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Indian Scientist identifies
genetic link to biological ageing in humans
7 February 2010
British
Heart Foundation Professor of Cardiology at the
University of Leicester Professor Nilesh Samani
and his team announced today (7 February 2010) that
they have identified for the first time definitive
variants associated with biological ageing in humans.
The team analyzed more than 500,000 genetic variations
across the entire human genome to identify the variants
which are located near a gene called TERC. The discovery
has important implications for the understanding
of cancer and age associated diseases.
Professor Samani, of the
Department of Cardiovascular Sciences, who co-led
the project explained that there are two forms
of ageing chronological ageing i.e. how
old you are in years and biological ageing whereby
the cells of some individuals are older (or younger)
than suggested by their actual age. He said: There
is accumulating evidence that the risk of age-associated
diseases including heart disease and some types
of cancers are more closely related to biological
rather than chronological age. What we studied
are structures called telomeres which are parts
of ones chromosomes. Individuals are born
with telomeres of certain length and in many cells
telomeres shorten as the cells divide and age.
Telomere length is therefore considered a marker
of biological ageing.
In this study what
we found was that those individuals carrying a
particular genetic variant had shorter telomeres
i.e. looked biologically older. Given the association
of shorter telomeres with age-associated diseases,
the finding raises the question whether individuals
carrying the variant are at greater risk of developing
such diseases
Professor Tim Spector from
Kings College London and director of the
TwinsUK study, who co-led this project, added:
The variants identified lies near a gene
called TERC which is already known to play an
important role in maintaining telomere length.
What our study suggests is that some people are
genetically programmed to age at a faster rate.
The effect was quite considerable in those with
the variant, equivalent to between 3-4 years of
biological ageing as measured by telomere
length loss. Alternatively genetically susceptible
people may age even faster when exposed to proven
bad environments for telomeres like
smoking, obesity or lack of exercise and
end up several years biologically older or succumbing
to more age-related diseases.
The study in Nature Genetics
published today by researchers from the University
of Leicester and Kings College London, working
with University of Groningen in the Netherlands,
was funded by The Wellcome Trust and the British
Heart Foundation.
Details of the study, published
online in Nature Genetics on 07 February 2010.
can be found at www.nature.com/naturegenetics
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