EP300-HDAC1-SWI/SNF functional unit defines transcription of some DNA repair enzymes during differentiation of human macrophages

“…In the current study, we show that BRG1 binding occurs at the promoters of functionally linked genes in proliferating breast cancer cells, revealing a new mechanism by which BRG1 defines gene transcription.Cancers 2020, 12, 349 2 of 17 with the proliferative status of the tumors [2]. Once again, direct molecular and mechanistical mutual interdependence has not been forthcoming.Our recently published results provide evidence that transcription of some of DNA repair genes, such as PARP1, BRCA1, and XRCC1, is controlled by SWI/SNF in a cell cycle-dependent manner [3]. In our model of monocyte-to-macrophage differentiation promoters of DNA repair genes, characterized by the presence of CpG island and E2F motifs, were enriched in SWI/SNF-EP300-HDAC1 complexes.…”

“…Our recently published results provide evidence that transcription of some of DNA repair genes, such as PARP1, BRCA1, and XRCC1, is controlled by SWI/SNF in a cell cycle-dependent manner [3]. In our model of monocyte-to-macrophage differentiation promoters of DNA repair genes, characterized by the presence of CpG island and E2F motifs, were enriched in SWI/SNF-EP300-HDAC1 complexes.…”

“…Lack of reciprocity between enzyme and H3, as well as weak negative co-occurrence with H3K27me3, seem to further confirm a previously postulated mechanism, where BRG1 evicted histones from transcriptionally permissive promoters and enabled gene expression. In human macrophages, BRG1/H3K27ac-positive promoters are characterized by binding motif for E2F (indicative of likely gene dependence on cell cycle status) and/or the CpG island [3]. To test whether distribution of BRG1 is associated with similar chromatin and DNA features in proliferating breast cancer cells, MDA-MB-231, we looked for overlapping regions adjacent to TSS (±2 kbp), which are characterized by the occurrence of BRG1, H3K27ac, E2F motifs, and CpG islands.…”

“…Cell cycle progression in MCF7 and MDA-MB-231 cells treated with iCDK4/6, iEP300 and iSWI/SNF for 48 h was analyzed by flow cytometry as described previously [3]. Additionally, protein level of Ki67, PCNA and CCNB was monitored in cell lysates by western blot.…”

BRG1 Activates Proliferation and Transcription of Cell Cycle-Dependent Genes in Breast Cancer Cells

“…In the current study, we show that BRG1 binding occurs at the promoters of functionally linked genes in proliferating breast cancer cells, revealing a new mechanism by which BRG1 defines gene transcription.Cancers 2020, 12, 349 2 of 17 with the proliferative status of the tumors [2]. Once again, direct molecular and mechanistical mutual interdependence has not been forthcoming.Our recently published results provide evidence that transcription of some of DNA repair genes, such as PARP1, BRCA1, and XRCC1, is controlled by SWI/SNF in a cell cycle-dependent manner [3]. In our model of monocyte-to-macrophage differentiation promoters of DNA repair genes, characterized by the presence of CpG island and E2F motifs, were enriched in SWI/SNF-EP300-HDAC1 complexes.…”

“…Our recently published results provide evidence that transcription of some of DNA repair genes, such as PARP1, BRCA1, and XRCC1, is controlled by SWI/SNF in a cell cycle-dependent manner [3]. In our model of monocyte-to-macrophage differentiation promoters of DNA repair genes, characterized by the presence of CpG island and E2F motifs, were enriched in SWI/SNF-EP300-HDAC1 complexes.…”

“…Lack of reciprocity between enzyme and H3, as well as weak negative co-occurrence with H3K27me3, seem to further confirm a previously postulated mechanism, where BRG1 evicted histones from transcriptionally permissive promoters and enabled gene expression. In human macrophages, BRG1/H3K27ac-positive promoters are characterized by binding motif for E2F (indicative of likely gene dependence on cell cycle status) and/or the CpG island [3]. To test whether distribution of BRG1 is associated with similar chromatin and DNA features in proliferating breast cancer cells, MDA-MB-231, we looked for overlapping regions adjacent to TSS (±2 kbp), which are characterized by the occurrence of BRG1, H3K27ac, E2F motifs, and CpG islands.…”

“…Cell cycle progression in MCF7 and MDA-MB-231 cells treated with iCDK4/6, iEP300 and iSWI/SNF for 48 h was analyzed by flow cytometry as described previously [3]. Additionally, protein level of Ki67, PCNA and CCNB was monitored in cell lysates by western blot.…”

BRG1 Activates Proliferation and Transcription of Cell Cycle-Dependent Genes in Breast Cancer Cells

“…W połowie tych regionów zidentyfikowano ponadto motyw dla wiązania czynników transkrypcyjnych z rodziny E2F, które łączą aktywność transkrypcyjną genu ze statusem proliferacji komórek. W ludzkich makrofagach oraz komórkach nowotworu piersi dla CpG/E2F-dodatnich promotorów funkcjonalnie powiązanych genów opisano nową jednostkę regulatorową, w skład której wchodzi kompleks SWI/SNF oparty na aktywności BRG1 oraz enzymy -acetylotransferaza EP300 i deacetylaza HDAC1 kontrolujące stopień acetylacji histonów [10,11]. Pierwszy z nich acetyluje reszty histonowe, które w formie zmienionej zostają rozpoznane przez BRG1.…”

Udział kompleksów SWI/SNF opartych na aktywności BRG1 w determinowaniu fenotypu komórek nowotworowych

TRIM25-mediated XRCC1 ubiquitination accelerates atherosclerosis by inducing macrophage M1 polarization and programmed death