Study may show way to cancer cure
Scientists who watched tumour cells spread in living mice said on
Sunday they had found a gene signal controlling how cancer cells move,
which could help companies design new drugs to fight the disease.
Scientists working for Cancer Research UK used hi-tech imaging
techniques to watch how breast cancer cells spread in mice. They found
that a genetic signal, known as TGF-beta, was crucial to whether cells
moved as single entities or in clumps.
TGF-beta signalling is only active in singly moving cells, not in
collectively moving cells. And in singly moving cells, the signal is on
when they move and off when they stop in a new place to grow, they
reported in the journal Nature Cell Biology.
"The results helped us to find the set of genes that are behind the
spread of breast cancer - and that the genes need to be first turned on
and then off in order for single cancer cells to be able to relocate,"
said Erik Sahai, head of the tumour cell biology lab at Cancer Research
UK's London institute.
He said several pharmaceutical firms were investigating how to stop
TGF-beta from functioning, but stressed they were "very much in the
development phase".
"As yet there is no new drug in the pipeline," said Sahai, "But
because we now know what these cancer cells are actually doing, it gives
us lots of new ideas about how to stop them."
Cancer
A study published in May 2007 in the Journal of Clinical
Investigation found that treating cancer with surgery, chemotherapy or
radiation raised levels of TGF-beta and could actually cause tumours to
spread.
But as yet, relatively little has been known about how cancer cells
spread through the body because it is very difficult to track them when
they are moving.
"In a medium-sized tumour there could be a billion cells - and only a
small proportion might break away and spread. So it is like trying to
find, and understand, a moving needle in a very big haystack," said
Sahai.
Sahai and his team used two groups of fluorescently labelled breast
cancer cells inside live mice and tracked them with a technique called
multiphoton confocal microscopy.
When the TGF-beta signal was blocked, the tumour spread via clumps of
cells in the lymphatic system - limiting how far it could go, the
researchers said.But cells that could receive the TGF-beta signal moved
as single entities, and the TGF-beta signal was first turned on -
allowing the cells to spread through the blood, and then turned off -
allowing them to grow again in a new location. "It seems they can't
multitask," said Sahai. "They can't move and grow at the same time, they
can only do one or the other."
LONDON, Oct 18 Reuters |
