Development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.

Development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.

Influenza is an infectious respiratory illness caused by influenza viruses. Despite yearly updates, the efficacy of influenza vaccines is significantly curtailed by the virus antigenic drift and antigenic shift. These constant changes to the influenza virus make-up also challenge the development of...

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Main Authors: Kamonthip Rungrojcharoenkit, Panya Sunintaboon, Damon Ellison, Louis Macareo, Panuwat Midoeng, Preamrudee Chaisuwirat, Stefan Fernandez, Sukathida Ubol
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2020-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0237218
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spelling doaj-a04a1c01e9d7483793c0a254a521d41b2021-06-19T05:09:12ZengPublic Library of Science (PLoS)PLoS ONE1932-62032020-01-01158e023721810.1371/journal.pone.0237218Development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.Kamonthip RungrojcharoenkitPanya SunintaboonDamon EllisonLouis MacareoPanuwat MidoengPreamrudee ChaisuwiratStefan FernandezSukathida UbolInfluenza is an infectious respiratory illness caused by influenza viruses. Despite yearly updates, the efficacy of influenza vaccines is significantly curtailed by the virus antigenic drift and antigenic shift. These constant changes to the influenza virus make-up also challenge the development of a universal flu vaccine, which requires conserved antigenic regions shared by influenza viruses of different subtypes. We propose that it is possible to bypass these challenges by the development of an influenza vaccine based on conserved proteins delivered in an adjuvanted nanoparticle system. In this study, we generated influenza nanoparticle constructs using trimethyl chitosan nanoparticles (TMC nPs) as the carrier of recombinant influenza hemagglutinin subunit 2 (HA2) and nucleoprotein (NP). The purified HA2 and NP recombinant proteins were encapsulated into TMC nPs to form HA2-TMC nPs and NP-TMC nPs, respectively. Primary human intranasal epithelium cells (HNEpCs) were used as an in vitro model to measure immunity responses. HA2-TMC nPs, NP-TMC nPs, and HA2-NP-TMC nPs (influenza nanoparticle constructs) showed no toxicity in HNEpCs. The loading efficiency of HA2 and NP into the TMC nPs was 97.9% and 98.5%, respectively. HA2-TMC nPs and NP-TMC nPs more efficiently delivered HA2 and NP proteins to HNEpCs than soluble HA2 and NP proteins alone. The induction of various cytokines and chemokines was more evident in influenza nanoparticle construct-treated HNEpCs than in soluble protein-treated HNEpCs. In addition, soluble factors secreted by influenza nanoparticle construct-treated HNEpCs significantly induced MoDCs maturation markers (CD80, CD83, CD86 and HLA-DR), as compared to soluble factors secreted by protein-treated HNEpCs. HNEpCs treated with the influenza nanoparticle constructs significantly reduced influenza virus replication in an in vitro challenge assay. The results indicate that TMC nPs can be used as influenza vaccine adjuvants and carriers capable of delivering HA2 and NP proteins to HNEpCs.https://doi.org/10.1371/journal.pone.0237218
collection DOAJ
language English
format Article
sources DOAJ
author Kamonthip Rungrojcharoenkit
Panya Sunintaboon
Damon Ellison
Louis Macareo
Panuwat Midoeng
Preamrudee Chaisuwirat
Stefan Fernandez
Sukathida Ubol
spellingShingle Kamonthip Rungrojcharoenkit
Panya Sunintaboon
Damon Ellison
Louis Macareo
Panuwat Midoeng
Preamrudee Chaisuwirat
Stefan Fernandez
Sukathida Ubol
Development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.
PLoS ONE
author_facet Kamonthip Rungrojcharoenkit
Panya Sunintaboon
Damon Ellison
Louis Macareo
Panuwat Midoeng
Preamrudee Chaisuwirat
Stefan Fernandez
Sukathida Ubol
author_sort Kamonthip Rungrojcharoenkit
title Development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.
title_short Development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.
title_full Development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.
title_fullStr Development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.
title_full_unstemmed Development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.
title_sort development of an adjuvanted nanoparticle vaccine against influenza virus, an in vitro study.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2020-01-01
description Influenza is an infectious respiratory illness caused by influenza viruses. Despite yearly updates, the efficacy of influenza vaccines is significantly curtailed by the virus antigenic drift and antigenic shift. These constant changes to the influenza virus make-up also challenge the development of a universal flu vaccine, which requires conserved antigenic regions shared by influenza viruses of different subtypes. We propose that it is possible to bypass these challenges by the development of an influenza vaccine based on conserved proteins delivered in an adjuvanted nanoparticle system. In this study, we generated influenza nanoparticle constructs using trimethyl chitosan nanoparticles (TMC nPs) as the carrier of recombinant influenza hemagglutinin subunit 2 (HA2) and nucleoprotein (NP). The purified HA2 and NP recombinant proteins were encapsulated into TMC nPs to form HA2-TMC nPs and NP-TMC nPs, respectively. Primary human intranasal epithelium cells (HNEpCs) were used as an in vitro model to measure immunity responses. HA2-TMC nPs, NP-TMC nPs, and HA2-NP-TMC nPs (influenza nanoparticle constructs) showed no toxicity in HNEpCs. The loading efficiency of HA2 and NP into the TMC nPs was 97.9% and 98.5%, respectively. HA2-TMC nPs and NP-TMC nPs more efficiently delivered HA2 and NP proteins to HNEpCs than soluble HA2 and NP proteins alone. The induction of various cytokines and chemokines was more evident in influenza nanoparticle construct-treated HNEpCs than in soluble protein-treated HNEpCs. In addition, soluble factors secreted by influenza nanoparticle construct-treated HNEpCs significantly induced MoDCs maturation markers (CD80, CD83, CD86 and HLA-DR), as compared to soluble factors secreted by protein-treated HNEpCs. HNEpCs treated with the influenza nanoparticle constructs significantly reduced influenza virus replication in an in vitro challenge assay. The results indicate that TMC nPs can be used as influenza vaccine adjuvants and carriers capable of delivering HA2 and NP proteins to HNEpCs.
url https://doi.org/10.1371/journal.pone.0237218
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