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吗啡急性和慢性处理后小鼠脑离散区域中GABA受体变化的分析。

An analysis of GABA receptor changes in the discrete regions of mouse brain after acute and chronic treatments with morphine.

作者信息

Sivam S P, Nabeshima T, Ho I K

出版信息

J Neurochem. 1982 Oct;39(4):933-9. doi: 10.1111/j.1471-4159.1982.tb11479.x.

Abstract

The effects of morphine on the affinity and distribution of GABA receptors in the mouse regions (striatum, medulla, diencephalon, cortex, and cerebellum) were investigated in relation to: (a) acute administration, (b) chronic administration (tolerance), (c) precipitated withdrawal by naloxone, an opiate antagonist, and (d) abrupt withdrawal for 8 and 24 h. The alterations in the affinity as reflected by the dissociation constant (KD) and the number of receptors (Bmax) in the synaptic membranes obtained from controls and various treatments were determined by radioligand binding assay using [3H]muscimol as a ligand. Significant changes were observed in striatum, medulla, and diencephalon, whereas other regions including whole brain exhibited marginal changes. In general the number of GABA receptors increased after tolerance development, which upon abrupt withdrawal returned to control levels except in the case of naloxone-induced precipitated withdrawal. The affinity changes in different regions were diverse in nature and were not evident in the whole brain membranes. These results indicate that: (as) the regional alterations in the affinity and distribution of GABA receptors may play a role in the induction, maintenance, and regression of morphine tolerance; (b) abrupt withdrawal and antagonist precipitated withdrawal affect the GABA system differently, (c) chronic morphine treatment appears to influence the GABA receptors in the cerebellum, a region generally known for its lack of opiate receptors.

摘要

研究了吗啡对小鼠不同脑区(纹状体、延髓、间脑、皮层和小脑)γ-氨基丁酸(GABA)受体亲和力和分布的影响,涉及以下方面:(a)急性给药;(b)慢性给药(耐受性);(c)用阿片类拮抗剂纳洛酮诱发戒断反应;(d)突然戒断8小时和24小时。通过使用[³H]蝇蕈醇作为配体的放射性配体结合试验,测定了对照组和各种处理组突触膜中解离常数(KD)和受体数量(Bmax)所反映的亲和力变化。在纹状体、延髓和间脑中观察到显著变化,而包括全脑在内的其他区域变化不明显。一般来说,耐受性形成后GABA受体数量增加,突然戒断后除纳洛酮诱发的戒断反应外均恢复到对照水平。不同脑区的亲和力变化性质各异,在全脑膜中不明显。这些结果表明:(a)GABA受体亲和力和分布的区域变化可能在吗啡耐受性的诱导、维持和消退中起作用;(b)突然戒断和拮抗剂诱发的戒断反应对GABA系统的影响不同;(c)慢性吗啡治疗似乎会影响小脑的GABA受体,而小脑通常被认为缺乏阿片受体。

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