Experimental Identification of Cross-Reacting IgG Hotspots to Predict Existing Immunity Evasion of SARS-CoV-2 Variants by a New Biotechnological Application of Phage Display

Multiple pathogens are competing against the human immune response, leading to outbreaks that are increasingly difficult to control. For example, the SARS-CoV-2 virus continually evolves, giving rise to new variants. The ability to evade the immune system is a crucial factor contributing to the spre...

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Published in:Viruses Vol. 16; no. 1; p. 58
Main Authors: Harhala, Marek Adam, Gembara, Katarzyna, Baniecki, Krzysztof, Pikies, Aleksandra, Nahorecki, Artur, Jędruchniewicz, Natalia, Kaźmierczak, Zuzanna, Rybicka, Izabela, Klimek, Tomasz, Witkiewicz, Wojciech, Barczyk, Kamil, Kłak, Marlena, Dąbrowska, Krystyna
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Language:English
Published: Switzerland MDPI AG 29-12-2023
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Abstract Multiple pathogens are competing against the human immune response, leading to outbreaks that are increasingly difficult to control. For example, the SARS-CoV-2 virus continually evolves, giving rise to new variants. The ability to evade the immune system is a crucial factor contributing to the spread of these variants within the human population. With the continuous emergence of new variants, it is challenging to comprehend all the possible combinations of previous infections, various vaccination types, and potential exposure to new variants in an individual patient. Rather than conducting variant-to-variant comparisons, an efficient approach could involve identifying key protein regions associated with the immune evasion of existing immunity against the virus. In this study, we propose a new biotechnological application of bacteriophages, the phage display platform for experimental identification of regions (linear epitopes) that may function as cross-reacting IgG hotspots in SARS-CoV-2 structural proteins. A total of 34,949 epitopes derived from genomes of all SARS-CoV-2 variants deposited prior to our library design were tested in a single assay. Cross-reacting IgG hotspots are protein regions frequently recognized by cross-reacting antibodies in many variants. The assay facilitated the one-step identification of immunogenic regions of proteins that effectively induced specific IgG in SARS-CoV-2-infected patients. We identified four regions demonstrating both significant immunogenicity and the activity of a cross-reacting IgG hotspot in protein S (located at NTD, RBD, HR1, and HR2/TM domains) and two such regions in protein N (at 197-280 and 358-419 aa positions). This novel method for identifying cross-reacting IgG hotspots holds promise for informing vaccine design and serological diagnostics for COVID-19 and other infectious diseases.
AbstractList Multiple pathogens are competing against the human immune response, leading to outbreaks that are increasingly difficult to control. For example, the SARS-CoV-2 virus continually evolves, giving rise to new variants. The ability to evade the immune system is a crucial factor contributing to the spread of these variants within the human population. With the continuous emergence of new variants, it is challenging to comprehend all the possible combinations of previous infections, various vaccination types, and potential exposure to new variants in an individual patient. Rather than conducting variant-to-variant comparisons, an efficient approach could involve identifying key protein regions associated with the immune evasion of existing immunity against the virus. In this study, we propose a new biotechnological application of bacteriophages, the phage display platform for experimental identification of regions (linear epitopes) that may function as cross-reacting IgG hotspots in SARS-CoV-2 structural proteins. A total of 34,949 epitopes derived from genomes of all SARS-CoV-2 variants deposited prior to our library design were tested in a single assay. Cross-reacting IgG hotspots are protein regions frequently recognized by cross-reacting antibodies in many variants. The assay facilitated the one-step identification of immunogenic regions of proteins that effectively induced specific IgG in SARS-CoV-2-infected patients. We identified four regions demonstrating both significant immunogenicity and the activity of a cross-reacting IgG hotspot in protein S (located at NTD, RBD, HR1, and HR2/TM domains) and two such regions in protein N (at 197–280 and 358–419 aa positions). This novel method for identifying cross-reacting IgG hotspots holds promise for informing vaccine design and serological diagnostics for COVID-19 and other infectious diseases.
Audience Academic
Author Witkiewicz, Wojciech
Kłak, Marlena
Klimek, Tomasz
Gembara, Katarzyna
Harhala, Marek Adam
Kaźmierczak, Zuzanna
Pikies, Aleksandra
Nahorecki, Artur
Dąbrowska, Krystyna
Barczyk, Kamil
Rybicka, Izabela
Jędruchniewicz, Natalia
Baniecki, Krzysztof
AuthorAffiliation 3 Healthcare Centre in Bolesławiec, Jeleniogórska 4, 59-700 Bolesławiec, Poland; krzysztofbaniecki@gmail.com (K.B.); aleksandrapikies@gmail.com (A.P.); anahorecki@zozbol.eu (A.N.); sekretariat@szpitalboleslawiec.pl (K.B.)
1 Research and Development Center, Regional Specialist Hospital in Wrocław, Kamieńskiego 73a St., 51-124 Wrocław, Poland; marek.harhala@hirszfeld.pl (M.A.H.); katarzyna.gembara@hirszfeld.pl (K.G.); natalia.jedruchniewicz@wssk.wroc.pl (N.J.); zuzanna.kazmierczak@hirszfeld.pl (Z.K.); tomasz.klimek@wssk.wroc.pl (T.K.); wojciech.witkiewicz@wssk.wroc.pl (W.W.); marlena.klak@wssk.wroc.pl (M.K.)
2 Hirszfeld Institute of Immunology and Experimental Therapy, Weigla 12 St., 53-114 Wrocław, Poland; izabela.rybicka@hirszfeld.pl
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Keywords COVID-19
serological profiling
epitopes
SARS-CoV-2
phage display
IgG
antibodies
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These authors contributed equally to this work.
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Snippet Multiple pathogens are competing against the human immune response, leading to outbreaks that are increasingly difficult to control. For example, the...
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StartPage 58
SubjectTerms Amino acids
Antibodies
Bacteriophages
Bioethics
Biotechnology
COVID-19
Epitopes
Genetic aspects
Genomes
Hospitalization
Humans
Identification
IgG
Immune Evasion
Immune response
Immunity
Immunogenicity
Immunoglobulin G
Immunology
Infections
Infectious diseases
Pandemics
Peptides
Phage display
Phages
Physiological aspects
Protein S
Proteins
Recombination hot spots
Regions
SARS-CoV-2
SARS-CoV-2 - genetics
Serology
Severe acute respiratory syndrome coronavirus 2
Software
Structural proteins
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Title Experimental Identification of Cross-Reacting IgG Hotspots to Predict Existing Immunity Evasion of SARS-CoV-2 Variants by a New Biotechnological Application of Phage Display
URI https://www.ncbi.nlm.nih.gov/pubmed/38257758
https://www.proquest.com/docview/2918792456
https://www.proquest.com/docview/2917868579
https://pubmed.ncbi.nlm.nih.gov/PMC10820762
https://doaj.org/article/91824f60f28b4aeda881ec1d94ece382
Volume 16
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