Essential and redundant functions of histone acetylation revealed by mutation of target lysines and loss of the Gcn5p acetyltransferase

Zhang, Wenzheng; Bone, James R.; Edmondson, Diane G.; Turner, Bryan M.; Roth, Sharon Y.

doi:10.1093/emboj/17.11.3155

Cited by 297 publications

(294 citation statements)

References 46 publications

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“…4D). Of interest, we previously determined that gcn5⌬ yeast cells accumulate in G2/M phase (Zhang et al, 1998). Together, these results indicate that Gcn5 is required for efficient mitotic progression.…”

Section: Gcn5 Is Not Required For Embryoid Body Formationmentioning

confidence: 80%

Developmental potential of Gcn5^−/− embryonic stem cells in vivo and in vitro

Lin

Srajer

Evrard

et al. 2007

Developmental Dynamics

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Gcn5 is a prototypical histone acetyltransferase (HAT) that serves as a coactivator for multiple DNA-bound transcription factors. We previously determined that deletion of Gcn512 (hereafter referred to as Gcn5) causes embryonic lethality in mice. Gcn5 null embryos undergo gastrulation but exhibit high levels of apoptosis, leading to loss of mesodermal lineages. To further define the functions of Gcn5 during development, we created Gcn5 ؊/؊ mouse embryonic stem (ES) cells. These cells survived in vitro and formed embryoid bodies (EBs) that expressed markers for ectodermal, mesodermal, and endodermal lineages.

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Section: Gcn5 Is Not Required For Embryoid Body Formationmentioning

confidence: 80%

Developmental potential of Gcn5^−/− embryonic stem cells in vivo and in vitro

Lin

Srajer

Evrard

et al. 2007

Developmental Dynamics

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“…YKY64 was generated by first transforming pHHF2-HHT2VSVx3 into the histone shuffle strain WZY42 (38) and selecting on 5-FOA-containing plates for cells that lost the original URA3 plasmid encoding H3 and H4. A second plasmid p316H4H3-HAx2 was then transformed to produce the final strain.…”

Section: Methodsmentioning

confidence: 99%

Splitting of H3–H4 tetramers at transcriptionally active genes undergoing dynamic histone exchange

Katan-Khaykovich

Struhl

2011

Proc. Natl. Acad. Sci. U.S.A.

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Nucleosome deposition occurs on newly synthesized DNA during DNA replication and on transcriptionally active genes via nucleosome-remodeling complexes recruited by activator proteins and elongating RNA polymerase II. It has been long believed that histone deposition involves stable H3-H4 tetramers, such that newly deposited nucleosomes do not contain H3 and H4 molecules with their associated histone modifications from preexisting nucleosomes. However, biochemical analyses and recent experiments in mammalian cells have raised the idea that preexisting H3-H4 tetramers might split into dimers, resulting in mixed nucleosomes composed of "old" and "new" histones. It is unknown to what extent different genomic loci might utilize such a mechanism and under which circumstances. Here, we address whether tetramer splitting occurs in a locus-specific manner by using sequential chromatin immunoprecipitation of mononucleosomes from yeast cells containing two differentially tagged versions of H3 that are expressed "old" and "new" histones. At many genomic loci, we observe little or no nucleosomal cooccupancy of old and new H3, indicating that tetramer splitting is generally infrequent. However, cooccupancy is detected at highly active genes, which have a high rate of histone exchange. Thus, DNA replication largely results in nucleosomes bearing exclusively old or new H3-H4, thereby precluding the acquisition of new histone modifications based on preexisting modifications within the same nucleosome. In contrast, tetramer splitting, dimer exchange, and nucleosomes with mixed H3-H4 tetramers occur at highly active genes, presumably linked to rapid histone exchange associated with robust transcription.T he packaging of eukaryotic DNA into chromatin influences many DNA-associated processes, including transcriptional regulation. Within the chromatin fiber, each basic nucleosome unit bears important chemical and structural information. The mechanisms by which nucleosomes are assembled on DNA during replication, transcription, DNA repair, etc., can thus impact not only the integrity of chromatin structure but also patterns of gene expression and epigenetic inheritance. The H3-H4 tetramer core of each nucleosome is the more stable component and contains most of the relatively persistent and functionally important histone methylation marks. Much attention has therefore been given to the questions of how the H3-H4 tetramers are formed and maintained on chromatin.Early studies attempted to distinguish between a conservative assembly model, by which old and new histones form separate tetramers on replicating DNA, and a semiconservative assembly mechanism, by which existing tetramers are split into H3-H4 dimers, followed by association of new H3-H4 dimers to complete each nucleosome core (1-3). In the semiconservative model, the resulting tetramers would bear a mixture of old and new histones, allowing transmission of epigenetic information within the basic nucleosome unit. Though mechanistically attractive, the mixed tetramer model receiv...

