A U1i RNA that Enhances HIV-1 RNA Splicing with an Elongated Recognition Domain Is an Optimal Candidate for Combination HIV-1 Gene Therapy

U1 interference (U1i) RNAs can be designed to correct splicing defects and target pathogenic RNA, such as HIV-1 RNA. In this study, we show that U1i RNAs that enhance HIV-1 RNA splicing are more effective at inhibiting HIV-1 production compared to top U1i RNAs that inhibit polyadenylation of HIV-1 R...

Descripción completa

Detalles Bibliográficos
Autores principales: Del Corpo, Olivier, Goguen, Ryan P., Malard, Camille M.G., Daher, Aïcha, Colby-Germinario, Susan, Scarborough, Robert J., Gatignol, Anne
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society of Gene & Cell Therapy 2019
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6861678/
https://www.ncbi.nlm.nih.gov/pubmed/31734561
http://dx.doi.org/10.1016/j.omtn.2019.10.011
_version_ 1783471403906891776
author Del Corpo, Olivier
Goguen, Ryan P.
Malard, Camille M.G.
Daher, Aïcha
Colby-Germinario, Susan
Scarborough, Robert J.
Gatignol, Anne
author_facet Del Corpo, Olivier
Goguen, Ryan P.
Malard, Camille M.G.
Daher, Aïcha
Colby-Germinario, Susan
Scarborough, Robert J.
Gatignol, Anne
author_sort Del Corpo, Olivier
collection PubMed
description U1 interference (U1i) RNAs can be designed to correct splicing defects and target pathogenic RNA, such as HIV-1 RNA. In this study, we show that U1i RNAs that enhance HIV-1 RNA splicing are more effective at inhibiting HIV-1 production compared to top U1i RNAs that inhibit polyadenylation of HIV-1 RNA. A U1i RNA was also identified targeting a site upstream of the first splice acceptor site in the Gag coding region that was effective at inhibiting HIV-1 production. U1-T6, which enhanced HIV-1 RNA splicing, was superior to an antiviral short hairpin RNA (shRNA) currently in clinical trials. To increase specificity, the recognition domain of U1-T6 was elongated by 3–6 nt. The elongated molecules inhibited HIV-1 production from different HIV-1 strains, including one with a mismatch in the target site. These results suggest that lengthening the recognition domain can enhance the specificity of U1i RNAs for their intended target sites while at the same time allowing them to tolerate single mismatch mutations. Overall, our results demonstrate that U1-T6 with an elongated recognition domain inhibits HIV-1 production and has both the efficacy and specificity to be a promising candidate for HIV-1 gene therapy.
format Online
Article
Text
id pubmed-6861678
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher American Society of Gene & Cell Therapy
record_format MEDLINE/PubMed
spelling pubmed-68616782019-11-22 A U1i RNA that Enhances HIV-1 RNA Splicing with an Elongated Recognition Domain Is an Optimal Candidate for Combination HIV-1 Gene Therapy Del Corpo, Olivier Goguen, Ryan P. Malard, Camille M.G. Daher, Aïcha Colby-Germinario, Susan Scarborough, Robert J. Gatignol, Anne Mol Ther Nucleic Acids Article U1 interference (U1i) RNAs can be designed to correct splicing defects and target pathogenic RNA, such as HIV-1 RNA. In this study, we show that U1i RNAs that enhance HIV-1 RNA splicing are more effective at inhibiting HIV-1 production compared to top U1i RNAs that inhibit polyadenylation of HIV-1 RNA. A U1i RNA was also identified targeting a site upstream of the first splice acceptor site in the Gag coding region that was effective at inhibiting HIV-1 production. U1-T6, which enhanced HIV-1 RNA splicing, was superior to an antiviral short hairpin RNA (shRNA) currently in clinical trials. To increase specificity, the recognition domain of U1-T6 was elongated by 3–6 nt. The elongated molecules inhibited HIV-1 production from different HIV-1 strains, including one with a mismatch in the target site. These results suggest that lengthening the recognition domain can enhance the specificity of U1i RNAs for their intended target sites while at the same time allowing them to tolerate single mismatch mutations. Overall, our results demonstrate that U1-T6 with an elongated recognition domain inhibits HIV-1 production and has both the efficacy and specificity to be a promising candidate for HIV-1 gene therapy. American Society of Gene & Cell Therapy 2019-10-18 /pmc/articles/PMC6861678/ /pubmed/31734561 http://dx.doi.org/10.1016/j.omtn.2019.10.011 Text en © 2019 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Del Corpo, Olivier
Goguen, Ryan P.
Malard, Camille M.G.
Daher, Aïcha
Colby-Germinario, Susan
Scarborough, Robert J.
Gatignol, Anne
A U1i RNA that Enhances HIV-1 RNA Splicing with an Elongated Recognition Domain Is an Optimal Candidate for Combination HIV-1 Gene Therapy
title A U1i RNA that Enhances HIV-1 RNA Splicing with an Elongated Recognition Domain Is an Optimal Candidate for Combination HIV-1 Gene Therapy
title_full A U1i RNA that Enhances HIV-1 RNA Splicing with an Elongated Recognition Domain Is an Optimal Candidate for Combination HIV-1 Gene Therapy
title_fullStr A U1i RNA that Enhances HIV-1 RNA Splicing with an Elongated Recognition Domain Is an Optimal Candidate for Combination HIV-1 Gene Therapy
title_full_unstemmed A U1i RNA that Enhances HIV-1 RNA Splicing with an Elongated Recognition Domain Is an Optimal Candidate for Combination HIV-1 Gene Therapy
title_short A U1i RNA that Enhances HIV-1 RNA Splicing with an Elongated Recognition Domain Is an Optimal Candidate for Combination HIV-1 Gene Therapy
title_sort u1i rna that enhances hiv-1 rna splicing with an elongated recognition domain is an optimal candidate for combination hiv-1 gene therapy
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6861678/
https://www.ncbi.nlm.nih.gov/pubmed/31734561
http://dx.doi.org/10.1016/j.omtn.2019.10.011
work_keys_str_mv AT delcorpoolivier au1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT goguenryanp au1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT malardcamillemg au1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT daheraicha au1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT colbygerminariosusan au1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT scarboroughrobertj au1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT gatignolanne au1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT delcorpoolivier u1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT goguenryanp u1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT malardcamillemg u1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT daheraicha u1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT colbygerminariosusan u1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT scarboroughrobertj u1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy
AT gatignolanne u1irnathatenhanceshiv1rnasplicingwithanelongatedrecognitiondomainisanoptimalcandidateforcombinationhiv1genetherapy

Ejemplares similares