Polymersomes with splenic avidity target red pulp myeloid cells for cancer immunotherapy

Author:

Wauters Annelies C.ORCID,Scheerstra Jari F.ORCID,van Leent Mandy M. T.ORCID,Teunissen Abraham J. P.ORCID,Priem Bram,Beldman Thijs J.,Rother NilsORCID,Duivenvoorden RaphaëlORCID,Prévot Geoffrey,Munitz Jazz,Toner Yohana C.ORCID,Deckers Jeroen,van Elsas YuriORCID,Mora-Raimundo Patricia,Chen Gal,Nauta Sheqouia A.,Verschuur Anna Vera D.,Griffioen Arjan W.,Schrijver David P.ORCID,Anbergen TomORCID,Li YudongORCID,Wu Hanglong,Mason Alexander F.ORCID,van Stevendaal Marleen H. M. E.,Kluza EwelinaORCID,Post Richard A. J.ORCID,Joosten Leo A. B.ORCID,Netea Mihai G.ORCID,Calcagno Claudia,Fayad Zahi A.ORCID,van der Meel RoyORCID,Schroeder AviORCID,Abdelmohsen Loai K. E. A.ORCID,Mulder Willem J. M.ORCID,van Hest Jan C. M.ORCID

Abstract

AbstractRegulating innate immunity is an emerging approach to improve cancer immunotherapy. Such regulation requires engaging myeloid cells by delivering immunomodulatory compounds to hematopoietic organs, including the spleen. Here we present a polymersome-based nanocarrier with splenic avidity and propensity for red pulp myeloid cell uptake. We characterized the in vivo behaviour of four chemically identical yet topologically different polymersomes by in vivo positron emission tomography imaging and innovative flow and mass cytometry techniques. Upon intravenous administration, relatively large and spherical polymersomes accumulated rapidly in the spleen and efficiently targeted myeloid cells in the splenic red pulp. When loaded with β-glucan, intravenously administered polymersomes significantly reduced tumour growth in a mouse melanoma model. We initiated our nanotherapeutic’s clinical translation with a biodistribution study in non-human primates, which revealed that the platform’s splenic avidity is preserved across species.

Publisher

Springer Science and Business Media LLC

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