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Theoretical and practical applications of the intracerebroventricular route for CSF sampling and drug administration in CNS drug discovery research: A mini review

机译:脑室内途径的脑脊液采样和给药在中枢神经系统药物发现研究中的理论和实际应用:综述

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Clinically, central nervous system (CNS) disorders account for more hospitalisations and prolonged care than almost all other diseases combined. In the preclinical setting, the intracerebroventricular (ICV) route for cerebrospinal fluid (CSF) sampling or dose administration in rodent models of human CNS disorders has potential to provide key insight on the pathobiology of these conditions. Low level neuroinflammation is present in >40% of patients with severe depression or schizophrenia and so comparative assessment of CSF composition between patients and rodent models of CNS disorders is potentially invaluable for hypothesis generation and for assessing rodent model validity. As molecules in the CSF have relatively low protein binding and are freely exchanged into the extracellular fluid of the brain parenchyma, supraspinal drug administration into the CSF can produce therapeutic drug concentrations in the brain. Direct administration of investigational agents into the CSF of the lateral ventricle of the brain enables intrinsic efficacy and adverse effect profiles to be evaluated without the confounding effects of drug metabolism, due to the low capacity of the CNS to metabolise exogenous compounds. It is our view that the ICV route for CSF sampling and for administration of novel drugs in development is under-utilised in preclinical research on CNS disorders. This is due to the high degree of technical skill and low margin for error associated with correct ICV guide cannula implantation in the rat. However, these technical challenges can be overcome by using standardised procedures and attention to detail during surgery and in the post-operative period.
机译:临床上,与几乎所有其他疾病的总和相比,中枢神经系统(CNS)疾病导致更多的住院和长期护理。在临床前环境中,在人类中枢神经系统疾病的啮齿动物模型中进行脑脊液(CSF)采样或剂量给药的脑室内(ICV)途径有可能为这些疾病的病理生物学提供关键见解。患有严重抑郁或精神分裂症的患者中,> 40%的患者存在低水平的神经炎症,因此,对患者和中枢神经系统疾病的啮齿动物模型之间的CSF组成进行比较评估,对于产生假说和评估啮齿动物模型的有效性具有潜在的价值。由于脑脊液中的分子具有相对较低的蛋白质结合能力,并且可以自由交换到脑实质的细胞外液中,因此脊柱上药物的给药可以在脑中产生治疗药物浓度。由于中枢神经系统代谢外源性化合物的能力低,将研究药物直接给药至大脑侧脑室的脑脊液可以评估内在功效和不良反应,而不会引起药物代谢的混淆。我们认为,在中枢神经系统疾病的临床前研究中,用于脑脊液采样和新药管理的ICV途径未得到充分利用。这归因于与正确的ICV引导套管植入大鼠相关的高度技术水平和较低的误差范围。但是,可以通过使用标准化的程序以及在手术期间和术后阶段注意细节来克服这些技术挑战。

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