TY - JOUR
T1 - Vincristine Disposition and Neurotoxicity Are Unchanged in Humanized CYP3A5 Mice
AU - Li, Yang
AU - Kazuki, Yasuhiro
AU - Drabison, Thomas
AU - Kobayashi, Kaoru
AU - Fujita, Ken Ichi
AU - Xu, Yue
AU - Jin, Yan
AU - Ahmed, Eman
AU - Li, Junan
AU - Eisenmann, Eric D.
AU - Baker, Sharyn D.
AU - Cavaletti, Guido
AU - Sparreboom, Alex
AU - Hu, Shuiying
N1 - Publisher Copyright:
Copyright © 2024 by The American Society for Pharmacology and Experimental Therapeutics.
PY - 2024/2/1
Y1 - 2024/2/1
N2 - Previous studies have suggested that the incidence of vincristine-induced peripheral neuropathy (VIPN) is potentially linked with cytochrome P450 (CYP)3A5, a polymorphic enzyme that metabolizes vincristine in vitro, and with concurrent use of azole antifungals such as ketoconazole. The assumed mechanism for these interactions is through modulation of CYP3A-mediated metabolism, leading to decreased vincristine clearance and increased susceptibility to VIPN. Given the controversy surrounding the contribution of these mechanisms, we directly tested these hypotheses in genetically engineered mouse models with a deficiency of the entire murine Cyp3a locus [Cyp3a(2/2) mice] and in humanized transgenic animals with hepatic expression of functional and nonfunctional human CYP3A5 variants. Compared with wild-type mice, the systemic exposure to vincristine was increased by only 1.15-fold (95% confidence interval, 0.84–1.58) in Cyp3a(2/2) mice, suggesting that the clearance of vincristine in mice is largely independent of hepatic Cyp3a function. In line with these observations, we found that Cyp3a deficiency or pretreatment with the CYP3A inhibitors ketoconazole or nilotinib did not influence the severity and time course of VIPN and that exposure to vincristine was not substantially altered in humanized CYP3A5*3 mice or humanized CYP3A5*1 mice compared with Cyp3a(2/2) mice. Our study suggests that the contribution of CYP3A5-mediated metabolism to vincristine elimination and the associated drug–drug interaction potential is limited and that plasma levels of vincristine are unlikely to be strongly predictive of VIPN. SIGNIFICANCE STATEMENT The current study suggests that CYP3A5 genotype status does not substantially influence vincristine disposition and neurotoxicity in translationally relevant murine models. These findings raise concerns about the causality of previously reported relationships between variant CYP3A5 genotypes or concomitant azole use with the incidence of vincristine neurotoxicity.
AB - Previous studies have suggested that the incidence of vincristine-induced peripheral neuropathy (VIPN) is potentially linked with cytochrome P450 (CYP)3A5, a polymorphic enzyme that metabolizes vincristine in vitro, and with concurrent use of azole antifungals such as ketoconazole. The assumed mechanism for these interactions is through modulation of CYP3A-mediated metabolism, leading to decreased vincristine clearance and increased susceptibility to VIPN. Given the controversy surrounding the contribution of these mechanisms, we directly tested these hypotheses in genetically engineered mouse models with a deficiency of the entire murine Cyp3a locus [Cyp3a(2/2) mice] and in humanized transgenic animals with hepatic expression of functional and nonfunctional human CYP3A5 variants. Compared with wild-type mice, the systemic exposure to vincristine was increased by only 1.15-fold (95% confidence interval, 0.84–1.58) in Cyp3a(2/2) mice, suggesting that the clearance of vincristine in mice is largely independent of hepatic Cyp3a function. In line with these observations, we found that Cyp3a deficiency or pretreatment with the CYP3A inhibitors ketoconazole or nilotinib did not influence the severity and time course of VIPN and that exposure to vincristine was not substantially altered in humanized CYP3A5*3 mice or humanized CYP3A5*1 mice compared with Cyp3a(2/2) mice. Our study suggests that the contribution of CYP3A5-mediated metabolism to vincristine elimination and the associated drug–drug interaction potential is limited and that plasma levels of vincristine are unlikely to be strongly predictive of VIPN. SIGNIFICANCE STATEMENT The current study suggests that CYP3A5 genotype status does not substantially influence vincristine disposition and neurotoxicity in translationally relevant murine models. These findings raise concerns about the causality of previously reported relationships between variant CYP3A5 genotypes or concomitant azole use with the incidence of vincristine neurotoxicity.
UR - http://www.scopus.com/inward/record.url?scp=85182091150&partnerID=8YFLogxK
U2 - 10.1124/dmd.123.001466
DO - 10.1124/dmd.123.001466
M3 - Article
C2 - 38071551
AN - SCOPUS:85182091150
SN - 0090-9556
VL - 52
SP - 80
EP - 85
JO - Drug Metabolism and Disposition
JF - Drug Metabolism and Disposition
IS - 2
ER -