Scientists generate the most precise map of genetic recombination ever
Press
Release 9 July 2008 [PDF]
Genetic recombination,
the process by which sexually reproducing organisms shuffle
their genetic material when producing germ cells, leads to offspring
with a new genetic make-up and influences the course
of evolution. In the current issue of Nature, researchers at the
European Molecular Biology Laboratory [EMBL] in
Heidelberg, Germany, and the EMBL-European
Bioinformatics Institute [EMBL-EBI] in Hinxton, UK, present
the most precise map of genetic recombination yet. The study
sheds light on fundamental questions about genetic shuffling
and has implications for the tracking of disease genes and their
inheritance.
In order to generate germ cells, sexually reproducing organisms
undergo a complex series of cell divisions [meiosis] that
includes the shuffling of genetic material inherited from the
two parents. Equivalent chromosomes from mother and
father pair up and exchange sections of DNA in a process
called crossover. In a different type of recombination, called
non-crossover, a small piece of DNA is copied from one chromosome
onto the other without reciprocal exchange leading
to gene conversion. Non-crossovers are minute events with a
subtler effect than the exchange of larger fragments, but both
types of recombination can increase genetic diversity and
explain why organisms of the same species differ in many
ways. Both types of recombination can also act to separate the
transmission of neighbouring genes, which are normally
inherited together.
The groups of Lars Steinmetz at EMBL and Wolfgang Huber
at EMBL-EBI have produced the most detailed map to date of
recombination events in the yeast genome.
"Our map has the highest resolution of recombination events
that currently exists for any organism. We can locate
crossovers and even hard-to-trace non-crossovers, typically
with a precision of about 80 bases. This resolution is 20 times
higher than in any existing yeast map and more than 360 times
higher than a recent human map," says Steinmetz.
The map revealed many new insights into the organisation of
recombination in yeast. On average over 150 recombination
events were observed during a typical meiosis. These events
did not occur uniformly across the genome. The recombination
rate varied according to location, with events concentrated
at so-called hotspots, some of which favoured either
crossovers or non-crossovers. The researchers also found evidence
for interference between crossovers and non-crossovers
- a phenomenon previously only known to occur between
crossovers - that makes it unlikely for two recombination
events to happen in close proximity.
The fundamental principles of recombination are likely to be
shared between yeast and humans. "Our map expands our
understanding of crossover and provides a wealth of new
information about non-crossovers and gene conversion. It will
act as a reference for future research into recombination," says
Richard Bourgon from Huber's group, who developed the statistical
methodology for this new type of data.
The insights gained will not only help tackle questions about
the basic mechanisms of recombination; they will also have
practical implications for the tracking of disease genes in
humans.
Source Article
E. Mancera, R. Bourgon, A. Brozzi, W. Huber & L.M. Steinmetz. High-resolution mapping of meiotic crossovers and noncrossovers in yeast. Nature, 9 July 2008
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