The fibronectin type-III (FNIII) domain of ATF7IP contributes to efficient transcriptional silencing mediated by the SETDB1 complex

Tsusaka, Takeshi; Fukuda, Kei; Shimura, Chikako; Kato, Masaki; Shinkai, Yoichi

doi:10.1186/s13072-020-00374-4

Cited by 14 publications

(19 citation statements)

References 38 publications

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“…Consistent with a direct role for MGA/MAX-mediated SETDB1 recruitment, MAX was recently shown to interact with SETDB1 via co-immunoprecipitation, and Ddx4 and Dazl promoters showed reduced H3K9me3 in Max KD pESCs 29 . However, a recent study suggests that SETDB1 may indirectly interact with PRC1.6, via its known binding partner ATF7IP 93 . ATF7IP contains a C-terminal fibronectin type-III (FNIII) domain, which was shown to interact with MGA in pESCs via mass spectrometry.…”

Section: Discussionmentioning

confidence: 99%

Repression of germline genes by PRC1.6 and SETDB1 in the early embryo precedes DNA methylation-mediated silencing

et al. 2021

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Silencing of a subset of germline genes is dependent upon DNA methylation (DNAme) post-implantation. However, these genes are generally hypomethylated in the blastocyst, implicating alternative repressive pathways before implantation. Indeed, in embryonic stem cells (ESCs), an overlapping set of genes, including germline “genome-defence” (GGD) genes, are upregulated following deletion of the H3K9 methyltransferase SETDB1 or subunits of the non-canonical PRC1 complex PRC1.6. Here, we show that in pre-implantation embryos and naïve ESCs (nESCs), hypomethylated promoters of germline genes bound by the PRC1.6 DNA-binding subunits MGA/MAX/E2F6 are enriched for RING1B-dependent H2AK119ub1 and H3K9me3. Accordingly, repression of these genes in nESCs shows a greater dependence on PRC1.6 than DNAme. In contrast, GGD genes are hypermethylated in epiblast-like cells (EpiLCs) and their silencing is dependent upon SETDB1, PRC1.6/RING1B and DNAme, with H3K9me3 and DNAme establishment dependent upon MGA binding. Thus, GGD genes are initially repressed by PRC1.6, with DNAme subsequently engaged in post-implantation embryos.

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Section: Discussionmentioning

confidence: 99%

Repression of germline genes by PRC1.6 and SETDB1 in the early embryo precedes DNA methylation-mediated silencing

et al. 2021

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“…Recently, the location of SETDB1 inside the nucleus was discovered to be mediated by ATF7IP, which increases the ubiquitination of SETDB1 to promote its enzymatic activity [ 84 , 85 , 86 ]. The fibronectin type-III (FNIII) domain of ATF7IP plays a certain role in the transcriptional repression function mediated by the SETDB1-ATF7IP complex.…”

Section: Biological Functions Of Setdb1mentioning

confidence: 99%

“…The fibronectin type-III (FNIII) domain of ATF7IP plays a certain role in the transcriptional repression function mediated by the SETDB1-ATF7IP complex. However, the FNIII domain seems to be unrelated to the nuclear localization of SETDB1 and to the ATF7IP-dependent integrated retroviral transgenes silencing [ 86 ]. Above all, by alternating the conformation of the X chromosome through SETDB1-ATF7IP-MBD1 complex, SETDB1 also plays an important role in XCI.…”

Section: Biological Functions Of Setdb1mentioning

confidence: 99%

The Updating of Biological Functions of Methyltransferase SETDB1 and Its Relevance in Lung Cancer and Mesothelioma

Sun

et al. 2021

IJMS

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SET domain bifurcated 1 (SETDB1) is a histone H3 lysine 9 (H3K9) methyltransferase that exerts important effects on epigenetic gene regulation. SETDB1 complexes (SETDB1-KRAB-KAP1, SETDB1-DNMT3A, SETDB1-PML, SETDB1-ATF7IP-MBD1) play crucial roles in the processes of histone methylation, transcriptional suppression and chromatin remodelling. Therefore, aberrant trimethylation at H3K9 due to amplification, mutation or deletion of SETDB1 may lead to transcriptional repression of various tumour-suppressing genes and other related genes in cancer cells. Lung cancer is the most common type of cancer worldwide in which SETDB1 amplification and H3K9 hypermethylation have been indicated as potential tumourigenesis markers. In contrast, frequent inactivation mutations of SETDB1 have been revealed in mesothelioma, an asbestos-associated, locally aggressive, highly lethal, and notoriously chemotherapy-resistant cancer. Above all, the different statuses of SETDB1 indicate that it may have different biological functions and be a potential diagnostic biomarker and therapeutic target in lung cancer and mesothelioma.

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Section: Accepted Manuscriptmentioning

confidence: 99%

“…One of the partners of ATF7IP is the histone methyltransferase SETDB1, a repressor of proinflammatory cytokine expression in macrophages. 43,44 Phospholipase B domain containing 1 (PLBD1) was first identified as a neutrophil phospholipase B precursor potentially involved in proinflammatory lipid release. 45 Accordingly, PLBD1 expression is increased in a variety of inflammatory conditions.…”

Section: Whole-exome Sequencing-based Overall Variant Callingmentioning

confidence: 99%

Somatic Genetic Mosaicism in the Apolipoprotein E-null Mouse Aorta

et al. 2021

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In addition to genetic and epigenetic inheritance, somatic variation may contribute to cardiovascular disease (CVD) risk. CVD-associated somatic mutations have been reported in human clonal haematopoiesis, but evidence in the atheroma is lacking. To probe for somatic variation in atherosclerosis, we sought single-nucleotide private variants (PVs) in whole-exome sequencing (WES) data of aorta, liver and skeletal muscle of two C57BL/6J coisogenic male ApoE-null/WT sibling pairs, and RNA-seq data of one of the two pairs. Relative to the C57BL/6 reference genome, we identified 9 and 11 ApoE-null aorta- and liver-specific PVs that were shared by all WES and RNA-seq data sets. Corresponding PVs in WT sibling aorta and liver were 1 and 0, respectively, and not overlapping with ApoE-null PVs. Pyrosequencing analysis of 4 representative PVs in 17 ApoE-null aortas and livers confirmed tissue-specific shifts towards the alternative allele, in addition to significant deviations from Mendelian allele ratios. Notably, all aorta and liver PVs were present in the dbSNP database and were predominantly transition mutations within atherosclerosis-related genes. The majority of PVs were in discrete clusters ~3 Mb and 65-73 Mb away from hypermutable immunoglobin loci in chromosome 6. These features were largely shared with previously reported CVD-associated somatic mutations in human clonal haematopoiesis. The observation that SNPs exhibit tissue-specific somatic DNA mosaicism in ApoE-null mice is potentially relevant for genetic association study design. The proximity of PVs to hypermutable loci suggests testable mechanistic hypotheses.

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The fibronectin type-III (FNIII) domain of ATF7IP contributes to efficient transcriptional silencing mediated by the SETDB1 complex

Cited by 14 publications

References 38 publications

Repression of germline genes by PRC1.6 and SETDB1 in the early embryo precedes DNA methylation-mediated silencing

Repression of germline genes by PRC1.6 and SETDB1 in the early embryo precedes DNA methylation-mediated silencing

The Updating of Biological Functions of Methyltransferase SETDB1 and Its Relevance in Lung Cancer and Mesothelioma

Somatic Genetic Mosaicism in the Apolipoprotein E-null Mouse Aorta

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