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429 results on '"Dekker, Cornelia L."'

1. KIR+CD8+ T cells suppress pathogenic T cells and are active in autoimmune diseases and COVID-19

Author

Li, Jing, Zaslavsky, Maxim, Su, Yapeng, Guo, Jing, Sikora, Michael J, van Unen, Vincent, Christophersen, Asbjørn, Chiou, Shin-Heng, Chen, Liang, Li, Jiefu, Ji, Xuhuai, Wilhelmy, Julie, McSween, Alana M, Palanski, Brad A, Mallajosyula, Venkata Vamsee Aditya, Bracey, Nathan A, Dhondalay, Gopal Krishna R, Bhamidipati, Kartik, Pai, Joy, Kipp, Lucas B, Dunn, Jeffrey E, Hauser, Stephen L, Oksenberg, Jorge R, Satpathy, Ansuman T, Robinson, William H, Dekker, Cornelia L, Steinmetz, Lars M, Khosla, Chaitan, Utz, Paul J, Sollid, Ludvig M, Chien, Yueh-Hsiu, Heath, James R, Fernandez-Becker, Nielsen Q, Nadeau, Kari C, Saligrama, Naresha, and Davis, Mark M

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Immunology, Autoimmune Disease, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Good Health and Well Being, Animals, Autoimmune Diseases, CD8-Positive T-Lymphocytes, COVID-19, Humans, Mice, Receptors, KIR, T-Lymphocytes, Regulatory, General Science & Technology
Abstract

In this work, we find that CD8+ T cells expressing inhibitory killer cell immunoglobulin-like receptors (KIRs) are the human equivalent of Ly49+CD8+ regulatory T cells in mice and are increased in the blood and inflamed tissues of patients with a variety of autoimmune diseases. Moreover, these CD8+ T cells efficiently eliminated pathogenic gliadin-specific CD4+ T cells from the leukocytes of celiac disease patients in vitro. We also find elevated levels of KIR+CD8+ T cells, but not CD4+ regulatory T cells, in COVID-19 patients, correlating with disease severity and vasculitis. Selective ablation of Ly49+CD8+ T cells in virus-infected mice led to autoimmunity after infection. Our results indicate that in both species, these regulatory CD8+ T cells act specifically to suppress pathogenic T cells in autoimmune and infectious diseases.

Published
2022

4. Continuous immunotypes describe human immune variation and predict diverse responses

Author

Kaczorowski, Kevin J, Shekhar, Karthik, Nkulikiyimfura, Dieudonné, Dekker, Cornelia L, Maecker, Holden, Davis, Mark M, Chakraborty, Arup K, and Brodin, Petter

Subjects
Biomedical and Clinical Sciences, Immunology, Clinical Research, Aging, Underpinning research, 1.1 Normal biological development and functioning, Inflammatory and immune system, Cohort Studies, Cytomegalovirus Infections, Flow Cytometry, Humans, Immune System, Immune System Phenomena, Immunity, Cellular, Leukocytes, Mononuclear, human immune variation, immune cell composition, systems immunology, aging
Abstract

The immune system consists of many specialized cell populations that communicate with each other to achieve systemic immune responses. Our analyses of various measured immune cell population frequencies in healthy humans and their responses to diverse stimuli show that human immune variation is continuous in nature, rather than characterized by discrete groups of similar individuals. We show that the same three key combinations of immune cell population frequencies can define an individual's immunotype and predict a diverse set of functional responses to cytokine stimulation. We find that, even though interindividual variations in specific cell population frequencies can be large, unrelated individuals of younger age have more homogeneous immunotypes than older individuals. Across age groups, cytomegalovirus seropositive individuals displayed immunotypes characteristic of older individuals. The conceptual framework for defining immunotypes suggested by our results could guide the development of better therapies that appropriately modulate collective immunotypes, rather than individual immune components.

