DNA Topoisomerase I differentially modulates R-loops across the human genome
Abstract Background Co-transcriptional R-loops are abundant non-B DNA structures in mammalian genomes. DNA Topoisomerase I (Top1) is often thought to regulate R-loop formation owing to its ability to resolve both positive and negative supercoils. How Top1 regulates R-loop structures at a global leve...
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doaj-d230920f9e4044538f0d8cb487c07b202020-11-24T21:49:18ZengBMCGenome Biology1474-760X2018-07-0119111810.1186/s13059-018-1478-1DNA Topoisomerase I differentially modulates R-loops across the human genomeStefano G. Manzo0Stella R. Hartono1Lionel A. Sanz2Jessica Marinello3Sara De Biasi4Andrea Cossarizza5Giovanni Capranico6Frederic Chedin7Department of Pharmacy and Biotechnology, University of BolognaDepartment of Molecular and Cellular Biology and Genome Center, University of CaliforniaDepartment of Molecular and Cellular Biology and Genome Center, University of CaliforniaDepartment of Pharmacy and Biotechnology, University of BolognaDepartment of Medical and Surgical Sciences for Children and Adults, University of Modena and Reggio EmiliaDepartment of Medical and Surgical Sciences for Children and Adults, University of Modena and Reggio EmiliaDepartment of Pharmacy and Biotechnology, University of BolognaDepartment of Molecular and Cellular Biology and Genome Center, University of CaliforniaAbstract Background Co-transcriptional R-loops are abundant non-B DNA structures in mammalian genomes. DNA Topoisomerase I (Top1) is often thought to regulate R-loop formation owing to its ability to resolve both positive and negative supercoils. How Top1 regulates R-loop structures at a global level is unknown. Results Here, we perform high-resolution strand-specific R-loop mapping in human cells depleted for Top1 and find that Top1 depletion results in both R-loop gains and losses at thousands of transcribed loci, delineating two distinct gene classes. R-loop gains are characteristic for long, highly transcribed, genes located in gene-poor regions anchored to Lamin B1 domains and in proximity to H3K9me3-marked heterochromatic patches. R-loop losses, by contrast, occur in gene-rich regions overlapping H3K27me3-marked active replication initiation regions. Interestingly, Top1 depletion coincides with a block of the cell cycle in G0/G1 phase and a trend towards replication delay. Conclusions Our findings reveal new properties of Top1 in regulating R-loop homeostasis in a context-dependent manner and suggest a potential role for Top1 in modulating the replication process via R-loop formation.http://link.springer.com/article/10.1186/s13059-018-1478-1 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Stefano G. Manzo Stella R. Hartono Lionel A. Sanz Jessica Marinello Sara De Biasi Andrea Cossarizza Giovanni Capranico Frederic Chedin |
spellingShingle |
Stefano G. Manzo Stella R. Hartono Lionel A. Sanz Jessica Marinello Sara De Biasi Andrea Cossarizza Giovanni Capranico Frederic Chedin DNA Topoisomerase I differentially modulates R-loops across the human genome Genome Biology |
author_facet |
Stefano G. Manzo Stella R. Hartono Lionel A. Sanz Jessica Marinello Sara De Biasi Andrea Cossarizza Giovanni Capranico Frederic Chedin |
author_sort |
Stefano G. Manzo |
title |
DNA Topoisomerase I differentially modulates R-loops across the human genome |
title_short |
DNA Topoisomerase I differentially modulates R-loops across the human genome |
title_full |
DNA Topoisomerase I differentially modulates R-loops across the human genome |
title_fullStr |
DNA Topoisomerase I differentially modulates R-loops across the human genome |
title_full_unstemmed |
DNA Topoisomerase I differentially modulates R-loops across the human genome |
title_sort |
dna topoisomerase i differentially modulates r-loops across the human genome |
publisher |
BMC |
series |
Genome Biology |
issn |
1474-760X |
publishDate |
2018-07-01 |
description |
Abstract Background Co-transcriptional R-loops are abundant non-B DNA structures in mammalian genomes. DNA Topoisomerase I (Top1) is often thought to regulate R-loop formation owing to its ability to resolve both positive and negative supercoils. How Top1 regulates R-loop structures at a global level is unknown. Results Here, we perform high-resolution strand-specific R-loop mapping in human cells depleted for Top1 and find that Top1 depletion results in both R-loop gains and losses at thousands of transcribed loci, delineating two distinct gene classes. R-loop gains are characteristic for long, highly transcribed, genes located in gene-poor regions anchored to Lamin B1 domains and in proximity to H3K9me3-marked heterochromatic patches. R-loop losses, by contrast, occur in gene-rich regions overlapping H3K27me3-marked active replication initiation regions. Interestingly, Top1 depletion coincides with a block of the cell cycle in G0/G1 phase and a trend towards replication delay. Conclusions Our findings reveal new properties of Top1 in regulating R-loop homeostasis in a context-dependent manner and suggest a potential role for Top1 in modulating the replication process via R-loop formation. |
url |
http://link.springer.com/article/10.1186/s13059-018-1478-1 |
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