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Oct 7, 2018
CANCER’s Spread May Depend on Weird, Newfound Fluid Physics, Oct 07, 2018
The spread of tumors and other growing tissues has revealed a whole new type of physics.
In new research, in the journal Nature Physics,
scientists found that living cells transition from 2D sheets to 3D
blobs by a previously unknown process called “active wetting.” And the
physics of active wetting may be able to explain why and how cancers
spread.
“If we could find the way to selectively modify these forces in a
real tumor, which is a very hard task, we could design a treatment to
avoid cancer dissemination,” study co-authors Xavier Trepat, of the
Institute for Bioengineering of Catalonia in Spain, and Carlos
Pérez-González, of the Universidad de La Laguna in Spain, told Live
Science in an email.
Active physics
Any sort of medical application for the findings is a long way off.
Trepat and Pérez-González said that their next steps will involve
delving further into the weird physics of active wetting, about which
little is yet known.
What the researchers have found is based on experiments done in a lab
dish using human breast cancer cells. It all started, Trepat and
Pérez-González said, with an investigation into a protein called
E-cadherin, which provides adhesion between cells. The researchers had
wanted to know how this protein regulates the tension within tissues, or
groups of cells. What they didn’t expect was that the tension within
the tissue could get so high that their sheet of tissue would
spontaneously detach from the collagen-coated gel they were using as a
substrate and retract into a spheroid shape.
“The first time we observed this phenomenon, we were not sure about how or why it was happening,” the researchers told.
The researchers contrasted active wetting with the behavior of
so-called passive fluids, in which there are no living structures to
alter fluid flow. Normally, in passive fluids, a set of physics
equations known as the Navier-Stokes equations dictates the fluid
dynamics. In passive fluids, the transition from 2D sheet to 3D spheroid
is called dewetting. The opposite, a 3D spheroid spreading out into two
dimensions, is called wetting. Whether wetting or dewetting happens is
governed by the surface tension of the interface, the liquid and the gas
involved.)
But as the researchers played with the cancer cells in their
experiment — varying parameters like tissue size and E-cadherin levels —
they found that the cells weren’t behaving like regular fluids do in
passive wetting and dewetting. This is because a number of active
processes, from the contractility of the tissue to the cell-substrate
adhesion, determine if the cells ball up or spread out, the researchers
found.
The transition between the spread-out wetting phase and balled-up
dewetting phase depends on competition between cell-cell forces and
forces that attach the cell to the substrate, the researchers said.
Here, the breast cancer cells are beginning to
detach from the surface to form a spheroid, with actin cytoskeleton
(red) stretching the bonds to the substrate (green).
Cancer transitions
Tissues grow and move in lots of ways, including during normal
development. But the active wetting transition is important, because it
is the key moment that cells go from a contained spherical to a
spreading, flat sheet Trepat and Pérez-González said. In other words,
once circular balls of tumor spread out and attach to a surface the
tumor is able to spread further.
“Our results set up a comprehensive framework to understand which
forces are important for cancer invasion,” the investigators said. Part
of the next phase of work will be to move the studies out of lab dishes
and into living tissue and real tumors, the researchers added.
Biological systems can be hard to fit into classical physics
frameworks, wrote Richard Morris and Alpha Yap in a comment accompanying
the new paper. Morris is a postdoctoral researcher at the Tata
Institute for Fundamental Research in India, and Yap is a cell biologist
at the University of Queensland in Australia. But the new article is a
“valuable step in the right direction” for making physics relevant to
problems of biology, Morris and Yap wrote.
“In this case,” they wrote, “we learn that, whereas ideas from
classical physics can be beneficial in the characterization of
biological systems, the analogy must not be pushed too far, and new
approaches are needed.”
Breast cancer cells attached to a surface coated
with collagen. The tumor contains actin cytoskeleton, or cellular
scaffolding proteins (green), motor proteins known as myosin (red) and
the adhesive protein E-cadherin (blue).
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