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使用平衡透析法测定血浆中不稳定共价调节剂的游离分数的策略。

Strategy for Determining the Free Fraction of Labile Covalent Modulators in Plasma Using Equilibrium Dialysis.

机构信息

Department of Drug Metabolism and Pharmacokinetics, Genentech Inc., South San Francisco, CA 94080.

Department of Drug Metabolism and Pharmacokinetics, Genentech Inc., South San Francisco, CA 94080.

出版信息

J Pharm Sci. 2020 Oct;109(10):3181-3189. doi: 10.1016/j.xphs.2020.06.029. Epub 2020 Jul 12.

Abstract

Determination of free drug fraction (f) in plasma can be challenging for labile covalent modulators due to the off-target reactivity of chemical warheads to matrix proteins. The resulting poor drug recovery yields low confidence in f. Two approaches using diluted plasma and low temperature (4 & 20 °C) for equilibrium dialysis (ED) have been investigated using covalent modulators including osimertinib, ibrutinib, rociletinib, afatinib, neratinib and acalabrutinib. Our data indicate that stability of covalent modulators in plasma varies in different species, and drug depletion may lead to overestimation of f if true equilibrium is not reached. Additionally, although ED at low temperature improves the recovery of covalent modulators, the impact of low temperature may lead to underestimate of f. Overall, ED using diluted plasma is a preferred method because of its faster equilibrium, improved recovery and free of temperature effect on f. If low temperature ED must be used for extremely labile compounds, precaution must be taken to ensure no temperature dependence of f in plasma. Nevertheless, an orthogonal ED approach is recommended for labile covalent modulators to confirm the true equilibrium and impact of temperature on f. Additionally, this strategy can be used for determining f of other liable compounds.

摘要

测定血浆中的游离药物分数(f)对于不稳定的共价调节剂来说具有挑战性,因为化学弹头会与基质蛋白发生非靶标反应。这导致药物回收率低,从而对 f 的可信度产生影响。本研究使用共价调节剂(包括奥希替尼、依鲁替尼、罗西替尼、阿法替尼、奈拉替尼和阿卡替尼),考察了两种使用稀释血浆和低温(4℃和 20℃)进行平衡透析(ED)的方法。我们的数据表明,共价调节剂在不同物种中的血浆稳定性存在差异,如果未达到真正的平衡,药物耗竭可能会导致 f 的高估。此外,虽然低温 ED 可提高共价调节剂的回收率,但低温的影响可能导致 f 的低估。总体而言,由于其更快的平衡、更高的回收率且不受温度对 f 的影响,使用稀释血浆的 ED 是首选方法。如果必须对极其不稳定的化合物使用低温 ED,则必须采取预防措施,以确保血浆中 f 无温度依赖性。然而,对于不稳定的共价调节剂,建议采用正交 ED 方法来确认真正的平衡和温度对 f 的影响。此外,该策略可用于测定其他易失化合物的 f。

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