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递增剂量甲基苯丙胺预处理会改变与高剂量甲基苯丙胺狂饮暴露相关的行为和神经化学特征。

Escalating dose methamphetamine pretreatment alters the behavioral and neurochemical profiles associated with exposure to a high-dose methamphetamine binge.

作者信息

Segal David S, Kuczenski Ronald, O'Neil Meghan L, Melega William P, Cho Arthur K

机构信息

Department of Psychiatry, University of California, San Diego, School of Medicine, La Jolla, CA 92093, USA.

出版信息

Neuropsychopharmacology. 2003 Oct;28(10):1730-40. doi: 10.1038/sj.npp.1300247.

DOI:10.1038/sj.npp.1300247
PMID:12865898
Abstract

The neurotoxic effects of methamphetamine (METH) have been characterized primarily from the study of high-dose binge regimens in rodents. However, this drug administration paradigm does not include a potentially important feature of stimulant abuse in humans, that is, the gradual escalation of stimulant doses that frequently occurs prior to high-dose exposure. We have argued that pretreatment with escalating doses (EDs) might significantly alter the neurotoxic profile produced by a single high-dose binge. In the present study, we tested this hypothesis by pretreating rats with saline or gradually increasing doses of METH (0.1-4.0 mg/kg over 14 days), prior to an acute METH binge (4 x 6 mg/kg at 2 h intervals). These animals, whose behavior was continuously monitored throughout drug treatment, were then killed 3 days later for determination of caudate-putamen dopamine (DA) content, levels of [(3)H]WIN 35,428 binding to the DA transporter, and levels of [(3)H]dihydrotetrabenazine ([(3)H]DTBZ) binding to the vesicular monoamine transporter. ED pretreatment markedly attenuated the stereotypy response, as well as the hyperthermia and indices of sympathetic activation associated with the acute binge. In addition, ED pretreatment prevented the decline in [(3)H]WIN 35,428 binding, and significantly diminished the decrease in DA levels, but did not affect the decrease in [(3)H]DTBZ binding associated with the acute binge. We suggest that further study of the effects produced by a regimen which includes a gradual escalation of doses prior to high-dose METH binge exposure could more accurately identify the neurochemical and behavioral changes relevant to those that occur as a consequence of high-dose METH abuse in humans.

摘要

甲基苯丙胺(METH)的神经毒性作用主要是通过对啮齿动物高剂量暴饮暴食给药方案的研究来确定的。然而,这种给药模式并未涵盖人类滥用兴奋剂的一个潜在重要特征,即高剂量暴露之前经常出现的兴奋剂剂量逐渐增加的情况。我们认为,用递增剂量(EDs)进行预处理可能会显著改变单次高剂量暴饮暴食所产生的神经毒性特征。在本研究中,我们通过在急性METH暴饮暴食(以2小时间隔给予4×6mg/kg)之前,用生理盐水或逐渐增加剂量的METH(在14天内从0.1 - 4.0mg/kg)对大鼠进行预处理来验证这一假设。在整个药物治疗过程中持续监测这些动物的行为,然后在3天后将其处死,以测定尾状核 - 壳核多巴胺(DA)含量、[³H]WIN 35,428与DA转运体的结合水平以及[³H]二氢四苯嗪([³H]DTBZ)与囊泡单胺转运体的结合水平。递增剂量预处理显著减弱了刻板反应,以及与急性暴饮暴食相关的体温过高和交感神经激活指标。此外,递增剂量预处理可防止[³H]WIN 35,428结合水平的下降,并显著减轻DA水平的降低,但不影响与急性暴饮暴食相关的[³H]DTBZ结合水平的降低。我们建议,进一步研究在高剂量METH暴饮暴食暴露之前采用剂量逐渐增加方案所产生的影响,可能会更准确地识别与人类高剂量滥用METH所导致的神经化学和行为变化相关的情况。

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