Your search keyword '"Mari Cobb"' showing total 6 results

1. Profiling B cell immunodominance after SARS-CoV-2 infection reveals antibody evolution to non-neutralizing viral targets

Author

Lei Li, Peter Halfmann, Maria Lucia Madariaga, Siriruk Changrob, Nicholas Asby, Florian Krammer, Kumaran Shanmugarajah, Maud O. Jansen, Isabelle Stewart, Ya Nan Dai, Andrzej Joachimiak, Steven A. Erickson, Haley L. Dugan, Yoshihiro Kawaoka, Jenna J. Guthmiller, Henry A. Utset, Paige D. Hall, Jiaolong Wang, Emma S. Winkler, Christopher T. Stamper, Mari Cobb, Olivia Stovicek, Daved H. Fremont, Michael S. Diamond, Fatima Amanat, Christopher A. Nelson, Patrick C. Wilson, Jun Huang, Robert Jedrzejczak, Dustin G. Shaw, Nai Ying Zheng, and Min Huang

Subjects

Male, 0301 basic medicine, medicine.drug_class, Immunology, Immunodominance, Cross Reactions, Antibodies, Viral, Monoclonal antibody, Article, 03 medical and health sciences, 0302 clinical medicine, Antigen, Neutralization Tests, medicine, Humans, Immunology and Allergy, Memory B cell, B cell, B-Lymphocytes, biology, Immunodominant Epitopes, SARS-CoV-2, Gene Expression Profiling, COVID-19, Computational Biology, High-Throughput Nucleotide Sequencing, virus diseases, Antibodies, Neutralizing, Virology, Nucleoprotein, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Epitope mapping, 030220 oncology & carcinogenesis, Antibody Formation, Host-Pathogen Interactions, Spike Glycoprotein, Coronavirus, biology.protein, Female, Single-Cell Analysis, Antibody, Transcriptome, Immunologic Memory, Epitope Mapping

Abstract

Dissecting the evolution of memory B cells (MBCs) against SARS-CoV-2 is critical for understanding antibody recall upon secondary exposure. Here, we utilized single-cell sequencing to profile SARS-CoV-2-reactive B cells in 38 COVID-19 patients. Using oligo-tagged antigen baits, we isolated B cells specific to the SARS-CoV-2 spike, nucleoprotein (NP), open reading frame 8 (ORF8), and endemic coronavirus (HCoV) spike proteins. SARS-CoV-2 spike-specific cells were enriched in the memory compartment of acutely infected and convalescent patients several months post-symptom onset. With severe acute infection, substantial populations of endemic HCoV-reactive antibody-secreting cells were identified and possessed highly mutated variable genes, signifying preexisting immunity. Finally, MBCs exhibited pronounced maturation to NP and ORF8 over time, especially in older patients. Monoclonal antibodies against these targets were non-neutralizing and non-protective in vivo. These findings reveal antibody adaptation to non-neutralizing intracellular antigens during infection, emphasizing the importance of vaccination for inducing neutralizing spike-specific MBCs., Graphical Abstract, Dugan et al. utilize a multi-antigen bait sorting and single cell sequencing approach to profile B cell immunodominance upon SARS-CoV-2 infection, revealing a dynamic response that evolves toward internal virus proteins over time. Antibodies to internal proteins were non-protective in vivo, suggesting vaccination may generate superior anti-spike immunological memory.

Published

2021

2. COVID-19 Infection Induces Substantial Memory B Cell Maturation to Non-Neutralizing Viral Targets

Author

Olivia Stovicek, Fatima Amanat, Robert Jedrzejczak, Steven A. Erickson, Kumaran Shanmugarajah, Yoshihiro Kawaoka, Maud O. Jansen, Dustin G. Shaw, Florian Krammer, Daved H. Fremont, Michael S. Diamond, Lei Li, Jiaolong Wang, Emma S. Winkler, Peter Halfmann, Paige D. Hall, Christopher T. Stamper, Henry A. Utset, Mari Cobb, Haley L. Dugan, Christopher A. Nelson, Patrick C. Wilson, Nai-Ying Zheng, Jenna J. Guthmiller, Maria Lucia Madariaga, Siriruk Changrob, Jun Huang, Min Huang, Nicholas Asby, Andrzej Joachimiak, Isabelle Stewart, and Ya-Nan Dai

