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人类大脑中单胺氧化酶蛋白的分布:对脑影像学研究的启示。

Distribution of monoamine oxidase proteins in human brain: implications for brain imaging studies.

机构信息

Human Brain Laboratory, Centre for Addiction and Mental Health, Toronto, Ontario, Canada M5T 1R8.

出版信息

J Cereb Blood Flow Metab. 2013 Jun;33(6):863-71. doi: 10.1038/jcbfm.2013.19. Epub 2013 Feb 13.

Abstract

Positron emission tomography (PET) imaging of monoamine oxidases (MAO-A: [(11)C]harmine, [(11)C]clorgyline, and [(11)C]befloxatone; MAO-B: [(11)C]deprenyl-D2) has been actively pursued given clinical importance of MAOs in human neuropsychiatric disorders. However, it is unknown how well PET outcome measures for the different radiotracers are quantitatively related to actual MAO protein levels. We measured regional distribution (n=38) and developmental/aging changes (21 hours to 99 years) of both MAOs by quantitative immunoblotting in autopsied normal human brain. MAO-A was more abundant than MAO-B in infants, which was reversed as MAO-B levels increased faster before 1 year and, unlike MAO-A, kept increasing steadily to senescence. In adults, regional protein levels of both MAOs were positively and proportionally correlated with literature postmortem data of MAO activities and binding densities. With the exception of [(11)C]befloxatone (binding potential (BP), r=0.61, P=0.15), correlations between regional PET outcome measures of binding in the literature and MAO protein levels were good (P<0.01) for [(11)C]harmine (distribution volume, r=0.86), [(11)C]clorgyline (λk3, r=0.82), and [(11)C]deprenyl-D2 (λk3 or modified Patlak slope, r=0.78 to 0.87), supporting validity of the latter imaging measures. However, compared with in vitro data, the latter PET measures underestimated regional contrast by ∼2-fold. Further studies are needed to address cause of the in vivo vs. in vitro nonproportionality.

摘要

正电子发射断层扫描(PET)成像单胺氧化酶(MAO-A:[(11)C]harmin,[(11)C]氯丙嗪和[(11)C]befloxatone;MAO-B:[(11)C]deprenyl-D2)一直受到积极的研究,因为 MAO 在人类神经精神疾病中的临床重要性。然而,目前尚不清楚不同放射性示踪剂的 PET 结果测量与实际 MAO 蛋白水平的定量关系如何。我们通过对尸检正常大脑进行定量免疫印迹,测量了两种 MAO 的区域分布(n=38)和发育/衰老变化(21 小时至 99 岁)。MAO-A 在婴儿中的含量高于 MAO-B,这种情况在 1 岁前 MAO-B 水平更快增加时发生逆转,并且与 MAO-A 不同,MAO-B 水平一直稳定增加到衰老。在成人中,两种 MAO 的区域蛋白水平与文献中死后 MAO 活性和结合密度的数据呈正相关和比例相关。除了 [(11)C]befloxatone(结合潜能(BP),r=0.61,P=0.15)外,文献中与结合相关的区域 PET 结果测量与 MAO 蛋白水平之间的相关性良好(P<0.01)为 [(11)C]harmin(分布容积,r=0.86),[(11)C]clorgyline(λk3,r=0.82)和 [(11)C]deprenyl-D2(λk3 或改良的 Patlak 斜率,r=0.78 至 0.87),支持后者成像测量的有效性。然而,与体外数据相比,后者 PET 测量值低估了区域对比度约 2 倍。需要进一步的研究来解决体内与体外不成比例的原因。

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