首页> 外文期刊>Behavioural Brain Research: An International Journal >The dopamine D2/D3 antagonist DS121 potentiates the effect of cocaine on locomotion and reduces tolerance in cocaine tolerant rats.
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The dopamine D2/D3 antagonist DS121 potentiates the effect of cocaine on locomotion and reduces tolerance in cocaine tolerant rats.

机译:多巴胺D2 / D3拮抗剂DS121增强了可卡因对运动的影响,并降低了可卡因耐受大鼠的耐受性。

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摘要

To explore the significance of dopamine (DA) autoreceptors in cocaine tolerance and cocaine induced locomotor activity rats were treated with saline and cocaine (40 mg/kg per day via osmotic minipump; normal and cocaine tolerant rats, respectively). Injections of DS121 (0-7 mg/kg, i.p.; S(-)-3-(3-(cyanophenyl)-N-n-propylpiperidine), a DA D2/3 and autoreceptor preferring antagonist, either alone (i.e. DS121 + saline injection) or in combination with cocaine (7.5 mg/kg, i.p.) were also given. DS121 (+ saline) increased locomotor activity in both saline and cocaine pump (CP) treated animals. DS121 also potentiated the effect of cocaine on locomotor activity; this effect was greatest in CP (tolerant) animals. It is concluded that DS121 can increase locomotor activity and that this effect is greatest when the DA tone is high, that is when cocaine is present, suggestive of a presynaptic mechanism. Furthermore, because DS121 potentiation of cocaine induced locomotor activity is greatest in tolerant animals it is concluded that supersensitive DA autoreceptors underlie this effect. These data further support our previous data, which show that DA autoreceptors are sensitized after continuous cocaine (minipump) treatment.
机译:为了探讨多巴胺(DA)自身受体在可卡因耐受性和可卡因诱导的运动活动中的重要性,分别用盐水和可卡因(分别通过渗透性微型泵每天40 mg / kg的剂量;正常和可卡因耐受的大鼠)处理大鼠。单独注射DS121(0-7 mg / kg,ip; S(-)-3-(3-(氰基苯基)-Nn-丙基哌啶),DA D2 / 3和优先接受拮抗剂的自身受体(即DS121 +盐水注射) )或与可卡因(7.5 mg / kg,腹腔注射)合用; DS121(+生理盐水)可增加生理盐水和可卡因泵(CP)治疗的动物的运动能力; DS121还增强了可卡因对运动能力的影响;结论:DS121可以增加运动能力,并且当DA音高时,即当存在可卡因时,这种作用最大,这表明存在突触前的机制;另外,由于DS121的增强,这种作用最大。可卡因引起的运动能力的变化在耐受性动物中最大,可以得出结论,超敏感的DA自身受体是这种作用的基础,这些数据进一步支持了我们以前的数据,这些数据表明,连续可卡因(minipump)治疗后,DA自身受体被致敏。

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