Anti-conflict effects of benzodiazepines in rhesus monkeys: relationship with therapeutic doses in humans and role of GABAA receptors.

Rowlett JK; Lelas S; Tornatzky W; Licata SC

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Anti-conflict effects of benzodiazepines in rhesus monkeys: relationship with therapeutic doses in humans and role of GABAA receptors.

机译：苯二氮卓类在恒河猴中的抗冲突作用：与人类治疗剂量的关系以及GABAA受体的作用。

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RATIONALE AND OBJECTIVES: Conflict procedures are used to study mechanisms underlying the anxiolytic effects of benzodiazepines (BZs). We established a conflict procedure with rhesus monkeys in order to examine the role of GABAA receptors in the anxiolytic-like effects of BZs. METHODS: Four rhesus monkeys responded under a two-component multiple schedule in which responding was maintained under a fixed-ratio schedule of food delivery in the absence (non-suppressed responding) and presence (suppressed responding) of response-contingent electric shock. RESULTS: Conventional BZs (alprazolam, flunitrazepam, clonazepam, nitrazepam, lorazepam, bromazepam, diazepam, flurazepam, clorazepate, chlordiazepoxide) engendered increases in the average rates of suppressed responding at low to intermediate doses and decreased the average rates of non-suppressed responding at higher doses. Positive correlations were observed when the therapeutic potencies of BZs in humans were compared with potencies to increase the rates of suppressed responding (R2=0.83) or decrease the rates of non-suppressed responding (R2=0.60). The 5-HT1A agonist buspirone increased the rates of suppressed responding, although the effects were modest, whereas the opioid morphine lacked anti-conflict effects. The BZ antagonist flumazenil also modestly increased the rates of suppressed responding. A relatively low dose of flumazenil enhanced, while a high dose blocked, alprazolam's anti-conflict effects. Compounds selective for alpha1 subunit-containing GABAA receptors (zolpidem, zaleplon, CL218,872) engendered relatively weak increases in the rates of suppressed responding. CONCLUSIONS: A rhesus monkey conflict procedure was established with predictive validity for therapeutic doses in people and provided evidence that anxiolytic-like effects of BZs can occur with relatively low intrinsic efficacy at GABAA receptors and are reduced by alpha1GABAA receptor selectivity.

机译：理由和目标：使用冲突程序研究苯二氮卓类药物（BZs）抗焦虑作用的潜在机制。我们建立了与恒河猴的冲突程序，以检查GABAA受体在BZ的抗焦虑作用中的作用。方法：四只恒河猴在两成分的多重时间表下做出反应，其中在不存在（非抑制性反应）和存在（抑制性反应）电击的情况下，以固定比例的食物递送速率维持反应。结果：常规BZs（阿普唑仑，氟尼西epa，氯硝西,、硝西epa，劳拉西m，溴马西m，地西epa，氟拉西m，氯拉西ate，氯二氮卓）导致中剂量低应答时的平均抑制率增加，而非抑制者的平均发生率降低。更高的剂量。当将人体内BZ的治疗效力与增加抑制应答率（R2 = 0.83）或降低未抑制应答率（R2 = 0.60）的效力进行比较时，观察到正相关。 5-HT1A激动剂丁螺环酮可增加抑制反应的速率，尽管作用不大，而阿片类吗啡缺乏抗冲突作用。 BZ拮抗剂氟马西尼也可适度增加抑制反应的速率。较低剂量的氟马西尼可增强，而高剂量则可抑制阿普唑仑的抗冲突作用。对含α1亚基的GABAA受体具有选择性的化合物（zolpidem，zaleplon，CL218,872）导致抑制响应率的增加相对较弱。结论：建立了恒河猴冲突程序，具有对人的治疗剂量的预测有效性，并提供证据表明，BZ的抗焦虑样作用可能以相对较低的内在功效发生在GABAA受体上，并被alpha1GABAA受体选择性降低。

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《Psychopharmacology》 |2006年第2期|共11页
作者
Rowlett JK; Lelas S; Tornatzky W; Licata SC;
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正文语种 eng
中图分类药学;
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Anti-Anxiety Agents; Benzodiazepines; Conflict (Psychology); Receptors; GABA-A; 抗焦虑药; 苯二氮ZHUO类; 冲突(心理学); 受体; GABA-A;

机译：Anti-Anxiety Agents;Benzodiazepines;Conflict (Psychology);Receptors;GABA-A;抗焦虑药;苯二氮|ZHUO|类;冲突(心理学);受体;GABA-A;

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1. Anti-conflict effects of benzodiazepines in rhesus monkeys: relationship with therapeutic doses in humans and role of GABAA receptors. [J] . Rowlett JK, Lelas S, Tornatzky W, Psychopharmacology . 2006,第2期

机译：苯二氮卓类在恒河猴中的抗冲突作用：与人类治疗剂量的关系以及GABAA受体的作用。
2. Cognition-impairing effects of benzodiazepine-type drugs: role of GABAA receptor subtypes in an executive function task in rhesus monkeys. [J] . Leah Makaron, Casey A Moran, Ojas Namjoshi, Pharmacology, Biochemistry and Behavior . 2013,第4期

机译：苯二氮卓类药物对认知的损害作用：GABAA受体亚型在恒河猴的执行功能任务中的作用。
3. Cognition-impairing effects of benzodiazepine-type drugs: role of GABAA receptor subtypes in an executive function task in rhesus monkeys. [J] . Leah Makaron, Casey A Moran, Ojas Namjoshi, Pharmacology, Biochemistry and Behavior . 2013,第4期

机译：苯并二氮杂毒药型药物的认知损害作用：Gabaa受体亚型在恒河猴执行职能任务中的作用。
4. Sar measurements in the rhesus monkey ankle: implications for humans [C] . R. G. Olsen NATO advanced research workshop on radio frequency radiation dosimetry and its relationship to the biological effects of electromagnetic fields . 2000

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5. Agonistic behavior between rhesus monkeys (Macaca mulatta) and humans in Nepal. [D] . Pedersen, Bonnie Lynn. 1997

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6. Cognition-Impairing Effects of Benzodiazepine-Type Drugs: Role of GABAA Receptor Subtypes in an Executive Function Task in Rhesus Monkeys [O] . Leah Makaron, Casey A. Moran, Ojas Namjoshi, -1

机译：苯二氮卓类药物的认知限制效果：在恒河猴的执行功能任务GaBaa受体亚型中的作用
7. Cognition-impairing effects of benzodiazepine-type drugs: Role of GABAA receptor subtypes in an executive function task in rhesus monkeys [O] . Leah Makaron, Casey A. Moran, Ojas Namjoshi, 2013

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机译：Nv 1895 Guanazole Triazole 3,5-二氨基-s的重复剂量毒性研究I.V.施用Beagle犬和恒河猴，小鼠和大鼠的单剂量毒性研究以及兔和豚鼠的局部作用和刺激作用

Anti-conflict effects of benzodiazepines in rhesus monkeys: relationship with therapeutic doses in humans and role of GABAA receptors.

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