2‐Deoxyglucose and hydroxychloroquine HPLC‐MS–MS analytical methods and pharmacokinetic interactions after oral co‐administration in male rats

Dongxiao Sun; Sangyub Kim; Deepkamal Karelia; Yibin Deng; Cheng Jiang; Junxuan Lü

doi:10.1002/prp2.1173

Pharmacology Research & Perspectives (Feb 2024)

2‐Deoxyglucose and hydroxychloroquine HPLC‐MS–MS analytical methods and pharmacokinetic interactions after oral co‐administration in male rats

Dongxiao Sun,
Sangyub Kim,
Deepkamal Karelia,
Yibin Deng,
Cheng Jiang,
Junxuan Lü

Affiliations

Dongxiao Sun: Department of Pharmacology Pennsylvania State University College of Medicine Hershey Pennsylvania USA
Sangyub Kim: Department of Pharmacology Pennsylvania State University College of Medicine Hershey Pennsylvania USA
Deepkamal Karelia: Department of Pharmacology Pennsylvania State University College of Medicine Hershey Pennsylvania USA
Yibin Deng: Department of Urology University of Minnesota College of Medicine Minneapolis Minnesota USA
Cheng Jiang: Department of Pharmacology Pennsylvania State University College of Medicine Hershey Pennsylvania USA
Junxuan Lü: Department of Pharmacology Pennsylvania State University College of Medicine Hershey Pennsylvania USA

DOI: https://doi.org/10.1002/prp2.1173
Journal volume & issue: Vol. 12, no. 1
pp. n/a – n/a

Abstract

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Abstract Our previous work has shown a synergistic tumoricidal efficacy of combining the hexokinase (HK) inhibitor 2‐deoxyglucose (2‐DG) and the autophagy inhibitor chloroquine (CQ) through intraperitoneal injections on HK2‐addicted prostate cancers in animal models. The pharmacokinetic (PK) behaviors of these oral drugs after simultaneous oral administration have not been reported. We developed high‐performance liquid chromatography–tandem mass spectrometry (HPLC‐MS–MS) analytical methods for 2‐DG and the clinically favored drug hydroxychloroquine (HCQ) for sera samples. Using a jugular vein‐cannulated male rat model with serial blood collection before and after a single gavage dose of each drug alone or in combination, we examined their PK metrics for drug–drug interactions. The data demonstrated a rapid and complete separation of 2‐DG from common monosaccharides by HPLC‐MS–MS multi‐reaction monitoring. Application of the HPLC‐MS–MS 2‐DG and HCQ methods to sera samples of nine rats showed a peak time (Tmax) for 2‐DG of 0.5 h after 2‐DG alone or with HCQ and identical post‐peak half‐life of approximately 1 h. With a seemingly bi‐modal time course for HCQ, the Tmax for HCQ alone (1.2 h) was faster than that for the combination (2 h; p = .017). After combination dosing, the peak concentration (Cmax) and area under the curve (AUC0‐4h) of 2‐DG were decreased by 53.8% (p = .0004) and 53.7% (p = .0001), whereas AUC0‐8h for HCQ was decreased by 30.8% (p = .0279) from the respective single dosing. Without changing the mean residence time (MRT0‐∞) of each drug, the combination affected the apparent volume of distribution (Vd) and clearance (CL) of 2‐DG, and CL for HCQ without affecting its Vd. We observed significant negative PK interactions, probably at the intestinal absorption level, between 2‐DG and HCQ taken simultaneously by mouth. Future optimization efforts are warranted for their combination regimen for clinical translation.

Published in Pharmacology Research & Perspectives

ISSN: 2052-1707 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: http://onlinelibrary.wiley.com/journal/10.1002/(ISSN)2052-1707

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