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苯二氮䓬类相关药物对清醒恒河猴的呼吸影响。

Respiratory effects of benzodiazepine-related drugs in awake rhesus monkeys.

作者信息

Wettstein J G, Teeple E S, Morse W H

机构信息

Department of Psychiatry, Harvard Medical School, Boston, Massachusetts.

出版信息

J Pharmacol Exp Ther. 1990 Dec;255(3):1328-34.

PMID:1979816
Abstract

The respiratory effects of several benzodiazepine (BZ) agonists and inverse agonists were compared with those of buspirone and pentobarbital in awake rhesus monkeys. Subjects, fitted with a helmet that served as a pressure displacement plethysmograph, were studied in a ventilated, sound-attenuating chamber; ventilatory frequency, tidal volume (VT) and minute volume (VE) were determined from the plethysmograph signal. During experimental sessions monkeys inhaled either 5% carbon dioxide (CO2) mixed in air or air alone according to a fixed alternating schedule. BZ agonists (alprazolam, 0.01-1.0 mg/kg; lorazepam, 0.3-10.0 mg/kg; quazepam, 1.0-5.6 mg/kg) decreased VT and VE during both 5% CO2 and air inhalation. Pentobarbital (3.0-30.0 mg/kg) also decreased VT and VE and additionally decreased respiratory frequency in monkeys breathing 5% CO2. Two BZ inverse agonists, the beta-carbolines beta-CCE and FG 7142 (0.3-5.6 or 10.00 mg/kg), increased frequency and had no effect on VT, resulting in an increase in VE in monkeys breathing either 5% CO2 or air. The weak BZ inverse agonist CGS 8216 (0.3-5.6 mg/kg) similarly increased ventilation only in monkeys breathing air. Buspirone (0.03-0.3 mg/kg), like the beta-carbolines, increased frequency and VE and, like the BZ agonists, decreased VT. The BZ antagonist Ro15-1788 (0.1-3.0 mg/kg) had little or no effect on ventilation, but Ro15-1788 and also CGS 8216 (both at 1.0 mg/kg) attenuated the respiratory depressant effects of lorazepam or alprazolam. In turn, alprazolam (0.03-0.3 mg/kg) and quazepam (1.0-3.0 mg/kg) attenuated the respiratory stimulant effects of FG 7142.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在清醒的恒河猴中,比较了几种苯二氮䓬(BZ)激动剂和反向激动剂与丁螺环酮和戊巴比妥的呼吸效应。给受试动物佩戴用作压力位移体积描记器的头盔,在通风、隔音的舱室内进行研究;通过体积描记器信号测定呼吸频率、潮气量(VT)和分钟通气量(VE)。在实验过程中,猴子按照固定的交替时间表吸入5%二氧化碳(CO2)与空气的混合气或仅吸入空气。BZ激动剂(阿普唑仑,0.01 - 1.0mg/kg;劳拉西泮,0.3 - 10.0mg/kg;夸西泮,1.0 - 5.6mg/kg)在吸入5% CO2和空气时均降低VT和VE。戊巴比妥(3.0 - 30.0mg/kg)也降低VT和VE,并且在吸入5% CO2的猴子中还降低呼吸频率。两种BZ反向激动剂,β-咔啉类β-CCE和FG 7142(0.3 - 5.6或10.00mg/kg)增加频率且对VT无影响,导致吸入5% CO2或空气的猴子的VE增加。弱BZ反向激动剂CGS 8216(0.3 - 5.6mg/kg)仅在吸入空气的猴子中同样增加通气。丁螺环酮(0.03 - 0.3mg/kg)与β-咔啉类一样增加频率和VE,与BZ激动剂一样降低VT。BZ拮抗剂Ro15 - 1788(0.1 - 3.0mg/kg)对通气几乎没有影响,但Ro15 - 1788以及CGS 8216(均为1.0mg/kg)减弱了劳拉西泮或阿普唑仑的呼吸抑制作用。反过来,阿普唑仑(0.03 - 0.3mg/kg)和夸西泮(1.0 - 3.0mg/kg)减弱了FG 7142的呼吸兴奋作用。(摘要截短于250字)

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