Ultra-low doses of methamphetamine suppress 5-hydroxytryptophan-induced head-twitch response in mice during aging.

IF 1.6 4区 心理学 Q3 BEHAVIORAL SCIENCES
Behavioural Pharmacology Pub Date : 2024-10-01 Epub Date: 2024-08-05 DOI:10.1097/FBP.0000000000000789
Yina Sun, Seetha Chebolu, Nissar A Darmani
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引用次数: 0

Abstract

The head-twitch response (HTR) in mice is considered a behavioral assay for activation of 5-HT 2A receptors in rodents. It can be evoked by direct-acting 5-HT 2A receptor agonists such as (±)-2,5-dimethoxy-4-iodoamphetamine, 5-hydroxytryptamine precursors [e.g. 5-hydroxytryptophan (5-HTP)], and selective 5-hydroxytryptamine releasers (e.g. d -fenfluramine). The nonselective monoamine releaser methamphetamine by itself does not produce the HTR but can suppress both (±)-2,5-dimethoxy-4-iodoamphetamine- and d -fenfluramine-evoked HTRs across ages via concomitant activation of the inhibitory serotonergic 5-HT 1A or adrenergic α 2 receptors. Currently, we investigated: (1) the ontogenic development of 5-HTP-induced HTR in 20-, 30-, and 60-day-old mice; (2) whether pretreatment with ultra-low doses of methamphetamine (0.1, 0.25, and 0.5 mg/kg, intraperitoneally) can suppress the frequency of 5-HTP-induced HTR at different ages; and (3) whether the inhibitory serotonergic 5-HT 1A or adrenergic α 2 receptors may account for the potential inhibitory effect of methamphetamine on 5-HTP-induced HTR. In the presence of a peripheral decarboxylase inhibitor (carbidopa), 5-HTP produced maximal frequency of HTRs in 20-day-old mice which rapidly subsided during aging. Methamphetamine dose-dependently suppressed 5-HTP-evoked HTR in 20- and 30-day-old mice. The selective 5-HT 1A -receptor antagonist WAY 100635 reversed the inhibitory effect of methamphetamine on 5-HTP-induced HTR in 30-day-old mice, whereas the selective adrenergic α 2 -receptor antagonist RS 79948 failed to reverse methamphetamine's inhibition at any tested age. These findings suggest an ontogenic rationale for methamphetamine's inhibitory 5-HT 1A receptor component of action in its suppressive effect on 5-HTP-induced HTR during development which is not maximally active at a very early age.

超低剂量的甲基苯丙胺能抑制小鼠在衰老过程中由 5- 羟色氨酸诱发的头部抽搐反应。
小鼠的头部牵张反应(HTR)被认为是啮齿类动物 5-HT2A 受体激活的一种行为检测方法。直接作用的 5-HT2A 受体激动剂,如 (±)-2,5-二甲氧基-4-碘苯丙胺、5-羟色胺前体[如 5-羟色氨酸 (5-HTP)]和选择性 5-羟色胺释放剂(如 d-芬氟拉明)可诱发这种反应。非选择性单胺释放剂甲基苯丙胺本身不会产生 HTR,但可通过同时激活抑制性血清素能 5-HT1A 或肾上腺素能 α2 受体,抑制(±)-2,5-二甲氧基-4-碘苯丙胺和 d-芬氟拉明诱发的跨年龄 HTR。目前,我们研究了:(1)20、30 和 60 日龄小鼠 5-HTP 诱导 HTR 的本体发育;(2)超低剂量甲基苯丙胺(0.1、0.25 和 0.5毫克/千克,腹腔注射)能否抑制不同年龄小鼠5-HTP诱导的HTR频率;以及(3)抑制性血清素能5-HT1A或肾上腺素能α2受体能否解释甲基苯丙胺对5-HTP诱导的HTR的潜在抑制作用。在外周脱羧酶抑制剂(卡比多巴)存在的情况下,5-HTP 在 20 天大的小鼠中产生最大频率的 HTR,并在衰老过程中迅速消退。甲基苯丙胺剂量依赖性地抑制了 5-HTP 在 20 天和 30 天大的小鼠中诱发的 HTR。选择性 5-HT1A 受体拮抗剂 WAY 100635 逆转了甲基苯丙胺对 30 天龄小鼠 5-HTP 诱导的 HTR 的抑制作用,而选择性肾上腺素能 α2 受体拮抗剂 RS 79948 在任何测试年龄都无法逆转甲基苯丙胺的抑制作用。这些研究结果表明,甲基苯丙胺的抑制性 5-HT1A 受体作用成分在发育过程中对 5-HTP 诱导的 HTR 有抑制作用,而这种抑制作用在小鼠很小的时候就没有达到最大活性。
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来源期刊
Behavioural Pharmacology
Behavioural Pharmacology 医学-行为科学
CiteScore
3.40
自引率
0.00%
发文量
84
审稿时长
6-12 weeks
期刊介绍: Behavioural Pharmacology accepts original full and short research reports in diverse areas ranging from ethopharmacology to the pharmacology of schedule-controlled operant behaviour, provided that their primary focus is behavioural. Suitable topics include drug, chemical and hormonal effects on behaviour, the neurochemical mechanisms under-lying behaviour, and behavioural methods for the study of drug action. Both animal and human studies are welcome; however, studies reporting neurochemical data should have a predominantly behavioural focus, and human studies should not consist exclusively of clinical trials or case reports. Preference is given to studies that demonstrate and develop the potential of behavioural methods, and to papers reporting findings of direct relevance to clinical problems. Papers making a significant theoretical contribution are particularly welcome and, where possible and merited, space is made available for authors to explore fully the theoretical implications of their findings. Reviews of an area of the literature or at an appropriate stage in the development of an author’s own work are welcome. Commentaries in areas of current interest are also considered for publication, as are Reviews and Commentaries in areas outside behavioural pharmacology, but of importance and interest to behavioural pharmacologists. Behavioural Pharmacology publishes frequent Special Issues on current hot topics. The editors welcome correspondence about whether a paper in preparation might be suitable for inclusion in a Special Issue.
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