Published
2017

5. An inflammatory aging clock (iAge) based on deep learning tracks multimorbidity, immunosenescence, frailty and cardiovascular aging

Author

Sayed, Nazish, Huang, Yingxiang, Nguyen, Khiem, Krejciova-Rajaniemi, Zuzana, Grawe, Anissa P., Gao, Tianxiang, Tibshirani, Robert, Hastie, Trevor, Alpert, Ayelet, Cui, Lu, Kuznetsova, Tatiana, Rosenberg-Hasson, Yael, Ostan, Rita, Monti, Daniela, Lehallier, Benoit, Shen-Orr, Shai S., Maecker, Holden T., Dekker, Cornelia L., Wyss-Coray, Tony, Franceschi, Claudio, Jojic, Vladimir, Haddad, François, Montoya, José G., Wu, Joseph C., Davis, Mark M., and Furman, David

Published
2021
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6. Molecular-level analysis of the serum antibody repertoire in young adults before and after seasonal influenza vaccination

Author

Lee, Jiwon, Boutz, Daniel R, Chromikova, Veronika, Joyce, M Gordon, Vollmers, Christopher, Leung, Kwanyee, Horton, Andrew P, DeKosky, Brandon J, Lee, Chang-Han, Lavinder, Jason J, Murrin, Ellen M, Chrysostomou, Constantine, Hoi, Kam Hon, Tsybovsky, Yaroslav, Thomas, Paul V, Druz, Aliaksandr, Zhang, Baoshan, Zhang, Yi, Wang, Lingshu, Kong, Wing-Pui, Park, Daechan, Popova, Lyubov I, Dekker, Cornelia L, Davis, Mark M, Carter, Chalise E, Ross, Ted M, Ellington, Andrew D, Wilson, Patrick C, Marcotte, Edward M, Mascola, John R, Ippolito, Gregory C, Krammer, Florian, Quake, Stephen R, Kwong, Peter D, and Georgiou, George

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Biotechnology, Infectious Diseases, Prevention, Immunization, Emerging Infectious Diseases, Pneumonia & Influenza, Vaccine Related, Influenza, Prevention of disease and conditions, and promotion of well-being, 3.4 Vaccines, Infection, Good Health and Well Being, Adult, Animals, Antibodies, Viral, B-Lymphocytes, Chromatography, Liquid, Cross Reactions, Epitopes, Female, Hemagglutinin Glycoproteins, Influenza Virus, High-Throughput Nucleotide Sequencing, Humans, Immunogenicity, Vaccine, Immunoglobulin G, Influenza A Virus, H1N1 Subtype, Influenza A Virus, H3N2 Subtype, Influenza Vaccines, Influenza, Human, Male, Mice, Orthomyxoviridae, RNA, Messenger, Receptors, Antigen, B-Cell, Sequence Analysis, RNA, Tandem Mass Spectrometry, Young Adult, Medical and Health Sciences, Immunology, Biomedical and clinical sciences, Health sciences
Abstract

Molecular understanding of serological immunity to influenza has been confounded by the complexity of the polyclonal antibody response in humans. Here we used high-resolution proteomics analysis of immunoglobulin (referred to as Ig-seq) coupled with high-throughput sequencing of transcripts encoding B cell receptors (BCR-seq) to quantitatively determine the antibody repertoire at the individual clonotype level in the sera of young adults before and after vaccination with trivalent seasonal influenza vaccine. The serum repertoire comprised between 40 and 147 clonotypes that were specific to each of the three monovalent components of the trivalent influenza vaccine, with boosted pre-existing clonotypes accounting for ∼60% of the response. An unexpectedly high fraction of serum antibodies recognized both the H1 and H3 monovalent vaccines. Recombinant versions of these H1 + H3 cross-reactive antibodies showed broad binding to hemagglutinins (HAs) from previously circulating virus strains; several of these antibodies, which were prevalent in the serum of multiple donors, recognized the same conserved epitope in the HA head domain. Although the HA-head-specific H1 + H3 antibodies did not show neutralization activity in vitro, they protected mice against infection with the H1N1 and H3N2 virus strains when administered before or after challenge. Collectively, our data reveal unanticipated insights regarding the serological response to influenza vaccination and raise questions about the added benefits of using a quadrivalent vaccine instead of a trivalent vaccine.

