Assessing Dose-Exposure-Response Relationships of Miltefosine in Adults and Children using Physiologically-Based Pharmacokinetic Modeling Approach

Shadrack J Madu; Ke Wang; Siri Kalyan Chirumamilla; David B Turner; Patrick G Steel; Mingzhong Li

doi:10.1007/s11095-023-03610-0

Assessing Dose-Exposure-Response Relationships of Miltefosine in Adults and Children using Physiologically-Based Pharmacokinetic Modeling Approach

Pharm Res. 2023 Dec;40(12):2983-3000. doi: 10.1007/s11095-023-03610-0. Epub 2023 Oct 10.

Authors

Shadrack J Madu¹, Ke Wang¹, Siri Kalyan Chirumamilla², David B Turner², Patrick G Steel³, Mingzhong Li⁴

Affiliations

¹ School of Pharmacy, De Montfort University, Leicester, LE1 9BH, UK.
² Certara UK Limited, Simcyp Division, Sheffield, S1 2BJ, UK.
³ Department of Chemistry, Durham University, Durham, DH1 3LE, UK.
⁴ School of Pharmacy, De Montfort University, Leicester, LE1 9BH, UK. mli@dmu.ac.uk.

Abstract

Objectives: Miltefosine is the first and only oral medication to be successfully utilized as an antileishmanial agent. However, the drug is associated with differences in exposure patterns and cure rates among different population groups e.g. ethnicity and age (i.e., children v adults) in clinical trials. In this work, mechanistic population physiologically-based pharmacokinetic (PBPK) models have been developed to study the dose-exposure-response relationship of miltefosine in in silico clinical trials and evaluate the differences in population groups, particularly children and adults.

Methods: The Simcyp population pharmacokinetics platform was employed to predict miltefosine exposure in plasma and peripheral blood mononuclear cells (PBMCs) in a virtual population under different dosing regimens. The cure rate of a simulation was based on the percentage of number of the individual virtual subjects with AUC_d0-28 > 535 µg⋅day/mL in the virtual population.

Results: It is shown that both adult and paediatric PBPK models of miltefosine can be developed to predict the PK data of the clinical trials accurately. There was no significant difference in the predicted dose-exposure-response of the miltefosine treatment for different simulated ethnicities under the same dose regime and the dose-selection strategies determined the clinical outcome of the miltefosine treatment. A lower cure rate of the miltefosine treatment in paediatrics was predicted because a lower exposure of miltefosine was simulated in virtual paediatric in comparison with adult virtual populations when they received the same dose of the treatment.

Conclusions: The mechanistic PBPK model suggested that the higher fraction of unbound miltefosine in plasma was responsible for a higher probability of failure in paediatrics because of the difference in the distribution of plasma proteins between adults and paediatrics. The developed PBPK models could be used to determine an optimal miltefosine dose regime in future clinical trials.

Keywords: PBPK modelling; dose-exposure–response relationships; miltefosine; pharmacokinetics.

MeSH terms

Adult
Antiprotozoal Agents*
Child
Computer Simulation
Humans
Leukocytes, Mononuclear*
Models, Biological
Phosphorylcholine

Substances

miltefosine
Phosphorylcholine
Antiprotozoal Agents

Grants and funding

EP/T020490/1/Engineering and Physical Sciences Research Council