Subjects

Clinical trial, Vaccination, medicine.medical_specialty, Infectious disease (medical specialty), Informed consent, Influenza vaccine, business.industry, Family medicine, medicine, Institutional review board, Medical research, Influenza research, business

Abstract

Dissecting the evolution of memory B cells (MBCs) against SARS-CoV-2 is critical for understanding antibody recall upon secondary exposure. Here, we utilized single-cell sequencing to profile SARS-CoV-2-reactive B cell subsets in 42 COVID-19 patients. We isolated thousands of B cells in multiple distinct subsets specific to the SARS-CoV-2 spike, endemic coronavirus (HCoV) spikes, nucleoprotein (NP), and open reading frame 8 (ORF8). Spike-specific cells were enriched in the memory compartment of acutely infected and convalescent patients 1.5–5 months post-infection. With severe acute infection, we identified substantial populations of endemic HCoV-reactive antibody-secreting cells with highly mutated variable genes, indicative of preexisting immunity. Finally, MBCs exhibited maturation to NP and ORF8 over time relative to spike, especially in older patients. Monoclonal antibodies against these targets were non-neutralizing and non-protective in vivo. These findings reveal considerable antibody adaptation to non-neutralizing antigens during infection, emphasizing the importance of vaccination for inducing neutralizing spike-specific MBCs. Trial Registration Number: This clinical trial was registered at ClinicalTrials.gov with identifier NCT04340050, and clinical information for patients included in the study is detailed in Table S1–S3. Funding: This project was funded in part by the National Institute of Allergy and Infectious Disease (NIAID); National Institutes of Health (NIH) grant numbers U19AI082724 (P.C.W.), U19AI109946 (P.C.W.), U19AI057266 (P.C.W.), the NIAID Centers of Excellence for Influenza Research and Surveillance (CEIRS) grant numbers HHSN272201400005C(P.C.W.). N.W.A. was supported by the Multi-disciplinary Training program in Cancer Research (MTCR) - NIH T32 CA009594. A.J. and R.P.J were supported by federal funds from the NIAID, NIH, and Department of Health and Human Services under Contract HHSN272201700060C. F.K and F.A. were funded by the NIAID CEIRS contractHHSN272201400008C, Collaborative Influenza Vaccine Innovation Centers (CIVIC) contract 75N93019C00051 and the generous support of the JPB foundation, the Open Philanthropy Project (#2020-215611) and other philanthropic donations. Y.K. and P.H.were funded by the Research Program on Emerging and Re-emerging Infectious Disease grant (JP19fk0108113) and the Japan Program for Infectious Diseases Research and Infrastructure (JP20fk0108272) from the Japan Agency for Medical Research and Development (AMED), NIAID CEIRS contract HHSN272201400008C, and CIVIC contract 75N93019C00051. D.F., C.N, Y.D., and P.D.H, were supported by NIAID contracts HHSN272201700060C and 75N93019C00062. M.S.D. and E.S.W. were supported by NIH grants R01 AI157155 and F30 AI152327, respectively. Conflict of Interest: Several antibodies generated from this work are being used by Now Diagnostics in Springdale, AR for the development of a diagnostic test. M.S.D. is a consultant for Inbios, Vir Biotechnology, NGM Biopharmaceuticals, and Carnival Corporation, and on the Scientific Advisory Boards of Moderna and Immunome. The Diamond laboratory has received funding support in sponsored research agreements from Moderna, Vir Biotechnology, and Emergent BioSolutions. Ethical Approval: All studies were performed with the approval of the University of Chicago institutional review board IRB20-0523 and University of Chicago, University of Wisconsin-Madison, and Washington University in St. Louis institutional biosafety committees. Informed consent was obtained after the research applications and possible consequences of the studies were disclosed to study subjects.

