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In Vitro Anti-Orthohantavirus Activity of the High-and Low-Molecular-Weight Fractions of Fucoidan from the Brown Alga Fucus evanescens

The Hantaan orthohantavirus (genovariant Amur–AMRV) is a rodent-borne zoonotic virus; it is the causative agent of haemorrhagic fever with renal syndrome in humans. The currently limited therapeutic options require the development of effective anti-orthohantavirus drugs. The ability of native fucoid...

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Autores principales: Krylova, Natalia V., Silchenko, Artem S., Pott, Anastasia B., Ermakova, Svetlana P., Iunikhina, Olga V., Rasin, Anton B., Kompanets, Galina G., Likhatskaya, Galina N., Shchelkanov, Mikhail Y.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8538225/
https://www.ncbi.nlm.nih.gov/pubmed/34677476
http://dx.doi.org/10.3390/md19100577
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author Krylova, Natalia V.
Silchenko, Artem S.
Pott, Anastasia B.
Ermakova, Svetlana P.
Iunikhina, Olga V.
Rasin, Anton B.
Kompanets, Galina G.
Likhatskaya, Galina N.
Shchelkanov, Mikhail Y.
author_facet Krylova, Natalia V.
Silchenko, Artem S.
Pott, Anastasia B.
Ermakova, Svetlana P.
Iunikhina, Olga V.
Rasin, Anton B.
Kompanets, Galina G.
Likhatskaya, Galina N.
Shchelkanov, Mikhail Y.
author_sort Krylova, Natalia V.
collection PubMed
description The Hantaan orthohantavirus (genovariant Amur–AMRV) is a rodent-borne zoonotic virus; it is the causative agent of haemorrhagic fever with renal syndrome in humans. The currently limited therapeutic options require the development of effective anti-orthohantavirus drugs. The ability of native fucoidan from Fucus evanescens (FeF) and its enzymatically prepared high-molecular-weight (FeHMP) and low-molecular-weight (FeLMP) fractions to inhibit different stages of AMRV infection in Vero cells was studied. The structures of derivatives obtained were determined using nuclear magnetic resonance (NMR) spectroscopy. We found that fucoidan and its derivatives exhibited significant antiviral activity by affecting the early stages of the AMRV lifecycle, notably virus attachment and penetration. The FeHMP and FeLMP fractions showed the highest anti-adsorption activity by inhibiting AMRV focus formation, with a selective index (SI) > 110; FeF had an SI of ~70. The FeLMP fraction showed a greater virucidal effect compared with FeF and the FeHMP fraction. It was shown by molecular docking that 2O-sulphated fucotetrasaccharide, a main component of the FeLMP fraction, is able to bind with the AMRV envelope glycoproteins Gn/Gc and with integrin β3 to prevent virus–cell interactions. The relatively small size of these sites of interactions explains the higher anti-AMRV activity of the FeLMP fraction.
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spelling pubmed-85382252021-10-24 In Vitro Anti-Orthohantavirus Activity of the High-and Low-Molecular-Weight Fractions of Fucoidan from the Brown Alga Fucus evanescens Krylova, Natalia V. Silchenko, Artem S. Pott, Anastasia B. Ermakova, Svetlana P. Iunikhina, Olga V. Rasin, Anton B. Kompanets, Galina G. Likhatskaya, Galina N. Shchelkanov, Mikhail Y. Mar Drugs Article The Hantaan orthohantavirus (genovariant Amur–AMRV) is a rodent-borne zoonotic virus; it is the causative agent of haemorrhagic fever with renal syndrome in humans. The currently limited therapeutic options require the development of effective anti-orthohantavirus drugs. The ability of native fucoidan from Fucus evanescens (FeF) and its enzymatically prepared high-molecular-weight (FeHMP) and low-molecular-weight (FeLMP) fractions to inhibit different stages of AMRV infection in Vero cells was studied. The structures of derivatives obtained were determined using nuclear magnetic resonance (NMR) spectroscopy. We found that fucoidan and its derivatives exhibited significant antiviral activity by affecting the early stages of the AMRV lifecycle, notably virus attachment and penetration. The FeHMP and FeLMP fractions showed the highest anti-adsorption activity by inhibiting AMRV focus formation, with a selective index (SI) > 110; FeF had an SI of ~70. The FeLMP fraction showed a greater virucidal effect compared with FeF and the FeHMP fraction. It was shown by molecular docking that 2O-sulphated fucotetrasaccharide, a main component of the FeLMP fraction, is able to bind with the AMRV envelope glycoproteins Gn/Gc and with integrin β3 to prevent virus–cell interactions. The relatively small size of these sites of interactions explains the higher anti-AMRV activity of the FeLMP fraction. MDPI 2021-10-15 /pmc/articles/PMC8538225/ /pubmed/34677476 http://dx.doi.org/10.3390/md19100577 Text en © 2021 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
Krylova, Natalia V.
Silchenko, Artem S.
Pott, Anastasia B.
Ermakova, Svetlana P.
Iunikhina, Olga V.
Rasin, Anton B.
Kompanets, Galina G.
Likhatskaya, Galina N.
Shchelkanov, Mikhail Y.
In Vitro Anti-Orthohantavirus Activity of the High-and Low-Molecular-Weight Fractions of Fucoidan from the Brown Alga Fucus evanescens
title In Vitro Anti-Orthohantavirus Activity of the High-and Low-Molecular-Weight Fractions of Fucoidan from the Brown Alga Fucus evanescens
title_full In Vitro Anti-Orthohantavirus Activity of the High-and Low-Molecular-Weight Fractions of Fucoidan from the Brown Alga Fucus evanescens
title_fullStr In Vitro Anti-Orthohantavirus Activity of the High-and Low-Molecular-Weight Fractions of Fucoidan from the Brown Alga Fucus evanescens
title_full_unstemmed In Vitro Anti-Orthohantavirus Activity of the High-and Low-Molecular-Weight Fractions of Fucoidan from the Brown Alga Fucus evanescens
title_short In Vitro Anti-Orthohantavirus Activity of the High-and Low-Molecular-Weight Fractions of Fucoidan from the Brown Alga Fucus evanescens
title_sort in vitro anti-orthohantavirus activity of the high-and low-molecular-weight fractions of fucoidan from the brown alga fucus evanescens
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8538225/
https://www.ncbi.nlm.nih.gov/pubmed/34677476
http://dx.doi.org/10.3390/md19100577
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