Published
2016

7. Defective Signaling in the JAK-STAT Pathway Tracks with Chronic Inflammation and Cardiovascular Risk in Aging Humans

Author

Shen-Orr, Shai S, Furman, David, Kidd, Brian A, Hadad, Francois, Lovelace, Patricia, Huang, Ying-Wen, Rosenberg-Hasson, Yael, Mackey, Sally, Grisar, Fatemeh A Gomari, Pickman, Yishai, Maecker, Holden T, Chien, Yueh-hsiu, Dekker, Cornelia L, Wu, Joseph C, Butte, Atul J, and Davis, Mark M

Subjects
Clinical Research, Cardiovascular, Aging, Heart Disease, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Good Health and Well Being, Cardiovascular Diseases, Cytokines, Humans, Inflammation, Interferon-gamma, Phosphorylation, Risk Factors, STAT Transcription Factors, Signal Transduction, aging, cardiovascular, cytokine responses, immune monitoring, immune signaling, immunosenescence, inflammaging, systems immunology, Biochemistry and Cell Biology
Abstract

Chronic inflammation, a decline in immune responsiveness, and reduced cardiovascular function are all associated with aging, but the relationships among these phenomena remain unclear. Here, we longitudinally profiled a total of 84 signaling conditions in 91 young and older adults and observed an age-related reduction in cytokine responsiveness within four immune cell lineages, most prominently T cells. The phenotype can be partially explained by elevated baseline levels of phosphorylated STAT (pSTAT) proteins and a different response capacity of naive versus memory T cell subsets to interleukin 6 (IL-6), interferon α (IFN-α), and, to a lesser extent, IL-21 and IFN-γ. Baseline pSTAT levels tracked with circulating levels of C-reactive protein (CRP), and we derived a cytokine response score that negatively correlates with measures of cardiovascular disease, specifically diastolic dysfunction and atherosclerotic burden, outperforming CRP. Thus, we identified an immunological link between inflammation, decreased cell responsiveness in the JAK-STAT pathway, and cardiovascular aging. Targeting chronic inflammation may ameliorate this deficiency in cellular responsiveness and improve cardiovascular function.

Published
2016

8. Lineage tracing of human B cells reveals the in vivo landscape of human antibody class switching.

Author

Horns, Felix, Vollmers, Christopher, Croote, Derek, Mackey, Sally F, Swan, Gary E, Dekker, Cornelia L, Davis, Mark M, and Quake, Stephen R

Subjects
B-Lymphocytes, Humans, Immunologic Factors, Immunoglobulin Isotypes, Sequence Analysis, DNA, Immunoglobulin Class Switching, Somatic Hypermutation, Immunoglobulin, Recombination, Genetic, antibody, cell decisions, class switching, computational biology, human, immunology, repertoire, systems biology, Recombination, Genetic, Sequence Analysis, DNA, Somatic Hypermutation, Immunoglobulin, Biochemistry and Cell Biology
Abstract

Antibody class switching is a feature of the adaptive immune system which enables diversification of the effector properties of antibodies. Even though class switching is essential for mounting a protective response to pathogens, the in vivo patterns and lineage characteristics of antibody class switching have remained uncharacterized in living humans. Here we comprehensively measured the landscape of antibody class switching in human adult twins using antibody repertoire sequencing. The map identifies how antibodies of every class are created and delineates a two-tiered hierarchy of class switch pathways. Using somatic hypermutations as a molecular clock, we discovered that closely related B cells often switch to the same class, but lose coherence as somatic mutations accumulate. Such correlations between closely related cells exist when purified B cells class switch in vitro, suggesting that class switch recombination is directed toward specific isotypes by a cell-autonomous imprinted state.

