Integration Preferences of Wildtype AAV-2 for Consensus Rep-Binding Sites at Numerous Loci in the Human Genome

Adeno-associated virus type 2 (AAV) is known to establish latency by preferential integration in human chromosome 19q13.42. The AAV non-structural protein Rep appears to target a site called AAVS1 by simultaneously binding to Rep-binding sites (RBS) present on the AAV genome and within AAVS1. In the...

Descripción completa

Detalles Bibliográficos
Autores principales: Hüser, Daniela, Gogol-Döring, Andreas, Lutter, Timo, Weger, Stefan, Winter, Kerstin, Hammer, Eva-Maria, Cathomen, Toni, Reinert, Knut, Heilbronn, Regine
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2900306/
https://www.ncbi.nlm.nih.gov/pubmed/20628575
http://dx.doi.org/10.1371/journal.ppat.1000985
_version_ 1782183622734774272
author Hüser, Daniela
Gogol-Döring, Andreas
Lutter, Timo
Weger, Stefan
Winter, Kerstin
Hammer, Eva-Maria
Cathomen, Toni
Reinert, Knut
Heilbronn, Regine
author_facet Hüser, Daniela
Gogol-Döring, Andreas
Lutter, Timo
Weger, Stefan
Winter, Kerstin
Hammer, Eva-Maria
Cathomen, Toni
Reinert, Knut
Heilbronn, Regine
author_sort Hüser, Daniela
collection PubMed
description Adeno-associated virus type 2 (AAV) is known to establish latency by preferential integration in human chromosome 19q13.42. The AAV non-structural protein Rep appears to target a site called AAVS1 by simultaneously binding to Rep-binding sites (RBS) present on the AAV genome and within AAVS1. In the absence of Rep, as is the case with AAV vectors, chromosomal integration is rare and random. For a genome-wide survey of wildtype AAV integration a linker-selection-mediated (LSM)-PCR strategy was designed to retrieve AAV-chromosomal junctions. DNA sequence determination revealed wildtype AAV integration sites scattered over the entire human genome. The bioinformatic analysis of these integration sites compared to those of rep-deficient AAV vectors revealed a highly significant overrepresentation of integration events near to consensus RBS. Integration hotspots included AAVS1 with 10% of total events. Novel hotspots near consensus RBS were identified on chromosome 5p13.3 denoted AAVS2 and on chromsome 3p24.3 denoted AAVS3. AAVS2 displayed seven independent junctions clustered within only 14 bp of a consensus RBS which proved to bind Rep in vitro similar to the RBS in AAVS3. Expression of Rep in the presence of rep-deficient AAV vectors shifted targeting preferences from random integration back to the neighbourhood of consensus RBS at hotspots and numerous additional sites in the human genome. In summary, targeted AAV integration is not as specific for AAVS1 as previously assumed. Rather, Rep targets AAV to integrate into open chromatin regions in the reach of various, consensus RBS homologues in the human genome.
format Text
id pubmed-2900306
institution National Center for Biotechnology Information
language English
publishDate 2010
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-29003062010-07-13 Integration Preferences of Wildtype AAV-2 for Consensus Rep-Binding Sites at Numerous Loci in the Human Genome Hüser, Daniela Gogol-Döring, Andreas Lutter, Timo Weger, Stefan Winter, Kerstin Hammer, Eva-Maria Cathomen, Toni Reinert, Knut Heilbronn, Regine PLoS Pathog Research Article Adeno-associated virus type 2 (AAV) is known to establish latency by preferential integration in human chromosome 19q13.42. The AAV non-structural protein Rep appears to target a site called AAVS1 by simultaneously binding to Rep-binding sites (RBS) present on the AAV genome and within AAVS1. In the absence of Rep, as is the case with AAV vectors, chromosomal integration is rare and random. For a genome-wide survey of wildtype AAV integration a linker-selection-mediated (LSM)-PCR strategy was designed to retrieve AAV-chromosomal junctions. DNA sequence determination revealed wildtype AAV integration sites scattered over the entire human genome. The bioinformatic analysis of these integration sites compared to those of rep-deficient AAV vectors revealed a highly significant overrepresentation of integration events near to consensus RBS. Integration hotspots included AAVS1 with 10% of total events. Novel hotspots near consensus RBS were identified on chromosome 5p13.3 denoted AAVS2 and on chromsome 3p24.3 denoted AAVS3. AAVS2 displayed seven independent junctions clustered within only 14 bp of a consensus RBS which proved to bind Rep in vitro similar to the RBS in AAVS3. Expression of Rep in the presence of rep-deficient AAV vectors shifted targeting preferences from random integration back to the neighbourhood of consensus RBS at hotspots and numerous additional sites in the human genome. In summary, targeted AAV integration is not as specific for AAVS1 as previously assumed. Rather, Rep targets AAV to integrate into open chromatin regions in the reach of various, consensus RBS homologues in the human genome. Public Library of Science 2010-07-08 /pmc/articles/PMC2900306/ /pubmed/20628575 http://dx.doi.org/10.1371/journal.ppat.1000985 Text en Hüser et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Hüser, Daniela
Gogol-Döring, Andreas
Lutter, Timo
Weger, Stefan
Winter, Kerstin
Hammer, Eva-Maria
Cathomen, Toni
Reinert, Knut
Heilbronn, Regine
Integration Preferences of Wildtype AAV-2 for Consensus Rep-Binding Sites at Numerous Loci in the Human Genome
title Integration Preferences of Wildtype AAV-2 for Consensus Rep-Binding Sites at Numerous Loci in the Human Genome
title_full Integration Preferences of Wildtype AAV-2 for Consensus Rep-Binding Sites at Numerous Loci in the Human Genome
title_fullStr Integration Preferences of Wildtype AAV-2 for Consensus Rep-Binding Sites at Numerous Loci in the Human Genome
title_full_unstemmed Integration Preferences of Wildtype AAV-2 for Consensus Rep-Binding Sites at Numerous Loci in the Human Genome
title_short Integration Preferences of Wildtype AAV-2 for Consensus Rep-Binding Sites at Numerous Loci in the Human Genome
title_sort integration preferences of wildtype aav-2 for consensus rep-binding sites at numerous loci in the human genome
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2900306/
https://www.ncbi.nlm.nih.gov/pubmed/20628575
http://dx.doi.org/10.1371/journal.ppat.1000985
work_keys_str_mv AT huserdaniela integrationpreferencesofwildtypeaav2forconsensusrepbindingsitesatnumerouslociinthehumangenome
AT gogoldoringandreas integrationpreferencesofwildtypeaav2forconsensusrepbindingsitesatnumerouslociinthehumangenome
AT luttertimo integrationpreferencesofwildtypeaav2forconsensusrepbindingsitesatnumerouslociinthehumangenome
AT wegerstefan integrationpreferencesofwildtypeaav2forconsensusrepbindingsitesatnumerouslociinthehumangenome
AT winterkerstin integrationpreferencesofwildtypeaav2forconsensusrepbindingsitesatnumerouslociinthehumangenome
AT hammerevamaria integrationpreferencesofwildtypeaav2forconsensusrepbindingsitesatnumerouslociinthehumangenome
AT cathomentoni integrationpreferencesofwildtypeaav2forconsensusrepbindingsitesatnumerouslociinthehumangenome
AT reinertknut integrationpreferencesofwildtypeaav2forconsensusrepbindingsitesatnumerouslociinthehumangenome
AT heilbronnregine integrationpreferencesofwildtypeaav2forconsensusrepbindingsitesatnumerouslociinthehumangenome

Ejemplares similares