V4C3 MXene Immune Profiling and Modulation of T Cell‐Dendritic Cell Function and Interaction

Author:

Fusco Laura123ORCID,Gazzi Arianna1ORCID,Shuck Christopher E.2ORCID,Orecchioni Marco4ORCID,Ahmed Eiman I3,Giro Linda1,Zavan Barbara56ORCID,Yilmazer Açelya78ORCID,Ley Klaus4ORCID,Bedognetti Davide3910ORCID,Gogotsi Yury2ORCID,Delogu Lucia Gemma111ORCID

Affiliation:

1. ImmuneNano Laboratory Department of Biomedical Sciences University of Padua Padua 35121 Italy

2. A. J. Drexel Nanomaterials Institute and Department of Materials Science and Engineering Drexel University Philadelphia PA 19104 USA

3. Translational Medicine Department Sidra Medicine Doha Qatar

4. La Jolla Institute for Immunology San Diego CA 92037 USA

5. Department of Medical Sciences University of Ferrara Ferrara 44121 Italy

6. Maria Cecilia Hospital GVM Care & Research Ravenna 48033 Italy

7. Stem Cell Institute Ankara University Ankara 06520 Turkey

8. Department of Biomedical Engineering Ankara University Ankara 06830 Turkey

9. Department of Internal Medicine and Medical Specialties University of Genoa Genoa 16132 Italy

10. College of Health and Life Sciences Hamad Bin Khalifa University Doha Qatar

11. New York University Abu Dhabi Abu Dhabi United Arab Emirates

Abstract

AbstractAlthough vanadium‐based metallodrugs are recently explored for their effective anti‐inflammatory activity, they frequently cause undesired side effects. Among 2D nanomaterials, transition metal carbides (MXenes) have received substantial attention for their promise as biomedical platforms. It is hypothesized that vanadium immune properties can be extended to MXene compounds. Therefore, vanadium carbide MXene (V4C3) is synthetized, evaluating its biocompatibility and intrinsic immunomodulatory effects. By combining multiple experimental approaches in vitro and ex vivo on human primary immune cells, MXene effects on hemolysis, apoptosis, necrosis, activation, and cytokine production are investigated. Furthermore, V4C3 ability is demonstrated to inhibit T cell‐dendritic cell interactions, evaluating the modulation of CD40–CD40 ligand interaction, two key costimulatory molecules for immune activation. The material biocompatibility at the single‐cell level on 17 human immune cell subpopulations by single‐cell mass cytometry is confirmed. Finally, the molecular mechanism underlying V4C3 immune modulation is explored, demonstrating a MXene‐mediated downregulation of antigen presentation‐associated genes in primary human immune cells. The findings set the basis for further V4C3 investigation and application as a negative modulator of the immune response in inflammatory and autoimmune diseases.

Publisher

Wiley

Subject

General Materials Science,General Chemistry

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