Transcription factor binding sites are genetic determinants of retroviral integration in the human genome.

Transcription factor binding sites are genetic determinants of retroviral integration in the human genome.

Gamma-retroviruses and lentiviruses integrate non-randomly in mammalian genomes, with specific preferences for active chromatin, promoters and regulatory regions. Gene transfer vectors derived from gamma-retroviruses target at high frequency genes involved in the control of growth, development and d...

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Main Authors: Barbara Felice, Claudia Cattoglio, Davide Cittaro, Anna Testa, Annarita Miccio, Giuliana Ferrari, Lucilla Luzi, Alessandra Recchia, Fulvio Mavilio
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2009-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2642719?pdf=render
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spelling doaj-5bfbd986e5784d29a53b9d39131641012020-11-24T22:21:32ZengPublic Library of Science (PLoS)PLoS ONE1932-62032009-01-0142e457110.1371/journal.pone.0004571Transcription factor binding sites are genetic determinants of retroviral integration in the human genome.Barbara FeliceClaudia CattoglioDavide CittaroAnna TestaAnnarita MiccioGiuliana FerrariLucilla LuziAlessandra RecchiaFulvio MavilioGamma-retroviruses and lentiviruses integrate non-randomly in mammalian genomes, with specific preferences for active chromatin, promoters and regulatory regions. Gene transfer vectors derived from gamma-retroviruses target at high frequency genes involved in the control of growth, development and differentiation of the target cell, and may induce insertional tumors or pre-neoplastic clonal expansions in patients treated by gene therapy. The gene expression program of the target cell is apparently instrumental in directing gamma-retroviral integration, although the molecular basis of this phenomenon is poorly understood. We report a bioinformatic analysis of the distribution of transcription factor binding sites (TFBSs) flanking >4,000 integrated proviruses in human hematopoietic and non-hematopoietic cells. We show that gamma-retroviral, but not lentiviral vectors, integrate in genomic regions enriched in cell-type specific subsets of TFBSs, independently from their relative position with respect to genes and transcription start sites. Analysis of sequences flanking the integration sites of Moloney leukemia virus (MLV)- and human immunodeficiency virus (HIV)-derived vectors carrying mutations in their long terminal repeats (LTRs), and of HIV vectors packaged with an MLV integrase, indicates that the MLV integrase and LTR enhancer are the viral determinants of the selection of TFBS-rich regions in the genome. This study identifies TFBSs as differential genomic determinants of retroviral target site selection in the human genome, and suggests that transcription factors binding the LTR enhancer may synergize with the integrase in tethering retroviral pre-integration complexes to transcriptionally active regulatory regions. Our data indicate that gamma-retroviruses and lentiviruses have evolved dramatically different strategies to interact with the host cell chromatin, and predict a higher risk in using gamma-retroviral vs. lentiviral vectors for human gene therapy applications.http://europepmc.org/articles/PMC2642719?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Barbara Felice
Claudia Cattoglio
Davide Cittaro
Anna Testa
Annarita Miccio
Giuliana Ferrari
Lucilla Luzi
Alessandra Recchia
Fulvio Mavilio
spellingShingle Barbara Felice
Claudia Cattoglio
Davide Cittaro
Anna Testa
Annarita Miccio
Giuliana Ferrari
Lucilla Luzi
Alessandra Recchia
Fulvio Mavilio
Transcription factor binding sites are genetic determinants of retroviral integration in the human genome.
PLoS ONE
author_facet Barbara Felice
Claudia Cattoglio
Davide Cittaro
Anna Testa
Annarita Miccio
Giuliana Ferrari
Lucilla Luzi
Alessandra Recchia
Fulvio Mavilio
author_sort Barbara Felice
title Transcription factor binding sites are genetic determinants of retroviral integration in the human genome.
title_short Transcription factor binding sites are genetic determinants of retroviral integration in the human genome.
title_full Transcription factor binding sites are genetic determinants of retroviral integration in the human genome.
title_fullStr Transcription factor binding sites are genetic determinants of retroviral integration in the human genome.
title_full_unstemmed Transcription factor binding sites are genetic determinants of retroviral integration in the human genome.
title_sort transcription factor binding sites are genetic determinants of retroviral integration in the human genome.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2009-01-01
description Gamma-retroviruses and lentiviruses integrate non-randomly in mammalian genomes, with specific preferences for active chromatin, promoters and regulatory regions. Gene transfer vectors derived from gamma-retroviruses target at high frequency genes involved in the control of growth, development and differentiation of the target cell, and may induce insertional tumors or pre-neoplastic clonal expansions in patients treated by gene therapy. The gene expression program of the target cell is apparently instrumental in directing gamma-retroviral integration, although the molecular basis of this phenomenon is poorly understood. We report a bioinformatic analysis of the distribution of transcription factor binding sites (TFBSs) flanking >4,000 integrated proviruses in human hematopoietic and non-hematopoietic cells. We show that gamma-retroviral, but not lentiviral vectors, integrate in genomic regions enriched in cell-type specific subsets of TFBSs, independently from their relative position with respect to genes and transcription start sites. Analysis of sequences flanking the integration sites of Moloney leukemia virus (MLV)- and human immunodeficiency virus (HIV)-derived vectors carrying mutations in their long terminal repeats (LTRs), and of HIV vectors packaged with an MLV integrase, indicates that the MLV integrase and LTR enhancer are the viral determinants of the selection of TFBS-rich regions in the genome. This study identifies TFBSs as differential genomic determinants of retroviral target site selection in the human genome, and suggests that transcription factors binding the LTR enhancer may synergize with the integrase in tethering retroviral pre-integration complexes to transcriptionally active regulatory regions. Our data indicate that gamma-retroviruses and lentiviruses have evolved dramatically different strategies to interact with the host cell chromatin, and predict a higher risk in using gamma-retroviral vs. lentiviral vectors for human gene therapy applications.
url http://europepmc.org/articles/PMC2642719?pdf=render
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