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首页> 外文期刊>Pharmacology, Biochemistry and Behavior >Genetically expressed HIV-1 viral proteins attenuate nicotine-induced behavioral sensitization and alter mesocorticolimbic ERK and CREB signaling in rats.
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Genetically expressed HIV-1 viral proteins attenuate nicotine-induced behavioral sensitization and alter mesocorticolimbic ERK and CREB signaling in rats.

机译:遗传表达的HIV-1病毒蛋白减弱了尼古丁引起的行为敏化并改变了大鼠中皮层皮质的ERK和CREB信号传导。

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The prevalence of tobacco smoking in HIV-1 positive individuals is 3-fold greater than that in the HIV-1 negative population; however, whether HIV-1 viral proteins and nicotine together produce molecular changes in mesolimbic structures that mediate psychomotor behavior has not been studied. This study determined whether HIV-1 viral proteins changed nicotine-induced behavioral sensitization in HIV-1 transgenic (HIV-1Tg) rats. Further, we examined cAMP response element binding protein (CREB) and extracellular regulated kinase (ERK1/2) signaling in the prefrontal cortex (PFC), nucleus accumbens (NAc) and ventral tegmental area (VTA). HIV-1Tg rats exhibited a transient decrease of activity during habituation, but showed attenuated nicotine (0.35mg/kg, s.c.)-induced behavioral sensitization compared to Fisher 344 (F344) rats. The basal levels of phosphorylated CREB and ERK2 were lower in the PFC of HIV-1Tg rats, but not in the NAc and VTA, relative to the controls. In the nicotine-treated groups, the levels of phosphorylated CREB and ERK2 in the PFC were increased in HIV-1Tg rats, but decreased in F344 animals. Moreover, repeated nicotine administration reduced phosphorylated ERK2 in the VTA of HIV-1Tg rats and in the NAc of F344 rats, but had no effect on phosphorylated CREB, indicating a region-specific change of intracellular signaling. These results demonstrate that HIV-1 viral proteins produce differences in basal and nicotine-induced alterations in CREB and ERK signaling that may contribute to the alteration in psychomotor sensitization. Thus, HIV-1 positive smokers are possibly more vulnerable to alterations in CREB and ERK signaling and this has implications for motivated behavior, including tobacco smoking, in HIV-1 positive individuals who self-administer nicotine.
机译:HIV-1阳性人群的吸烟率是HIV-1阴性人群的3倍。但是,尚未研究HIV-1病毒蛋白和尼古丁是否共同产生介导精神运动行为的中脑边缘结构的分子变化。这项研究确定了HIV-1病毒蛋白是否改变了尼古丁诱发的HIV-1转基因(HIV-1Tg)大鼠的行为敏化。此外,我们检查了前额叶皮层(PFC),伏隔核(NAc)和腹侧被盖区(VTA)中的cAMP反应元件结合蛋白(CREB)和细胞外调节激酶(ERK1 / 2)信号传导。与Fisher 344(F344)大鼠相比,HIV-1Tg大鼠在适应过程中表现出短暂的活动减少,但尼古丁(0.35mg / kg,s.c.)诱导的行为敏化减弱。相对于对照组,在HIV-1Tg大鼠的PFC中,磷酸化的CREB和ERK2的基础水平较低,但在NAc和VTA中则较低。在尼古丁治疗组中,HIV-1Tg大鼠中PFC中磷酸化的CREB和ERK2的水平升高,而F344动物中的降低。此外,重复给予尼古丁可减少HIV-1Tg大鼠的VTA和F344大鼠的NAc中的磷酸化ERK2,但对磷酸化的CREB没有影响,表明细胞内信号传导的区域特异性变化。这些结果表明,HIV-1病毒蛋白在CREB和ERK信号传导的基础和尼古丁诱导的变化中产生差异,这可能有助于精神运动敏化的变化。因此,HIV-1阳性吸烟者可能更容易受到CREB和ERK信号转导的影响,这对自我管理尼古丁的HIV-1阳性个体的动机行为(包括吸烟)具有影响。

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