In vivo mRNA expression of a multi-mechanistic mAb combination protects against Staphylococcus aureus infection

多种机制 mAb 组合的体内 mRNA 表达可预防金黄色葡萄球菌感染

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作者:Christine Tkaczyk, Michael Newton, Mun Mun Patnaik, George Thom, Martin Strain, Adam Gamson, Olalekan Daramola, Andal Murthy, Julie Douthwaite, Oleg Stepanov, Elin Boger, Haitao Yang, Mark T Esser, Ashley Lidwell, Antonio DiGiandomenico, Luis Santos, Bret R Sellman

Abstract

Single monoclonal antibodies (mAbs) can be expressed in vivo through gene delivery of their mRNA formulated with lipid nanoparticles (LNPs). However, delivery of a mAb combination could be challenging due to the risk of heavy and light variable chain mispairing. We evaluated the pharmacokinetics of a three mAb combination against Staphylococcus aureus first in single chain variable fragment scFv-Fc and then in immunoglobulin G 1 (IgG1) format in mice. Intravenous delivery of each mRNA/LNP or the trio (1 mg/kg each) induced functional antibody expression after 24 h (10-100 μg/mL) with 64%-78% cognate-chain paired IgG expression after 3 days, and an absence of non-cognate chain pairing for scFv-Fc. We did not observe reduced neutralizing activity for each mAb compared with the level of expression of chain-paired mAbs. Delivery of the trio mRNA protected mice in an S. aureus-induced dermonecrosis model. Intravenous administration of the three mRNA in non-human primates achieved peak serum IgG levels ranging between 2.9 and 13.7 μg/mL with a half-life of 11.8-15.4 days. These results suggest nucleic acid delivery of mAb combinations holds promise and may be a viable option to streamline the development of therapeutic antibodies.

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