Pre-existing vector immunity does not prevent replication deficient adenovirus from inducing efficient CD8 T-cell memory and recall responses

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Pre-existing vector immunity does not prevent replication deficient adenovirus from inducing efficient CD8 T-cell memory and recall responses. / Steffensen, Maria Abildgaard; Jensen, Benjamin Anderschou Holbech; Holst, Peter Johannes; Bassi, Maria Rosaria; Christensen, Jan Pravsgaard; Thomsen, Allan Randrup.

In: P L o S One, Vol. 7, No. 4, e34884, 04.2012.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Steffensen, MA, Jensen, BAH, Holst, PJ, Bassi, MR, Christensen, JP & Thomsen, AR 2012, 'Pre-existing vector immunity does not prevent replication deficient adenovirus from inducing efficient CD8 T-cell memory and recall responses', P L o S One, vol. 7, no. 4, e34884. https://doi.org/10.1371/journal.pone.0034884

APA

Steffensen, M. A., Jensen, B. A. H., Holst, P. J., Bassi, M. R., Christensen, J. P., & Thomsen, A. R. (2012). Pre-existing vector immunity does not prevent replication deficient adenovirus from inducing efficient CD8 T-cell memory and recall responses. P L o S One, 7(4), [e34884]. https://doi.org/10.1371/journal.pone.0034884

Vancouver

Steffensen MA, Jensen BAH, Holst PJ, Bassi MR, Christensen JP, Thomsen AR. Pre-existing vector immunity does not prevent replication deficient adenovirus from inducing efficient CD8 T-cell memory and recall responses. P L o S One. 2012 Apr;7(4). e34884. https://doi.org/10.1371/journal.pone.0034884

Author

Steffensen, Maria Abildgaard ; Jensen, Benjamin Anderschou Holbech ; Holst, Peter Johannes ; Bassi, Maria Rosaria ; Christensen, Jan Pravsgaard ; Thomsen, Allan Randrup. / Pre-existing vector immunity does not prevent replication deficient adenovirus from inducing efficient CD8 T-cell memory and recall responses. In: P L o S One. 2012 ; Vol. 7, No. 4.

Bibtex

@article{83e48c898bcb4cebbf471678e8801482,
title = "Pre-existing vector immunity does not prevent replication deficient adenovirus from inducing efficient CD8 T-cell memory and recall responses",
abstract = "Adenoviral vectors have shown a great potential for vaccine development due to their inherent ability to induce potent and protective CD8 T-cell responses. However, a critical issue regarding the use of these vectors is the existence of inhibitory immunity against the most commonly used Ad5 vector in a large part of the human population. We have recently developed an improved adenoviral vaccine vector system in which the vector expresses the transgene tethered to the MHC class II associated invariant chain (Ii). To further evaluate the potential of this system, the concept of pre-existing inhibitory immunity to adenoviral vectors was revisited to investigate whether the inhibition previously seen with the Ad5 vector also applied to the optimized vector system. We found this to be the case, and antibodies dominated as the mechanism underlying inhibitory vector immunity. However, presence of CD8 T cells directed against epitopes in the adenoviral vector seemed to correlate with repression of the induced response in re-vaccinated B-cell deficient mice. More importantly, despite a repressed primary effector CD8 T-cell response in Ad5-immune animals subjected to vaccination, memory T cells were generated that provided the foundation for an efficient recall response and protection upon subsequent viral challenge. Furthermore, the transgene specific response could be efficiently boosted by homologous re-immunization. Taken together, these studies indicate that adenoviral vectors can be used to induce efficient CD8 T-cell memory even in individuals with pre-existing vector immunity.",
author = "Steffensen, {Maria Abildgaard} and Jensen, {Benjamin Anderschou Holbech} and Holst, {Peter Johannes} and Bassi, {Maria Rosaria} and Christensen, {Jan Pravsgaard} and Thomsen, {Allan Randrup}",
year = "2012",
month = apr,
doi = "10.1371/journal.pone.0034884",
language = "English",
volume = "7",
journal = "PLoS ONE",
issn = "1932-6203",
publisher = "Public Library of Science",
number = "4",

}

RIS

TY - JOUR

T1 - Pre-existing vector immunity does not prevent replication deficient adenovirus from inducing efficient CD8 T-cell memory and recall responses

AU - Steffensen, Maria Abildgaard

AU - Jensen, Benjamin Anderschou Holbech

AU - Holst, Peter Johannes

AU - Bassi, Maria Rosaria

AU - Christensen, Jan Pravsgaard

AU - Thomsen, Allan Randrup

PY - 2012/4

Y1 - 2012/4

N2 - Adenoviral vectors have shown a great potential for vaccine development due to their inherent ability to induce potent and protective CD8 T-cell responses. However, a critical issue regarding the use of these vectors is the existence of inhibitory immunity against the most commonly used Ad5 vector in a large part of the human population. We have recently developed an improved adenoviral vaccine vector system in which the vector expresses the transgene tethered to the MHC class II associated invariant chain (Ii). To further evaluate the potential of this system, the concept of pre-existing inhibitory immunity to adenoviral vectors was revisited to investigate whether the inhibition previously seen with the Ad5 vector also applied to the optimized vector system. We found this to be the case, and antibodies dominated as the mechanism underlying inhibitory vector immunity. However, presence of CD8 T cells directed against epitopes in the adenoviral vector seemed to correlate with repression of the induced response in re-vaccinated B-cell deficient mice. More importantly, despite a repressed primary effector CD8 T-cell response in Ad5-immune animals subjected to vaccination, memory T cells were generated that provided the foundation for an efficient recall response and protection upon subsequent viral challenge. Furthermore, the transgene specific response could be efficiently boosted by homologous re-immunization. Taken together, these studies indicate that adenoviral vectors can be used to induce efficient CD8 T-cell memory even in individuals with pre-existing vector immunity.

AB - Adenoviral vectors have shown a great potential for vaccine development due to their inherent ability to induce potent and protective CD8 T-cell responses. However, a critical issue regarding the use of these vectors is the existence of inhibitory immunity against the most commonly used Ad5 vector in a large part of the human population. We have recently developed an improved adenoviral vaccine vector system in which the vector expresses the transgene tethered to the MHC class II associated invariant chain (Ii). To further evaluate the potential of this system, the concept of pre-existing inhibitory immunity to adenoviral vectors was revisited to investigate whether the inhibition previously seen with the Ad5 vector also applied to the optimized vector system. We found this to be the case, and antibodies dominated as the mechanism underlying inhibitory vector immunity. However, presence of CD8 T cells directed against epitopes in the adenoviral vector seemed to correlate with repression of the induced response in re-vaccinated B-cell deficient mice. More importantly, despite a repressed primary effector CD8 T-cell response in Ad5-immune animals subjected to vaccination, memory T cells were generated that provided the foundation for an efficient recall response and protection upon subsequent viral challenge. Furthermore, the transgene specific response could be efficiently boosted by homologous re-immunization. Taken together, these studies indicate that adenoviral vectors can be used to induce efficient CD8 T-cell memory even in individuals with pre-existing vector immunity.

U2 - 10.1371/journal.pone.0034884

DO - 10.1371/journal.pone.0034884

M3 - Journal article

C2 - 22514686

VL - 7

JO - PLoS ONE

JF - PLoS ONE

SN - 1932-6203

IS - 4

M1 - e34884

ER -

ID: 38493707