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The latest work on the genetic causes of one of the world’s
biggest killers, coronary artery disease, will be published in the March 2009
issue of Nature Genetics. The research done by teams from the Cardiogenics
consortium used the Enabling Grids for E-sciencE (EGEE) infrastructure. EGEE
manages the world’s largest multi-disciplinary computing grid and enabled the
researchers to do two years’ work in fewer than 45 days. This allowed them to
identify possible genetic candidates for the causes of a disease which kills
over two million people a year in Europe alone.
Coronary artery disease (CAD) is the most common form of heart
disease and is a leading cause of death worldwide. It is one of the root causes
of angina, heart failure and arrhythmias. This work could allow researchers to
better understand why the disease develops and may offer new approaches for
pharmacological prevention and treatment.
“Until recently, we looked at one variation at a time when trying
to find new genes associated with disease”, said David Tregouet, Pierre &
Marie Curie University (UPMC), France. “In this work we are using an original
approach which lets us look at several variations at once. So, instead of
investigating the effect on CAD risk of the 378,000 individual genetic markers
available in this project, more than 8.1 million combinations were tested. We
could do this large number of calculations thanks to EGEE”.
The work was done in three stages to successfully narrow down the
genetic sequences within a person's chromosomes that could make them
susceptible to CAD. In the first stage, almost 8.1 million configurations of
genetic markers were examined and 29 specific combinations were identified as
possibly associated with susceptibility to CAD. Focussing on these 29
combinations, the second stage was able to bring this number down to just one
combination of four genetic markers confirmed to be strongly associated with
the risk of CAD. When these four genetic markers were investigated in
additional studies, covering a total of almost 12,000 individuals, there was a
strong correlation between their presence and the risk of having CAD.
One of the possible explanations behind why these four genetic markers seem to
indicate that a person may be at an increased risk of CAD, is that they overlap
with genes that regulate an enzyme called lipoprotein (a). A raised level of
lipoprotein (a) is used by doctors around the world to diagnose CAD. When the
Cardiogenics consortium compared the levels of the enzyme in one of the
studies, they found that there was a strong correlation between high
lipoprotein levels and the presence of the identified gene sequences.
Notes for Editors
Follow the EGEE User Forum live via GridCast at http://gridtalk-project.blogspot.com/
and Twitter at
http://twitter.com/EnablingGrids.
Photos from the conference will be tagged on Flickr with "egeeuf09."
Press contact: Neasan O’Neil, EGEE Press and Events Manager, +44 (0)79 6281
8712, n.oneill@qmul.ac.uk. For
conference details visit http://egee-uf4.eu-egee.org/
Cardiogenics, an EU-project coordinated in Lübeck, Germany, aims to discover
genetic variations leading to coronary artery disease, to uncover the
underlying disease mechanisms and help to develop new treatments. For more
information see www.cardiogenics.eu.
The Enabling Grids for E-sciencE (EGEE) project is co-funded by the European
Commission. The project aims to provide researchers, in both academia and
industry, with access to major computing resources, independent of their
geographic locations.
EGEE's main aims are:
1. To build a secure, reliable and robust grid infrastructure
2. To supply a computing service for many scientific disciplines
3. To attract, engage and support a wide range of users from science and
industry, and provide them with extensive technical and training support.
For more information see http://www.eu-egee.org
or contact Catherine Gater, EGEE Dissemination, Outreach and
Communications Manager, on + 41 (0)22 767 41 76 or email Catherine.Gater@cern.ch.