A Minimal PBPK/PD Model with Expansion-Enhanced Target-Mediated Drug Disposition to Support a First-in-Human Clinical Study Design for a FLT3L-Fc Molecule

Overview

Journal Pharmaceutics

Publisher MDPI

Date 2024 May 25

PMID 38794321

Authors

Iraj Hosseini

Brett Fleisher

Jennifer Getz

Jeremie Decalf

Mandy Kwong

Meric Ovacik

Travis W Bainbridge

Christine Moussion

Gautham K Rao

Kapil Gadkar

Amrita V Kamath

Saroja Ramanujan

Affiliations

Soon will be listed here.

Abstract

FLT3L-Fc is a half-life extended, effectorless Fc-fusion of the native human FLT3-ligand. In cynomolgus monkeys, treatment with FLT3L-Fc leads to a complex pharmacokinetic/pharmacodynamic (PK/PD) relationship, with observed nonlinear PK and expansion of different immune cell types across different dose levels. A minimal physiologically based PK/PD model with expansion-enhanced target-mediated drug disposition (TMDD) was developed to integrate the molecule's mechanism of action, as well as the complex preclinical and clinical PK/PD data, to support the preclinical-to-clinical translation of FLT3L-Fc. In addition to the preclinical PK data of FLT3L-Fc in cynomolgus monkeys, clinical PK and PD data from other FLT3-agonist molecules (GS-3583 and CDX-301) were used to inform the model and project the expansion profiles of conventional DC1s (cDC1s) and total DCs in peripheral blood. This work constitutes an essential part of our model-informed drug development (MIDD) strategy for clinical development of FLT3L-Fc by projecting PK/PD in healthy volunteers, determining the first-in-human (FIH) dose, and informing the efficacious dose in clinical settings. Model-generated results were incorporated in regulatory filings to support the rationale for the FIH dose selection.

Citing Articles

A single point mutation on FLT3L-Fc protein increases the risk of immunogenicity.

Qin D, Phung Q, Wu P, Yin Z, Tam S, Tran P Front Immunol. 2025; 16:1519452.

PMID: 40018031 PMC: 11865242. DOI: 10.3389/fimmu.2025.1519452.

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