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地卓西平与体温降低并不能预防黑长尾猴中甲基苯丙胺诱导的神经毒性:[11C]WIN 35,428-正电子发射断层扫描研究。

Dizocilpine and reduced body temperature do not prevent methamphetamine-induced neurotoxicity in the vervet monkey: [11C]WIN 35,428 - positron emission tomography studies.

作者信息

Melega W P, Lacan G, Harvey D C, Huang S C, Phelps M E

机构信息

Department of Molecular and Medical Pharmacology, UCLA School of Medicine, Los Angeles, CA 90095-1735, USA.

出版信息

Neurosci Lett. 1998 Dec 11;258(1):17-20. doi: 10.1016/s0304-3940(98)00845-3.

DOI:10.1016/s0304-3940(98)00845-3
PMID:9876041
Abstract

[11C]WIN 35,428 (WIN), a cocaine analog that binds to the dopamine transporter (DAT), and positron emission tomography (PET) were used to evaluate the potential neuroprotective effects of dizocilpine (MK-801) on methamphetamine (MeAmp) induced neurotoxicity in the striatal dopamine system of the vervet monkey. MK-801 (1 mg/kg, i.m.) was administered 30 min prior to a neurotoxic MeAmp dosage for this species (2 x 2 mg/kg, 4 h apart); control subjects received MeAmp. MK-801 treated subjects were anesthetized by the drug for 6-8 h; throughout that period, a 2-3 degrees C decrease in body temperature was measured. At 1-2 weeks post-MeAmp, decreases of approximately 75% in striatal WIN binding were observed for both MK-801/MeAmp and MeAmp subjects. Thus, in this non-human primate species, the combination of MK-801 pretreatment and reduced body temperature did not provide protection from the MeAmp-induced loss of DAT. Further, the absence of an elevated body temperature during the acute MeAmp exposure period indicated that hyperthermia, per se, was not a necessary concomitant of the MeAmp neurotoxicity profile as has been previously demonstrated in rodents. These results provide evidence that different regulatory factors maintain the integrity of the rodent and primate striatal dopamine systems.

摘要

可卡因类似物[11C]WIN 35,428(WIN)可与多巴胺转运体(DAT)结合,利用正电子发射断层扫描(PET)评估地佐环平(MK-801)对黑长尾猴纹状体多巴胺系统中甲基苯丙胺(MeAmp)诱导的神经毒性的潜在神经保护作用。在给予该物种神经毒性剂量的MeAmp(2×2mg/kg,间隔4小时)前30分钟,注射MK-801(1mg/kg,肌肉注射);对照组接受MeAmp。接受MK-801治疗的受试动物被该药物麻醉6-8小时;在此期间,体温下降了2-3摄氏度。在给予MeAmp后1-2周,MK-801/MeAmp组和MeAmp组的纹状体WIN结合均下降了约75%。因此,在这种非人类灵长类动物中,MK-801预处理和体温降低并不能防止MeAmp诱导的DAT丢失。此外,在急性MeAmp暴露期间体温没有升高,这表明高热本身并非MeAmp神经毒性特征的必要伴随因素,这与之前在啮齿动物中的研究结果一致。这些结果证明,不同的调节因素维持着啮齿动物和灵长类动物纹状体多巴胺系统的完整性。

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