Novel Endogenous Engineering Platform for Robust Loading and Delivery of Functional mRNA by Extracellular Vesicles

Author:

Zickler Antje M.123ORCID,Liang Xiuming1234ORCID,Gupta Dhanu125ORCID,Mamand Doste R.1236,De Luca Mariacristina78,Corso Giulia129,Errichelli Lorenzo7ORCID,Hean Justin7,Sen Titash710ORCID,Elsharkasy Omnia M.123,Kamei Noriyasu1211ORCID,Niu Zheyu1212,Zhou Guannan1213,Zhou Houze123,Roudi Samantha123ORCID,Wiklander Oscar P. B.136ORCID,Görgens André12314ORCID,Nordin Joel Z.1315ORCID,Castilla‐Llorente Virginia716ORCID,EL Andaloussi Samir123ORCID

Affiliation:

1. Division of Biomolecular and Cellular Medicine Department of Laboratory Medicine Karolinska Institutet ANA Futura Alfred‐Nobels‐Allé 8, Huddinge Stockholm 14152 Sweden

2. Department of Cellular Therapy and Allogeneic Stem Cell Transplantation (CAST) Karolinska University Hospital Stockholm 14186 Sweden

3. Karolinska ATMP Center, Karolinska Institutet ANA Futura Alfred‐Nobels‐Allé 8, Huddinge Stockholm 14152 Sweden

4. Cancer Research Laboratory Shandong University‐Karolinska Institutet collaborative Laboratory School of Basic Medical Science Shandong University No. 44, Wenhua Xi Road Ji'nan Shandong 250012 P. R. China

5. Institute of Developmental and Regenerative Medicine, Department of Paediatrics. University of Oxford Old Road Campus, Roosevelt Dr, Headington Oxford OX3 7TY UK

6. Breast Center, Karolinska Comprehensive Cancer Center Karolinska University Hospital Stockholm 14186 Sweden

7. Evox Therapeutics Ltd. Oxford Science Park Medawar Centre Robert Robinson Avenue Oxford OX4 4HG UK

8. Human Technopole Viale Rita Levi Montalcini, 1 Milan 20157 Italy

9. Evercyte GmbH Leberstrasse 20 Vienna 1110 Austria

10. Lonza Biologics Chesterford Research Park Cambridge CB10 1XL UK

11. Laboratory of Drug Delivery Systems Faculty of Pharmaceutical Sciences Kobe Gakuin University 1‐1‐3 Minatojima, Chuo‐ku Kobe Hyogo 650‐8586 Japan

12. Department of Hepatobiliary Surgery Shandong Provincial Hospital Affiliated to Shandong First Medical University No. 324, Five Jing Road Ji'nan Shandong 250012 P. R. China

13. Department of Gynecology The Obstetrics and Gynecology Hospital of Fudan University No. 419, Fangxie Road Shanghai 200011 P. R. China

14. Institute for Transfusion Medicine University Hospital Essen University of Duisburg‐Essen 45147 Essen Germany

15. Department of Clinical Immunology and Transfusion Medicine (KITM) Karolinska University Hospital Stockholm 14186 Sweden

16. Uncommon Bio Cambridge Technopark Newmarket Rd Cambridge CB5 8PB UK

Abstract

AbstractMessenger RNA (mRNA) has emerged as an attractive therapeutic molecule for a plethora of clinical applications. For in vivo functionality, mRNA therapeutics require encapsulation into effective, stable, and safe delivery systems to protect the cargo from degradation and reduce immunogenicity. Here, a bioengineering platform for efficient mRNA loading and functional delivery using bionormal nanoparticles, extracellular vesicles (EVs), is established by expressing a highly specific RNA‐binding domain fused to CD63 in EV producer cells stably expressing the target mRNA. The additional combination with a fusogenic endosomal escape moiety, Vesicular Stomatitis Virus Glycoprotein, enables functional mRNA delivery in vivo at doses substantially lower than currently used clinically with synthetic lipid‐based nanoparticles. Importantly, the application of EVs loaded with effective cancer immunotherapy proves highly effective in an aggressive melanoma mouse model. This technology addresses substantial drawbacks currently associated with EV‐based nucleic acid delivery systems and is a leap forward to clinical EV applications.

Funder

Center for Innovative Medicine

Vetenskapsrådet

Cancerfonden

Stiftelsen för Strategisk Forskning

Horizon 2020 Framework Programme

HORIZON EUROPE European Research Council

Publisher

Wiley

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