| Literature DB >> 36202974 |
Anthony Beucher1,2, Irene Miguel-Escalada3,4,5, Diego Balboa4,5, Matías G De Vas3, Miguel Angel Maestro4,5, Javier Garcia-Hurtado4,5, Aina Bernal4,5, Roser Gonzalez-Franco3, Pierfrancesco Vargiu6, Holger Heyn4,7,8, Philippe Ravassard9, Sagrario Ortega6, Jorge Ferrer10,11,12.
Abstract
The biological purpose of long non-coding RNAs (lncRNAs) is poorly understood. Haploinsufficient mutations in HNF1A homeobox A (HNF1A), encoding a homeodomain transcription factor, cause diabetes mellitus. Here, we examine HASTER, the promoter of an lncRNA antisense to HNF1A. Using mouse and human models, we show that HASTER maintains cell-specific physiological HNF1A concentrations through positive and negative feedback loops. Pancreatic β cells from Haster mutant mice consequently showed variegated HNF1A silencing or overexpression, resulting in hyperglycaemia. HASTER-dependent negative feedback was essential to prevent HNF1A binding to inappropriate genomic regions. We demonstrate that the HASTER promoter DNA, rather than the lncRNA, modulates HNF1A promoter-enhancer interactions in cis and thereby regulates HNF1A transcription. Our studies expose a cis-regulatory element that is unlike classic enhancers or silencers, it stabilizes the transcription of its target gene and ensures the fidelity of a cell-specific transcription factor program. They also show that disruption of a mammalian lncRNA promoter can cause diabetes mellitus.Entities:
Year: 2022 PMID: 36202974 PMCID: PMC9586874 DOI: 10.1038/s41556-022-00996-8
Source DB: PubMed Journal: Nat Cell Biol ISSN: 1465-7392 Impact factor: 28.213