Beyond the Charge: Interplay of Nanogels’ Functional Group and Zeta‐Potential for Antifungal Drug Delivery to Human Pathogenic Fungus Aspergillus Fumigatus

Author:

Vogel Theresa1,Kohlmann Simon1,Abboud Zahraa2,Thusek Sina2,Fella Franziska1,Teßmar Joerg1ORCID,Sekimizu Kazuhisa3,Miyashita Atsushi4,Beilhack Andreas2ORCID,Groll Jürgen1ORCID,Yu Yidong25ORCID,Albrecht Krystyna1ORCID

Affiliation:

1. Department for Functional Materials in Medicine and Dentistry Institute of Functional Materials and Biofabrication University of Würzburg 97070 Würzburg Germany

2. Department of Internal Medicine II Center for Experimental Molecular Medicine Würzburg University Hospital 97078 Würzburg Germany

3. Endowed Course “Drug Discoveries by Silkworm Models,” Faculty of Pharmaceutical Sciences Teikyo University Tokyo 192‐0395 Japan

4. Institute of Medical Mycology Teikyo University Tokyo 192‐0395 Japan

5. JSPS International Research Fellow Endowed Course “Drug Discoveries by Silkworm Models,” Faculty of Pharmaceutical Sciences Teikyo University Tokyo 192‐0395 Japan

Abstract

AbstractThe ubiquitous mold Aspergillus fumigatus (A. fumigatus) is one of the main fungal pathogens causing invasive infections in immunocompromised humans. Conventional antifungal agents exhibit limited efficacy and often cause severe side effects. Nanoparticle‐based antifungal delivery provides a promising alternative, which can increase local drug concentration; while, mitigating toxicity, thereby enhancing treatment efficacy. Previous research underscores the potential of poly(glycidol)‐based nanogels (NG) with negative surface charge as carriers for delivering antifungals to A. fumigatus hyphae. In this study, NG is tailored with 2‐carboxyethyl acrylate (CEA) or with phosphoric acid 2‐hydroxyethyl acrylate (PHA). It is discovered that quenching with PHA clearly improves the adhesion of NG to hyphal surface and the internalization of NG into the hyphae under protein‐rich conditions, surpassing the outcomes of non‐quenched and CEA‐quenched NG. This enhancement cannot be solely attributed to an increase in negative surface charge but appears to be contingent on the functional group of the quencher. Further, it is demonstrated that itraconazole‐loaded, PHA‐functionalized nanogels (NGxPHA‐ITZ) show lower MIC in vitro and superior therapeutic effect in vivo against A. fumigatus compared to pure itraconazole. This confirms NGxPHA as a promising antifungal delivery system.

Funder

Japan Society for the Promotion of Science

Uehara Memorial Foundation

Bayerisches Staatsministerium für Wissenschaft und Kunst

Deutsche Forschungsgemeinschaft

Publisher

Wiley

Reference70 articles.

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