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首页> 外文期刊>Pharmacology, Biochemistry and Behavior >Locomotion, stereotypy, and dopamine D(1) receptors after chronic 'binge' cocaine in C57BL/6J and 129/J mice.
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Locomotion, stereotypy, and dopamine D(1) receptors after chronic 'binge' cocaine in C57BL/6J and 129/J mice.

机译:运动,刻板印象和多巴胺D(1)受体后慢性“暴饮”可卡因在C57BL / 6J和129 / J小鼠。

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We have shown that C57BL/6J and 129/J mice differ in their behavioral response to "binge" pattern cocaine (three daily injections of 15 mg/kg separated by 1 h). To determine if these differences persist during chronic binge cocaine administration, we examined the effects of 14-day binge pattern cocaine on home cage behavior. Since the dopamine D(1) receptor may be an important mediator of cocaine-induced locomotor activity, we examined binding to the dopamine D(1) receptor. Locomotor activity was increased by chronic binge cocaine in C57BL/6J (P<.0001) but not in 129/J mice. C57BL/6J mice developed tolerance to the locomotor-activating effects of cocaine. Stereotypic responses were greater in C57BL/6J than in 129/J mice (P=.03), with neither tolerance nor sensitization in either strain. Dopamine D(1) receptor binding in the nucleus accumbens and olfactory tubercle did not differ between strains and was not affected by chronic binge cocaine. In the caudate putamen, subregion specific strain differences in dopamine D(1) receptor binding were observed; chronic binge cocaine increased dopamine D(1) receptor binding in the caudal (P<.05), but not rostral caudate putamen. There was no correlation between locomotor activity or stereotypy and dopamine D(1) receptor density. Thus, with chronic binge cocaine administration, behavioral differences persist between the C57BL/6J and 129/J mice, and cocaine-induced locomotor activity is not correlated with changes in dopamine D(1) receptor binding.
机译:我们已经显示,C57BL / 6J和129 / J小鼠在对“可卡因”模式可卡因的行为反应上存在差异(每天3次注射15 mg / kg,间隔1 h)。为了确定在长期暴饮可卡因期间这些差异是否持续存在,我们检查了14天暴饮可卡因对家庭笼养行为的影响。由于多巴胺D(1)受体可能是可卡因诱导的运动活性的重要介质,因此我们检查了与多巴胺D(1)受体的结合。在C57BL / 6J中,慢性暴饮可卡因可提高运动能力(P <.0001),而在129 / J小鼠中则没有。 C57BL / 6J小鼠对可卡因的运动激活作用产生了耐受性。 C57BL / 6J的刻板印象反应比129 / J小鼠大(P = .03),在这两种菌株中均没有耐受性或致敏性。多巴胺D(1)受体结合伏隔核和嗅结节之间没有差异,并且不受慢性暴饮可卡因的影响。在尾状壳核中,观察到多巴胺D(1)受体结合的亚区域特定应变差异;慢性暴饮可卡因增加了尾巴中的多巴胺D(1)受体结合(P <.05),但不是尾状尾状壳核。运动活动或刻板印象与多巴胺D(1)受体密度之间没有相关性。因此,与慢性暴饮可卡因管理,C57BL / 6J和129 / J小鼠之间的行为差​​异仍然存在,可卡因诱导的自发活动与多巴胺D(1)受体结合的变化不相关。

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