Scientists discover that long-term regulation of the human genome is much more
dynamic than assumed
Press
Release 6 March 2008 [PDF]
Epigenetic regulation - modifications
to the structure of chromatin that influence which genes
are expressed in a cell - is a key player in embryonic development
and cancer formation. Researchers at the European
Molecular Biology Laboratory [EMBL] in Heidelberg now
gained new insight into one crucial epigenetic mechanism and
reveal that it acts much faster than assumed. In this week's
issue of Nature they report that estrogen causes rapid epigenetic
changes in breast cancer cells. The new findings impact
upon our understanding of how cells interpret their DNA and
suggest that epigenetic regulation can affect gene expression
immediately and long-term.
Epigenetic changes to the structure of chromatin - tightly
packaged DNA - grant or deny access to the molecular
machinery that transcribes DNA and thereby regulate gene
expression. One of these mechanisms is DNA methylation,
where a small chemical residue called a methyl group is added
to strategic bases on the DNA. The methyl group prevents the
transcription machinery from docking and thereby shuts
down gene expression. For a long time scientists have considered
methylation a mechanism of long-term regulation of a
gene's activity, because the methylation marks are stable and
maintained through cellular replication.
EMBL researchers of the group of Frank Gannon, current
director of the Science Foundation Ireland, now found out that
methylation marks occur rapidly in breast cancer cells in
response to hormones such as estrogen or drug compounds.
Estrogen withdrawal or treatment with the established anticancer
drug doxorubicin cause the methyl groups to be
removed from regulatory regions of specific genes within tens
of minutes in human breast cancer cells. The treatment sets off
a whole cycle of events: initial demethylation renders silent
genes active and subsequent remethylation shuts them down
again. This cycle repeats itself every 1.5 hours.
"We observed that unlike assumed for a long time methylation
can act on a very short timescale. The results challenge our
understanding of epigenetics as a means to regulate gene
expression permanently," says Sara Kangaspeska, who carried
out the research together with Brenda Stride.
The new insights into the cyclical nature of methylation might
shed light on the molecular bases of cancer and development,
both processes involving epigenetic mechanisms.
"In particular breast cancer is affected by estrogen signalling
and changes in epigenetic control," says George Reid, co-senior
author of the study. "Our next step will be to find small
molecules that target the cyclical methylation processes to elucidate
their precise role."
Source Article
S. Kangaspeska, B. Stride, R. Métivier, M. Polycarpou-Schwarz, D. Ibberson, R.P. Carmouche, V. Benes, F. Gannon & G. Reid.
Transient cyclical methylation of promoter DNA. Nature, 6 March 2008
Press Contact
Anna-Lynn Wegener
Press Officer
EMBL Heidelberg
Tel: +49 6221 387-8452
Email: wegener@embl.de
|
