Sulfated Polysaccharide, Curdlan Sulfate, Efficiently Prevents Entry/Fusion and Restricts Antibody-Dependent Enhancement of Dengue Virus Infection In Vitro: A Possible Candidate for Clinical Application

Curdlan sulfate (CRDS), a sulfated 1→3-β-D glucan, previously shown to be a potent HIV entry inhibitor, is characterized in this study as a potent inhibitor of the Dengue virus (DENV). CRDS was identified by in silico blind docking studies to exhibit binding potential to the envelope (E) protein of...

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Autores principales: Ichiyama, Koji, Gopala Reddy, Sindhoora Bhargavi, Zhang, Li Feng, Chin, Wei Xin, Muschin, Tegshi, Heinig, Lars, Suzuki, Youichi, Nanjundappa, Haraprasad, Yoshinaka, Yoshiyuki, Ryo, Akihide, Nomura, Nobuo, Ooi, Eng Eong, Vasudevan, Subhash G., Yoshida, Takashi, Yamamoto, Naoki
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3636050/
https://www.ncbi.nlm.nih.gov/pubmed/23658845
http://dx.doi.org/10.1371/journal.pntd.0002188
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author Ichiyama, Koji
Gopala Reddy, Sindhoora Bhargavi
Zhang, Li Feng
Chin, Wei Xin
Muschin, Tegshi
Heinig, Lars
Suzuki, Youichi
Nanjundappa, Haraprasad
Yoshinaka, Yoshiyuki
Ryo, Akihide
Nomura, Nobuo
Ooi, Eng Eong
Vasudevan, Subhash G.
Yoshida, Takashi
Yamamoto, Naoki
author_facet Ichiyama, Koji
Gopala Reddy, Sindhoora Bhargavi
Zhang, Li Feng
Chin, Wei Xin
Muschin, Tegshi
Heinig, Lars
Suzuki, Youichi
Nanjundappa, Haraprasad
Yoshinaka, Yoshiyuki
Ryo, Akihide
Nomura, Nobuo
Ooi, Eng Eong
Vasudevan, Subhash G.
Yoshida, Takashi
Yamamoto, Naoki
author_sort Ichiyama, Koji
collection PubMed
description Curdlan sulfate (CRDS), a sulfated 1→3-β-D glucan, previously shown to be a potent HIV entry inhibitor, is characterized in this study as a potent inhibitor of the Dengue virus (DENV). CRDS was identified by in silico blind docking studies to exhibit binding potential to the envelope (E) protein of the DENV. CRDS was shown to inhibit the DENV replication very efficiently in different cells in vitro. Minimal effective concentration of CRDS was as low as 0.1 µg/mL in LLC-MK2 cells, and toxicity was observed only at concentrations over 10 mg/mL. CRDS can also inhibit DENV-1, 3, and 4 efficiently. CRDS did not inhibit the replication of DENV subgenomic replicon. Time of addition experiments demonstrated that the compound not only inhibited viral infection at the host cell binding step, but also at an early post-attachment step of entry (membrane fusion). The direct binding of CRDS to DENV was suggested by an evident reduction in the viral titers after interaction of the virus with CRDS following an ultrafiltration device separation, as well as after virus adsorption to an alkyl CRDS-coated membrane filter. The electron microscopic features also showed that CRDS interacted directly with the viral envelope, and caused changes to the viral surface. CRDS also potently inhibited DENV infection in DC-SIGN expressing cells as well as the antibody-dependent enhancement of DENV-2 infection. Based on these data, a probable binding model of CRDS to DENV E protein was constructed by a flexible receptor and ligand docking study. The binding site of CRDS was predicted to be at the interface between domains II and III of E protein dimer, which is unique to this compound, and is apparently different from the β-OG binding site. Since CRDS has already been tested in humans without serious side effects, its clinical application can be considered.
