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Systems Biology Methods Applied to Blood and Tissue for a Comprehensive Analysis of Immune Response to Hepatitis B Vaccine in Adults
Conventional vaccine design has been based on trial-and-error approaches, which have been generally successful. However, there have been some major failures in vaccine development and we still do not have highly effective licensed vaccines for tuberculosis, HIV, respiratory syncytial virus, and othe...
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , |
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| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Frontiers Media S.A.
2020
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| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7672042/ https://www.ncbi.nlm.nih.gov/pubmed/33250895 http://dx.doi.org/10.3389/fimmu.2020.580373 |
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| author | Ben-Othman, Rym Cai, Bing Liu, Aaron C. Varankovich, Natallia He, Daniel Blimkie, Travis M. Lee, Amy H. Gill, Erin E. Novotny, Mark Aevermann, Brian Drissler, Sibyl Shannon, Casey P. McCann, Sarah Marty, Kim Bjornson, Gordean Edgar, Rachel D. Lin, David Tse Shen Gladish, Nicole Maclsaac, Julia Amenyogbe, Nelly Chan, Queenie Llibre, Alba Collin, Joyce Landais, Elise Le, Khoa Reiss, Samantha M. Koff, Wayne C. Havenar-Daughton, Colin Heran, Manraj Sangha, Bippan Walt, David Krajden, Mel Crotty, Shane Sok, Devin Briney, Bryan Burton, Dennis R. Duffy, Darragh Foster, Leonard J. Mohn, William W. Kobor, Michael S. Tebbutt, Scott J. Brinkman, Ryan R. Scheuermann, Richard H. Hancock, Robert E. W. Kollmann, Tobias R. Sadarangani, Manish |
| author_facet | Ben-Othman, Rym Cai, Bing Liu, Aaron C. Varankovich, Natallia He, Daniel Blimkie, Travis M. Lee, Amy H. Gill, Erin E. Novotny, Mark Aevermann, Brian Drissler, Sibyl Shannon, Casey P. McCann, Sarah Marty, Kim Bjornson, Gordean Edgar, Rachel D. Lin, David Tse Shen Gladish, Nicole Maclsaac, Julia Amenyogbe, Nelly Chan, Queenie Llibre, Alba Collin, Joyce Landais, Elise Le, Khoa Reiss, Samantha M. Koff, Wayne C. Havenar-Daughton, Colin Heran, Manraj Sangha, Bippan Walt, David Krajden, Mel Crotty, Shane Sok, Devin Briney, Bryan Burton, Dennis R. Duffy, Darragh Foster, Leonard J. Mohn, William W. Kobor, Michael S. Tebbutt, Scott J. Brinkman, Ryan R. Scheuermann, Richard H. Hancock, Robert E. W. Kollmann, Tobias R. Sadarangani, Manish |
| author_sort | Ben-Othman, Rym |
| collection | PubMed |
| description | Conventional vaccine design has been based on trial-and-error approaches, which have been generally successful. However, there have been some major failures in vaccine development and we still do not have highly effective licensed vaccines for tuberculosis, HIV, respiratory syncytial virus, and other major infections of global significance. Approaches at rational vaccine design have been limited by our understanding of the immune response to vaccination at the molecular level. Tools now exist to undertake in-depth analysis using systems biology approaches, but to be fully realized, studies are required in humans with intensive blood and tissue sampling. Methods that support this intensive sampling need to be developed and validated as feasible. To this end, we describe here a detailed approach that was applied in a study of 15 healthy adults, who were immunized with hepatitis B vaccine. Sampling included ~350 mL of blood, 12 microbiome samples, and lymph node fine needle aspirates obtained over a ~7-month period, enabling comprehensive analysis of the immune response at the molecular level, including single cell and tissue sample analysis. Samples were collected for analysis of immune phenotyping, whole blood and single cell gene expression, proteomics, lipidomics, epigenetics, whole blood response to key immune stimuli, cytokine responses, in vitro T cell responses, antibody repertoire analysis and the microbiome. Data integration was undertaken using different approaches—NetworkAnalyst and DIABLO. Our results demonstrate that such intensive sampling studies are feasible in healthy adults, and data integration tools exist to analyze the vast amount of data generated from a multi-omics systems biology approach. This will provide the basis for a better understanding of vaccine-induced immunity and accelerate future rational vaccine design. |
| format | Online Article Text |
| id | pubmed-7672042 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2020 |
