System Vaccinology for the Evaluation of Influenza Vaccine Safety by Multiplex Gene Detection of Novel Biomarkers in a Preclinical Study and Batch Release Test

Vaccines are beneficial and universal tools to prevent infectious disease. Thus, safety of vaccines is strictly evaluated in the preclinical phase of trials and every vaccine batch must be tested by the National Control Laboratories according to the guidelines published by each country. Despite many...

Descripción completa

Detalles Bibliográficos
Autores principales: Mizukami, Takuo, Momose, Haruka, Kuramitsu, Madoka, Takizawa, Kazuya, Araki, Kumiko, Furuhata, Keiko, Ishii, Ken J., Hamaguchi, Isao, Yamaguchi, Kazunari
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4092028/
https://www.ncbi.nlm.nih.gov/pubmed/25010690
http://dx.doi.org/10.1371/journal.pone.0101835
_version_ 1782480825003016192
author Mizukami, Takuo
Momose, Haruka
Kuramitsu, Madoka
Takizawa, Kazuya
Araki, Kumiko
Furuhata, Keiko
Ishii, Ken J.
Hamaguchi, Isao
Yamaguchi, Kazunari
author_facet Mizukami, Takuo
Momose, Haruka
Kuramitsu, Madoka
Takizawa, Kazuya
Araki, Kumiko
Furuhata, Keiko
Ishii, Ken J.
Hamaguchi, Isao
Yamaguchi, Kazunari
author_sort Mizukami, Takuo
collection PubMed
description Vaccines are beneficial and universal tools to prevent infectious disease. Thus, safety of vaccines is strictly evaluated in the preclinical phase of trials and every vaccine batch must be tested by the National Control Laboratories according to the guidelines published by each country. Despite many vaccine production platforms and methods, animal testing for safety evaluation is unchanged thus far. We recently developed a systems biological approach to vaccine safety evaluation where identification of specific biomarkers in a rat pre-clinical study evaluated the safety of vaccines for pandemic H5N1 influenza including Irf7, Lgals9, Lgalsbp3, Cxcl11, Timp1, Tap2, Psmb9, Psme1, Tapbp, C2, Csf1, Mx2, Zbp1, Ifrd1, Trafd1, Cxcl9, β2m, Npc1, Ngfr and Ifi47. The current study evaluated whether these 20 biomarkers could evaluate the safety, batch-to-batch and manufacturer-to-manufacturer consistency of seasonal trivalent influenza vaccine using a multiplex gene detection system. When we evaluated the influenza HA vaccine (HAv) from four different manufactures, the biomarker analysis correlated to findings from conventional animal use tests, such as abnormal toxicity test. In addition, sensitivity of toxicity detection and differences in HAvs were higher and more accurate than with conventional methods. Despite a slight decrease in body weight caused by HAv from manufacturer B that was not statistically significant, our results suggest that HAv from manufacturer B is significantly different than the other HAvs tested with regard to Lgals3bp, Tapbp, Lgals9, Irf7 and C2 gene expression in rat lungs. Using the biomarkers confirmed in this study, we predicted batch-to-batch consistency and safety of influenza vaccines within 2 days compared with the conventional safety test, which takes longer. These biomarkers will facilitate the future development of new influenza vaccines and provide an opportunity to develop in vitro methods of evaluating batch-to-batch consistency and vaccine safety as an alternative to animal testing.
format Online
Article
Text
id pubmed-4092028
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-40920282014-07-18 System Vaccinology for the Evaluation of Influenza Vaccine Safety by Multiplex Gene Detection of Novel Biomarkers in a Preclinical Study and Batch Release Test Mizukami, Takuo Momose, Haruka Kuramitsu, Madoka Takizawa, Kazuya Araki, Kumiko Furuhata, Keiko Ishii, Ken J. Hamaguchi, Isao Yamaguchi, Kazunari PLoS One Research Article Vaccines are beneficial and universal tools to prevent infectious disease. Thus, safety of vaccines is strictly evaluated in the preclinical phase of trials and every vaccine batch must be tested by the National Control Laboratories according to the guidelines published by each country. Despite many vaccine production platforms and methods, animal testing for safety evaluation is unchanged thus far. We recently developed a systems biological approach to vaccine safety evaluation where identification of specific biomarkers in a rat pre-clinical study evaluated the safety of vaccines for pandemic H5N1 influenza including Irf7, Lgals9, Lgalsbp3, Cxcl11, Timp1, Tap2, Psmb9, Psme1, Tapbp, C2, Csf1, Mx2, Zbp1, Ifrd1, Trafd1, Cxcl9, β2m, Npc1, Ngfr