A Toxicology Study of Complementation and Pulmonary Macrophage Transplantation Therapy of Hereditary PAP in Mice

Overview

Journal Mol Ther Methods Clin Dev

Publisher Cell Press

Date 2024 Apr 10

PMID 38596536

Authors

Paritha Arumugam

Brenna C Carey

Kathryn A Wikenheiser-Brokamp

Jeffrey Krischer

Matthew Wessendarp

Kenjiro Shima

Claudia Chalk

Jennifer Stock

Yan Ma

Diane Black

Michelle Imbrogno

Margaret Collins

Dan Justin Kalenda Yombo

Haripriya Sakthivel

Takuji Suzuki

Carolyn Lutzko

Jose A Cancelas

Michelle Adams

Elizabeth Hoskins

Dawn Lowe-Daniels

Lilith Reeves

Anne Kaiser

Bruce C Trapnell

Affiliations

Soon will be listed here.

Abstract

Pulmonary macrophage transplantation (PMT) is a gene and cell transplantation approach in development as therapy for hereditary pulmonary alveolar proteinosis (hPAP), a surfactant accumulation disorder caused by mutations in (and murine homologs). We conducted a toxicology study of PMT of gene-corrected macrophages (mGM-RαMϕs) or saline-control intervention in or wild-type (WT) mice including single ascending dose and repeat ascending dose studies evaluating safety, tolerability, pharmacokinetics, and pharmacodynamics. Lentiviral-mediated cDNA transfer restored GM-CSF signaling in mGM-RαMϕs. Following PMT, mGM-RαMϕs engrafted, remained within the lungs, and did not undergo uncontrolled proliferation or result in bronchospasm, pulmonary function abnormalities, pulmonary or systemic inflammation, anti-transgene product antibodies, or pulmonary fibrosis. Aggressive male fighting caused a similarly low rate of serious adverse events in saline- and PMT-treated mice. Transient, minor pulmonary neutrophilia and exacerbation of pre-existing hPAP-related lymphocytosis were observed 14 days after PMT of the safety margin dose but not the target dose (5,000,000 or 500,000 mGM-RαMϕs, respectively) and only in mice but not in WT mice. PMT reduced lung disease severity in mice. Results indicate PMT of mGM-RαMϕs was safe, well tolerated, and therapeutically efficacious in mice, and established a no adverse effect level and 10-fold safety margin.

Citing Articles

OCallaghan M, McCarthy C Mol Ther Methods Clin Dev. 2024; 32(1):101180.

PMID: 38249935 PMC: 10797184. DOI: 10.1016/j.omtm.2023.101180.

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