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February 28, 2026Open Access

Effects of CYP1A2 genetic polymorphisms on the pharmacokinetics of pentoxifylline and its active metabolites

Key Points

The study aims to explore the impact of CYP1A2 genetic polymorphisms on the pharmacokinetics of pentoxifylline and its metabolites.
Administered a single 400 mg oral dose of pentoxifylline to 46 healthy Chinese volunteers.
Quantified plasma concentrations using LC-MS/MS.
Determined CYP1A2 genotypes using the SnapShot technique.
Participants with the CYP1A2 -3860G/A genotype had a 22.3% reduction in maximum plasma concentration of metabolite M5 compared to homozygous genotypes.
Significant reductions in exposure (AUC0–t and AUC0–∞) for metabolite M5 were seen in heterozygotes compared to homozygous carriers.
The CYP1A2 -163 C/A genotype significantly lowered pentoxifylline exposure by 29.14% and 28.62%.

Abstract

To investigate whether the CYP1A2 genetic polymorphisms could affect the pharmacokinetics of pentoxifylline and its two active metabolites in Chinese healthy participants. Forty-six healthy Chinese volunteers were administered a single 400 mg oral dose of pentoxifylline. The plasma concentrations of pentoxifylline and its active metabolites were quantified using LC-MS/MS. The CYP1A2 genotypes for the following loci were determined by the SnapShot technique: -5347T > C (rs2470890), -3860G > A (rs2069514), -3594T > G (rs2069520), -3113 C > A (rs2069521), -2467delT (rs35694136), -739T > G (rs2069526), -163 C > A (rs762551), and 2159G > A (rs2472304). Participants heterozygous for the CYP1A2 -3860G/A genotype exhibited a 22.3% and 17.6% reduction in the Cmax of metabolite M5 compared to homozygous − 3860G/G and − 3860 A/A carriers, respectively. Participants carrying the CYP1A2 -3860G/A genotype exhibited reduced AUC0–t and AUC0–∞ values of metabolite M5 compared to both homozygous − 3860G/G and − 3860 A/A carriers. Additionally, participants with the CYP1A2 -163 C/A genotype had significantly lower pentoxifylline AUC0–t and AUC0–∞ than those with the − 163 C/C genotype (reduced by 29.14% and 28.62%, respectively). In contrast, no significant differences were observed in the pharmacokinetic parameters of the primary metabolites M1 and M5 across the different CYP1A2 genotype groups. The two CYP1A2 polymorphisms significantly affected pharmacokinetics: the − 3860G > A variant was associated with a significant reduction in systemic exposure to metabolite M5, while potentially increasing exposure to pentoxifylline and M1. Conversely, the − 163 C > A variant significantly reduced the plasma exposure of the parent drug pentoxifylline, with a trend toward decreased exposure for metabolites M1 and M5. This clinical trial has been registered in the Chinese Clinical Trial Register (accessible at http://www.chinadrugtrials.org.cn/index.htmL) with the registration number CTR20233180 on October 08, 2023.

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Cite This Study

Guo et al. (Thu,) studied this question.

synapsesocial.com/papers/69a286240a974eb0d3c00f41 https://doi.org/https://doi.org/10.1186/s40360-026-01106-2

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