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依替斯的明抑制胆碱酯酶对正常大鼠脑血流-代谢比值的长期影响。

Prolonged effects of cholinesterase inhibition with eptastigmine on the cerebral blood flow-metabolism ratio of normal rats.

作者信息

Scremin O U, Scremin A M, Heuser D, Hudgell R, Romero E, Imbimbo B P

机构信息

Veterans Affairs Medical Center, Los Angeles, California.

出版信息

J Cereb Blood Flow Metab. 1993 Jul;13(4):702-11. doi: 10.1038/jcbfm.1993.89.

Abstract

The cerebrovascular and metabolic effects of the novel cholinesterase inhibitor eptastigmine were tested in conscious rats. The drug was administered by single intravenous injection, and blood flow or glucose utilization were assessed in 38 brain regions by quantitative autoradiographic techniques. A dose-dependent increase in regional cerebral blood flow (rCBF) was obtained for i.v. doses ranging from 0.5 to 3 mg kg-1. Forty minutes after the dose of 1.5 mg kg-1, average rCBF of the 38 regions studied was (mean +/- SD) 2.62 +/- 0.62 ml g-1 min-1, a value significantly higher than that of saline-injected controls (1.46 +/- 0.26; p < 0.005). In contrast, a similar dose of eptastigmine did not significantly alter regional cerebral glucose utilization (rCGU) (0.90 +/- 0.21 mumol g-1 min-1) when compared with saline-injected controls (0.99 +/- 0.08 mumol g-1 min-1). A linear correlation between rCBF and rCGU was observed both in saline (r = 0.871) and eptastigmine (r = 0.873)-injected animals but the slope of the regression line of rCBF on rCGU was significantly higher (p < 0.01) in the eptastigmine group (2.863 +/- 0.266) than in the controls that received saline (1.00 +/- 0.094). The cerebral vasodilatation induced by eptastigmine peaked at 40 min after drug administration. No toxic signs were observed at the doses used. Mean arterial blood pressure decreased after 0.5 mg kg-1 (control = 109.3 +/- 10.56 mm Hg; eptastigmine = 96.6 +/- 8.10 mm Hg) but did not differ from control at the higher doses. It is concluded that eptastigmine induces a long-lasting increase in rCBF and a significant enhancement of the rCBF:rCGU ratio in most regions. The results suggest an important role of endogenous acetylcholine in the control of cerebral perfusion.

摘要

在清醒大鼠中测试了新型胆碱酯酶抑制剂依他斯的明对脑血管和代谢的影响。通过单次静脉注射给药,采用定量放射自显影技术评估38个脑区的血流量或葡萄糖利用率。静脉注射剂量为0.5至3mg/kg时,局部脑血流量(rCBF)呈剂量依赖性增加。给予1.5mg/kg剂量40分钟后,所研究的38个区域的平均rCBF为(均值±标准差)2.62±0.62ml/g-1min-1,该值显著高于注射生理盐水的对照组(1.46±0.26;p<0.005)。相比之下,与注射生理盐水的对照组(0.99±0.08μmol/g-1min-1)相比,相同剂量的依他斯的明并未显著改变局部脑葡萄糖利用率(rCGU)(0.90±0.21μmol/g-1min-1)。在注射生理盐水(r=0.871)和依他斯的明(r=0.873)的动物中均观察到rCBF与rCGU之间存在线性相关性,但依他斯的明组(2.863±0.266)中rCBF对rCGU的回归线斜率显著高于接受生理盐水的对照组(1.00±0.094)(p<0.01)。依他斯的明诱导的脑血管舒张在给药后40分钟达到峰值。在所使用的剂量下未观察到毒性迹象。给予0.5mg/kg后平均动脉血压下降(对照组=109.3±10.56mmHg;依他斯的明=96.6±8.10mmHg),但在较高剂量下与对照组无差异。结论是依他斯的明可诱导rCBF长期增加,并显著提高大多数区域的rCBF:rCGU比值。结果表明内源性乙酰胆碱在脑灌注控制中起重要作用。

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