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spelling pubmed-36360502013-05-08 Sulfated Polysaccharide, Curdlan Sulfate, Efficiently Prevents Entry/Fusion and Restricts Antibody-Dependent Enhancement of Dengue Virus Infection In Vitro: A Possible Candidate for Clinical Application Ichiyama, Koji Gopala Reddy, Sindhoora Bhargavi Zhang, Li Feng Chin, Wei Xin Muschin, Tegshi Heinig, Lars Suzuki, Youichi Nanjundappa, Haraprasad Yoshinaka, Yoshiyuki Ryo, Akihide Nomura, Nobuo Ooi, Eng Eong Vasudevan, Subhash G. Yoshida, Takashi Yamamoto, Naoki PLoS Negl Trop Dis Research Article Curdlan sulfate (CRDS), a sulfated 1→3-β-D glucan, previously shown to be a potent HIV entry inhibitor, is characterized in this study as a potent inhibitor of the Dengue virus (DENV). CRDS was identified by in silico blind docking studies to exhibit binding potential to the envelope (E) protein of the DENV. CRDS was shown to inhibit the DENV replication very efficiently in different cells in vitro. Minimal effective concentration of CRDS was as low as 0.1 µg/mL in LLC-MK2 cells, and toxicity was observed only at concentrations over 10 mg/mL. CRDS can also inhibit DENV-1, 3, and 4 efficiently. CRDS did not inhibit the replication of DENV subgenomic replicon. Time of addition experiments demonstrated that the compound not only inhibited viral infection at the host cell binding step, but also at an early post-attachment step of entry (membrane fusion). The direct binding of CRDS to DENV was suggested by an evident reduction in the viral titers after interaction of the virus with CRDS following an ultrafiltration device separation, as well as after virus adsorption to an alkyl CRDS-coated membrane filter. The electron microscopic features also showed that CRDS interacted directly with the viral envelope, and caused changes to the viral surface. CRDS also potently inhibited DENV infection in DC-SIGN expressing cells as well as the antibody-dependent enhancement of DENV-2 infection. Based on these data, a probable binding model of CRDS to DENV E protein was constructed by a flexible receptor and ligand docking study. The binding site of CRDS was predicted to be at the interface between domains II and III of E protein dimer, which is unique to this compound, and is apparently different from the β-OG binding site. Since CRDS has already been tested in humans without serious side effects, its clinical application can be considered. Public Library of Science 2013-04-25 /pmc/articles/PMC3636050/ /pubmed/23658845 http://dx.doi.org/10.1371/journal.pntd.0002188 Text en © 2013 Ichiyama et al http://creativecommons.org/licenses/by/4.0/ 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 author and source are properly credited.
spellingShingle Research Article
Ichiyama, Koji
Gopala Reddy, Sindhoora Bhargavi
Zhang, Li Feng
Chin, Wei Xin
Muschin, Tegshi
Heinig, Lars
Suzuki, Youichi
Nanjundappa, Haraprasad
Yoshinaka, Yoshiyuki
Ryo, Akihide
Nomura, Nobuo
Ooi, Eng Eong
Vasudevan, Subhash G.
Yoshida, Takashi
Yamamoto, Naoki
Sulfated Polysaccharide, Curdlan Sulfate, Efficiently Prevents Entry/Fusion and Restricts Antibody-Dependent Enhancement of Dengue Virus Infection In Vitro: A Possible Candidate for Clinical Application
title Sulfated Polysaccharide, Curdlan Sulfate, Efficiently Prevents Entry/Fusion and Restricts Antibody-Dependent Enhancement of Dengue Virus Infection In Vitro: A Possible Candidate for Clinical Application
title_full Sulfated Polysaccharide, Curdlan Sulfate, Efficiently Prevents Entry/Fusion and Restricts Antibody-Dependent Enhancement of Dengue Virus Infection In Vitro: A Possible Candidate for Clinical Application
title_fullStr Sulfated Polysaccharide, Curdlan Sulfate, Efficiently Prevents Entry/Fusion and Restricts Antibody-Dependent Enhancement of Dengue Virus Infection In Vitro: A Possible Candidate for Clinical Application
title_full_unstemmed Sulfated Polysaccharide, Curdlan Sulfate, Efficiently Prevents Entry/Fusion and Restricts Antibody-Dependent Enhancement of Dengue Virus Infection In Vitro: A Possible Candidate for Clinical Application
title_short Sulfated Polysaccharide, Curdlan Sulfate, Efficiently Prevents Entry/Fusion and Restricts Antibody-Dependent Enhancement of Dengue Virus Infection In Vitro: A Possible Candidate for Clinical Application
title_sort sulfated polysaccharide, curdlan sulfate, efficiently prevents entry/fusion and restricts antibody-dependent enhancement of dengue virus infection in vitro: a possible candidate for clinical application
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3636050/
https://www.ncbi.nlm.nih.gov/pubmed/23658845
http://dx.doi.org/10.1371/journal.pntd.0002188
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