Published
2016

10. Variation in the Human Immune System Is Largely Driven by Non-Heritable Influences

Author

Brodin, Petter, Jojic, Vladimir, Gao, Tianxiang, Bhattacharya, Sanchita, Angel, Cesar J Lopez, Furman, David, Shen-Orr, Shai, Dekker, Cornelia L, Swan, Gary E, Butte, Atul J, Maecker, Holden T, and Davis, Mark M

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Infectious Diseases, Influenza, Vaccine Related, Pneumonia & Influenza, Pediatric Research Initiative, Adolescent, Adult, Aged, Aged, 80 and over, Blood Proteins, Child, Cytokines, Cytomegalovirus Infections, Humans, Immunity, Influenza Vaccines, Middle Aged, Twins, Dizygotic, Twins, Monozygotic, Young Adult, Biological Sciences, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

There is considerable heterogeneity in immunological parameters between individuals, but its sources are largely unknown. To assess the relative contribution of heritable versus non-heritable factors, we have performed a systems-level analysis of 210 healthy twins between 8 and 82 years of age. We measured 204 different parameters, including cell population frequencies, cytokine responses, and serum proteins, and found that 77% of these are dominated (>50% of variance) and 58% almost completely determined (>80% of variance) by non-heritable influences. In addition, some of these parameters become more variable with age, suggesting the cumulative influence of environmental exposure. Similarly, the serological responses to seasonal influenza vaccination are also determined largely by non-heritable factors, likely due to repeated exposure to different strains. Lastly, in MZ twins discordant for cytomegalovirus infection, more than half of all parameters are affected. These results highlight the largely reactive and adaptive nature of the immune system in healthy individuals.

Published
2015

16. Author Correction: An inflammatory aging clock (iAge) based on deep learning tracks multimorbidity, immunosenescence, frailty and cardiovascular aging

Author

Sayed, Nazish, Huang, Yingxiang, Nguyen, Khiem, Krejciova-Rajaniemi, Zuzana, Grawe, Anissa P., Gao, Tianxiang, Tibshirani, Robert, Hastie, Trevor, Alpert, Ayelet, Cui, Lu, Kuznetsova, Tatiana, Rosenberg-Hasson, Yael, Ostan, Rita, Monti, Daniela, Lehallier, Benoit, Shen-Orr, Shai S., Maecker, Holden T., Dekker, Cornelia L., Wyss-Coray, Tony, Franceschi, Claudio, Jojic, Vladimir, Haddad, François, Montoya, José G., Wu, Joseph C., Davis, Mark M., and Furman, David

Published
2021
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17. Considerations for unblinding individual study participants during vaccine trials

Author

Halsey, Neal, primary, Evans, Stephen, additional, Santosham, Mathuram, additional, Hacker, Adam, additional, Edwards, Kathryn M., additional, Chandler, Rebecca E., additional, Dudley, Matthew Z., additional, Dekker, Cornelia L., additional, Al-Abri, Seif, additional, Arora, Narendra, additional, Buttery, Jim, additional, Dodoo, Alex, additional, Eskola, Juhani, additional, Heininger, Ulrich, additional, Jee, Youngmee, additional, Khuri, Najwa, additional, Obaro, Stephen, additional, Orenstein, Walt, additional, Pitisuttithum, Punnee, additional, Safadi, Marco, additional, Whitney, Cynthia G., additional, and Black, Steve, additional

Published
2023
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20. Abstract A014: Cytokines surge in the blood years prior to a cancer diagnosis in elderly individuals

