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5΄-Vinylphosphonate improves tissue accumulation and efficacy of conjugated siRNAs in vivo

5΄-Vinylphosphonate modification of siRNAs protects them from phosphatases, and improves silencing activity. Here, we show that 5΄-vinylphosphonate confers novel properties to siRNAs. Specifically, 5΄-vinylphosphonate (i) increases siRNA accumulation in tissues, (ii) extends duration of silencing in...

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Autores principales: Haraszti, Reka A., Roux, Loic, Coles, Andrew H., Turanov, Anton A., Alterman, Julia F., Echeverria, Dimas, Godinho, Bruno M.D.C., Aronin, Neil, Khvorova, Anastasia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5570069/
https://www.ncbi.nlm.nih.gov/pubmed/28591791
http://dx.doi.org/10.1093/nar/gkx507
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author Haraszti, Reka A.
Roux, Loic
Coles, Andrew H.
Turanov, Anton A.
Alterman, Julia F.
Echeverria, Dimas
Godinho, Bruno M.D.C.
Aronin, Neil
Khvorova, Anastasia
author_facet Haraszti, Reka A.
Roux, Loic
Coles, Andrew H.
Turanov, Anton A.
Alterman, Julia F.
Echeverria, Dimas
Godinho, Bruno M.D.C.
Aronin, Neil
Khvorova, Anastasia
author_sort Haraszti, Reka A.
collection PubMed
description 5΄-Vinylphosphonate modification of siRNAs protects them from phosphatases, and improves silencing activity. Here, we show that 5΄-vinylphosphonate confers novel properties to siRNAs. Specifically, 5΄-vinylphosphonate (i) increases siRNA accumulation in tissues, (ii) extends duration of silencing in multiple organs and (iii) protects siRNAs from 5΄-to-3΄ exonucleases. Delivery of conjugated siRNAs requires extensive chemical modifications to achieve stability in vivo. Because chemically modified siRNAs are poor substrates for phosphorylation by kinases, and 5΄-phosphate is required for loading into RNA-induced silencing complex, the synthetic addition of a 5΄-phosphate on a fully modified siRNA guide strand is expected to be beneficial. Here, we show that synthetic phosphorylation of fully modified cholesterol-conjugated siRNAs increases their potency and efficacy in vitro, but when delivered systemically to mice, the 5΄-phosphate is removed within 2 hours. The 5΄-phosphate mimic 5΄-(E)-vinylphosphonate stabilizes the 5΄ end of the guide strand by protecting it from phosphatases and 5΄-to-3΄ exonucleases. The improved stability increases guide strand accumulation and retention in tissues, which significantly enhances the efficacy of cholesterol-conjugated siRNAs and the duration of silencing in vivo. Moreover, we show that 5΄-(E)-vinylphosphonate stabilizes 5΄ phosphate, thereby enabling systemic delivery to and silencing in kidney and heart.
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spelling pubmed-55700692017-08-29 5΄-Vinylphosphonate improves tissue accumulation and efficacy of conjugated siRNAs in vivo Haraszti, Reka A. Roux, Loic Coles, Andrew H. Turanov, Anton A. Alterman, Julia F. Echeverria, Dimas Godinho, Bruno M.D.C. Aronin, Neil Khvorova, Anastasia Nucleic Acids Res Chemical Biology and Nucleic Acid Chemistry 5΄-Vinylphosphonate modification of siRNAs protects them from phosphatases, and improves silencing activity. Here, we show that 5΄-vinylphosphonate confers novel properties to siRNAs. Specifically, 5΄-vinylphosphonate (i) increases siRNA accumulation in tissues, (ii) extends duration of silencing in multiple organs and (iii) protects siRNAs from 5΄-to-3΄ exonucleases. Delivery of conjugated siRNAs requires extensive chemical modifications to achieve stability in vivo. Because chemically modified siRNAs are poor substrates for phosphorylation by kinases, and 5΄-phosphate is required for loading into RNA-induced silencing complex, the synthetic addition of a 5΄-phosphate on a fully modified siRNA guide strand is expected to be beneficial. Here, we show that synthetic phosphorylation of fully modified cholesterol-conjugated siRNAs increases their potency and efficacy in vitro, but when delivered systemically to mice, the 5΄-phosphate is removed within 2 hours. The 5΄-phosphate mimic 5΄-(E)-vinylphosphonate stabilizes the 5΄ end of the guide strand by protecting it from phosphatases and 5΄-to-3΄ exonucleases. The improved stability increases guide strand accumulation and retention in tissues, which significantly enhances the efficacy of cholesterol-conjugated siRNAs and the duration of silencing in vivo. Moreover, we show that 5΄-(E)-vinylphosphonate stabilizes 5΄ phosphate, thereby enabling systemic delivery to and silencing in kidney and heart. Oxford University Press 2017-07-27 2017-06-07 /pmc/articles/PMC5570069/ /pubmed/28591791 http://dx.doi.org/10.1093/nar/gkx507 Text en © The Author(s) 2017. Published by Oxford University Press on behalf of Nucleic Acids Research. http://creativecommons.org/licenses/by-nc/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Chemical Biology and Nucleic Acid Chemistry
Haraszti, Reka A.
Roux, Loic
Coles, Andrew H.
Turanov, Anton A.
Alterman, Julia F.
Echeverria, Dimas
Godinho, Bruno M.D.C.
Aronin, Neil
Khvorova, Anastasia
5΄-Vinylphosphonate improves tissue accumulation and efficacy of conjugated siRNAs in vivo
title 5΄-Vinylphosphonate improves tissue accumulation and efficacy of conjugated siRNAs in vivo
title_full 5΄-Vinylphosphonate improves tissue accumulation and efficacy of conjugated siRNAs in vivo
title_fullStr 5΄-Vinylphosphonate improves tissue accumulation and efficacy of conjugated siRNAs in vivo
title_full_unstemmed 5΄-Vinylphosphonate improves tissue accumulation and efficacy of conjugated siRNAs in vivo
title_short 5΄-Vinylphosphonate improves tissue accumulation and efficacy of conjugated siRNAs in vivo
title_sort 5΄-vinylphosphonate improves tissue accumulation and efficacy of conjugated sirnas in vivo
topic Chemical Biology and Nucleic Acid Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5570069/
https://www.ncbi.nlm.nih.gov/pubmed/28591791
http://dx.doi.org/10.1093/nar/gkx507
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