Learning how cancer cells coordinate and collaborate to multiply and metastasise

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Cancer cells are known to migrate and collaborate to form networks that function as conduits providing access to nutrients and blood vessels.

Now, researchers in Japan have generated similar large-scale structures from cancer cells in the laboratory and thus gained a better understanding of the underlying forces and their interactions.

Proliferating cells often cooperate in order to form self-beneficial large-scale structures; these include bacterial biofilms, protective epithelial monolayers or even more complex configurations such as endothelial capillaries.

Malignant cells, in a process called vasculogenic mimicry, form structures that facilitate access to nutrients for tumour growth and to blood vessels for metastasis.

The biochemical and biophysical mechanisms are not well understood, as this purposive behaviour was difficult to reproduce experimentally until now.

In a study published in the Biophysical Journal, researchers from Osaka University in collaboration with Advanced ICT Research Institute, the National Institute of Information and Communications Technology (NICT), have demonstrated migration and large-scale structure formation by cancer cells grown on Matrigel substrate, and have developed simple simulated models that reproduce their observations.

The research team first cultured HeLa cells, a strain of epithelial-like cervical cancer cells, on Matrigel, a gelatinous protein mixture resembling the extracellular environment of many tissues, and showed that the cells migrate aggressively and form large-scale structures.

This was previously difficult to achieve in vitro as HeLa cells are relatively non-motile on glass.

Using time-lapse imaging they analysed the cell migration patterns and quantified the large-scale structures with a two-point correlation function.

“We observed that HeLa cells first exhibited increased motility on Matrigel, which later decreased after they integrated into a spatially distinct structure,” explained Dr Tokuko Haraguchi, senior researcher at NICT. “We also noted that HeLa cells in close proximity formed bridges between cell aggregates, and that structures were formed in a cell-density dependent manner.”

To explain these results, the researchers developed a simulated model in which cells migrate and interact using two distinct forces: remote forces that act at a distance through substrate deformation, and contact forces between cells in physical proximity.

By selectively enabling these forces, they modelled the three types of structures formed – islands, network-like structures and continents–according to cell density.

Tadashi Nakano, lead author, explained the potential implications of their findings: “Cancer cells may rely on vasculogenic mimicry for survival and proliferation,” he said. “A complete understanding of this process can, by manipulation of the relevant cell density and force parameters, inhibit these network-like structures. This may have great potential for combating cancer.”

Source: Osaka University


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The ONA Editor curates oncology news, views and reviews from Australia and around the world for our readers. In aggregated content, original sources will be acknowledged in the article footer.

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