CovidV2, Main, Exploration, bibRecord, 001764

Development of nonhuman adenoviruses as vaccine vectors

Identifieur interne : 001764 ( Main/Exploration ); précédent : 001763; suivant : 001765

Development of nonhuman adenoviruses as vaccine vectors

Auteurs : Dinesh S. Bangari ; Suresh K. Mittal

Source :

Vaccine [ 0264-410X ] ; 2005.

RBID : PMC:1462960

Abstract

Human adenoviral (HAd) vectors have demonstrated great potential as vaccine vectors. Preclinical and clinical studies have demonstrated the feasibility of vector design, robust antigen expression and protective immunity using this system. However, clinical use of adenoviral vectors for vaccine purposes is anticipated to be limited by vector immunity that is either preexisting or develops rapidly following the first inoculation with adenoviral vectors. Vector immunity inactivates the vector particles and rapidly removes the transduced cells, thereby limiting the duration of transgene expression. Due to strong vector immunity, subsequent use of the same vector is usually less efficient. In order to circumvent this limitation, nonhuman adenoviral vectors have been proposed as alternative vectors. In addition to eluding HAd immunity, these vectors possess most of the attractive features of HAd vectors. Several replication-competent or replication-defective nonhuman adenoviral vectors have been developed and investigated for their potential as vaccine delivery vectors. Here, we review recent advances in the design and characterization of various nonhuman adenoviral vectors, and discuss their potential applications for human and animal vaccination.

Url:

http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1462960

DOI: 10.1016/j.vaccine.2005.08.101
PubMed: 16297508
PubMed Central: 1462960

Affiliations:

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<front><div type="abstract" xml:lang="en"><p id="P1">Human adenoviral (HAd) vectors have demonstrated great potential as vaccine vectors. Preclinical and clinical studies have demonstrated the feasibility of vector design, robust antigen expression and protective immunity using this system. However, clinical use of adenoviral vectors for vaccine purposes is anticipated to be limited by vector immunity that is either preexisting or develops rapidly following the first inoculation with adenoviral vectors. Vector immunity inactivates the vector particles and rapidly removes the transduced cells, thereby limiting the duration of transgene expression. Due to strong vector immunity, subsequent use of the same vector is usually less efficient. In order to circumvent this limitation, nonhuman adenoviral vectors have been proposed as alternative vectors. In addition to eluding HAd immunity, these vectors possess most of the attractive features of HAd vectors. Several replication-competent or replication-defective nonhuman adenoviral vectors have been developed and investigated for their potential as vaccine delivery vectors. Here, we review recent advances in the design and characterization of various nonhuman adenoviral vectors, and discuss their potential applications for human and animal vaccination.</p>
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Development of nonhuman adenoviruses as vaccine vectors

Development of nonhuman adenoviruses as vaccine vectors

Source :

Abstract

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Le document en format XML

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Pour générer des pages wiki

	Serveur d'exploration Covid (26 mars)
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