2020
DOI: 10.3390/ijms21218320
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Hypoxic Regulation of Gene Transcription and Chromatin: Cause and Effect

Abstract: Cellular responses to low oxygen (hypoxia) are fundamental to normal physiology and to the pathology of many common diseases. Hypoxia-inducible factor (HIF) is central to this by enhancing the transcriptional activity of many hundreds of genes. The cellular response to HIF is cell-type-specific and is largely governed by the pre-existing epigenetic landscape. Prior to activation, HIF-binding sites and the promoters of HIF-target genes are already accessible, in contact with each other through chromatin looping… Show more

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Cited by 36 publications
(27 citation statements)
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References 144 publications
(257 reference statements)
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“…Several bHLH factors, such as USF1/2 [213], TCF3 (in B cells) [213], yeast Pho4 [214], HIF1A-ARNT [215], and MYC [138,142,216] among others, have shown to preferentially target accessible chromatin. This preference for open chromatin is particularly evident when comparing binding of TFs across different cell types.…”
Section: Chromatin Accessibility and Pioneer Factorsmentioning
confidence: 99%
See 1 more Smart Citation
“…Several bHLH factors, such as USF1/2 [213], TCF3 (in B cells) [213], yeast Pho4 [214], HIF1A-ARNT [215], and MYC [138,142,216] among others, have shown to preferentially target accessible chromatin. This preference for open chromatin is particularly evident when comparing binding of TFs across different cell types.…”
Section: Chromatin Accessibility and Pioneer Factorsmentioning
confidence: 99%
“…Cytosines in CpG sites frequently present a methyl group bound to their 5th position, which can be progressively oxidized to 5-hydroximethylcythosine (5hmC), then 5-formylcytosine (5fC), and then be subsequently transformed into 5-carboxylcytosine (5caC) [230]. Symmetrical methylation of the central CpG of E-boxes has shown to prevent Myc-Max, Max-Max and HIF1A-ARNT binding to DNA [215,[231][232][233]. In the case of Max homodimers, and oxidation to a 5caC restores the affinity to the level of the unmodified cytosine [233].…”
Section: Dna Modificationsmentioning
confidence: 99%
“…Ключевым патофизиологическим компонентом ИМ является гипоксия, которая активирует сигнальный путь HIF [36] и запускает широкий спектр клеточных реакций, включая регуляцию экспрессии генов и посттрансляционные модификации белков. Для изучения влияния тканевой гипоксии на активность клеток эпикарда были исследованы срезы сердец животных, полученных после моделирования ИМ.…”
Section: результатыunclassified
“…In addition, PAM is among the top 176 human genes identified by both HIF1A-ChIP-seq and HIF2A/EPAS1-ChIPseq (Bono & Hirota, 2020). Based on multiple studies, a consensus hypoxia response element (HRE) has been defined (Figure 8a; Dengler et al, 2014;Kaelin et al, 2016;Kindrick & Mole, 2020; F I G U R E 8 Identification of putative hypoxia-response elements (HREs) in the human and mouse PAM genes. (a) The consensus HRE sequence is VBRCGTG where R═A or G; B═C, G or T; V═C, G or A (Dengler et al, 2014;Kindrick & Mole, 2020;Wenger et al, 2005).…”
Section: Pam Is a Hif-responsive Genementioning
confidence: 99%
“…. Functional HREs are most commonly found in the proximal 2 kb of the 5ʹ-flanking region, with some within a few nucleotides (nts) of the transcriptional initiation site, but are also found in 5ʹ-untranslated regions (UTRs), nearby intervening sequences and distant 3ʹ-UTRs (Kindrick & Mole, 2020;Wenger et 2005). Consistent with this, three of the five putative HREs identified in hPAM are in its 5ʹ-UTR, with two of the putative sites in the upstream genomic region (Figure 8b).…”
Section: Acknowledgmentsmentioning
confidence: 99%