DNA methylation and late replication probably aid cell memory, and type I DNA reeling could aid chromosome folding and enhancer function

Riggs, Arthur D.

doi:10.1098/rstb.1990.0012

Cited by 125 publications

(48 citation statements)

References 42 publications

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“…lian development (Riggs 1989}. There is rather convincing evidence that DNA methylation is important for the maintenance of X chromosome inactivation (for review, see Monk 1986; Grant and Chapman 1988;Lyon 1988;Riggs 1990).…”

Section: Pfeifer Et Almentioning

confidence: 99%

“…There is rather convincing evidence that DNA methylation is important for the maintenance of X chromosome inactivation (for review, see Monk 1986; Grant and Chapman 1988;Lyon 1988;Riggs 1990). Some of the critical methylation sites involved in the maintenance of X chromosome inactivation may be found in CpG islands, because sex-specific island methylation is correlated with stability of the inactive state (Kaslow and Migeon 1987;Migeon et al 1989).…”

Section: Pfeifer Et Almentioning

confidence: 99%

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In vivo footprint and methylation analysis by PCR-aided genomic sequencing: comparison of active and inactive X chromosomal DNA at the CpG island and promoter of human PGK-1.

Pfeifer

Tanguay²,

Steigerwald³

et al. 1990

Genes Dev.

240

182

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The promoter region of the X-linked human phosphoglycerate kinase-I [PGK-I) gene is a CpG island, similar to those often found near autosomal genes. We used ligation-mediated polymerase chain reaction (PCR) for a genomie sequencing study in which 450 bp of the human PGK-1 promoter region was analyzed for the presence of in vivo protein footprints and cytosine methylation at all CpG sites. A technique was devised to selectively visualize the DNA of the inactive X chromosome (Xi), even in the presence of the active X chromosome (Xa). We found that the human Xa in both normal male lymphoeytes and hamster-human hybrids is completely unmethylated at all 120 CpG sites. In contrast, 118 of the CpG sites are methylated on the human Xi in hamster-human hybrids. The Xi in normal female lymphoeytes is also highly methylated, but some GCG or CGC trinueleotides partially escape methylation; all other CpGs are fully methylated. In vivo footprinting studies with dimethylsulfate (DMS) revealed eight regions of apparent protein-DNA contacts on the Xa. Four of the footprints contained the consensus sequence of the binding site for transcription factor Spl. The other regions include potential binding sites for transcription factors ATF, NF1, and a CCAAT-binding protein. The Xi did not show any specifically protected sequences, and with the exception of four hyperreaetive sites, the in vivo DMS reactivity profile of Xi DNA was very similar to that of purified, linear Xi DNA. The implications of these findings with regard to the maintenance of methylation-free islands, X chromosome inactivation, and the ehromatin structure of faeultative heteroehromatin are discussed.

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Section: Pfeifer Et Almentioning

confidence: 99%

Section: Pfeifer Et Almentioning

confidence: 99%

In vivo footprint and methylation analysis by PCR-aided genomic sequencing: comparison of active and inactive X chromosomal DNA at the CpG island and promoter of human PGK-1.

Pfeifer

Tanguay²,

Steigerwald³

et al. 1990

Genes Dev.

240

182

View full text Add to dashboard Cite

show abstract

“…Perhaps the higher-order chromatin structure that we have begun to analyze on the Xi can only form in the second half of S phase and, once formed, is stable until the next late S phase. This idea leads to an experimentally testable model for cell memory (Riggs 1990a).…”

Section: The Maintenance Of X Chromosome Inactivation and Chromatin Amentioning

confidence: 99%

“…The stable, somatically heritable maintenance of differentiated states is of central importance for vertebrate development. However, little is known about the required cell memory mechanisms (see Riggs 1989Riggs , 1990a, although methylated CpG sites are somatically heritable entities (Pfeifer et al 1990b) and a strong case can be made for DNA cytosine methylation being involved as an important component of X chromosome inactivation. The transcription start sites for PGK-1 are located near the center of what appears to be a typical CpG-rich island.…”

mentioning

confidence: 99%

Chromatin differences between active and inactive X chromosomes revealed by genomic footprinting of permeabilized cells using DNase I and ligation-mediated PCR.

