4.6 Article

Magnetic Compression of Tumor Spheroids Increases Cell Proliferation In Vitro and Cancer Progression In Vivo

Journal

CANCERS
Volume 14, Issue 2, Pages -

Publisher

MDPI
DOI: 10.3390/cancers14020366

Keywords

cancer spheroids; forces and cancer; magnetic nanoparticles; magnetic force

Categories

Funding

  1. European Union [MaTissE 648779, NanoBioMade 865629]

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This study demonstrates that anisotropic compression of tumor spheroids enhances cancer cell proliferation and metastasis, with significant increases in cancer index and liver metastasis observed in experimental animals. These findings have important implications for clinical procedures involving tumor compression.
Simple Summary Clinical studies are still debating on the long-term benefits and consequences of endoscopic procedures that expand a stent through a tumor, leading to its compression. Herein, due to the development of magnetic tumor spheroids as magnetically deformable models of a mature tumor, we evidence that anisotropic tumor compression can trigger an increase in vitro of cancer cell proliferation and can induce in vivo amplified malignancy. It confirms other evidence of the impact of a mechanical compression on the metastasis ability and invasion potential of cancer cells. A growing tumor is submitted to ever-evolving mechanical stress. Endoscopic procedures add additional constraints. However, the impact of mechanical forces on cancer progression is still debated. Herein, a set of magnetic methods is proposed to form tumor spheroids and to subject them to remote deformation, mimicking stent-imposed compression. Upon application of a permanent magnet, the magnetic tumor spheroids (formed from colon cancer cells or from glioblastoma cells) are compressed by 50% of their initial diameters. Such significant deformation triggers an increase in the spheroid proliferation for both cell lines, correlated with an increase in the number of proliferating cells toward its center and associated with an overexpression of the matrix metalloproteinase-9 (MMP-9). In vivo peritoneal injection of the spheroids made from colon cancer cells confirmed the increased aggressiveness of the compressed spheroids, with almost a doubling of the peritoneal cancer index (PCI), as compared with non-stimulated spheroids. Moreover, liver metastasis of labeled cells was observed only in animals grafted with stimulated spheroids. Altogether, these results demonstrate that a large compression of tumor spheroids enhances cancer proliferation and metastatic process and could have implications in clinical procedures where tumor compression plays a role.

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