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Construction of a pIX-modified Adenovirus Vector Able to Effectively Bind to Nanoantibodies for Targeting

Current targeting strategies for genetic vectors imply the creation of a specific vector for every targeted receptor, which is time-consuming and expensive. Therefore, the development of a universal vector system whose surface can specifically bind molecules to provide efficient targeting is of part...

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Autores principales: Garas, M. N., Tillib, S. V., Zubkova, O. V., Rogozhin, V. N., Ivanova, T. I., Vasilev, L. A., Logunov, D. Yu., Shmarov, M. M., Tutykhina, I. L., Esmagambetov, I. B., Gribova, I. Yu., Bandelyuk, A. S., Naroditsky, B. S., Gintsburg, A. L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: A.I. Gordeyev 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4115231/
https://www.ncbi.nlm.nih.gov/pubmed/25093116
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author Garas, M. N.
Tillib, S. V.
Zubkova, O. V.
Rogozhin, V. N.
Ivanova, T. I.
Vasilev, L. A.
Logunov, D. Yu.
Shmarov, M. M.
Tutykhina, I. L.
Esmagambetov, I. B.
Gribova, I. Yu.
Bandelyuk, A. S.
Naroditsky, B. S.
Gintsburg, A. L.
author_facet Garas, M. N.
Tillib, S. V.
Zubkova, O. V.
Rogozhin, V. N.
Ivanova, T. I.
Vasilev, L. A.
Logunov, D. Yu.
Shmarov, M. M.
Tutykhina, I. L.
Esmagambetov, I. B.
Gribova, I. Yu.
Bandelyuk, A. S.
Naroditsky, B. S.
Gintsburg, A. L.
author_sort Garas, M. N.
collection PubMed
description Current targeting strategies for genetic vectors imply the creation of a specific vector for every targeted receptor, which is time-consuming and expensive. Therefore, the development of a universal vector system whose surface can specifically bind molecules to provide efficient targeting is of particular interest. In this study, we propose a new approach in creating targeted vectors based on the genome of human adenovirus serotype 5 carrying the modified gene of the capsid protein pIX (Ad5-EGFP-pIX-ER): recombinant pseudoadenoviral nanoparticles (RPANs). The surfaces of such RPANs are able to bind properly modified chimeric nanoantibodies that specifically recognize a particular target antigen (carcinoembryonic antigen (CEA)) with high affinity. The efficient binding of nanoantibodies (aCEA-RE) to the RPAN capsid surfaces has been demonstrated by ELISA. The ability of the constructed vector to deliver target genes has been confirmed by experiments with the tumor cell lines A549 and Lim1215 expressing CEA. It has been shown that Ad5-EGFP-pIX-ER carrying aCEA-RE on its surface penetrates into the tumor cell lines A549 and Lim1215 via the CAR-independent pathway three times more efficiently than unmodified RPAN and Ad5-EGFP-pIX-ER without nanoantibodies on the capsid surface. Thus, RPAN Ad5-EGFP-pIX-ER is a universal platform that may be useful for targeted gene delivery in specific cells due to “nanoantibody–modified RPAN” binding.
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spelling pubmed-41152312014-08-04 Construction of a pIX-modified Adenovirus Vector Able to Effectively Bind to Nanoantibodies for Targeting Garas, M. N. Tillib, S. V. Zubkova, O. V. Rogozhin, V. N. Ivanova, T. I. Vasilev, L. A. Logunov, D. Yu. Shmarov, M. M. Tutykhina, I. L. Esmagambetov, I. B. Gribova, I. Yu. Bandelyuk, A. S. Naroditsky, B. S. Gintsburg, A. L. Acta Naturae Research Article Current targeting strategies for genetic vectors imply the creation of a specific vector for every targeted receptor, which is time-consuming and expensive. Therefore, the development of a universal vector system whose surface can specifically bind molecules to provide efficient targeting is of particular interest. In this study, we propose a new approach in creating targeted vectors based on the genome of human adenovirus serotype 5 carrying the modified gene of the capsid protein pIX (Ad5-EGFP-pIX-ER): recombinant pseudoadenoviral nanoparticles (RPANs). The surfaces of such RPANs are able to bind properly modified chimeric nanoantibodies that specifically recognize a particular target antigen (carcinoembryonic antigen (CEA)) with high affinity. The efficient binding of nanoantibodies (aCEA-RE) to the RPAN capsid surfaces has been demonstrated by ELISA. The ability of the constructed vector to deliver target genes has been confirmed by experiments with the tumor cell lines A549 and Lim1215 expressing CEA. It has been shown that Ad5-EGFP-pIX-ER carrying aCEA-RE on its surface penetrates into the tumor cell lines A549 and Lim1215 via the CAR-independent pathway three times more efficiently than unmodified RPAN and Ad5-EGFP-pIX-ER without nanoantibodies on the capsid surface. Thus, RPAN Ad5-EGFP-pIX-ER is a universal platform that may be useful for targeted gene delivery in specific cells due to “nanoantibody–modified RPAN” binding. A.I. Gordeyev 2014 /pmc/articles/PMC4115231/ /pubmed/25093116 Text en Copyright ® 2014 Park-media Ltd. http://creativecommons.org/licenses/by/2.0/ 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 work is properly cited.
spellingShingle Research Article
Garas, M. N.
Tillib, S. V.
Zubkova, O. V.
Rogozhin, V. N.
Ivanova, T. I.
Vasilev, L. A.
Logunov, D. Yu.
Shmarov, M. M.
Tutykhina, I. L.
Esmagambetov, I. B.
Gribova, I. Yu.
Bandelyuk, A. S.
Naroditsky, B. S.
Gintsburg, A. L.
Construction of a pIX-modified Adenovirus Vector Able to Effectively Bind to Nanoantibodies for Targeting
title Construction of a pIX-modified Adenovirus Vector Able to Effectively Bind to Nanoantibodies for Targeting
title_full Construction of a pIX-modified Adenovirus Vector Able to Effectively Bind to Nanoantibodies for Targeting
title_fullStr Construction of a pIX-modified Adenovirus Vector Able to Effectively Bind to Nanoantibodies for Targeting
title_full_unstemmed Construction of a pIX-modified Adenovirus Vector Able to Effectively Bind to Nanoantibodies for Targeting
title_short Construction of a pIX-modified Adenovirus Vector Able to Effectively Bind to Nanoantibodies for Targeting
title_sort construction of a pix-modified adenovirus vector able to effectively bind to nanoantibodies for targeting
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4115231/
https://www.ncbi.nlm.nih.gov/pubmed/25093116
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