Pfeifer

Riggs²

1991

Genes Dev.

189

121

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Ligation-mediated polymerase chain reaction (LMPCR) provides adequate sensitivity for nucleotide-level analysis of single-copy genes. Here, we report that chromatin structure can be studied by enzyme treatment of permeabilized cells followed by LMPCR. DNase I treatment of lysolecithin-permeabilized cells was found to give very clear footprints and to show differences between active and inactive X chromosomes (Xa and Xi, respectively 1 at the human X-linked phosphoglycerate kinase (PGK-11 locus. Beginning 380 bp upstream and continuing 70 bp downstream of the major transcription start site of PGK-1, we analyzed both strands of this promoter and CpG island and discovered the following: {1) The transcriptionally active Xa in permeabilized cells has several upstream regions that are almost completely protected on both strands from DNase I nicking. {2) Nuclei isolated in polyamine-containing buffers lack these footprints, suggesting that data from isolated nuclei can be flawed; other buffers are less disruptive. (3) The Xa has no detectable footprints at the transcription start and HIP1 consensus sequence. {4) The heterochromatic and transcriptionally inactive Xi has no footprints but has two regions showing increased DNase I sensitivity at 10-bp intervals, suggesting that the DNA is wrapped on the surface of a particle; one nucleosome-sized particle seems to be positioned over the transcription start site and another is centered -260 bp upstream. (51 Potassium permanganate and micrococcal nuclease {MNase) studies indicate no melted or otherwise unusual DNA structures in the region analyzed, and MNase, unlike restriction endonuclease MspI, does cut within the positioned particles on the Xi. Results are discussed in the context of X chromosome inactivation and the maintenance of protein and DNA methylation differences between euchromatin and facuhative heterochromatin at CpG islands.

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“…DNA methylation: In mammals, DNA methylation is associated with the regulation of gene expression and the maintenance of the differential state in cell lineages [1]. It is also present in other phylogenetic groups such as some invertebrates: sponges, some insects, sea urchins.…”

mentioning

confidence: 99%

DNA repair in sea star asterias rubens: genomic aspects

Leclerc¹

2017

Histol Cytol Embryol

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Both genetic and biochemical approaches have been used, to study the molecular mechanisms, by which damaged DNA is repaired, in a number of species. The fundamental DNA repair pathways have been functionally conserved for the most part among, prokaryotes, lower eukaryotes and higher eukaryotes. The proteins and protein families, involved, in these repair processes, show high degrees of amino-acid sequence conservation. However, there are also a number of cases in which lack of conservation of particular polypeptides may reveal interesting species specific differences in how certain repair functions are performed. These genes are mainly used in cellular response to X-Ray, to gamma radiation, in Vertebrates.It is surprising to find them in an ancestral invertebrate: the sea star Asterias rubens: The enigmatic sea star! Another explication can be done. These genes named : Xrcc6 and Xrrc5 play a role in the immune process in which immune receptor V,D and J,orV and J gene segments, depending on the specific receptor are recombined within a single locus utilizing the conserved heptamer and nonomer recombination signal sequence (RSS) regional genes (V,D,J) used to generate Ig molecules.This last aspect of sea star genomic studies corroborates the existence of the sea star primitive antibody. References1. Riggs AD (1990) DNA methylation and late replication probably aid cell memory, and type I DNA reeling could aid chromosome folding and enhancer function.

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DNA methylation and late replication probably aid cell memory, and type I DNA reeling could aid chromosome folding and enhancer function

Cited by 125 publications

References 42 publications

In vivo footprint and methylation analysis by PCR-aided genomic sequencing: comparison of active and inactive X chromosomal DNA at the CpG island and promoter of human PGK-1.

In vivo footprint and methylation analysis by PCR-aided genomic sequencing: comparison of active and inactive X chromosomal DNA at the CpG island and promoter of human PGK-1.

Chromatin differences between active and inactive X chromosomes revealed by genomic footprinting of permeabilized cells using DNase I and ligation-mediated PCR.

DNA repair in sea star asterias rubens: genomic aspects

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