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Publication : Fetal γ-globin genes are regulated by the <i>BGLT3</i> long noncoding RNA locus.

First Author  Ivaldi MS Year  2018
Journal  Blood Volume  132
Issue  18 Pages  1963-1973
PubMed ID  30150205 Mgi Jnum  J:269927
Mgi Id  MGI:6273046 Doi  10.1182/blood-2018-07-862003
Citation  Ivaldi MS, et al. (2018) Fetal gamma-globin genes are regulated by the BGLT3 long noncoding RNA locus. Blood 132(18):1963-1973
abstractText  Long noncoding RNAs (lncRNAs) are increasingly being appreciated as participants in regulation of important cellular processes, including transcription. Because lncRNAs are highly cell type specific, they have the potential to contribute to the unique transcriptional repertoire of diverse cells, but underlying mechanisms are unclear. We studied BGLT3, an erythroid lncRNA encoded downstream of (A)gamma-globin (HBG1). BGLT3 and gamma-globin genes are dynamically cotranscribed in erythroid cells in vivo. Deletion of BGLT3 using CRISPR/Cas9 editing shows that it specifically contributes to regulation of gamma-globin genes. We used reduction or overexpression of the RNA and inhibition of transcription through the locus by CRISPRi to distinguish functions of the transcript vs the underlying sequence. Transcription of the BGLT3 locus is critical for looping between the gamma-globin genes and BGLT3 sequences. In contrast, the BGLT3 transcript is dispensable for gamma-globin/BGLT3 looping but interacts with the mediator complex on chromatin. Manipulation of the BGLT3 locus does not compromise gamma-globin gene long-range looping interactions with the beta-globin locus control region (LCR). These data reveal that BGLT3 regulates gamma-globin transcription in a developmental stage-specific fashion together with the LCR by serving as a separate means to increase RNA Pol II density at the gamma-globin promoters.
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