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Architectural insight into inovirus-associated vectors (IAVs) and development of IAV-based vaccines inducing humoral and cellular responses: Implications in HIV-1 vaccines

dc.contributor.authorHassapis, K. A.en
dc.contributor.authorStylianou, Dora C.en
dc.contributor.authorKostrikis, Leontios G.en
dc.creatorHassapis, K. A.en
dc.creatorStylianou, Dora C.en
dc.creatorKostrikis, Leontios G.en
dc.date.accessioned2019-11-04T12:50:41Z
dc.date.available2019-11-04T12:50:41Z
dc.date.issued2014
dc.identifier.issn1999-4915
dc.identifier.urihttp://gnosis.library.ucy.ac.cy/handle/7/53124
dc.description.abstractInovirus-associated vectors (IAVs) are engineered, non-lytic, filamentous bacteriophages that are assembled primarily from thousands of copies of the major coat protein gp8 and just five copies of each of the four minor coat proteins gp3, gp6, gp7 and gp9. Inovirus display studies have shown that the architecture of inoviruses makes all coat proteins of the inoviral particle accessible to the outside. This particular feature of IAVs allows foreign antigenic peptides to be displayed on the outer surface of the virion fused to its coat proteins and for more than two decades has been exploited in many applications including antibody or peptide display libraries, drug design, and vaccine development against infectious and non-infectious diseases. As vaccine carriers, IAVs have been shown to elicit both a cellular and humoral response against various pathogens through the display of antibody epitopes on their coat proteins. Despite their high immunogenicity, the goal of developing an effective vaccine against HIV-1 has not yet materialized. One possible limitation of previous efforts was the use of broadly neutralizing antibodies, which exhibited autoreactivity properties. In the past five years, however, new, more potent broadly neutralizing antibodies that do not exhibit autoreactivity properties have been isolated from HIV-1 infected individuals, suggesting that vaccination strategies aimed at producing such broadly neutralizing antibodies may confer protection against infection. The utilization of these new, broadly neutralizing antibodies in combination with the architectural traits of IAVs have driven the current developments in the design of an inovirus-based vaccine against HIV-1. This article reviews the applications of IAVs in vaccine development, with particular emphasis on the design of inoviral-based vaccines against HIV-1. © 2014 by the authorsen
dc.description.abstractlicensee MDPI, Basel, Switzerland.en
dc.sourceVirusesen
dc.source.urihttps://www.scopus.com/inward/record.uri?eid=2-s2.0-84919354166&doi=10.3390%2fv6125047&partnerID=40&md5=4a6d1e9395ef67838dc4598dbb849dd5
dc.subjectReviewen
dc.subjecthumanen
dc.subjectHumansen
dc.subjectHuman immunodeficiency virus infectionen
dc.subjectamino acid sequenceen
dc.subjectmonoclonal antibodyen
dc.subjectunclassified drugen
dc.subjectHIV Infectionsen
dc.subjectcellular immunityen
dc.subjectnonhumanen
dc.subjectvasculotropinen
dc.subjectmetabolismen
dc.subjectpolyclonal antibodyen
dc.subjectCD4+ T lymphocyteen
dc.subjectimmunologyen
dc.subjectAnimalsen
dc.subjectanimalen
dc.subjectT lymphocyte activationen
dc.subjectgeneticsen
dc.subjectmajor histocompatibility antigen class 1en
dc.subjectmajor histocompatibility antigen class 2en
dc.subjectHuman immunodeficiency virus antibodyen
dc.subjectCD8+ T lymphocyteen
dc.subjectvirologyen
dc.subjectphase 3 clinical trial (topic)en
dc.subjectchemistryen
dc.subjectHuman immunodeficiency virus 1en
dc.subjectHIV-1en
dc.subjectvirus replicationen
dc.subjectnucleotide sequenceen
dc.subjectDNA sequenceen
dc.subjectantigen expressionen
dc.subjectvaccinationen
dc.subjecthumoral immunityen
dc.subjectGenetic Vectorsen
dc.subjectvirus vectoren
dc.subjectphase 1 clinical trial (topic)en
dc.subjectphase 2 clinical trial (topic)en
dc.subjectneutralizing antibodyen
dc.subjectHuman immunodeficiency virus vaccineen
dc.subjectvirus pathogenesisen
dc.subjectbacteriophageen
dc.subjectprotein structureen
dc.subjectgene vectoren
dc.subjectAIDS Vaccinesen
dc.subjectglycoprotein gp 120en
dc.subjectglycoprotein gp 41en
dc.subjectimmunogenicityen
dc.subjectscanning transmission electron microscopyen
dc.subjectViral vectorsen
dc.subjectadenovirus vectoren
dc.subjectantibody and immunoglobulin productionen
dc.subjectAntigen displayen
dc.subjectcapsid proteinen
dc.subjectcoat proteinen
dc.subjectepitopeen
dc.subjectFilamentous bacteriophageen
dc.subjectHIV-1 vaccineen
dc.subjectImmunity, Cellularen
dc.subjectImmunity, Humoralen
dc.subjectimmunological toleranceen
dc.subjectinoviridae vaccineen
dc.subjectInovirusen
dc.subjectInovirus displayen
dc.subjectInovirus-associated vectorsen
dc.subjectmelanoma antigen 1en
dc.subjectPhage displayen
dc.subjectprotein DNA bindingen
dc.subjectsecondary immune responseen
dc.subjectsingle stranded DNA binding proteinen
dc.subjecttranscription terminationen
dc.subjectvirus glycoproteinen
dc.subjectvirus neutralizationen
dc.titleArchitectural insight into inovirus-associated vectors (IAVs) and development of IAV-based vaccines inducing humoral and cellular responses: Implications in HIV-1 vaccinesen
dc.typeinfo:eu-repo/semantics/article
dc.identifier.doi10.3390/v6125047
dc.description.volume6
dc.description.startingpage5047
dc.description.endingpage5076
dc.author.facultyΣχολή Θετικών και Εφαρμοσμένων Επιστημών / Faculty of Pure and Applied Sciences
dc.author.departmentΤμήμα Βιολογικών Επιστημών / Department of Biological Sciences
dc.type.uhtypeArticleen
dc.source.abbreviationVirusesen
dc.contributor.orcidKostrikis, Leontios G. [0000-0002-5340-7109]
dc.contributor.orcidStylianou, Dora C. [0000-0003-4167-1380]
dc.gnosis.orcid0000-0002-5340-7109


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