Engineering Toxoplasma gondii secretion systems for intracellular delivery of multiple large therapeutic proteins to neurons

Author:

Bracha ShaharORCID,Johnson Hannah J.,Pranckevicius Nicole A.,Catto Francesca,Economides Athena E.ORCID,Litvinov Sergey,Hassi Karoliina,Rigoli Marco Tullio,Cheroni Cristina,Bonfanti Matteo,Valenti Alessia,Stucchi Sarah,Attreya Shruti,Ross Paul D.,Walsh DanielORCID,Malachi Nati,Livne Hagay,Eshel Reut,Krupalnik Vladislav,Levin Doron,Cobb Stuart,Koumoutsakos Petros,Caporale Nicolò,Testa Giuseppe,Aguzzi AdrianoORCID,Koshy Anita A.,Sheiner LilachORCID,Rechavi OdedORCID

Abstract

AbstractDelivering macromolecules across biological barriers such as the blood–brain barrier limits their application in vivo. Previous work has demonstrated that Toxoplasma gondii, a parasite that naturally travels from the human gut to the central nervous system (CNS), can deliver proteins to host cells. Here we engineered T. gondii’s endogenous secretion systems, the rhoptries and dense granules, to deliver multiple large (>100 kDa) therapeutic proteins into neurons via translational fusions to toxofilin and GRA16. We demonstrate delivery in cultured cells, brain organoids and in vivo, and probe protein activity using imaging, pull-down assays, scRNA-seq and fluorescent reporters. We demonstrate robust delivery after intraperitoneal administration in mice and characterize 3D distribution throughout the brain. As proof of concept, we demonstrate GRA16-mediated brain delivery of the MeCP2 protein, a putative therapeutic target for Rett syndrome. By characterizing the potential and current limitations of the system, we aim to guide future improvements that will be required for broader application.

Publisher

Springer Science and Business Media LLC

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