Loss of Gcn5l2 leads to increased apoptosis and mesodermal defects during mouse development
Histone acetyltransferases regulate transcription, but little is known about the role of these enzymes in developmental processes. Gcn5 (encoded by Gcn5l2 ) and Pcaf, mouse histone acetyltransferases, share similar sequences and enzymatic activities 1 . Both interact with p300 and CBP (encoded by Ep...
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Veröffentlicht in: | Nature genetics 2000-10, Vol.26 (2), p.229-232 |
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Zusammenfassung: | Histone acetyltransferases regulate transcription, but little is known about the role of these enzymes in developmental processes. Gcn5 (encoded by
Gcn5l2
) and Pcaf, mouse histone acetyltransferases, share similar sequences and enzymatic activities
1
. Both interact with p300 and CBP (encoded by
Ep300
and
Crebbp
, respectively), two other histone acetyltransferases that integrate multiple signalling pathways
1
. Pcaf is thought to participate in many of the cellular processes regulated by p300/CBP (refs
2
–
8
), but the functions of Gcn5 are unknown in mammalian cells. Here we show that the gene
Pcaf
is dispensable in mice. In contrast,
Gcn5l2
-null embryos die during embryogenesis. These embryos develop normally to 7.5 days post coitum (d.p.c.), but their growth is severely retarded by 8.5 d.p.c. and they fail to form dorsal mesoderm lineages, including chordamesoderm and paraxial mesoderm. Differentiation of extra-embryonic and cardiac mesoderm seems to be unaffected. Loss of the dorsal mesoderm lineages is due to a high incidence of apoptosis in the
Gcn5l2
mutants that begins before the onset of morphological abnormality. Embryos null for both
Gcn5l2
and
Pcaf
show even more severe defects, indicating that these histone acetyltransferases have overlapping functions during embryogenesis. Our studies are the first to demonstrate that specific acetyltransferases are required for cell survival and mesoderm formation during mammalian development. |
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ISSN: | 1061-4036 1546-1718 |
DOI: | 10.1038/79973 |