Author

Chen, Guangbo, primary, Zheng, Hong, additional, Rosenberg-Hasson, Yael, additional, Araya, Saron, additional, Padilla, Cindy, additional, Sarin, Kavita, additional, Dekker, Cornelia L., additional, Grant, Philip, additional, Maecker, Holden T., additional, Furman, David, additional, Shen-Orr, Shai, additional, Khatri, Purvesh, additional, and Davis, Mark M., additional

Published
2023
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21. Abstract PR002: Cytokines surge in the blood years prior to a cancer diagnosis in elderly individuals

Author

Chen, Guangbo, primary, Zheng, Hong, additional, Rosenberg-Hasson, Yael, additional, Araya, Saron, additional, Padilla, Cindy, additional, Sarin, Kavita, additional, Dekker, Cornelia L., additional, Grant, Philip, additional, Maecker, Holden T., additional, Furman, David, additional, Shen-Orr, Shai, additional, Khatri, Purvesh, additional, and Davis, Mark M., additional

Published
2023
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22. Expression of specific inflammasome gene modules stratifies older individuals into two extreme clinical and immunological states

Author

Furman, David, Chang, Junlei, Lartigue, Lydia, Bolen, Christopher R, Haddad, François, Gaudilliere, Brice, Ganio, Edward A, Fragiadakis, Gabriela K, Spitzer, Matthew H, Douchet, Isabelle, Daburon, Sophie, Moreau, Jean-François, Nolan, Garry P, Blanco, Patrick, Déchanet-Merville, Julie, Dekker, Cornelia L, Jojic, Vladimir, Kuo, Calvin J, Davis, Mark M, and Faustin, Benjamin

Subjects
Inflammasomes -- Health aspects, Elderly -- Genetic aspects -- Health aspects, Immune response -- Genetic aspects, Gene expression -- Health aspects, Biological sciences, Health
Abstract

Low-grade, chronic inflammation has been associated with many diseases of aging, but the mechanisms responsible for producing this inflammation remain unclear. Inflammasomes can drive chronic inflammation in the context of an infectious disease or cellular stress, and they trigger the maturation of interleukin-1[beta] (IL-1[beta]). Here we find that the expression of specific inflammasome gene modules stratifies older individuals into two extremes: those with constitutive expression of IL-1[beta], nucleotide metabolism dysfunction, elevated oxidative stress, high rates of hypertension and arterial stiffness; and those without constitutive expression of IL-1[beta], who lack these characteristics. Adenine and N[sup.4]-acetylcytidine, nucleotide-derived metabolites that are detectable in the blood of the former group, prime and activate the NLRC4 inflammasome, induce the production of IL-1[beta], activate platelets and neutrophils and elevate blood pressure in mice. In individuals over 85 years of age, the elevated expression of inflammasome gene modules was associated with all-cause mortality. Thus, targeting inflammasome components may ameliorate chronic inflammation and various other age-associated conditions., Author(s): David Furman (corresponding author) [1, 2]; Junlei Chang [3]; Lydia Lartigue [4]; Christopher R Bolen [5]; François Haddad [6]; Brice Gaudilliere [5]; Edward A Ganio [5]; Gabriela K Fragiadakis [...]

Published
2017
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34. KIR + CD8 + T cells suppress pathogenic T cells and are active in autoimmune diseases and COVID-19

Author

Li, Jing, primary, Zaslavsky, Maxim, additional, Su, Yapeng, additional, Guo, Jing, additional, Sikora, Michael J., additional, van Unen, Vincent, additional, Christophersen, Asbjørn, additional, Chiou, Shin-Heng, additional, Chen, Liang, additional, Li, Jiefu, additional, Ji, Xuhuai, additional, Wilhelmy, Julie, additional, McSween, Alana M., additional, Palanski, Brad A., additional, Mallajosyula, Venkata Vamsee Aditya, additional, Bracey, Nathan A., additional, Dhondalay, Gopal Krishna R., additional, Bhamidipati, Kartik, additional, Pai, Joy, additional, Kipp, Lucas B., additional, Dunn, Jeffrey E., additional, Hauser, Stephen L., additional, Oksenberg, Jorge R., additional, Satpathy, Ansuman T., additional, Robinson, William H., additional, Dekker, Cornelia L., additional, Steinmetz, Lars M., additional, Khosla, Chaitan, additional, Utz, Paul J., additional, Sollid, Ludvig M., additional, Chien, Yueh-Hsiu, additional, Heath, James R., additional, Fernandez-Becker, Nielsen Q., additional, Nadeau, Kari C., additional, Saligrama, Naresha, additional, and Davis, Mark M., additional

