Risk Assessment Using Cytochrome P450 Time-Dependent Inhibition Assays at Single Time and Concentration in the Early Stage of Drug Discovery

J Pharm Sci. 2017 Sep;106(9):2839-2846. doi: 10.1016/j.xphs.2017.04.077.

Mai Kosaka ¹, Yohei Kosugi ², Hideki Hirabayashi ²

Affiliations

1 Drug Metabolism and Pharmacokinetics Research Laboratories, Research, Takeda Pharmaceutical Company Limited, 26-1, Muraoka-Higashi 2-chome, Fujisawa, Kanagawa, Japan. Electronic address: [email protected].
2 Drug Metabolism and Pharmacokinetics Research Laboratories, Research, Takeda Pharmaceutical Company Limited, 26-1, Muraoka-Higashi 2-chome, Fujisawa, Kanagawa, Japan.

PMID: 28483425 DOI: 10.1016/j.xphs.2017.04.077

Abstract

In this article, we proposed a risk assessment strategy for CYP3A time-dependent inhibition (TDI) during drug discovery based on a thorough retrospective study of 13 reference drugs, some of which are known to have in vitro TDI potential but have unknown clinical relevance. First, the traditional parameter k_inact/K_I, recommended by regulatory authorities for necessity decision making in clinical drug-drug interaction (DDI) studies, was investigated as a predictive index for clinical TDI liability. The cutoff value of 1.1 for k_inact/K_I, established by the Food and Drug Administration, tended to produce false-positive prediction results for clinical DDI occurrence. The value of 1.25 recommended in the European Medicines Evaluation Agency draft guideline yielded better predictions with only 1 false negative for diltiazem. Second, to enable earlier risk assessment, remaining activity, defined as the residual CYP3A activity in vitro obtained in the screening conditions, was investigated as an alternative index. As a result, the ratios of unbound C_max or area under the curve to remaining activity precisely predicted clinical DDI occurrence. In conclusion, we demonstrated the predictive power of k_inact/K_I and remaining activity values for clinical DDIs. These findings provide insights that enable TDI risk assessment, even during drug discovery.

Keywords

cytochrome P450; drug interactions; inhibition; metabolism; microsomes; protein binding.

Products

Cat. No.

Product Name

Description

Target

Research Area
HY-17007

Saquinavir

99.73%, HIV Protease Inhibitor

HIV; HIV Protease; SARS-CoV

Infection; Cancer

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