Antibody-displaying extracellular vesicles for targeted cancer therapy.

Oscar P B Wiklander,Oscar P B Wiklander,Oscar P B Wiklander,Doste R Mamand,Doste R Mamand,Doste R Mamand,Dara K Mohammad,Dara K Mohammad,Wenyi Zheng,Wenyi Zheng,Wenyi Zheng,Rim Jawad Wiklander,Rim Jawad Wiklander,Taras Sych,Antje M Zickler,Antje M Zickler,Antje M Zickler,Xiuming Liang,Xiuming Liang,Xiuming Liang,Heena Sharma,Andrea Lavado,Jeremy Bost,Jeremy Bost,Samantha Roudi,Samantha Roudi,Samantha Roudi,Giulia Corso,Giulia Corso,Angus J Lennaárd,Angus J Lennaárd,Manuchehr Abedi-Valugerdi,Manuchehr Abedi-Valugerdi,Imre Mäger,Evren Alici,Evren Alici,Erdinc Sezgin,Joel Z Nordin,Joel Z Nordin,Joel Z Nordin,Dhanu Gupta,Dhanu Gupta,Dhanu Gupta,André Görgens,André Görgens,André Görgens,André Görgens,Samir El Andaloussi,Samir El Andaloussi,Samir El Andaloussi

doi:10.1038/s41551-024-01214-6

Abstract

Extracellular vesicles (EVs) function as natural delivery vectors and mediators of biological signals across tissues. Here, by leveraging these functionalities, we show that EVs decorated with an antibody-binding moiety specific for the fragment crystallizable (Fc) domain can be used as a modular delivery system for targeted cancer therapy. The Fc-EVs can be decorated with different types of immunoglobulin G antibody and thus be targeted to virtually any tissue of interest. Following optimization of the engineered EVs by screening Fc-binding and EV-sorting moieties, we show the targeting of EVs to cancer cells displaying the human epidermal receptor 2 or the programmed-death ligand 1, as well as lower tumour burden and extended survival of mice with subcutaneous melanoma tumours when systemically injected with EVs displaying an antibody for the programmed-death ligand 1 and loaded with the chemotherapeutic doxorubicin. EVs with Fc-binding domains may be adapted to display other Fc-fused proteins, bispecific antibodies and antibody-drug conjugates.

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