First published online July 25, 2008
Development 135, 1601e (2008)
© The Company of Biologists Limited
CTCF gets maternal
Maternal effect genes are transcribed in the oocyte and are essential for
embryonic development. Few are known in mammals, but now Marisa Bartolomei and
co-workers add Ctcf to this short list (see
p. 2729). In
vertebrates, CTCF regulates transcription at genomic loci by binding to
enhancer and insulator sequences. In an earlier study into CTCF binding and
activity at the maternally imprinted H19/Igf2 locus, the Bartolomei
lab generated a transgenic mouse in which growing oocytes are specifically
depleted of CTCF by RNAi. Using microarrays, they have now identified hundreds
of genes that are misregulated in these CTCF-depleted oocytes. Most genes are
downregulated; moreover, downregulated genes occur closer to CTCF-binding
sites. Oocyte CTCF depletion, they report, delays not only meiosis onset but
also the second, post-fertilisation division; it also perturbs zygotic genome
activation, alters nuclear morphology and causes apoptotic early embryonic
death. These abnormalities, further experiments show, are very likely to be a
maternal effect caused by transcriptional, rather than chromatin, defects.
Together, these findings reveal new and independent CTCF functions in oocyte
and embryonic growth.
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Related articles in Development:
- Maternal depletion of CTCF reveals multiple functions during oocyte and preimplantation embryo development
- Le-Ben Wan, Hua Pan, Sridhar Hannenhalli, Yong Cheng, Jun Ma, Andrew Fedoriw, Victor Lobanenkov, Keith E. Latham, Richard M. Schultz, and Marisa S. Bartolomei
Development 2008 135: 2729-2738.
[Abstract]
[Full Text]