Published

2021

3. Single-cell RNA-sequencing reveals pervasive but highly cell type-specific genetic ancestry effects on the response to viral infection

Author

Zepeng Mu, Jessica K. Fiege, Haley E. Randolph, Mari Cobb, Beth K Thielen, Julie Hussein, Ryan A. Langlois, Jean-Christophe Grenier, Yang I. Li, and Luis B. Barreiro

Subjects

Genetics, Cell type, Immune system, Infectious disease (medical specialty), Interferon, Genetic genealogy, Expression quantitative trait loci, medicine, Biology, Gene, Peripheral blood mononuclear cell, medicine.drug

Abstract

Humans vary in their susceptibility to infectious disease, partly due to variation in the immune response following infection. Here, we used single-cell RNA-sequencing to quantify genetic contributions to this variation in peripheral blood mononuclear cells, focusing specifically on the transcriptional response to influenza infection. We find that monocytes are the most responsive to influenza infection, but that all cell types mount a conserved interferon response, which is stronger in individuals with increased European ancestry. By comparing European American and African American individuals, we show that genetic ancestry effects on expression are common, influencing 29% of genes, but highly cell type-specific. Further, we demonstrate that much of this population-associated expression variation is explained by cis expression quantitative trait loci, which are enriched for signatures of recent positive selection. Our findings establish common cis-regulatory variants—including those that are differentiated by genetic ancestry—as important determinants of the antiviral immune response.

Published

2020

4. Clinical predictors of donor antibody titre and correlation with recipient antibody response in a COVID‐19 convalescent plasma clinical trial

Author

Nai-Ying Zheng, Jeffrey B. Matthews, John C. Alverdy, Amy Durkin-Celauro, Geoffrey D. Wool, Mari Cobb, Henry A. Utset, David O. Meltzer, Won Hee Oh, Jessica S. Donington, Mark K. Ferguson, Patrick C. Wilson, Kumaran Shanmugarajah, Scott Matushek, Maud O. Jansen, Haley L. Dugan, John P. Kress, Micah T. Prochaska, Cindy Bethel, Kathleen G. Beavis, John F. Fung, Diego di Sabato, Janani Vigneswaran, Maria Lucia Madariaga, Dustin G. Shaw, Madan Kumar, Jenna J. Guthmiller, Laura Trockman, Jiaolong Wang, Stephen Schrantz, Chancey Christensen, Mihai Giurcanu, Olivia Stovicek, and Robert Keskey

Subjects

0301 basic medicine, myalgia, Adult, Male, medicine.medical_specialty, 030204 cardiovascular system & hematology, antibody titre, Antibodies, Viral, Gastroenterology, Serology, COVID-19 Serological Testing, 03 medical and health sciences, 0302 clinical medicine, COVID‐19, Internal medicine, ABO blood group system, medicine, Internal Medicine, Humans, COVID-19 Serotherapy, Aged, Blood type, biology, business.industry, SARS-CoV-2, Immunization, Passive, COVID-19, Original Articles, Middle Aged, Antibodies, Neutralizing, United States, Clinical trial, Titer, 030104 developmental biology, Treatment Outcome, Immunoglobulin G, Toxicity, convalescent plasma, Antibody Formation, biology.protein, Original Article, Female, Antibody, medicine.symptom, Symptom Assessment, business

Abstract

Background Convalescent plasma therapy for COVID‐19 relies on transfer of anti‐viral antibody from donors to recipients via plasma transfusion. The relationship between clinical characteristics and antibody response to COVID‐19 is not well defined. We investigated predictors of convalescent antibody production and quantified recipient antibody response in a convalescent plasma therapy clinical trial. Methods Multivariable analysis of clinical and serological parameters in 103 confirmed COVID‐19 convalescent plasma donors 28 days or more following symptom resolution was performed. Mixed‐effects regression models with piecewise linear trends were used to characterize serial antibody responses in 10 convalescent plasma recipients with severe COVID‐19. Results Donor antibody titres ranged from 0 to 1 : 3892 (anti‐receptor binding domain (RBD)) and 0 to 1 : 3289 (anti‐spike). Higher anti‐RBD and anti‐spike titres were associated with increased age, hospitalization for COVID‐19, fever and absence of myalgia (all P