Published
2022
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42. Vaccine-associated enhanced disease: Case definition and guidelines for data collection, analysis, and presentation of immunization safety data

Author

Munoz, Flor M., primary, Cramer, Jakob P., additional, Dekker, Cornelia L., additional, Dudley, Matthew Z., additional, Graham, Barney S., additional, Gurwith, Marc, additional, Law, Barbara, additional, Perlman, Stanley, additional, Polack, Fernando P., additional, Spergel, Jonathan M., additional, Van Braeckel, Eva, additional, Ward, Brian J., additional, Didierlaurent, Arnaud M., additional, and Lambert, Paul Henri, additional

Published
2021
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44. The critical role of background rates of possible adverse events in the assessment of COVID-19 vaccine safety

Author

Data Science & Biostatistiek, JC onderzoeksprogramma Cardiovasculaire Epidemiologie, Black, Steven B, Law, Barbara, Chen, Robert T, Dekker, Cornelia L, Sturkenboom, Miriam, Huang, Wan-Ting, Gurwith, Marc, Poland, Greg, Data Science & Biostatistiek, JC onderzoeksprogramma Cardiovasculaire Epidemiologie, Black, Steven B, Law, Barbara, Chen, Robert T, Dekker, Cornelia L, Sturkenboom, Miriam, Huang, Wan-Ting, Gurwith, Marc, and Poland, Greg

Published
2021

45. Limited efficacy of inactivated influenza vaccine in elderly individuals is associated with decreased production of vaccine-specific antibodies

Author

Sasaki, Sanae, Sullivan, Meghan, Narvaez, Carlos F., Holmes, Tyson H., Furman, David, Zheng, Nai-Ying, Nishtala, Madhuri, Wrammert, Jens, Smith, Kenneth, James, Judith A., Dekker, Cornelia L., Davis, Mark M., Wilson, Patrick C., Greenberg, Harry B., and He, Xiao-Song

Subjects
Aged -- Health aspects, Influenza vaccines -- Production management -- Health aspects -- Research, Viral antibodies -- Physiological aspects -- Research, Antibodies -- Physiological aspects -- Research, Health care industry
Abstract

During seasonal influenza epidemics, disease burden is shouldered predominantly by the very young and the elderly. Elderly individuals are particularly affected, in part because vaccine efficacy wanes with age. This has been linked to a reduced ability to induce a robust serum antibody response. Here, we show that this is due to reduced quantities of vaccine-specific antibodies, rather than a lack of antibody avidity or affinity. We measured levels of vaccine-specific plasmablasts by ELISPOT 1 week after immunization of young and elderly adults with inactivated seasonal influenza vaccine. Plasmablast-derived polyclonal antibodies (PPAbs) were generated from bulk-cultured B cells, while recombinant monoclonal antibodies (re-mAbs) were produced from single plasmablasts. The frequency of vaccine-specific plasmablasts and the concentration of PPAbs were lower in the elderly than in young adults, whereas the yields of secreted IgG per plasmablast were not different. Differences were not detected in the overall vaccine-specific avidity or affinity of PPAbs and re-mAbs between the 2 age groups. In contrast, reactivity of the antibodies induced by the inactivated seasonal influenza vaccine toward the 2009 pandemic H1N1 virus, which was not present in the vaccine, was higher in the elderly than in the young. These results indicate that the inferior antibody response to influenza vaccination in the elderly is primarily due to reduced quantities of vaccine-specific antibodies. They also suggest that exposure history affects the cross-reactivity of vaccination-induced antibodies., Introduction Influenza viruses are respiratory pathogens that cause annual epidemics and intermittent pandemics. Disease burden is especially significant among young children and elderly individuals. Although influenza vaccines effectively protect children [...]

