精神药理学中的低剂量效应:个体发生的考虑。

Linda Patia Spear, Elena I Varlinskaya
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引用次数: 9

摘要

低剂量的精神活性药物通常会引起与服用更大剂量药物后观察到的相反的行为特征。我们的实验室观察到,这些影响在大鼠身上往往是年龄特异性的。例如,中剂量到高剂量的多巴胺激动剂阿波啡会增加运动能力,而低剂量暴露后会抑制运动活动,这种低剂量效应直到青春期才持续出现。5HT(1a)受体激动剂8-OH-DPAT较早出现低剂量“矛盾”效应,在断奶后期,而不是新生期,大鼠在低剂量时表现出摄食行为增加,而在高剂量时表现出抑制。与这些低剂量药物效应表达的个体发生性增加相反,低剂量乙醇只在青春期大鼠中出现社会行为的促进作用,而在成年大鼠中则没有,尽管在两个年龄的大鼠中都可以看到高剂量乙醇对社会互动的抑制作用。这种类似激效的低剂量刺激似乎部分与过度补偿有关,在随后的刺激反应之前有短暂的社会抑制,并且与急性耐受性有许多个体发生上的相似之处,急性耐受性是对乙醇的一种特征明确、迅速出现的适应。本文讨论了这些和其他个体发生学发现对激效研究的意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Low dose effects in psychopharmacology: ontogenetic considerations.

Low doses of psychoactive drugs often elicit a behavioral profile opposite to that observed following administration of more substantial doses. Our laboratory has observed that these effects are often age-specific in rats. For instance, whereas moderate to high doses of the dopamine agonist apomorphine increase locomotion, suppressed locomotor activity is seen following low dose exposure, with this low dose effect not emerging consistently until adolescence. A somewhat earlier emergence of a low dose "paradoxical" effect is seen with the 5HT(1a) receptor agonist, 8-OH-DPAT, with late preweanling, but not neonatal, rats showing increases in ingestive behavior at low doses but suppression at higher doses. In contrast to these ontogenetic increases in expression of low dose drug effects, low dose facilitation of social behavior is seen following ethanol only in adolescent rats and not their mature counterparts, although suppression of social interactions at higher doses is seen at both ages. This hormesis-like low dose stimulation appears related in part to overcompensation, with brief social suppression preceding the subsequent stimulation response, and also bears a number of ontogenetic similarities to acute tolerance, a well characterized, rapidly emerging adaptation to ethanol. Implications of these and other ontogenetic findings for studies of hormesis are discussed.

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