and Ifi47. The current study evaluated whether these 20 biomarkers could evaluate the safety, batch-to-batch and manufacturer-to-manufacturer consistency of seasonal trivalent influenza vaccine using a multiplex gene detection system. When we evaluated the influenza HA vaccine (HAv) from four different manufactures, the biomarker analysis correlated to findings from conventional animal use tests, such as abnormal toxicity test. In addition, sensitivity of toxicity detection and differences in HAvs were higher and more accurate than with conventional methods. Despite a slight decrease in body weight caused by HAv from manufacturer B that was not statistically significant, our results suggest that HAv from manufacturer B is significantly different than the other HAvs tested with regard to Lgals3bp, Tapbp, Lgals9, Irf7 and C2 gene expression in rat lungs. Using the biomarkers confirmed in this study, we predicted batch-to-batch consistency and safety of influenza vaccines within 2 days compared with the conventional safety test, which takes longer. These biomarkers will facilitate the future development of new influenza vaccines and provide an opportunity to develop in vitro methods of evaluating batch-to-batch consistency and vaccine safety as an alternative to animal testing. Public Library of Science 2014-07-10 /pmc/articles/PMC4092028/ /pubmed/25010690 http://dx.doi.org/10.1371/journal.pone.0101835 Text en © 2014 Mizukami 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
Mizukami, Takuo
Momose, Haruka
Kuramitsu, Madoka
Takizawa, Kazuya
Araki, Kumiko
Furuhata, Keiko
Ishii, Ken J.
Hamaguchi, Isao
Yamaguchi, Kazunari
System Vaccinology for the Evaluation of Influenza Vaccine Safety by Multiplex Gene Detection of Novel Biomarkers in a Preclinical Study and Batch Release Test
title System Vaccinology for the Evaluation of Influenza Vaccine Safety by Multiplex Gene Detection of Novel Biomarkers in a Preclinical Study and Batch Release Test
title_full System Vaccinology for the Evaluation of Influenza Vaccine Safety by Multiplex Gene Detection of Novel Biomarkers in a Preclinical Study and Batch Release Test
title_fullStr System Vaccinology for the Evaluation of Influenza Vaccine Safety by Multiplex Gene Detection of Novel Biomarkers in a Preclinical Study and Batch Release Test
title_full_unstemmed System Vaccinology for the Evaluation of Influenza Vaccine Safety by Multiplex Gene Detection of Novel Biomarkers in a Preclinical Study and Batch Release Test
title_short System Vaccinology for the Evaluation of Influenza Vaccine Safety by Multiplex Gene Detection of Novel Biomarkers in a Preclinical Study and Batch Release Test
title_sort system vaccinology for the evaluation of influenza vaccine safety by multiplex gene detection of novel biomarkers in a preclinical study and batch release test
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4092028/
https://www.ncbi.nlm.nih.gov/pubmed/25010690
http://dx.doi.org/10.1371/journal.pone.0101835
work_keys_str_mv AT mizukamitakuo systemvaccinologyfortheevaluationofinfluenzavaccinesafetybymultiplexgenedetectionofnovelbiomarkersinapreclinicalstudyandbatchreleasetest
AT momoseharuka systemvaccinologyfortheevaluationofinfluenzavaccinesafetybymultiplexgenedetectionofnovelbiomarkersinapreclinicalstudyandbatchreleasetest
AT kuramitsumadoka systemvaccinologyfortheevaluationofinfluenzavaccinesafetybymultiplexgenedetectionofnovelbiomarkersinapreclinicalstudyandbatchreleasetest
AT takizawakazuya systemvaccinologyfortheevaluationofinfluenzavaccinesafetybymultiplexgenedetectionofnovelbiomarkersinapreclinicalstudyandbatchreleasetest
AT arakikumiko systemvaccinologyfortheevaluationofinfluenzavaccinesafetybymultiplexgenedetectionofnovelbiomarkersinapreclinicalstudyandbatchreleasetest
AT furuhatakeiko systemvaccinologyfortheevaluationofinfluenzavaccinesafetybymultiplexgenedetectionofnovelbiomarkersinapreclinicalstudyandbatchreleasetest
AT ishiikenj systemvaccinologyfortheevaluationofinfluenzavaccinesafetybymultiplexgenedetectionofnovelbiomarkersinapreclinicalstudyandbatchreleasetest
AT hamaguchiisao systemvaccinologyfortheevaluationofinfluenzavaccinesafetybymultiplexgenedetectionofnovelbiomarkersinapreclinicalstudyandbatchreleasetest
AT yamaguchikazunari systemvaccinologyfortheevaluationofinfluenzavaccinesafetybymultiplexgenedetectionofnovelbiomarkersinapreclinicalstudyandbatchreleasetest

Ejemplares similares