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脱氢表雄酮7-羟化酶CYP7B:在灵长类动物海马中主要表达,在阿尔茨海默病中表达降低。

Dehydroepiandrosterone 7-hydroxylase CYP7B: predominant expression in primate hippocampus and reduced expression in Alzheimer's disease.

作者信息

Yau J L W, Rasmuson S, Andrew R, Graham M, Noble J, Olsson T, Fuchs E, Lathe R, Seckl J R

机构信息

Molecular Medicine Centre, Western General Hospital, Edinburgh EH4 2XU, UK.

出版信息

Neuroscience. 2003;121(2):307-14. doi: 10.1016/s0306-4522(03)00438-x.

Abstract

Neurosteroids such as dehydroepiandrosterone (DHEA), pregnenolone and 17beta-estradiol are synthesized by cytochrome P450s from endogenous cholesterol. We previously reported a new cytochrome P450 enzyme, CYP7B, highly expressed in rat and mouse brain that metabolizes DHEA and related steroids by hydroxylation at the 7alpha position. Such 7-hydroxylation can enhance DHEA bioactivity in vivo. Here we show that the reaction is conserved across mammalian species: in addition to mouse and rat, DHEA hydroxylation activity was present in brain extracts from sheep, marmoset and human. Northern blotting using a human CYP7B complementary deoxyribonucleic acid (cDNA) probe confirmed the presence of CYP7B mRNA in marmoset and human hippocampus; CYP7B mRNA was present in marmoset cerebellum and brainstem, with lower levels in hypothalamus and cortex. In situ hybridization to human brain revealed higher levels of CYP7B mRNA in the hippocampus than in cerebellum, cortex, or other brain regions. We also measured CYP7B expression in Alzheimer's disease (AD). CYP7B mRNA was significantly decreased (approximately 50% decline; P<0.05) in dentate neurons from AD subjects compared with controls. A decline in CYP7B activity may contribute the loss of effects of DHEA with ageing and perhaps to the pathophysiology of AD.

摘要

神经甾体如脱氢表雄酮(DHEA)、孕烯醇酮和17β-雌二醇由细胞色素P450从内源性胆固醇合成。我们之前报道了一种新的细胞色素P450酶CYP7B,在大鼠和小鼠脑中高度表达,它通过在7α位羟基化来代谢DHEA及相关甾体。这种7-羟基化可增强DHEA在体内的生物活性。在此我们表明该反应在哺乳动物物种中是保守的:除小鼠和大鼠外,绵羊、狨猴和人类的脑提取物中也存在DHEA羟基化活性。使用人CYP7B互补脱氧核糖核酸(cDNA)探针进行的Northern印迹证实狨猴和人类海马体中存在CYP7B mRNA;CYP7B mRNA存在于狨猴的小脑和脑干中,下丘脑和皮质中的水平较低。对人脑进行原位杂交显示,海马体中CYP7B mRNA水平高于小脑、皮质或其他脑区。我们还检测了阿尔茨海默病(AD)中CYP7B的表达。与对照组相比,AD患者齿状神经元中的CYP7B mRNA显著降低(约下降50%;P<0.05)。CYP7B活性的下降可能导致随着年龄增长DHEA作用的丧失,也许还与AD的病理生理学有关。

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