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Naloxone blocks 'anxiolytic' effects of neuropeptide Y.

机译:纳洛酮阻断神经肽Y的“抗焦虑”作用。

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Intracerebroventricular injection of neuropeptide Y (NPY) produces potent 'anxiolytic' effects in animal models of anxiety. Administration of opioid receptor antagonists suppresses NPY-induced food intake and thermogenesis. The present study examined whether the opiate antagonist naloxone would also suppress the 'anxiolytic' effects of neuropeptide Y. Following training and stabilization of responding in an operant conflict model of anxiety, rats were injected with either NPY or diazepam. Both NPY (veh., 2, 4, 6 microg, i.c.v.) and chlordiazepoxide (veh., 2, 4, 6 mg/kg, i.p.) produced a dose-dependent increase in punished responding in the conflict test. The 'anxiolytic' effects of NPY were not blocked by the administration of flumazenil (3, 6, 12 mg/kg, i.p.). The administration of naloxone (0.25-2.0 mg/kg, s.c.) antagonized the effects of NPY. Central administration of the selective mu opiate antagonist CTAP (1 microg, i.c.v.) partially blocked NPY-induced conflict responding. These results support the hypothesis that NPY may play an important role in experimental anxiety independent of the benzodiazepine receptor and further implicate the opioid system in the behavioral expression of anxiety.
机译:脑室内注射神经肽Y(NPY)在焦虑动物模型中产生有效的“抗焦虑”作用。阿片受体拮抗剂的给药抑制了NPY诱导的食物摄入和生热。本研究检查了阿片拮抗剂纳洛酮是否还会抑制神经肽Y的“抗焦虑”作用。在焦虑的操作性冲突模型中训练和稳定反应后,给大鼠注射NPY或地西epa。在冲突测试中,NPY(2、4、6微克,v.v。)和氯二氮杂卓(2、4、6mg / kg,v.v。)均产生剂量依赖性增加的惩罚反应。氟马西尼(3、6、12 mg / kg,腹腔注射)的给药并未阻止NPY的“抗焦虑”作用。纳洛酮(0.25-2.0mg / kg,皮下注射)的给药拮抗了NPY的作用。中央施用选择性阿片拮抗剂CTAP(1 microg,i.c.v.)部分阻断了NPY诱导的冲突反应。这些结果支持以下假设:NPY在独立于苯二氮卓受体的实验性焦虑中可能起重要作用,并进一步使阿片类药物系统参与焦虑的行为表达。

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