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利用脑开放流动微灌注技术对脑药代动力学和药效学进行体内监测。

In vivo monitoring of brain pharmacokinetics and pharmacodynamics with cerebral open flow microperfusion.

作者信息

Altendorfer-Kroath Thomas, Hummer Joanna, Birngruber Thomas

机构信息

Institute for Biomedical Research and Technologies, JOANNEUM RESEARCH - HEALTH, Graz, Austria.

出版信息

Biopharm Drug Dispos. 2023 Feb;44(1):84-93. doi: 10.1002/bdd.2343. Epub 2023 Feb 3.

DOI:10.1002/bdd.2343
PMID:36650922
Abstract

In vivo investigation of brain pharmacokinetics and pharmacodynamics (PK/PD) is an integral part of neurological drug development. However, drugs intended to act in the brain may reach it at very low concentrations due to the protective effect of the blood-brain barrier (BBB). Consequently, very sensitive measurement methods are required to investigate PK/PD of drugs in the brain. Also, these methods must be capable of continuously assessing cerebral drug concentrations with verifiable intact BBB, as disrupted BBB may lead to compound efflux from blood into brain and to biased results. To date, only a few techniques are available that can sensitively measure drug concentrations in the brain over time; one of which is cerebral open flow microperfusion (cOFM). cOFM's key features are that it enables measurement of cerebral compound concentrations with intact BBB, induces only minor tissue reactions, and that no scar formation occurs around the probe. The membrane-free cOFM probes collect diluted cerebral interstitial fluid (ISF) samples that are containing the whole molecule spectrum of the ISF. Further, combining cOFM with an in vivo calibration protocol (e.g. Zero Flow Rate) enables absolute quantification of compounds in cerebral ISF. In general, three critical aspects have to be considered when measuring cerebral drug concentrations and recording PK/PD profiles with cOFM: (a) the BBB integrity during sampling, (b) the status of the brain tissue next to the cOFM probe during sampling, and (c) the strategy to absolutely quantify drugs in cerebral ISF. This work aims to review recent applications of cOFM for PK/PD assessment with a special focus on these critical aspects.

摘要

脑药代动力学和药效学(PK/PD)的体内研究是神经药物开发不可或缺的一部分。然而,由于血脑屏障(BBB)的保护作用,旨在作用于大脑的药物可能以非常低的浓度到达大脑。因此,需要非常灵敏的测量方法来研究大脑中的药物PK/PD。此外,这些方法必须能够在血脑屏障完整可验证的情况下持续评估脑内药物浓度,因为血脑屏障破坏可能导致化合物从血液流入大脑并产生有偏差的结果。迄今为止,只有少数几种技术能够灵敏地随时间测量脑内药物浓度;其中之一是脑开放流微灌注(cOFM)。cOFM的关键特性在于它能够在血脑屏障完整的情况下测量脑内化合物浓度,仅引起轻微的组织反应,并且在探头周围不会形成瘢痕。无膜cOFM探头收集稀释的脑间质液(ISF)样本,这些样本包含ISF的全部分子谱。此外,将cOFM与体内校准方案(例如零流速)相结合能够对脑内ISF中的化合物进行绝对定量。一般来说,使用cOFM测量脑内药物浓度并记录PK/PD曲线时必须考虑三个关键方面:(a)采样期间的血脑屏障完整性,(b)采样期间cOFM探头旁边的脑组织状态,以及(c)对脑内ISF中的药物进行绝对定量的策略。这项工作旨在回顾cOFM在PK/PD评估中的最新应用,特别关注这些关键方面。

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