首页> 美国卫生研究院文献>The Journal of Neuroscience >Overexpression of the Steroidogenic Enzyme Cytochrome P450 Side Chain Cleavage in the Ventral Tegmental Area Increases 3α5α-THP and Reduces Long-Term Operant Ethanol Self-Administration
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Overexpression of the Steroidogenic Enzyme Cytochrome P450 Side Chain Cleavage in the Ventral Tegmental Area Increases 3α5α-THP and Reduces Long-Term Operant Ethanol Self-Administration

机译:类固醇酶细胞色素P450侧链切割在腹侧被盖区的过度表达增加3α5α-THP并减少长期可操作的乙醇自我管理

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摘要

Neuroactive steroids are endogenous neuromodulators capable of altering neuronal activity and behavior. In rodents, systemic administration of endogenous or synthetic neuroactive steroids reduces ethanol self-administration. We hypothesized this effect arises from actions within mesolimbic brain regions that we targeted by viral gene delivery. Cytochrome P450 side chain cleavage (P450scc) converts cholesterol to pregnenolone, the rate-limiting enzymatic reaction in neurosteroidogenesis. Therefore, we constructed a recombinant adeno-associated serotype 2 viral vector (rAAV2), which drives P450scc expression and neuroactive steroid synthesis. The P450scc-expressing vector (rAAV2-P450scc) or control GFP-expressing vector (rAAV2-GFP) were injected bilaterally into the ventral tegmental area (VTA) or nucleus accumbens (NAc) of alcohol preferring (P) rats trained to self-administer ethanol. P450scc overexpression in the VTA significantly reduced ethanol self-administration by 20% over the 3 week test period. P450scc overexpression in the NAc, however, did not alter ethanol self-administration. Locomotor activity was unaltered by vector administration to either region. P450scc overexpression produced a 36% increase in (3α,5α)-3-hydroxypregnan-20-one (3α,5α-THP, allopregnanolone)-positive cells in the VTA, but did not increase 3α,5α-THP immunoreactivity in NAc. These results suggest that P450scc overexpression and the resultant increase of 3α,5α-THP-positive cells in the VTA reduces ethanol reinforcement. 3α,5α-THP is localized to neurons in the VTA, including tyrosine hydroxylase neurons, but not astrocytes. Overall, the results demonstrate that using gene delivery to modulate neuroactive steroids shows promise for examining the neuronal mechanisms of moderate ethanol drinking, which could be extended to other behavioral paradigms and neuropsychiatric pathology.
机译:神经活性类固醇是能够改变神经元活动和行为的内源性神经调节剂。在啮齿动物中,内源性或合成性神经活性类固醇的全身性给药会减少乙醇的自我给药。我们假设这种效果是由于我们以病毒基因传递为目标的中脑边缘大脑区域内的作用引起的。细胞色素P450侧链裂解(P450scc)将胆固醇转化为孕烯醇酮,这是神经甾体生成过程中的限速酶促反应。因此,我们构建了一个重组腺相关血清型2病毒载体(rAAV2),该载体可驱动P450scc表达和神经活性类固醇合成。将表达P450scc的载体(rAAV2-P450scc)或对照表达GFP的载体(rAAV2-GFP)双向注射到酒精偏爱(P)受过自我管理的大鼠的腹侧被盖区(VTA)或伏隔核(NAc)中乙醇。在3周的测试期内,VTA中的P450scc过表达显着降低了乙醇的自用率,降低了20%。但是,NAc中的P450scc过表达并没有改变乙醇的自我管理。通过向任一区域施用载体,运动活性没有改变。 P450scc过表达使VTA中的(3α,5α)-3-羟基pregnan-20-one(3α,5α-THP,allopregnanolone)阳性细胞增加36%,但在NAc中未增加3α,5α-THP免疫反应性。这些结果表明,V450中P450scc的过表达和3α,5α-THP阳性细胞的增加减少了乙醇的强化。 3α,5α-THP定位于VTA中的神经元,包括酪氨酸羟化酶神经元,而非星形胶质细胞。总体而言,结果表明,使用基因传递来调节神经活性类固醇显示出有望检查适度饮酒的神经元机制,这可能会扩展到其他行为范例和神经精神病学病理学。

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