Microfluidic immuno-serology assay revealed a limited diversity of protection against COVID-19 in patients with altered immunity

The immune response to SARS-CoV-2 for patients with altered immunity such as hematologic malignancies and autoimmune disease may differ substantially from that in general population. These patients remain at high risk despite wide-spread adoption of vaccination. It is critical to examine the differe...

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Autores principales: Kim, Dongjoo, Biancon, Giulia, Bai, Zhiliang, VanOudenhove, Jennifer, Liu, Yuxin, Kothari, Shalin, Gowda, Lohith, Kwan, Jennifer M., Buitrago-Pocasangre, Nicholas Carlos, Lele, Nikhil, Asashima, Hiromitsu, Racke, Michael K., Wilson, JoDell E., Givens, Tara S., Tomayko, Mary M., Schulz, Wade L., Longbrake, Erin E., Hafler, David A., Halene, Stephanie, Fan, Rong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9460970/
https://www.ncbi.nlm.nih.gov/pubmed/36093346
http://dx.doi.org/10.1101/2022.08.31.506117
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author Kim, Dongjoo
Biancon, Giulia
Bai, Zhiliang
VanOudenhove, Jennifer
Liu, Yuxin
Kothari, Shalin
Gowda, Lohith
Kwan, Jennifer M.
Buitrago-Pocasangre, Nicholas Carlos
Lele, Nikhil
Asashima, Hiromitsu
Racke, Michael K.
Wilson, JoDell E.
Givens, Tara S.
Tomayko, Mary M.
Schulz, Wade L.
Longbrake, Erin E.
Hafler, David A.
Halene, Stephanie
Fan, Rong
author_facet Kim, Dongjoo
Biancon, Giulia
Bai, Zhiliang
VanOudenhove, Jennifer
Liu, Yuxin
Kothari, Shalin
Gowda, Lohith
Kwan, Jennifer M.
Buitrago-Pocasangre, Nicholas Carlos
Lele, Nikhil
Asashima, Hiromitsu
Racke, Michael K.
Wilson, JoDell E.
Givens, Tara S.
Tomayko, Mary M.
Schulz, Wade L.
Longbrake, Erin E.
Hafler, David A.
Halene, Stephanie
Fan, Rong
author_sort Kim, Dongjoo
collection PubMed
description The immune response to SARS-CoV-2 for patients with altered immunity such as hematologic malignancies and autoimmune disease may differ substantially from that in general population. These patients remain at high risk despite wide-spread adoption of vaccination. It is critical to examine the differences at the systems level between the general population and the patients with altered immunity in terms of immunologic and serological responses to COVID-19 infection and vaccination. Here, we developed a novel microfluidic chip for high-plex immuno-serological assay to simultaneously measure up to 50 plasma or serum samples for up to 50 soluble markers including 35 plasma proteins, 11 anti-spike/RBD IgG antibodies spanning all major variants, and controls. Our assay demonstrated the quintuplicate test in a single run with high throughput, low sample volume input, high reproducibility and high accuracy. It was applied to the measurement of 1,012 blood samples including in-depth analysis of sera from 127 patients and 21 healthy donors over multiple time points, either with acute COVID infection or vaccination. The protein association matrix analysis revealed distinct immune mediator protein modules that exhibited a reduced degree of diversity in protein-protein cooperation in patients with hematologic malignancies and patients with autoimmune disorders receiving B cell depletion therapy. Serological analysis identified that COVID infected patients with hematologic malignancies display impaired anti-RBD antibody response despite high level of anti-spike IgG, which could be associated with limited clonotype diversity and functional deficiency in B cells and was further confirmed by single-cell BCR and transcriptome sequencing. These findings underscore the importance to individualize immunization strategy for these high-risk patients and provide an informative tool to monitor their responses at the systems level.
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spelling pubmed-94609702022-09-10 Microfluidic immuno-serology assay revealed a limited diversity of protection against COVID-19 in patients with altered immunity Kim, Dongjoo Biancon, Giulia Bai, Zhiliang VanOudenhove, Jennifer Liu, Yuxin Kothari, Shalin Gowda, Lohith Kwan, Jennifer M. Buitrago-Pocasangre, Nicholas Carlos Lele, Nikhil Asashima, Hiromitsu Racke, Michael K. Wilson, JoDell E. Givens, Tara S. Tomayko, Mary M. Schulz, Wade L. Longbrake, Erin E. Hafler, David A. Halene, Stephanie Fan, Rong bioRxiv Article The immune response to SARS-CoV-2 for patients with altered immunity such as hematologic malignancies and autoimmune disease may differ substantially from that in general population. These patients remain at high risk despite wide-spread adoption of vaccination. It is critical to examine the differences at the systems level between the general population and the patients with altered immunity in terms of immunologic and serological responses to COVID-19 infection and vaccination. Here, we developed a novel microfluidic chip for high-plex immuno-serological assay to simultaneously measure up to 50 plasma or serum samples for up to 50 soluble markers including 35 plasma proteins, 11 anti-spike/RBD IgG antibodies spanning all major variants, and controls. Our assay demonstrated the quintuplicate test in a single run with high throughput, low sample volume input, high reproducibility and high accuracy. It was applied to the measurement of 1,012 blood samples including in-depth analysis of sera from 127 patients and 21 healthy donors over multiple time points, either with acute COVID infection or vaccination. The protein association matrix analysis revealed distinct immune mediator protein modules that exhibited a reduced degree of diversity in protein-protein cooperation in patients with hematologic malignancies and patients with autoimmune disorders receiving B cell depletion therapy. Serological analysis identified that COVID infected patients with hematologic malignancies display impaired anti-RBD antibody response despite high level of anti-spike IgG, which could be associated with limited clonotype diversity and functional deficiency in B cells and was further confirmed by single-cell BCR and transcriptome sequencing. These findings underscore the importance to individualize immunization strategy for these high-risk patients and provide an informative tool to monitor their responses at the systems level. Cold Spring Harbor Laboratory 2022-09-02 /pmc/articles/PMC9460970/ /pubmed/36093346 http://dx.doi.org/10.1101/2022.08.31.506117 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Kim, Dongjoo
Biancon, Giulia
Bai, Zhiliang
VanOudenhove, Jennifer
Liu, Yuxin
Kothari, Shalin
Gowda, Lohith
Kwan, Jennifer M.
Buitrago-Pocasangre, Nicholas Carlos
Lele, Nikhil
Asashima, Hiromitsu
Racke, Michael K.
Wilson, JoDell E.
Givens, Tara S.
Tomayko, Mary M.
Schulz, Wade L.
Longbrake, Erin E.
Hafler, David A.
Halene, Stephanie
Fan, Rong
Microfluidic immuno-serology assay revealed a limited diversity of protection against COVID-19 in patients with altered immunity
title Microfluidic immuno-serology assay revealed a limited diversity of protection against COVID-19 in patients with altered immunity
title_full Microfluidic immuno-serology assay revealed a limited diversity of protection against COVID-19 in patients with altered immunity
title_fullStr Microfluidic immuno-serology assay revealed a limited diversity of protection against COVID-19 in patients with altered immunity
title_full_unstemmed Microfluidic immuno-serology assay revealed a limited diversity of protection against COVID-19 in patients with altered immunity
title_short Microfluidic immuno-serology assay revealed a limited diversity of protection against COVID-19 in patients with altered immunity
title_sort microfluidic immuno-serology assay revealed a limited diversity of protection against covid-19 in patients with altered immunity
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9460970/
https://www.ncbi.nlm.nih.gov/pubmed/36093346
http://dx.doi.org/10.1101/2022.08.31.506117
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