Semi-Mechanism-Based Pharmacokinetic-Toxicodynamic Model of Oxaliplatin-Induced Acute and Chronic Neuropathy

Oxaliplatin (L-OHP) is widely prescribed for treating gastroenterological cancer. L-OHP-induced peripheral neuropathy is a critical toxic effect that limits the dosage of L-OHP. An ideal chemotherapeutic strategy that does not result in severe peripheral neuropathy but confers high anticancer effica...

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Main Authors: Shinji Kobuchi, Risa Shimizu, Yukako Ito
Format: Article
Language:English
Published: MDPI AG 2020-02-01
Series:Pharmaceutics
Subjects:
Online Access:https://www.mdpi.com/1999-4923/12/2/125
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spelling doaj-2a3c6e6d51734a7ea9992e7d5bd67bb32020-11-25T01:42:25ZengMDPI AGPharmaceutics1999-49232020-02-0112212510.3390/pharmaceutics12020125pharmaceutics12020125Semi-Mechanism-Based Pharmacokinetic-Toxicodynamic Model of Oxaliplatin-Induced Acute and Chronic NeuropathyShinji Kobuchi0Risa Shimizu1Yukako Ito2Department of Pharmacokinetics, Kyoto Pharmaceutical University, Kyoto 607-8414, JapanDepartment of Pharmacokinetics, Kyoto Pharmaceutical University, Kyoto 607-8414, JapanDepartment of Pharmacokinetics, Kyoto Pharmaceutical University, Kyoto 607-8414, JapanOxaliplatin (L-OHP) is widely prescribed for treating gastroenterological cancer. L-OHP-induced peripheral neuropathy is a critical toxic effect that limits the dosage of L-OHP. An ideal chemotherapeutic strategy that does not result in severe peripheral neuropathy but confers high anticancer efficacy has not been established. To establish an optimal evidence-based dosing regimen, a pharmacokinetic-toxicodynamic (PK-TD) model that can characterize the relationship between drug administration regimen and L-OHP-induced peripheral neuropathy is required. We developed a PK-TD model of L-OHP for peripheral neuropathy using Phoenix<sup>&#174;</sup> NLME&#8482; Version 8.1. Plasma concentration of L-OHP, the number of withdrawal responses in the acetone test, and the threshold value in the von Frey test following 3, 5, or 8 mg/kg L-OHP administration were used. The PK-TD model consisting of an indirect response model and a transit compartment model adequately described and simulated time-course alterations of onset and grade of L-OHP-induced cold and mechanical allodynia. The results of model analysis suggested that individual fluctuation of plasma L-OHP concentration might be a more important factor for individual variability of neuropathy than cell sensitivity to L-OHP. The current PK-TD model might contribute to investigation and establishment of an optimal dosing strategy that can reduce L-OHP-induced neuropathy.https://www.mdpi.com/1999-4923/12/2/125pharmacokinetic-toxicodynamic modelingperipheral neuropathycancer chemotherapyplatinum compoundpersonalized therapytoxicology
collection DOAJ
language English
format Article
sources DOAJ
author Shinji Kobuchi
Risa Shimizu
Yukako Ito
spellingShingle Shinji Kobuchi
Risa Shimizu
Yukako Ito
Semi-Mechanism-Based Pharmacokinetic-Toxicodynamic Model of Oxaliplatin-Induced Acute and Chronic Neuropathy
Pharmaceutics
pharmacokinetic-toxicodynamic modeling
peripheral neuropathy
cancer chemotherapy
platinum compound
personalized therapy
toxicology
author_facet Shinji Kobuchi
Risa Shimizu
Yukako Ito
author_sort Shinji Kobuchi
title Semi-Mechanism-Based Pharmacokinetic-Toxicodynamic Model of Oxaliplatin-Induced Acute and Chronic Neuropathy
title_short Semi-Mechanism-Based Pharmacokinetic-Toxicodynamic Model of Oxaliplatin-Induced Acute and Chronic Neuropathy
title_full Semi-Mechanism-Based Pharmacokinetic-Toxicodynamic Model of Oxaliplatin-Induced Acute and Chronic Neuropathy
title_fullStr Semi-Mechanism-Based Pharmacokinetic-Toxicodynamic Model of Oxaliplatin-Induced Acute and Chronic Neuropathy
title_full_unstemmed Semi-Mechanism-Based Pharmacokinetic-Toxicodynamic Model of Oxaliplatin-Induced Acute and Chronic Neuropathy
title_sort semi-mechanism-based pharmacokinetic-toxicodynamic model of oxaliplatin-induced acute and chronic neuropathy
publisher MDPI AG
series Pharmaceutics
issn 1999-4923
publishDate 2020-02-01
description Oxaliplatin (L-OHP) is widely prescribed for treating gastroenterological cancer. L-OHP-induced peripheral neuropathy is a critical toxic effect that limits the dosage of L-OHP. An ideal chemotherapeutic strategy that does not result in severe peripheral neuropathy but confers high anticancer efficacy has not been established. To establish an optimal evidence-based dosing regimen, a pharmacokinetic-toxicodynamic (PK-TD) model that can characterize the relationship between drug administration regimen and L-OHP-induced peripheral neuropathy is required. We developed a PK-TD model of L-OHP for peripheral neuropathy using Phoenix<sup>&#174;</sup> NLME&#8482; Version 8.1. Plasma concentration of L-OHP, the number of withdrawal responses in the acetone test, and the threshold value in the von Frey test following 3, 5, or 8 mg/kg L-OHP administration were used. The PK-TD model consisting of an indirect response model and a transit compartment model adequately described and simulated time-course alterations of onset and grade of L-OHP-induced cold and mechanical allodynia. The results of model analysis suggested that individual fluctuation of plasma L-OHP concentration might be a more important factor for individual variability of neuropathy than cell sensitivity to L-OHP. The current PK-TD model might contribute to investigation and establishment of an optimal dosing strategy that can reduce L-OHP-induced neuropathy.
topic pharmacokinetic-toxicodynamic modeling
peripheral neuropathy
cancer chemotherapy
platinum compound
personalized therapy
toxicology
url https://www.mdpi.com/1999-4923/12/2/125
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AT yukakoito semimechanismbasedpharmacokinetictoxicodynamicmodelofoxaliplatininducedacuteandchronicneuropathy
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