Published

2020

5. Integrated COVID-19 Convalescent Plasma Treatment and Antibody Research Program at a Single Academic Medical Center

Author

Maria Lucia Madariaga, Stephen Schrantz, Maud O. Jansen, Chancey Christensen, Madan Kumar, Micah Prochaska, Geoffrey Wool, Amy Durkin-Celauro, Won Hee Oh, Laura Trockman, Janani Vigneswaran, Robert Keskey, Jenna J. Guthmiller, Dustin Shaw, Haley L. Dugan, Nai-Ying Zheng, Mari Cobb, Henry Utset, Jiaolong Wang, Olivia Stovicek, Cindy Bethel, Scott Matushek, Kathleen Beavis, Diego di Sabato, Mark K. Ferguson, John P. Kress, Kumaran Shanmugarajah, Jeffrey B. Matthews, John F. Fung, Patrick C. Wilson, John Alverdy, and Jessica S. Donington

Subjects

2019-20 coronavirus outbreak, medicine.medical_specialty, Convalescent plasma, biology, Coronavirus disease 2019 (COVID-19), business.industry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Emergency medicine, biology.protein, medicine, Center (algebra and category theory), Antibody, business

Abstract

Background: Convalescent plasma is a potential therapy for COVID-19 Using existing resources at a single academic medical center, we established an integrated

Published

2020

6. Clinical Predictors of Donor Antibody Titer and Correlation with Recipient Antibody Response in a COVID-19 Convalescent Plasma Clinical Trial

Author

Jiaolong Wang, Olivia Stovicek, Kathleen G. Beavis, Patrick C. Wilson, Haley L. Dugan, Jeffrey B. Matthews, Robert Keskey, Chancey Christensen, Geoffrey D. Wool, Micah T. Prochaska, Maria Lucia Madariaga, Dustin G. Shaw, Henry A. Utset, Madan Kumar, Janani Vigneswaran, David O. Meltzer, Maud O. Jansen, Mark K. Ferguson, Cindy Bethel, John F. Fung, Won Hee Oh, Mari Cobb, Nai-Ying Zheng, Jessica S. Donington, Diego di Sabato, Amy Durkin-Celauro, Laura Trockman, John P. Kress, Scott Matushek, John C. Alverdy, Jenna J. Guthmiller, Stephen Schrantz, Mihai Giurcanu, and Kumaran Shanmugarajah

Subjects

myalgia, Blood type, medicine.medical_specialty, biology, business.industry, Influenza vaccine, Antibody titer, Serology, Clinical trial, Titer, Internal medicine, biology.protein, Medicine, medicine.symptom, Antibody, business

Abstract

BackgroundConvalescent plasma therapy for COVID-19 relies on the transfer of anti-viral antibody from donors to recipients via plasma transfusion. The relationship between clinical characteristics and antibody response to COVID-19 is not well defined. We investigated predictors of convalescent antibody production and quantified recipient antibody response in a convalescent plasma therapy clinical trial.MethodsMultivariable analysis of clinical and serological parameters in 103 confirmed COVID-19 convalescent plasma donors 28 days or more following symptom resolution was performed. Mixed effects regression models with piecewise linear trends were used to characterize serial antibody responses in 10 convalescent plasma recipients with severe COVID-19.FindingsMean symptom duration of plasma donors was 11.9±5.9 days and 7.8% (8/103) had been hospitalized. Antibody titers ranged from 0 to 1:3,892 (anti-receptor binding domain (RBD)) and 0 to 1:3,289 (anti-spike). Multivariable analysis demonstrated that higher anti-RBD and anti-spike titer were associated with increased age, hospitalization for COVID-19, fever, and absence of myalgia (all pInterpretationAdvanced age, fever, absence of myalgia, fatigue, blood type and hospitalization were associated with higher convalescent antibody titer to COVID-19. Despite variability in donor titer, 80% of convalescent plasma recipients showed significant increase in antibody levels post-transfusion. A more complete understanding of the dose-response effect of plasma transfusion among COVID-19 patients is needed to determine the clinical efficacy of this therapy.Trial RegistrationNCT04340050FundingDepartment of Surgery University of Chicago, National Institute of Allergy and Infectious Diseases (NIAID) Collaborative Influenza Vaccine Innovation Centers (CIVIC) contract 75N93019C00051

Published

2020