Deletion of the H19 differentially methylated domain results in loss of imprinted expression of H19 and Igf2

Thorvaldsen, Joanne L.; Duran, Kristen L.; Bartolomei, Marisa S.

doi:10.1101/gad.12.23.3693

Cited by 612 publications

(556 citation statements)

References 52 publications

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“…CpG islands are normally unmethylated, but allele-specific methylation of CpG islands appears to mark both the inactive X chromosome (Yen et al 1984) and many imprinted genes, for example, H19, Snrpn, and Igf2r (Brandeis et al 1993;Shemer et al 1997;Wutz et al 1997). In addition, GC-rich sequences that are not CpG islands (i.e., they meet the first, but not the second criterion above) may also be differentially methylated (termed a differentially methylated region) in the vicinity of imprinted genes, for example Igf2 (Sullivan et al 1999) and a second site 2-4 kb upstream of the H19 CpG island (Thorvaldsen et al 1998). Therefore, one of our goals was to identify conserved CpG islands and GC-rich sequences that might serve as a substrate for future experiments to investigate allelespecific methylation.…”

Section: A Two-island Rule For Imprinted Genesmentioning

confidence: 99%

“…Thus it is likely that both local and regional cis-acting elements are involved in the regulation of genomic imprinting. However, almost nothing is known about the identity or location of such regulatory elements, with the notable exception of a region that has been intensively studied upstream of and downstream from the H19 gene (Thorvaldsen et al 1998;Bell and Felsenfeld 2000;Hark et al 2000;Srivastava et al 2000).…”

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confidence: 99%

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Sequence and Comparative Analysis of the Mouse 1-Megabase Region Orthologous to the Human 11p15 Imprinted Domain

et al. 2000

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A major barrier to conceptual advances in understanding the mechanisms and regulation of imprinting of a genomic region is our relatively poor understanding of the overall organization of genes and of the potentially important cis-acting regulatory sequences that lie in the nonexonic segments that make up 97% of the genome. Interspecies sequence comparison offers an effective approach to identify sequence from conserved functional elements. In this article we describe the successful use of this approach in comparing a ∼1-Mb imprinted genomic domain on mouse chromosome 7 to its orthologous region on human 11p15.5. Within the region, we identified 112 exons of known genes as well as a novel gene identified uniquely in the mouse region, termed Msuit, that was found to be imprinted. In addition to these coding elements, we identified 33 CpG islands and 49 orthologous nonexonic, nonisland sequences that met our criteria as being conserved, and making up 4.1% of the total sequence. These conserved noncoding sequence elements were generally clustered near imprinted genes and the majority were between Igf2 and H19 or within Kvlqt1.

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Section: A Two-island Rule For Imprinted Genesmentioning

confidence: 99%

mentioning

confidence: 99%

Sequence and Comparative Analysis of the Mouse 1-Megabase Region Orthologous to the Human 11p15 Imprinted Domain

et al. 2000

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“…Particularly, deletion of the H19 ICR resulted in biallelic expression of Igf2 ('loss of imprinting'), when maternally transmitted. (16) Deletion of the KvDMR1 Imprinting control region abrogates imprinting of the paternally repressed genes in this domain, when paternally inherited. This causes growth retardation, which supports the hypothesis that abnormal silencing at CDKN1C and other genes along the domain negatively affects growth.…”

Section: Introductionmentioning

confidence: 99%

Epigenetic deregulation of imprinting in congenital diseases of aberrant growth

2006

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“…The 5 0 region of H19 is methylated only on the paternal allele in both mouse (Bartolomei et al, 1993;Ferguson-Smith et al, 1993) and human (Jinno et al, 1996). This region is regarded as a key domain in the control of imprinting at this locus (Thorvaldsen et al, 1998). The DMR of H19 contains seven potential CTCF-binding sites.…”

Section: Introductionmentioning

confidence: 99%

Erasure of methylation imprint at the promoter and CTCF-binding site upstream of H19 in human testicular germ cell tumors of adolescents indicate their fetal germ cell origin

et al. 2006

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Genome-wide epigenetic modification plays a crucial role in regulating genome functions at critical stages of development. In particular, DNA methylation is known to be reprogrammed on a genome-wide level in germ cells and in preimplantation embryos, although it is relatively stable in somatic cells. In this reprogramming process, the genome becomes demethylated, and methylated de novo during later stages of development. Reprogramming of DNA methylation in male germ cells has not been fully investigated. Testicular germ cell tumors (TGCTs) possess a pluripotential nature and display protean histology from germ cells to embryonal and somatic cell differentiation. These properties make TGCT a unique model for studying germ cell development and gametogenesis in respect of DNA reprogramming. In order to obtain an insight into the epigenetic dynamics of TGCTs, we conducted a comprehensive analysis of differential methylated regions (DMRs) on H19 and IGF2 in TGCTs compared with testicular malignant lymphomas. In the present study, we show that methylation imprint at the promoter and CTCF-binding site upstream of H19 was completely erased in both seiminomatous and nonseminomatous TGCTs, whereas differential methylation was observed in testicular lymphomas. The erasure of methylation imprint was also observed in TGCTs with malignant transformation. We found biallelic unmethylation at the promoter and the CTCF-binding site upstream of H19 is required, but not sufficient for the biallelic expression of H19 in TGCTs. These data suggest that factors other than methylation contribute to transcriptional regulation of imprinted genes in TGCTs. The present data have shown that TGCTs carry distinctive epigenetic profiles at the core-imprinting domain of H19/ IGF2 from other neoplasms of somatic cell origin. The data also suggest that both seminomatous and nonseminomatous TGCTs carry methylation profiles similar to fetal germ cells, but not adult germ cells, indicating the origin of TGCTs as fetal germ cells.

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Deletion of the H19 differentially methylated domain results in loss of imprinted expression of H19 and Igf2

Cited by 612 publications

References 52 publications

Sequence and Comparative Analysis of the Mouse 1-Megabase Region Orthologous to the Human 11p15 Imprinted Domain

Sequence and Comparative Analysis of the Mouse 1-Megabase Region Orthologous to the Human 11p15 Imprinted Domain

Epigenetic deregulation of imprinting in congenital diseases of aberrant growth

Erasure of methylation imprint at the promoter and CTCF-binding site upstream of H19 in human testicular germ cell tumors of adolescents indicate their fetal germ cell origin

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