β-Globin LCR and Intron Elements Cooperate and Direct Spatial Reorganization for Gene Therapy

The Locus Control Region (LCR) requires intronic elements within β-globin transgenes to direct high level expression at all ectopic integration sites. However, these essential intronic elements cannot be transmitted through retrovirus vectors and their deletion may compromise the therapeutic potenti...

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Autores principales: Buzina, Alla, Lo, Mandy Y. M., Moffett, Angela, Hotta, Akitsu, Fussner, Eden, Bharadwaj, Rikki R., Pasceri, Peter, Garcia-Martinez, J. Victor, Bazett-Jones, David P., Ellis, James
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2271131/
https://www.ncbi.nlm.nih.gov/pubmed/18404216
http://dx.doi.org/10.1371/journal.pgen.1000051
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author Buzina, Alla
Lo, Mandy Y. M.
Moffett, Angela
Hotta, Akitsu
Fussner, Eden
Bharadwaj, Rikki R.
Pasceri, Peter
Garcia-Martinez, J. Victor
Bazett-Jones, David P.
Ellis, James
author_facet Buzina, Alla
Lo, Mandy Y. M.
Moffett, Angela
Hotta, Akitsu
Fussner, Eden
Bharadwaj, Rikki R.
Pasceri, Peter
Garcia-Martinez, J. Victor
Bazett-Jones, David P.
Ellis, James
author_sort Buzina, Alla
collection PubMed
description The Locus Control Region (LCR) requires intronic elements within β-globin transgenes to direct high level expression at all ectopic integration sites. However, these essential intronic elements cannot be transmitted through retrovirus vectors and their deletion may compromise the therapeutic potential for gene therapy. Here, we systematically regenerate functional β-globin intron 2 elements that rescue LCR activity directed by 5′HS3. Evaluation in transgenic mice demonstrates that an Oct-1 binding site and an enhancer in the intron cooperate to increase expression levels from LCR globin transgenes. Replacement of the intronic AT-rich region with the Igμ 3′MAR rescues LCR activity in single copy transgenic mice. Importantly, a combination of the Oct-1 site, Igμ 3′MAR and intronic enhancer in the BGT158 cassette directs more consistent levels of expression in transgenic mice. By introducing intron-modified transgenes into the same genomic integration site in erythroid cells, we show that BGT158 has the greatest transcriptional induction. 3D DNA FISH establishes that induction stimulates this small 5′HS3 containing transgene and the endogenous locus to spatially reorganize towards more central locations in erythroid nuclei. Electron Spectroscopic Imaging (ESI) of chromatin fibers demonstrates that ultrastructural heterochromatin is primarily perinuclear and does not reorganize. Finally, we transmit intron-modified globin transgenes through insulated self-inactivating (SIN) lentivirus vectors into erythroid cells. We show efficient transfer and robust mRNA and protein expression by the BGT158 vector, and virus titer improvements mediated by the modified intron 2 in the presence of an LCR cassette composed of 5′HS2-4. Our results have important implications for the mechanism of LCR activity at ectopic integration sites. The modified transgenes are the first to transfer intronic elements that potentiate LCR activity and are designed to facilitate correction of hemoglobinopathies using single copy vectors.
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spelling pubmed-22711312008-04-18 β-Globin LCR and Intron Elements Cooperate and Direct Spatial Reorganization for Gene Therapy Buzina, Alla Lo, Mandy Y. M. Moffett, Angela Hotta, Akitsu Fussner, Eden Bharadwaj, Rikki R. Pasceri, Peter Garcia-Martinez, J. Victor Bazett-Jones, David P. Ellis, James PLoS Genet Research Article The Locus Control Region (LCR) requires intronic elements within β-globin transgenes to direct high level expression at all ectopic integration sites. However, these essential intronic elements cannot be transmitted through retrovirus vectors and their deletion may compromise the therapeutic potential for gene therapy. Here, we systematically regenerate functional β-globin intron 2 elements that rescue LCR activity directed by 5′HS3. Evaluation in transgenic mice demonstrates that an Oct-1 binding site and an enhancer in the intron cooperate to increase expression levels from LCR globin transgenes. Replacement of the intronic AT-rich region with the Igμ 3′MAR rescues LCR activity in single copy transgenic mice. Importantly, a combination of the Oct-1 site, Igμ 3′MAR and intronic enhancer in the BGT158 cassette directs more consistent levels of expression in transgenic mice. By introducing intron-modified transgenes into the same genomic integration site in erythroid cells, we show that BGT158 has the greatest transcriptional induction. 3D DNA FISH establishes that induction stimulates this small 5′HS3 containing transgene and the endogenous locus to spatially reorganize towards more central locations in erythroid nuclei. Electron Spectroscopic Imaging (ESI) of chromatin fibers demonstrates that ultrastructural heterochromatin is primarily perinuclear and does not reorganize. Finally, we transmit intron-modified globin transgenes through insulated self-inactivating (SIN) lentivirus vectors into erythroid cells. We show efficient transfer and robust mRNA and protein expression by the BGT158 vector, and virus titer improvements mediated by the modified intron 2 in the presence of an LCR cassette composed of 5′HS2-4. Our results have important implications for the mechanism of LCR activity at ectopic integration sites. The modified transgenes are the first to transfer intronic elements that potentiate LCR activity and are designed to facilitate correction of hemoglobinopathies using single copy vectors. Public Library of Science 2008-04-18 /pmc/articles/PMC2271131/ /pubmed/18404216 http://dx.doi.org/10.1371/journal.pgen.1000051 Text en Buzina 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
Buzina, Alla
Lo, Mandy Y. M.
Moffett, Angela
Hotta, Akitsu
Fussner, Eden
Bharadwaj, Rikki R.
Pasceri, Peter
Garcia-Martinez, J. Victor
Bazett-Jones, David P.
Ellis, James
β-Globin LCR and Intron Elements Cooperate and Direct Spatial Reorganization for Gene Therapy
title β-Globin LCR and Intron Elements Cooperate and Direct Spatial Reorganization for Gene Therapy
title_full β-Globin LCR and Intron Elements Cooperate and Direct Spatial Reorganization for Gene Therapy
title_fullStr β-Globin LCR and Intron Elements Cooperate and Direct Spatial Reorganization for Gene Therapy
title_full_unstemmed β-Globin LCR and Intron Elements Cooperate and Direct Spatial Reorganization for Gene Therapy
title_short β-Globin LCR and Intron Elements Cooperate and Direct Spatial Reorganization for Gene Therapy
title_sort β-globin lcr and intron elements cooperate and direct spatial reorganization for gene therapy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2271131/
https://www.ncbi.nlm.nih.gov/pubmed/18404216
http://dx.doi.org/10.1371/journal.pgen.1000051
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