/kg i.v.). rCBF in AJ-3941-treated rats completely returned to the basal values after 30 min. The present suggest that AJ-3941 may be useful in the prevention of late spasm and in the improvement of cerebral circulation impaired with SAH.

摘要

通过向大鼠小脑延髓池注射同源血液建立蛛网膜下腔出血(SAH)模型。在此模型中研究了AJ - 3941((±)-(E)-1 -(3 - 氟 - 6,11 - 二氢二苯并[b,e] - 氧杂环庚三烯 - 11 - 基)-4 -(3 - 苯基 - 2 - 丙烯基)- 哌嗪二马来酸盐,CAS 143110 - 70 - 7)对SAH后脑血管痉挛发展及局部脑血流量(rCBF)变化的影响。SAH后的脑血管痉挛呈双相模式,血液注射后10分钟出现早期阶段,1天后出现晚期阶段。在整个实验过程中,生理参数(血压、心率和血气含量)在生理范围内保持稳定。AJ - 3941(静脉注射0.01mg/kg或口服0.3mg/kg)显著预防了晚期脑血管痉挛的发展。小脑延髓池注射同源血液后立即显著降低rCBF,且在观察期(30分钟)内持续降低。AJ - 3941(静脉注射0.01mg/kg)可预防同源血液注射后rCBF的降低。AJ - 3941治疗的大鼠的rCBF在30分钟后完全恢复到基础值。目前的研究表明,AJ - 3941可能有助于预防晚期痉挛并改善SAH所致的脑循环障碍。

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