Adaptive adhesion systems mediate glioma cell invasion in complex environments

Author:

Gritsenko Pavlo G.1,Friedl Peter123ORCID

Affiliation:

1. Microscopical Imaging of the Cell, Department of Cell Biology, Radboud Institute for Molecular Life Sciences, Radboud University Nijmegen Medical Centre, The Netherlands

2. David H Koch Center for Applied Research of Genitourinary Cancers, Department of Genitourinary Medical Oncology, The University of Texas, MD Anderson Cancer Center, Houston, Texas, USA

3. Cancer Genomics Centre (CGC.nl), 3584 Utrecht, The Netherlands

Abstract

Diffuse brain invasion by glioma cells prevents effective surgical or molecular-targeted therapy and underlies detrimental outcome. Migrating glioma cells are guided by complex anatomical brain structures, however exact mechanisms remain poorly defined. To identify adhesion receptor systems and matrix structures supporting glioma cell invasion into brain-like environments we used 2D and 3D organotypic invasion assays in combination with antibody-, peptide- and RNA-based interference. Combined interference with β1 and αV integrins abolished the migration of U-251 and E-98 glioma cells on reconstituted basement membrane, however invasion into primary brain slices or 3D astrocyte-based scaffolds and migration on astrocyte-deposited matrix was only partly inhibited. Any residual invasion was supported by vascular structures as well as laminin 511, a central constituent of basement membrane of brain blood vessels. Multi-targeted interference against β1, αV and α6 integrins expressed by U-251 and E-98 cells proved insufficient to achieve complete migration arrest. These data suggest that mechanocoupling by integrins are relatively resistant to antibody/peptide based targeting, and cooperates with additional, yet unidentified adhesion systems in mediating glioma cell invasion in complex brain stroma.

Funder

NWO-VICI

FP7 Ideas: European Research Council

NIH

Cancer Genomics Center

Publisher

The Company of Biologists

Subject

Cell Biology

Reference82 articles.

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