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“…Gcn5 Ϫ/Ϫ embryos exhibit a large increase in apoptotic cells as early as E7.5 (Xu et al, 2000), and deletion of Gcn5 in chicken cells (Kikuchi et al, 2005) or yeast (Zhang et al, 1998) leads to defective cell cycle progression. Therefore, we next determined whether neural tube closure defects in the Gcn5 flox(neo)/⌬ mutants might be due to changes in cell proliferation or survival.…”

Section: Cell Death and Cell Proliferation Are Normal In Hypomorphic mentioning

confidence: 99%

“…Immunoblots were performed as described (Lin et al, 2007) using a Gcn5-specific antisera (Abcam) at 1:400 dilution, a H3 K9,18Ac-specific antisera (Zhang et al, 1998) at 1:1,000 dilution, an H3-secific antisera (Abcam) at 1:5,000 dilution, and an actin-specific antibody (Sigma) at 1:4,000 dilution.…”

Section: Immunoblotsmentioning

confidence: 99%

Proper expression of the Gcn5 histone acetyltransferase is required for neural tube closure in mouse embryos

Lin

Zhang

Srajer

et al. 2008

Developmental Dynamics

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Histone acetyltransferases (HATs) are important to gene activation, altering chromatin structures to facilitate association of transcription proteins with gene promoters. The functions of individual HATs in mammalian developmental are not well defined. Our previous studies demonstrated that Gcn5, a prototypical HAT, is required for mesodermal maintenance in early embryos. Homozygous Gcn5 null embryos die soon after gastrulation, preventing determination of Gcn5 functions later during development. We report here the creation of a Gcn5 flox(neo) allele, which is only partially functional and gives rise to a hypomorphic phenotype. Mice homozygous for this allele had an increased risk of cranial neural tube closure defects (NTDs) and exencephaly. These defects were found at an even greater penetrance in

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Essential and redundant functions of histone acetylation revealed by mutation of target lysines and loss of the Gcn5p acetyltransferase

Cited by 297 publications

References 46 publications

Developmental potential of Gcn5^−/− embryonic stem cells in vivo and in vitro

Developmental potential of Gcn5^−/− embryonic stem cells in vivo and in vitro

Splitting of H3–H4 tetramers at transcriptionally active genes undergoing dynamic histone exchange

Proper expression of the Gcn5 histone acetyltransferase is required for neural tube closure in mouse embryos

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Essential and redundant functions of histone acetylation revealed by mutation of target lysines and loss of the Gcn5p acetyltransferase

Cited by 297 publications

References 46 publications

Developmental potential of Gcn5−/− embryonic stem cells in vivo and in vitro

Developmental potential of Gcn5−/− embryonic stem cells in vivo and in vitro

Splitting of H3–H4 tetramers at transcriptionally active genes undergoing dynamic histone exchange

Proper expression of the Gcn5 histone acetyltransferase is required for neural tube closure in mouse embryos

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Developmental potential of Gcn5^−/− embryonic stem cells in vivo and in vitro

Developmental potential of Gcn5^−/− embryonic stem cells in vivo and in vitro