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Brain-to-Blood Transporters for Endogenous Substrates and Xenobiotics at the Blood-Brain Barrier: An Overview of Biology and Methodology

机译:血脑屏障中内源性底物和异生物的脑到血转运蛋白:生物学和方法论概述

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摘要

>Summary: In the past decade, research into P-glycoprotein involving the blood-brain barrier (BBB) has seen a shift in the concept of the BBB as a structural barrier to that of a functional barrier for xenobiotics and changed simultaneously the strategy for the discovery and development of drugs acting in the CNS. As far as making advances in neurotherapeutics are concerned, the brain-to-blood transport function at the BBB will be one of the most important issues. Knowing the limitations of the in vivo and in vitro methods for BBB efflux research, it is essential to adopt a multidisciplinary approach in investigating the true physiological role of the BBB. Among several methods, the Brain Efflux Index method and the use of conditionally immortalized brain capillary endothelial cell lines, established from transgenic rats harboring temperature-sensitive simian virus 40 large T-antigen gene, are likely to be very useful tools for the BBB efflux transport research. According to our recent findings using these methods, several transporters in the brain capillary endothelial cells appear to play an important role in reducing the brain level of hydrophilic endogenous substrates produced either in the brain or peripheral organs, e.g., neurotransmitters, neuromodulators, metabolites of neurotransmitters, and uremic toxins. It has been reported also that large hydrophilic molecules, such as IgG, apo-transferrin, and amyloid-β peptide, are susceptible to brain-to-blood efflux transport. In the light of the latest findings, we have formed the hypothesis that the BBB acts as a CNS detoxifying system for both endogenous substrates and xenobiotics in the brain. A fuller understanding of the physiological role of BBB efflux transporters will provide rational insights to assist in the development of safer neurotherapeutics.
机译:>摘要:在过去的十年中,对涉及血脑屏障(BBB)的P糖蛋白的研究已将BBB的概念转变为异源生物功能性屏障的结构性屏障同时改变了发现和开发在中枢神经系统中起作用的药物的策略。就神经治疗学的进步而言,BBB的脑血转运功能将是最重要的问题之一。了解BBB外排研究的体内和体外方法的局限性,在研究BBB的真正生理作用时采用多学科方法至关重要。在几种方法中,脑外流指数法和使用具有温度敏感性猿猴病毒40大T抗原基因的转基因大鼠建立的条件永生化的脑毛细血管内皮细胞系可能是BBB外向运输的非常有用的工具研究。根据我们使用这些方法的最新发现,脑毛细血管内皮细胞中的几种转运蛋白似乎在降低大脑在脑部或周围器官中产生的亲水性内源性底物的水平方面起着重要作用,例如,神经递质,神经调节剂,神经递质的代谢产物和尿毒症毒素。也有报道说,较大的亲水分子,例如IgG,脱辅基转铁蛋白和淀粉样β肽,很容易发生脑到血的外排运输。根据最新发现,我们形成了这样的假设,即血脑屏障对大脑中的内源性底物和异种生物都起着中枢神经系统的排毒作用。对BBB外排转运蛋白的生理作用的更全面的了解将提供理性的见解,以协助开发更安全的神经疗法。

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