| Literature DB >> 35573091 |
Ilias Georgakopoulos-Soares1,2, Jesus Victorino3,4,5, Guillermo E Parada6,7,5, Vikram Agarwal8, Jingjing Zhao1,2, Hei Yuen Wong9, Mubarak Ishaq Umar9, Orry Elor1, Allan Muhwezi6, Joon-Yong An10,11, Stephan J Sanders2,10, Chun Kit Kwok9,12, Fumitaka Inoue1,2,13, Martin Hemberg6,7,14, Nadav Ahituv1,2,15.
Abstract
lternative DNA conformations, termed non-B DNA structures, can affect transcription, but the underlying mechanisms and their functional impact have not been systematically characterized. Here, we used computational genomic analyses coupled with massively parallel reporter assays (MPRAs) to show that certain non-B DNA structures have a substantial effect on gene expression. Genomic analyses found that non-B DNA structures at promoters harbor an excess of germline variants. Analysis of multiple MPRAs, including a promoter library specifically designed to perturb non-B DNA structures, functionally validated that Z-DNA can significantly affect promoter activity. We also observed that biophysical properties of non-B DNA motifs, such as the length of Z-DNA motifs and the orientation of G-quadruplex structures relative to transcriptional direction, have a significant effect on promoter activity. Combined, their higher mutation rate and functional effect on transcription implicate a subset of non-B DNA motifs as major drivers of human gene-expression-associated phenotypes.Entities:
Year: 2022 PMID: 35573091 PMCID: PMC9105345 DOI: 10.1016/j.xgen.2022.100111
Source DB: PubMed Journal: Cell Genom ISSN: 2666-979X