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健康个体和痴呆症患者的人血脑屏障 SLC 和 ABC 转运蛋白的蛋白质组学定量分析。

Proteomic Quantification of Human Blood-Brain Barrier SLC and ABC Transporters in Healthy Individuals and Dementia Patients.

机构信息

Centre for Applied Pharmacokinetic Research (CAPKR) , University of Manchester , Manchester M13 9PT , U.K.

Biological Mass Spectrometry Core Facility , University of Manchester , Manchester M13 9PT , U.K.

出版信息

Mol Pharm. 2019 Mar 4;16(3):1220-1233. doi: 10.1021/acs.molpharmaceut.8b01189. Epub 2019 Feb 8.

Abstract

The blood-brain barrier (BBB) maintains brain homeostasis by controlling traffic of molecules from the circulation into the brain. This function is predominantly dependent on proteins expressed at the BBB, especially transporters and tight junction proteins. Alterations to the level and function of BBB proteins can impact the susceptibility of the central nervous system to exposure to xenobiotics in the systemic circulation with potential consequent effects on brain function. In this study, expression profiles of drug transporters and solute carriers in the BBB were assessed in tissues from healthy individuals ( n = 12), Alzheimer's patients ( n = 5), and dementia with Lewy bodies patients ( n = 5), using targeted, accurate mass retention time (AMRT) and global proteomic methods. A total of 53 transporters were quantified, 19 for the first time in the BBB. A further 20 novel transporters were identified but not quantified. The global proteomic method identified another 3333 BBB proteins. Transporter abundances, taken together with the scaling factor, microvessel protein content per unit tissue (BMvPGB also measured here), can be used in quantitative systems pharmacology models predicting drug disposition in the brain and permitting dose adjustment (precision dosing) in special populations of patients, such as those with dementia. Even in this small study, we see differences in transporter profile between healthy and diseased brain tissue.

摘要

血脑屏障 (BBB) 通过控制分子从循环系统进入大脑的流量来维持大脑内环境的稳定。这种功能主要依赖于 BBB 上表达的蛋白质,特别是转运体和紧密连接蛋白。BBB 蛋白的水平和功能的改变会影响中枢神经系统对外周循环中异物的易感性,从而可能对大脑功能产生潜在的影响。在这项研究中,使用靶向、准确质量保留时间 (AMRT) 和整体蛋白质组学方法,评估了来自健康个体(n=12)、阿尔茨海默病患者(n=5)和路易体痴呆患者(n=5)组织中药物转运体和溶质载体的表达谱。共定量了 53 种转运体,其中 19 种是 BBB 中的首次定量。还鉴定了另外 20 种新型转运体,但未进行定量。整体蛋白质组学方法鉴定了另外 3333 种 BBB 蛋白。转运体丰度,连同缩放因子,即单位组织中的微血管蛋白含量 (BMvPGB,这里也进行了测量),可用于定量系统药理学模型,以预测药物在大脑中的分布,并允许对特定患者群体(如痴呆患者)进行剂量调整(精准给药)。即使在这项小型研究中,我们也看到了健康和患病脑组织之间转运体谱的差异。

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