Breast Tumor Cell Survival and Morphology in a Brain‐like Extracellular Matrix Depends on Matrix Composition and Mechanical Properties

Author:

Türker Esra1,Andrade Mier Mateo S.1,Faber Jessica2,Padilla Padilla Selma J.3,Murenu Nicoletta1,Stahlhut Philipp4,Lang Gregor4,Lamberger Zan4,Weigelt Jeanette4,Schaefer Natascha1,Tessmar Jörg4,Strissel Pamela L.567,Blunk Torsten8,Budday Silvia2,Strick Reiner7,Villmann Carmen1ORCID

Affiliation:

1. Institute for Clinical Neurobiology University Hospital Würzburg Versbacherstr. 5 97078 Würzburg Germany

2. Institute of Continuum Mechanics and Biomechanics FAU Erlangen‐Nürnberg Egerlandstr. 5 91058 Erlangen Germany

3. Department of Biomaterials Engineering Faculty University of Bayreuth Prof.‐Rüdiger‐Bormann‐Straße 1 95447 Bayreuth Germany

4. Department of Functional Materials in Medicine and Dentistry and Bavarian Polymer Institute University Hospital Würzburg Pleicherwall 2 97070 Würzburg Germany

5. Institute of Pathology Krankenhausstrasse 8–10 91054 Erlangen Germany

6. Department of Radiation Oncology University of Maryland School of Medicine Baltimore MD USA

7. University Hospital Erlangen Department of Gynecology and Obstetrics Laboratory for Molecular Medicine FAU Erlangen‐Nürnberg Universitätsstr. 21/23 91054 Erlangen Germany

8. Department of Trauma Hand, Plastic and Reconstructive Surgery University Hospital Würzburg Oberdürrbacherstr. 6 97080 Würzburg Germany

Abstract

AbstractTriple‐negative breast cancer (TNBC) is the most invasive type of breast cancer with high risk of brain metastasis. To better understand interactions between breast tumors with the brain extracellular matrix (ECM), a 3D cell culture model is implemented using a thiolated hyaluronic acid (HA‐SH) based hydrogel. The latter is used as HA represents a major component of brain ECM. Melt‐electrowritten (MEW) scaffolds of box‐ and triangular‐shaped polycaprolactone (PCL) micro‐fibers for hydrogel reinforcement are utilized. Two different molecular weight HA‐SH materials (230 and 420 kDa) are used with elastic moduli of 148 ± 34 Pa (soft) and 1274 ± 440 Pa (stiff). Both hydrogels demonstrate similar porosities. The different molecular weight of HA‐SH, however, significantly changes mechanical properties, e.g., stiffness, nonlinearity, and hysteresis. The breast tumor cell line MDA‐MB‐231 forms mainly multicellular aggregates in both HA‐SH hydrogels but sustains high viability (75%). Supplementation of HA‐SH hydrogels with ECM components does not affect gene expression but improves cell viability and impacts cellular distribution and morphology. The presence of other brain cell types further support numerous cell–cell interactions with tumor cells. In summary, the present 3D cell culture model represents a novel tool establishing a disease cell culture model in a systematic way.

Funder

Deutsche Forschungsgemeinschaft

Publisher

Wiley

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