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Pharmacologic Stimulation of Cytochrome P450 46A1 and Cerebral Cholesterol Turnover in Mice

机译:小鼠细胞色素P450 46A1的药理刺激和脑胆固醇转换

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摘要

Cytochrome P450 46A1 (CYP46A1) is a brain-specific cholesterol 24-hydroxylase responsible for the majority of cholesterol elimination from the brain. Genetically increased CYP46A1 expression in mice leads to improved cognition and decreases manifestations of Alzheimer disease. We found that four pharmaceuticals (efavirenz (EFV), acetaminophen, mirtazapine, and galantamine) prescribed for indications unrelated to cholesterol maintenance increased CYP46A1 activity in vitro. We then evaluated the anti-HIV medication EFV for the mode of interaction with CYP46A1 and the effect on mice. We propose a model for CYP46A1 activation by EFV and show that EFV enhanced CYP46A1 activity and cerebral cholesterol turnover in animals with no effect on the levels of brain cholesterol. The doses of EFV administered to mice and required for the stimulation of their cerebral cholesterol turnover are a hundred times lower than those prescribed to HIV patients. At such small doses, EFV may be devoid of adverse effects elicited by high drug concentrations. CYP46A1 could be a novel therapeutic target and a tool to further investigate the physiological and medical significance of cerebral cholesterol turnover.
机译:细胞色素P450 46A1(CYP46A1)是一种大脑特异性胆固醇24-羟化酶,负责从大脑清除大部分胆固醇。 CYP46A1基因在小鼠中的基因表达增加可导致认知功能改善,并减少阿尔茨海默氏病的表现。我们发现四种与胆固醇维持无关的药物处方(依非韦伦(EFV),对乙酰氨基酚,米氮平和加兰他敏)在体外增加了CYP46A1的活性。然后,我们评估了抗HIV药物EFV与CYP46A1相互作用的方式以及对小鼠的影响。我们提出了由EFV激活CYP46A1的模型,并显示EFV增强了动物体内的CYP46A1活性和脑胆固醇更新,而对脑胆固醇水平没有影响。给予小鼠并刺激其脑胆固醇更新所需的EFV剂量比HIV患者处方的剂量低一百倍。在如此小的剂量下,EFV可能没有高药物浓度引起的不良反应。 CYP46A1可能是一种新型的治疗靶点,也是进一步研究脑胆固醇代谢的生理和医学意义的工具。

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