A cis-acting control region is required exclusively for the tissue-specific imprinting of Gnas
Genomic imprinting brings about allele-specific silencing according to parental origin 1 . Silencing is controlled by cis -acting regulatory regions that are differentially marked during gametogenesis and can act over hundreds of kilobases to silence many genes 2 , 3 , 4 , 5 , 6 . Two candidate impr...
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Veröffentlicht in: | Nature genetics 2004-08, Vol.36 (8), p.894-899 |
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Zusammenfassung: | Genomic imprinting brings about allele-specific silencing according to parental origin
1
. Silencing is controlled by
cis
-acting regulatory regions that are differentially marked during gametogenesis and can act over hundreds of kilobases to silence many genes
2
,
3
,
4
,
5
,
6
. Two candidate imprinting control regions (ICRs) have been identified at the compact imprinted
Gnas
cluster on distal mouse chromosome 2, one at exon 1A upstream of
Gnas
itself
7
and one covering the promoters for
Gnasxl
and the antisense
Nespas
(ref.
8
). This imprinted cluster is complex, containing biallelic, maternally and paternally expressed transcripts that share exons
9
.
Gnas
itself is mainly biallelically expressed but is weakly paternally repressed in specific tissues
10
. Here we show that a paternally derived targeted deletion of the germline differentially methylated region at exon 1A abolishes tissue-specific imprinting of
Gnas
. This rescues the abnormal phenotype of mice with a maternally derived
Gnas
mutation
11
,
12
. Imprinting of alternative transcripts,
Nesp
,
Gnasxl
and
Nespas
(ref.
13
), in the cluster is unaffected. The results establish that the differentially methylated region at exon 1A contains an imprinting control element that specifically regulates
Gnas
and comprises a characterized ICR for a gene that is only weakly imprinted in a minority of tissues. There must be a second ICR regulating the alternative transcripts. |
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ISSN: | 1061-4036 1546-1718 |
DOI: | 10.1038/ng1398 |