| Literature DB >> 29358049 |
Diane E Dickel1, Athena R Ypsilanti2, Ramón Pla2, Yiwen Zhu3, Iros Barozzi3, Brandon J Mannion3, Yupar S Khin2, Yoko Fukuda-Yuzawa3, Ingrid Plajzer-Frick3, Catherine S Pickle3, Elizabeth A Lee3, Anne N Harrington3, Quan T Pham3, Tyler H Garvin3, Momoe Kato3, Marco Osterwalder3, Jennifer A Akiyama3, Veena Afzal3, John L R Rubenstein2, Len A Pennacchio4, Axel Visel5.
Abstract
Non-coding "ultraconserved" regions containing hundreds of consecutive bases of perfect sequence conservation across mammalian genomes can function as distant-acting enhancers. However, initial deletion studies in mice revealed that loss of such extraordinarily constrained sequences had no immediate impact on viability. Here, we show that ultraconserved enhancers are required for normal development. Focusing on some of the longest ultraconserved sites genome wide, located near the essential neuronal transcription factor Arx, we used genome editing to create an expanded series of knockout mice lacking individual or combinations of ultraconserved enhancers. Mice with single or pairwise deletions of ultraconserved enhancers were viable and fertile but in nearly all cases showed neurological or growth abnormalities, including substantial alterations of neuron populations and structural brain defects. Our results demonstrate the functional importance of ultraconserved enhancers and indicate that remarkably strong sequence conservation likely results from fitness deficits that appear subtle in a laboratory setting.Entities:
Keywords: Arx; brain development; enhancer; gene regulation; hippocampus; in vivo; knockout; neurons; noncoding; ultraconserved
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Year: 2018 PMID: 29358049 PMCID: PMC5786478 DOI: 10.1016/j.cell.2017.12.017
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582