Cambridge: Normal skin contains an unexpectedly high number of cancer-associated mutations, according to a study published in Science.
The findings illuminate the first steps cells take towards becoming a
cancer and demonstrate the value of analysing normal tissue to learn
more about the origins of the disease. The
study revealed that each cell in normal facial skin carries many
thousands of mutations, mainly caused by exposure to sunlight. Around
one in four skin cells in samples from people without cancer were found
to carry at least one cancer-associated mutation.
Ultra-deep genetic sequencing was performed on 234 biopsies taken from
four patients revealing 3,760 mutations, with more than 100
cancer-associated mutations per square centimetre of skin. Cells with
these mutations formed clusters of cells, known as clones, that had
grown to be around twice the size of normal clones, but none of them had
become cancerous.
“With this technology, we can now peer into the first steps a cell takes
to become cancerous,” explains Dr Peter Campbell, a corresponding
author from the Wellcome Trust Sanger Institute. “These first
cancer-associated mutations give cells a boost compared to their normal
neighbours. They have a burst of growth that increases the pool of cells
waiting for the next mutation to push them even further. We can even
see some cells in normal skin that have taken two or three such steps
towards cancer. How many of these steps are needed to become fully
cancerous? Maybe five, maybe 10, we don’t know yet.”
The mutations observed showed the patterns associated with the most
common and treatable form of skin cancer linked to sun exposure, known
as cutaneous squamous cell carcinoma, rather than melanoma, a rarer and
sometimes fatal form of skin cancer.
“The burden of mutations observed is high but almost certainly none of
these clones would have developed into skin cancer,” says Dr Iñigo
Martincorena, first author from the Sanger Institute. “Because skin
cancers are so common in the population, it makes sense that individuals
would carry a large number of mutations. What we are seeing here are
the hidden depths of the iceberg, not just the relatively small number
that break through the surface waters to become cancer.”
Skin samples used in this study were taken from four people aged between
55 and 73 who were undergoing routine surgery to remove excess eyelid
skin that was obscuring vision. The mutations had accumulated over each
individual’s lifetime as the eyelids were exposed to sunshine. The
researchers estimate that each sun-exposed skin cell accumulated on
average a new mutation in its genome for nearly every day of life.
“These kinds of mutations accumulate over time – whenever our skin is
exposed to sunlight, we are at risk of adding to them,” explains Dr Phil
Jones, a corresponding author from the Sanger Institute and the MRC
Cancer Unit at the University of Cambridge. “Throughout our lives we
need to protect our skin by using sun-block lotions, staying away from
midday sun and covering exposed skin wherever possible. These
precautions are important at any stage of life but particularly in
children, who are busy growing new skin, and older people, who have
already built up an array of mutations.”
Recent studies analysing blood samples from people who do not have
cancer had revealed a lower burden of mutations, with only a small
percentage of individuals carrying a cancer-causing mutation in their
blood cells. Owing to sun exposure, skin is much more heavily mutated,
with thousands of cancer-associated mutations expected in any adult’s
skin.
The research was primarily supported by the Wellcome Trust, the Medical Research Council, Cancer Research UK and EMBO.
Adapted from a press release from the Wellcome Trust Sanger Institute
Reference
Martincorena I, et al. (2015). High burden and pervasive positive selection of somatic mutations in normal human skin. Science.
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