| publisher | Frontiers Media S.A. |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-76720422020-11-26 Systems Biology Methods Applied to Blood and Tissue for a Comprehensive Analysis of Immune Response to Hepatitis B Vaccine in Adults Ben-Othman, Rym Cai, Bing Liu, Aaron C. Varankovich, Natallia He, Daniel Blimkie, Travis M. Lee, Amy H. Gill, Erin E. Novotny, Mark Aevermann, Brian Drissler, Sibyl Shannon, Casey P. McCann, Sarah Marty, Kim Bjornson, Gordean Edgar, Rachel D. Lin, David Tse Shen Gladish, Nicole Maclsaac, Julia Amenyogbe, Nelly Chan, Queenie Llibre, Alba Collin, Joyce Landais, Elise Le, Khoa Reiss, Samantha M. Koff, Wayne C. Havenar-Daughton, Colin Heran, Manraj Sangha, Bippan Walt, David Krajden, Mel Crotty, Shane Sok, Devin Briney, Bryan Burton, Dennis R. Duffy, Darragh Foster, Leonard J. Mohn, William W. Kobor, Michael S. Tebbutt, Scott J. Brinkman, Ryan R. Scheuermann, Richard H. Hancock, Robert E. W. Kollmann, Tobias R. Sadarangani, Manish Front Immunol Immunology Conventional vaccine design has been based on trial-and-error approaches, which have been generally successful. However, there have been some major failures in vaccine development and we still do not have highly effective licensed vaccines for tuberculosis, HIV, respiratory syncytial virus, and other major infections of global significance. Approaches at rational vaccine design have been limited by our understanding of the immune response to vaccination at the molecular level. Tools now exist to undertake in-depth analysis using systems biology approaches, but to be fully realized, studies are required in humans with intensive blood and tissue sampling. Methods that support this intensive sampling need to be developed and validated as feasible. To this end, we describe here a detailed approach that was applied in a study of 15 healthy adults, who were immunized with hepatitis B vaccine. Sampling included ~350 mL of blood, 12 microbiome samples, and lymph node fine needle aspirates obtained over a ~7-month period, enabling comprehensive analysis of the immune response at the molecular level, including single cell and tissue sample analysis. Samples were collected for analysis of immune phenotyping, whole blood and single cell gene expression, proteomics, lipidomics, epigenetics, whole blood response to key immune stimuli, cytokine responses, in vitro T cell responses, antibody repertoire analysis and the microbiome. Data integration was undertaken using different approaches—NetworkAnalyst and DIABLO. Our results demonstrate that such intensive sampling studies are feasible in healthy adults, and data integration tools exist to analyze the vast amount of data generated from a multi-omics systems biology approach. This will provide the basis for a better understanding of vaccine-induced immunity and accelerate future rational vaccine design. Frontiers Media S.A. 2020-11-04 /pmc/articles/PMC7672042/ /pubmed/33250895 http://dx.doi.org/10.3389/fimmu.2020.580373 Text en Copyright © 2020 Ben-Othman, Cai, Liu, Varankovich, He, Blimkie, Lee, Gill, Novotny, Aevermann, Drissler, Shannon, McCann, Marty, Bjornson, Edgar, Lin, Gladish, Maclsaac, Amenyogbe, Chan, Llibre, Collin, Landais, Le, Reiss, Koff, Havenar-Daughton, Heran, Sangha, Walt, Krajden, Crotty, Sok, Briney, Burton, Duffy, Foster, Mohn, Kobor, Tebbutt, Brinkman, Scheuermann, Hancock, Kollmann and Sadarangani http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms. |
| spellingShingle | Immunology Ben-Othman, Rym Cai, Bing Liu, Aaron C. Varankovich, Natallia He, Daniel Blimkie, Travis M. Lee, Amy H. Gill, Erin E. Novotny, Mark Aevermann, Brian Drissler, Sibyl Shannon, Casey P. McCann, Sarah Marty, Kim Bjornson, Gordean Edgar, Rachel D. Lin, David Tse Shen Gladish, Nicole Maclsaac, Julia Amenyogbe, Nelly Chan, Queenie Llibre, Alba Collin, Joyce Landais, Elise Le, Khoa Reiss, Samantha M. Koff, Wayne C. Havenar-Daughton, Colin Heran, Manraj Sangha, Bippan Walt, David Krajden, Mel Crotty, Shane Sok, Devin Briney, Bryan Burton, Dennis R. Duffy, Darragh Foster, Leonard J. Mohn, William W. Kobor, Michael S. Tebbutt, Scott J. Brinkman, Ryan R. Scheuermann, Richard H. Hancock, Robert E. W. Kollmann, Tobias R. Sadarangani, Manish Systems Biology Methods Applied to Blood and Tissue for a Comprehensive Analysis of Immune Response to Hepatitis B Vaccine in Adults |
| title | Systems Biology Methods Applied to Blood and Tissue for a Comprehensive Analysis of Immune Response to Hepatitis B Vaccine in Adults |
| title_full | Systems Biology Methods Applied to Blood and Tissue for a Comprehensive Analysis of Immune Response to Hepatitis B Vaccine in Adults |
| title_fullStr | Systems Biology Methods Applied to Blood and Tissue for a Comprehensive Analysis of Immune Response to Hepatitis B Vaccine in Adults |
| title_full_unstemmed | Systems Biology Methods Applied to Blood and Tissue for a Comprehensive Analysis of Immune Response to Hepatitis B Vaccine in Adults |
| title_short | Systems Biology Methods Applied to Blood and Tissue for a Comprehensive Analysis of Immune Response to Hepatitis B Vaccine in Adults |
| title_sort | systems biology methods applied to blood and tissue for a comprehensive analysis of immune response to hepatitis b vaccine in adults |
| topic | Immunology |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7672042/ https://www.ncbi.nlm.nih.gov/pubmed/33250895 http://dx.doi.org/10.3389/fimmu.2020.580373 |
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