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The Regioselective Conjugation of the 15-nt Thrombin Aptamer with an Optimized Tripeptide Sequence Greatly Increases the Anticoagulant Activity of the Aptamer

Currently, oligonucleotide therapy has emerged as a new paradigm in the treatment of human diseases. In many cases, however, therapeutic oligonucleotides cannot be used directly without modification. Chemical modification or the conjugation of therapeutic oligonucleotides is required to increase the...

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Autores principales: Varizhuk, Irina V., Tsvetkov, Vladimir B., Toropygin, Ilya Yu., Stomakhin, Andrey A., Kolganova, Natalia A., Surzhikov, Sergei A., Timofeev, Edward N.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9967020/
https://www.ncbi.nlm.nih.gov/pubmed/36839926
http://dx.doi.org/10.3390/pharmaceutics15020604
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author Varizhuk, Irina V.
Tsvetkov, Vladimir B.
Toropygin, Ilya Yu.
Stomakhin, Andrey A.
Kolganova, Natalia A.
Surzhikov, Sergei A.
Timofeev, Edward N.
author_facet Varizhuk, Irina V.
Tsvetkov, Vladimir B.
Toropygin, Ilya Yu.
Stomakhin, Andrey A.
Kolganova, Natalia A.
Surzhikov, Sergei A.
Timofeev, Edward N.
author_sort Varizhuk, Irina V.
collection PubMed
description Currently, oligonucleotide therapy has emerged as a new paradigm in the treatment of human diseases. In many cases, however, therapeutic oligonucleotides cannot be used directly without modification. Chemical modification or the conjugation of therapeutic oligonucleotides is required to increase their stability or specificity, improve their affinity or inhibitory characteristics, and address delivery issues. Recently, we proposed a conjugation strategy for a 15-nt G-quadruplex thrombin aptamer aimed at extending the recognition interface of the aptamer. In particular, we have prepared a series of designer peptide conjugates of the thrombin aptamer, showing improved anticoagulant activity. Herein, we report a new series of aptamer–peptide conjugates with optimized peptide sequences. The anti-thrombotic activity of aptamer conjugates was notably improved. The lead conjugate, TBA–GLE, was able to inhibit thrombin-induced coagulation approximately six-fold more efficiently than the unmodified aptamer. In terms of its anticoagulant activity, the TBA–GLE conjugate approaches NU172, one of the most potent G-quadruplex thrombin aptamers. Molecular dynamics studies have confirmed that the principles applied to the design of the peptide side chain are efficient instruments for improving aptamer characteristics for the proposed TBA conjugate model.
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spelling pubmed-99670202023-02-26 The Regioselective Conjugation of the 15-nt Thrombin Aptamer with an Optimized Tripeptide Sequence Greatly Increases the Anticoagulant Activity of the Aptamer Varizhuk, Irina V. Tsvetkov, Vladimir B. Toropygin, Ilya Yu. Stomakhin, Andrey A. Kolganova, Natalia A. Surzhikov, Sergei A. Timofeev, Edward N. Pharmaceutics Article Currently, oligonucleotide therapy has emerged as a new paradigm in the treatment of human diseases. In many cases, however, therapeutic oligonucleotides cannot be used directly without modification. Chemical modification or the conjugation of therapeutic oligonucleotides is required to increase their stability or specificity, improve their affinity or inhibitory characteristics, and address delivery issues. Recently, we proposed a conjugation strategy for a 15-nt G-quadruplex thrombin aptamer aimed at extending the recognition interface of the aptamer. In particular, we have prepared a series of designer peptide conjugates of the thrombin aptamer, showing improved anticoagulant activity. Herein, we report a new series of aptamer–peptide conjugates with optimized peptide sequences. The anti-thrombotic activity of aptamer conjugates was notably improved. The lead conjugate, TBA–GLE, was able to inhibit thrombin-induced coagulation approximately six-fold more efficiently than the unmodified aptamer. In terms of its anticoagulant activity, the TBA–GLE conjugate approaches NU172, one of the most potent G-quadruplex thrombin aptamers. Molecular dynamics studies have confirmed that the principles applied to the design of the peptide side chain are efficient instruments for improving aptamer characteristics for the proposed TBA conjugate model. MDPI 2023-02-10 /pmc/articles/PMC9967020/ /pubmed/36839926 http://dx.doi.org/10.3390/pharmaceutics15020604 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Varizhuk, Irina V.
Tsvetkov, Vladimir B.
Toropygin, Ilya Yu.
Stomakhin, Andrey A.
Kolganova, Natalia A.
Surzhikov, Sergei A.
Timofeev, Edward N.
The Regioselective Conjugation of the 15-nt Thrombin Aptamer with an Optimized Tripeptide Sequence Greatly Increases the Anticoagulant Activity of the Aptamer
title The Regioselective Conjugation of the 15-nt Thrombin Aptamer with an Optimized Tripeptide Sequence Greatly Increases the Anticoagulant Activity of the Aptamer
title_full The Regioselective Conjugation of the 15-nt Thrombin Aptamer with an Optimized Tripeptide Sequence Greatly Increases the Anticoagulant Activity of the Aptamer
title_fullStr The Regioselective Conjugation of the 15-nt Thrombin Aptamer with an Optimized Tripeptide Sequence Greatly Increases the Anticoagulant Activity of the Aptamer
title_full_unstemmed The Regioselective Conjugation of the 15-nt Thrombin Aptamer with an Optimized Tripeptide Sequence Greatly Increases the Anticoagulant Activity of the Aptamer
title_short The Regioselective Conjugation of the 15-nt Thrombin Aptamer with an Optimized Tripeptide Sequence Greatly Increases the Anticoagulant Activity of the Aptamer
title_sort regioselective conjugation of the 15-nt thrombin aptamer with an optimized tripeptide sequence greatly increases the anticoagulant activity of the aptamer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9967020/
https://www.ncbi.nlm.nih.gov/pubmed/36839926
http://dx.doi.org/10.3390/pharmaceutics15020604
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