Selective Uptake Into Inflamed Human Intestinal Tissue and Immune Cell Targeting by Wormlike Polymer Micelles

Author:

Gardey Elena12,Cseresnyes Zoltan3ORCID,Sobotta Fabian H.245ORCID,Eberhardt Juliane24ORCID,Haziri Drilon1,Grunert Philip C.1ORCID,Kuchenbrod Maren T.24,Gruschwitz Franka V.24,Hoeppener Stephanie2ORCID,Schumann Michael6ORCID,Gaßler Nikolaus7,Figge Marc T.38ORCID,Stallmach Andreas12ORCID,Brendel Johannes C.24ORCID

Affiliation:

1. Department of Internal Medicine IV (Gastroenterology Hepatology Infectious Diseases and Central Endoscopy) Jena University Hospital Am Klinikum 1 07747 Jena Germany

2. Jena Center for Soft Matter (JCSM) Friedrich Schiller University Jena Philosophenweg 7 07743 Jena Germany

3. Applied Systems Biology Leibniz Institute for Natural Product Research and Infection Biology Hans Knöll Institute (HKI) Beutenbergstraße 11a 07745 Jena Germany

4. Laboratory of Organic and Macromolecular Chemistry (IOMC) Friedrich Schiller University Jena Humboldtstraße 10 07743 Jena Germany

5. Department of Chemical Engineering and Chemistry & Institute for Complex Molecular Systems Eindhoven University of Technology Eindhoven 5612 AZ the Netherlands

6. Department of Gastroenterology Infectious Diseases and Rheumatology Campus Benjamin Franklin Charité‐University Medicine Hindenburgdamm 30 12200 Berlin Germany

7. Jena University Hospital Section of Pathology Institute of Forensic Medicine Friedrich Schiller University Jena Am Klinikum 1 07747 Jena Germany

8. Institute of Microbiology Faculty of Biological Sciences Friedrich Schiller University Jena Neugasse 25 07743 Jena Germany

Abstract

AbstractInflammatory bowel disease (IBD) has become a globally prevalent chronic disease with no causal therapeutic options. Targeted drug delivery systems with selectivity for inflamed areas in the gastrointestinal tract promise to reduce severe drug‐related side effects. By creating three distinct nanostructures (vesicles, spherical, and wormlike micelles) from the same amphiphilic block copolymer poly(butyl acrylate)‐block‐poly(ethylene oxide) (PBA‐b‐PEO), the effect of nanoparticle shape on human mucosal penetration is systematically identified. An Ussing chamber technique is established to perform the ex vivo experiments on human colonic biopsies, demonstrating that the shape of polymeric nanostructures represents a rarely addressed key to tissue selectivity required for efficient IBD treatment. Wormlike micelles specifically enter inflamed mucosa from patients with IBD, but no significant uptake is observed in healthy tissue. Spheres (≈25 nm) and vesicles (≈120 nm) enter either both normal and inflamed tissue types or do not penetrate any tissue. According to quantitative image analysis, the wormlike nanoparticles localize mainly within immune cells, facilitating specific targeting, which is crucial for further increasing the efficacy of IBD treatment. These findings therefore demonstrate the untapped potential of wormlike nanoparticles not only to selectively target the inflamed human mucosa, but also to target key pro‐inflammatory cells.

Publisher

Wiley

Subject

Biomaterials,Biotechnology,General Materials Science,General Chemistry

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