Scalable in silico Simulation of Transdermal Drug Permeability: Application of BIOiSIM Platform

Neha Maharao; Victor Antontsev; Hypatia Hou; Jason Walsh; Jyotika Varshney

doi:10.2147/DDDT.S253064

Scalable in silico Simulation of Transdermal Drug Permeability: Application of BIOiSIM Platform

Drug Des Devel Ther. 2020 Jun 11:14:2307-2317. doi: 10.2147/DDDT.S253064. eCollection 2020.

Authors

Neha Maharao^#¹, Victor Antontsev^#¹, Hypatia Hou¹, Jason Walsh¹, Jyotika Varshney¹

Affiliation

¹ VeriSIM Life Inc., San Francisco, CA, USA.

^# Contributed equally.

Abstract

Introduction: Transdermal drug delivery is gaining popularity as an alternative to traditional routes of administration. It can increase patient compliance because of its painless and noninvasive nature, aid compounds in bypassing presystemic metabolic effects, and reduce the likelihood of adverse effects through decreased systemic exposure. In silico physiological modeling is critical to predicting dermal exposure for a therapeutic and assessing the impact of different formulations on transdermal disposition.

Methods: The present study aimed at developing a physiologically based transdermal platform, "BIOiSIM", that could be globally applied to a wide variety of compounds to predict their transdermal disposition. The platform integrates a 16-compartment model of compound pharmacokinetics and was used to simulate and predict drug exposure of three chemically and biologically distinct drug-like compounds. Machine learning optimization was composed of two components: exhaustive search algorithm (coarse-tuning) and descent (fine-tuning) integrated with the platform used to quantitatively determine parameters influencing pharmacokinetics (eg permeability, k_perm) of test compounds.

Results: The model successfully predicted drug exposure (AUC, C_max and T_max) following transdermal application of morphine, buprenorphine and nicotine in human subjects, mostly with less than two-fold absolute average fold error (AAFE). The model was further able to successfully characterize the relationship between observed systemic exposure and intended pharmacological effect. The predicted systemic concentration of morphine and plasma levels of endogenous pain biomarkers were used to estimate the effectiveness of a given therapeutic regimen.

Conclusion: BIOiSIM marks a novel approach to in silico prediction that will enable leveraging of machine learning technology in the pharmaceutical space. The approach to model development outlined results in scalable, accurate models and enables the generation of large parameter/coefficient datasets from in vivo clinical data that can be used in future work to train quantitative structure activity relationship (QSAR) models for predicting likelihood of compound utility as a transdermally administered therapeutic.

Keywords: BIOiSIM; computational modeling; machine learning; transdermal absorption.

MeSH terms

Administration, Cutaneous
Buprenorphine / administration & dosage
Buprenorphine / metabolism*
Buprenorphine / pharmacokinetics
Computer Simulation
Humans
Models, Biological*
Morphine / administration & dosage
Morphine / metabolism*
Morphine / pharmacokinetics
Nicotine / administration & dosage
Nicotine / metabolism*
Nicotine / pharmacokinetics
Permeability
Quantitative Structure-Activity Relationship

Substances

Buprenorphine
Nicotine
Morphine