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Immunoengineering via Chimeric Antigen Receptor-T Cell Therapy: Reprogramming Nanodrug Delivery.

ΤίτλοςImmunoengineering via Chimeric Antigen Receptor-T Cell Therapy: Reprogramming Nanodrug Delivery.
Publication TypeJournal Article
Year of Publication2023
AuthorsKatopodi, T., Petanidis S., Anestakis D., Charalampidis C., Chatziprodromidou I., Floros G., Eskitzis P., Zarogoulidis P., Koulouris C., Sevva C., Papadopoulos K., Dagher M., Varsamis N., Theodorou V., Mystakidou C. Maria, Katsios N. Iason, Farmakis K., & Kosmidis C.
JournalPharmaceutics
Volume15
Issue10
Date Published2023 Oct 13
ISSN1999-4923
Abstract

Following its therapeutic effect in hematological metastasis, chimeric antigen receptor (CAR) T cell therapy has gained a great deal of attention during the last years. However, the effectiveness of this treatment has been hampered by a number of challenges, including significant toxicities, difficult access to tumor locations, inadequate therapeutic persistence, and manufacturing problems. Developing novel techniques to produce effective CARs, administer them, and monitor their anti-tumor activity in CAR-T cell treatment is undoubtedly necessary. Exploiting the advantages of nanotechnology may possibly be a useful strategy to increase the efficacy of CAR-T cell treatment. This study outlines the current drawbacks of CAR-T immunotherapy and identifies promising developments and significant benefits of using nanotechnology in order to introduce CAR transgene motifs into primary T cells, promote T cell expansion, enhance T cell trafficking, promote intrinsic T cell activity and rewire the immunosuppressive cellular and vascular microenvironments. Therefore, the development of powerful CART cells can be made possible with genetic and functional alterations supported by nanotechnology. In this review, we discuss the innovative and possible uses of nanotechnology for clinical translation, including the delivery, engineering, execution, and modulation of immune functions to enhance and optimize the anti-tumor efficacy of CAR-T cell treatment.

DOI10.3390/pharmaceutics15102458
Alternate JournalPharmaceutics
PubMed ID37896218
PubMed Central IDPMC10610474
Grant ListERAPERMED2020-342 / / European Council /

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