Transplanted Organoids Empower Human Preclinical Assessment of Drug Candidate for the Clinic

Overview

Journal Sci Adv

Specialties Biology
Science

Date 2022 Jul 20

PMID 35857479

Authors

Amy D Westerling-Bui

Eva Maria Fast

Thomas W Soare

Srinivasan Venkatachalan

Michael DeRan

Alyssa B Fanelli

Sergii Kyrychenko

Hien Hoang

Grinal M Corriea

Wei Zhang

Maolin Yu

Matthew Daniels

Goran Malojcic

Xin-Ru Pan-Zhou

Mark W Ledeboer

Jean-Christophe Harmange

Maheswarareddy Emani

Thomas T Tibbitts

John F Reilly

Peter Mundel

Affiliations

Soon will be listed here.

Abstract

Pharmacodynamic (PD) studies are an essential component of preclinical drug discovery. Current approaches for PD studies, including the analysis of novel kidney disease targeting therapeutic agents, are limited to animal models with unclear translatability to the human condition. To address this challenge, we developed a novel approach for PD studies using transplanted, perfused human kidney organoids. We performed pharmacokinetic (PK) studies with GFB-887, an investigational new drug now in phase 2 trials. Orally dosed GFB-887 to athymic rats that had undergone organoid transplantation resulted in measurable drug exposure in transplanted organoids. We established the efficacy of orally dosed GFB-887 in PD studies, where quantitative analysis showed significant protection of kidney filter cells in human organoids and endogenous rat host kidneys. This widely applicable approach demonstrates feasibility of using transplanted human organoids in preclinical PD studies with an investigational new drug, empowering organoids to revolutionize drug discovery.

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