MANNosylation of Mesoporous Silica Nanoparticles Modifies TLR4 Localization and NF‐κB Translocation in T24 Bladder Cancer Cells

Author:

Hohagen Mariam1ORCID,Sánchez Laura2,Herbst Ann‐Jacqueline13,Kählig Hanspeter4,Shin Jae Won5,Berry David2,Del Favero Giorgia67ORCID,Kleitz Freddy1ORCID

Affiliation:

1. Department of Functional Materials and Catalysis Faculty of Chemistry University of Vienna Währinger Straße 42 Vienna 1090 Austria

2. Division of Microbial Ecology Department of Microbiology and Ecosystem Science Centre for Microbiology and Environmental Systems Science University of Vienna Djerassiplatz 1 Vienna 1030 Austria

3. Vienna Doctoral School in Chemistry (DoSChem) University of Vienna Währinger Str. 42 Vienna 1090 Austria

4. Department of Organic Chemistry Faculty of Chemistry University of Vienna Währinger Straße 38 Vienna 1090 Austria

5. Center for Nanomaterials and Chemical Reactions Institute for Basic Science (IBS) Daejeon 34141 Republic of Korea

6. Core Facility Multimodal Imaging Faculty of Chemistry University of Vienna Währinger Straße 42 Vienna 1090 Austria

7. Department of Food Chemistry and Toxicology Faculty of Chemistry University of Vienna Währinger Straße 38–40 Vienna 1090 Austria

Abstract

AbstractD‐mannose is widely used as non‐antibiotic treatment for bacterial urinary tract infections. This application is based on a well‐studied mechanism of binding to the type 1 bacterial pili and, therefore, blocking bacteria adhesion to the uroepithelial cells. To implement D‐mannose into carrier systems, the mechanism of action of the sugar in the bladder environment is also relevant and requires investigation. Herein, two different MANNosylation strategies using mesoporous silica nanoparticles (MSNs) are described. The impact of different chemical linkers on bacterial adhesion and bladder cell response is studied via confocal microscopy imaging of the MSN interactions with the respective organisms. Cytotoxicity is assessed and the expression of Toll‐like receptor 4 (TLR4) and caveolin‐1 (CAV‐1), in the presence or absence of simulated infection with bacterial lipopolysaccharide (LPS), is evaluated using the human urinary bladder cancer cell line T24. Further, localisation of the transcription factor NF‐κB due to the MANNosylated materials is examined over time. The results show that MANNosylation modifies bacterial adhesion to the nanomaterials and significantly affects TLR4, caveolin‐1, and NF‐κB in bladder cells. These elements are essential components of the inflammatory cascade/pathogens response during urinary tract infections. These findings demonstrate that MANNosylation is a versatile tool to design hybrid nanocarriers for targeted biomedical applications.

Funder

Universität Wien

Institute for Basic Science

Publisher

Wiley

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