Genomic and epigenetic characterization of the arsenic-induced oncogenic microRNA-21

Genomic and epigenetic characterization of the arsenic-induced oncogenic microRNA-21

As one of the first identified oncogenic microRNAs, the precise details concerning the transcriptional regulation and function of microRNA-21 (miR-21) are still not completely established. The miR-21 gene is situated on chromosome 17q23.2, positioned at the 3′-UTR of the gene that encodes vacuole me...

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Veröffentlicht in:Environmental pollution (1987) 2024-03, Vol.345, p.123396-123396, Article 123396
Hauptverfasser: Ji, Haoyan, Bi, Zhuoyue, Pawar, Aashna S., Seno, Akimasa, Almutairy, Bandar Saeed, Fu, Yao, Qiu, Yiran, Zhang, Wenxuan, Wang, Ziwei, Thakur, Chitra, Cui, Hongjuan, Yang, Liqun, Chen, Fei
Format: Artikel
Sprache:eng
Schlagworte:
Arsenic
Carcinogenesis
chromatin immunoprecipitation
chromosomes
DNA
Epigenetics
epithelium
genomics
humans
introns
microRNA
miR-21
Nrf2
pollution
Super-enhancer
transcription termination
vacuoles
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Zusammenfassung:As one of the first identified oncogenic microRNAs, the precise details concerning the transcriptional regulation and function of microRNA-21 (miR-21) are still not completely established. The miR-21 gene is situated on chromosome 17q23.2, positioned at the 3′-UTR of the gene that encodes vacuole membrane protein-1 (VMP1). In this current study, we presented evidence indicating that miR-21 possesses its own gene promoter, which can be found in the intron 10 of the VMP1 gene. Chromatin immunoprecipitation followed by global DNA sequencing (ChIP-seq) revealed the presence of a broad H3K4me3 peak spanning the entire gene body of the primary miR-21 and the existence of super-enhancer clusters in the close proximity to both the miR-21 gene promoter and the transcription termination site in arsenic (As3+)-induced cancer stem-like cells (CSCs) and human induced pluripotent stem cells (hiPSCs). In non-transformed human bronchial epithelial cells (BEAS-2B), As3+ treatment enhanced Nrf2 binding to both the host gene VMP1 of miR-21 and the miR-21 gene. Knockout of Nrf2 inhibited both the basal and As3+-induced expressions of miR-21. Furthermore, the As3+-enhanced Nrf2 peaks in ChIP-seq fully overlap with these super-enhancers enriched with H3K4me1 and H3K27ac in the miR-21 gene, suggesting that Nrf2 may coordinate with other transcription factors through the super-enhancers to regulate the expression of miR-21 in cellular response to As3+. These findings demonstrate the unique genetic and epigenetic characteristics of miR-21 and may provide insights into understanding the novel mechanisms linking environmental As3+ exposure and human cancers. [Display omitted] •Pri-miR-21 gene overlaps with VMP1 gene from intron 10 to 3′-UTR.•Pri-miR-21 possesses its own gene promoter regulatable by arsenic.•Super-enhancers were identified on pri-miR-21 gene.•Arsenic-induced miR-21 is Nrf2 as well as ATF3 dependent.•Higher level of miR-21 is associated with poorer survival of the cancer patients.
ISSN:0269-7491
1873-6424
DOI:10.1016/j.envpol.2024.123396