Epigenetic mechanisms underlying the imprinting of the mouse H19 gene.

Bartolomei, Marisa S.; Webber, Andrea L.; Brunkow, Mary E.; Tilghman, Shirley M.

doi:10.1101/gad.7.9.1663

Cited by 456 publications

(341 citation statements)

References 48 publications

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“…In addition, we examined methylation at the imprinted genes H19 (Bartolomei et al, 1993) and Snrpn (Sutcliffe et al, 1994). DNA from control and mutant cerebral cortex showed the expected monoallelic methylation pattern, with roughly half the sequences being heavily methylated (Fig.…”

Section: Cre1 Mutant Micementioning

confidence: 99%

Ablation of de novo DNA methyltransferase Dnmt3a in the nervous system leads to neuromuscular defects and shortened lifespan

Nguyen¹,

Meletis²,

Fu³

et al. 2007

Developmental Dynamics

174

130

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DNA methylation is an epigenetic mechanism involved in gene regulation and implicated in the functioning of the nervous system. The de novo DNA methyltransferase Dnmt3a is expressed in neurons, but its specific role has not been clarified. Dnmt3a is activated around embryonic day 10.5 in mouse neuronal precursor cells and remains active in postmitotic neurons in the adult. We assessed the role of neuronal Dnmt3a by conditional gene targeting. Mice lacking functional Dnmt3a in the nervous system were born healthy, but degenerated in adulthood and died prematurely. Mutant mice were hypoactive, walked abnormally, and underperformed on tests of neuromuscular function and motor coordination. Loss of Dnmt3a also led to fewer motor neurons in the hypoglossal nucleus and more fragmented endplates in neuromuscular junctions of the diaphragm muscle. Our results implicate a role for Dnmt3a in the neuromuscular control of motor movement.

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Section: Cre1 Mutant Micementioning

confidence: 99%

Ablation of de novo DNA methyltransferase Dnmt3a in the nervous system leads to neuromuscular defects and shortened lifespan

Nguyen¹,

Meletis²,

Fu³

et al. 2007

Developmental Dynamics

174

130

View full text Add to dashboard Cite

show abstract

“…The closely linked and reciprocally imprinted mouse H19 gene is methylated specifically on the repressed paternal chro mosome (Bartolomei et al, 1993;Ferguson-Smith et al, 1993;Brandeis et al, 1993;Feil et aL, 1994). In addi tion, tissue-specific méthylation, directly proportional to the transcriptional levels, was found (Feil et al, 1994).…”

Section: Cpg 1 Is Completely Unmethylated On Both Parental Igf2r Allementioning

confidence: 99%

“…At pres ent, the nature of the primary im print and the molecu lar basis by which genes are recognized as paternally or maternally derived are still unknown. First evidence that méthylation plays an important role in genomic im printing came from the observation that many transgenes become hypomethylated after passage through the male germline and hypermethylated after passage through the female germline (Surani et a l,, 1988), Analysis of four imprinted genes in the mouse, H19 (Bartolomei et al, 1993;Ferguson-Smith et a l, 1993;Brandeis et al, 1993;Feil et al, 1994), insulinlike growth factor II {Igf2) (Sasaki et a l, 1992;Bran deis et al, 1993;Feil et al, 1994), Igf2 receptor (Igf2r) (Stôger et a lv 1993), and U2afl-rsl (SP2) (Hatada et al, 1995), has revealed that regions within the gene or adjacent to it are methylated in a parent-specific manner, The mouse Igf2r gene is expressed exclusively from the maternally inherited chromosome in fetal and adult tissues (Barlow et al, 1991), with the exception of the head and the brain, where biallelic expression has been observed (Villar and Pedersen, 1994). During preimplantation development, both maternal and pa ternal Ig f2 r alleles are expressed (Latham et al, 1994;Szabô and Mann, 1995), indicating that silencing of the paternal allele is a secondary event.…”

Section: Introductionmentioning

confidence: 99%

Maternal-Specific Methylation of the HumanIGF2RGene Is Not Accompanied by Allele-Specific Transcription

et al. 1996

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The hum an in su lin -lik e grow th factor type 2 recep tor gen e (IGF2R) is b ia llelica lly expressed in a variety o f fetal and adult tissu es. In contrast, the im printed m ouse Igf2r gen e is exp ressed exclu sively from the ma ternally in h erited chrom osom e. The m ouse gene con tains tw o CpG isla n d s th at are m ethylated in a parentspecific m anner. M éthylation o f th e CpG island in the prom oter region occu rs on th e repressed paternal gene copy. M éthylation of th e CpG island in intron 2 is specific for th e a ctiv e m aternal allele and m ay repre sen t the prim ary im print. H ere, we have analyzed the hum an IGF2R gen e to in v estig a te w hether these m otifs and th eir parent-of-origin-specific epigenetic modifi cation have b een conserved. As in th e mouse, the hu man IGF2R gen e w as found to contain two CpG is lands, one en com p assin g th e transcription start site (CpG 1) and th e oth er in th e second intron (CpG 2). CpG 2 is h yp erm eth ylated on th e m aternal IGF2R al lele. In contrast to th e situ a tio n in th e m ouse, how ever, the hum an CpG 1 is com p letely unm ethylated on both parental chrom osom es, The hum an and m ouse intronic CpG islan d s la ck sign ifican t sequence hom ol ogy* w h ich su g g ests th a t DNA conform ation plays a role in allele-Specific m éthylation.

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“…Maternally expressed H19 is one of the best-characterized imprinted genes. 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).…”

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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Epigenetic mechanisms underlying the imprinting of the mouse H19 gene.

Cited by 456 publications

References 48 publications

Ablation of de novo DNA methyltransferase Dnmt3a in the nervous system leads to neuromuscular defects and shortened lifespan

Ablation of de novo DNA methyltransferase Dnmt3a in the nervous system leads to neuromuscular defects and shortened lifespan

Maternal-Specific Methylation of the HumanIGF2RGene Is Not Accompanied by Allele-Specific Transcription

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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