Published
2011
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47. Signatures of immune dysfunction in HIV and HCV infection share features with chronic inflammation in aging and persist after viral reduction or elimination

Author

Lopez Angel, Cesar J., primary, Pham, Edward A., additional, Du, Huixun, additional, Vallania, Francesco, additional, Fram, Benjamin J., additional, Perez, Kevin, additional, Nguyen, Thai, additional, Rosenberg-Hasson, Yael, additional, Ahmed, Aijaz, additional, Dekker, Cornelia L., additional, Grant, Philip M., additional, Khatri, Purvesh, additional, Maecker, Holden T., additional, Glenn, Jeffrey S., additional, Davis, Mark M., additional, and Furman, David, additional

Published
2021
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49. Risk factors for developing apnea after immunization in the neonatal intensive care unit

Author

Klein, Nicola P., Massolo, Maria L., Greene, John, Dekker, Cornelia L., Black, Steven, and Escobar, Gabriel J.

Subjects
Sleep apnea syndromes -- Risk factors, Sleep apnea syndromes -- Demographic aspects, Infants (Premature) -- Health aspects, Vaccination -- Patient outcomes, Vaccination -- Demographic aspects, Vaccination -- Research, Neonatal intensive care -- Research
Published
2008

50. Guidance on safety data collection for COVID-19 vaccine safety (SO2-D2.4a)

Author

Dekker, Cornelia L., Black, Steve, Law, Barbara, and Sturkenboom, Miriam

Subjects
Guidance for developers, CEPI, Brighton Collaboration
Abstract

A novel coronavirus (CoV), Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2), emerged in late 2019 in Wuhan, China and has since spread as a global pandemic. Safe and effective vaccines are urgently needed to reduce the significant morbidity and mortality of Coronavirus Disease 2019 (COVID-19) and ease the major economic impact. There has been an unprecedented rapid response by vaccine developers with >140 vaccine candidates in preclinical development and >20 having reached clinical trials. However, a major challenge during rapid development is to avoid safety issues both by thoughtful vaccine design and by thorough safety evaluation in a timely manner. This SO2 D2.4 deliverable was meant to summarize recommendations for vaccine safety data collection, CRF, presentation and analysis for clinical trials of CEPI funded vaccine candidates targeting COVID-19. SPEAC has responded to this challenge by summarizing recommendations by the Brighton Collaboration and SPEAC project for vaccine safety data collection, CRF, presentation and analysis for clinical trials of CEPI funded vaccine candidates targeting COVID-19 with sample CRF presented in Appendix 1. In response to a request by CEPI to provide comments to the 19April version of the WHO Solidarity Protocol, SPEAC outlined the safety evaluations that should be included for trials of COVID-19 vaccine candidates with input from some Meta-DSMB members. As an example, we provided a memory aid for collection of solicited local and systemic reactions following immunization included as Appendix 2. A guide for presentation and analysis of these solicited local and systemic reaction data is included as Appendix 3 using the Brighton Collaboration case definitions as a reference where available. We also reviewed the information about enhanced disease following immunization with prior coronavirus vaccine candidates for SARS and MERS, establishing an initial literature search to gather the available information on this topic and then with the support of CEPI (Appendix 4), and organized a virtual 2-day consensus meeting on March 12 and 13, 2020 to review the preclinical data with a panel of experts. This meeting led to consensus recommendations for developers with the input of regulators attending the meeting that has been published and is included as Appendix 5., The SPEAC Project is funded in whole by CEPI.

Published
2020
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