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Assessment of Crosslinkers between Peptide Antigen and Carrier Protein for Fusion Peptide-Directed Vaccines against HIV-1

Conjugate-vaccine immunogens require three components: a carrier protein, an antigen, and a crosslinker, capable of coupling antigen to carrier protein, while preserving both T-cell responses from carrier protein and B-cell responses from antigen. We previously showed that the N-terminal eight resid...

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Autores principales: Ou, Li, Gulla, Krishana, Biju, Andrea, Biner, Daniel W., Bylund, Tatsiana, Changela, Anita, Chen, Steven J., Zheng, Cheng-Yan, Cibelli, Nicole, Corrigan, Angela R., Duan, Hongying, Gonelli, Christopher A., Kong, Wing-Pui, Cheng, Cheng, O’Dell, Sijy, Sarfo, Edward K., Shaddeau, Andrew, Wang, Shuishu, Vinitsky, Alison, Yang, Yanhong, Zhang, Baoshan, Zhang, Yaqiu, Koup, Richard A., Doria-Rose, Nicole A., Gall, Jason G., Mascola, John R., Kwong, Peter D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9698951/
https://www.ncbi.nlm.nih.gov/pubmed/36423012
http://dx.doi.org/10.3390/vaccines10111916
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author Ou, Li
Gulla, Krishana
Biju, Andrea
Biner, Daniel W.
Bylund, Tatsiana
Changela, Anita
Chen, Steven J.
Zheng, Cheng-Yan
Cibelli, Nicole
Corrigan, Angela R.
Duan, Hongying
Gonelli, Christopher A.
Kong, Wing-Pui
Cheng, Cheng
O’Dell, Sijy
Sarfo, Edward K.
Shaddeau, Andrew
Wang, Shuishu
Vinitsky, Alison
Yang, Yanhong
Zhang, Baoshan
Zhang, Yaqiu
Koup, Richard A.
Doria-Rose, Nicole A.
Gall, Jason G.
Mascola, John R.
Kwong, Peter D.
author_facet Ou, Li
Gulla, Krishana
Biju, Andrea
Biner, Daniel W.
Bylund, Tatsiana
Changela, Anita
Chen, Steven J.
Zheng, Cheng-Yan
Cibelli, Nicole
Corrigan, Angela R.
Duan, Hongying
Gonelli, Christopher A.
Kong, Wing-Pui
Cheng, Cheng
O’Dell, Sijy
Sarfo, Edward K.
Shaddeau, Andrew
Wang, Shuishu
Vinitsky, Alison
Yang, Yanhong
Zhang, Baoshan
Zhang, Yaqiu
Koup, Richard A.
Doria-Rose, Nicole A.
Gall, Jason G.
Mascola, John R.
Kwong, Peter D.
author_sort Ou, Li
collection PubMed
description Conjugate-vaccine immunogens require three components: a carrier protein, an antigen, and a crosslinker, capable of coupling antigen to carrier protein, while preserving both T-cell responses from carrier protein and B-cell responses from antigen. We previously showed that the N-terminal eight residues of the HIV-1 fusion peptide (FP8) as an antigen could prime for broad cross-clade neutralizing responses, that recombinant heavy chain of tetanus toxin (rTTHC) as a carrier protein provided optimal responses, and that choice of crosslinker could impact both antigenicity and immunogenicity. Here, we delve more deeply into the impact of varying the linker between FP8 and rTTHC. In specific, we assessed the physical properties, the antigenicity, and the immunogenicity of conjugates for crosslinkers ranging in spacer-arm length from 1.5 to 95.2 Å, with varying hydrophobicity and crosslinking-functional groups. Conjugates coupled with different degrees of multimerization and peptide-to-rTTHC stoichiometry, but all were well recognized by HIV-fusion-peptide-directed antibodies VRC34.01, VRC34.05, PGT151, and ACS202 except for the conjugate with the longest linker (24-PEGylated SMCC; SM(PEG)24), which had lower affinity for ACS202, as did the conjugate with the shortest linker (succinimidyl iodoacetate; SIA), which also had the lowest peptide-to-rTTHC stoichiometry. Murine immunizations testing seven FP8-rTTHC conjugates elicited fusion-peptide-directed antibody responses, with SIA- and SM(PEG)24-linked conjugates eliciting lower responses than the other five conjugates. After boosting with prefusion-closed envelope trimers from strains BG505 clade A and consensus clade C, trimer-directed antibody-binding responses were lower for the SIA-linked conjugate; elicited neutralizing responses were similar, however, though statistically lower for the SM(PEG)24-linked conjugate, when tested against a strain especially sensitive to fusion-peptide-directed responses. Overall, correlation analyses revealed the immunogenicity of FP8-rTTHC conjugates to be negatively impacted by hydrophilicity and extremes of length or low peptide-carrier stoichiometry, but robust to other linker parameters, with several commonly used crosslinkers yielding statistically indistinguishable serological results.
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spelling pubmed-96989512022-11-26 Assessment of Crosslinkers between Peptide Antigen and Carrier Protein for Fusion Peptide-Directed Vaccines against HIV-1 Ou, Li Gulla, Krishana Biju, Andrea Biner, Daniel W. Bylund, Tatsiana Changela, Anita Chen, Steven J. Zheng, Cheng-Yan Cibelli, Nicole Corrigan, Angela R. Duan, Hongying Gonelli, Christopher A. Kong, Wing-Pui Cheng, Cheng O’Dell, Sijy Sarfo, Edward K. Shaddeau, Andrew Wang, Shuishu Vinitsky, Alison Yang, Yanhong Zhang, Baoshan Zhang, Yaqiu Koup, Richard A. Doria-Rose, Nicole A. Gall, Jason G. Mascola, John R. Kwong, Peter D. Vaccines (Basel) Article Conjugate-vaccine immunogens require three components: a carrier protein, an antigen, and a crosslinker, capable of coupling antigen to carrier protein, while preserving both T-cell responses from carrier protein and B-cell responses from antigen. We previously showed that the N-terminal eight residues of the HIV-1 fusion peptide (FP8) as an antigen could prime for broad cross-clade neutralizing responses, that recombinant heavy chain of tetanus toxin (rTTHC) as a carrier protein provided optimal responses, and that choice of crosslinker could impact both antigenicity and immunogenicity. Here, we delve more deeply into the impact of varying the linker between FP8 and rTTHC. In specific, we assessed the physical properties, the antigenicity, and the immunogenicity of conjugates for crosslinkers ranging in spacer-arm length from 1.5 to 95.2 Å, with varying hydrophobicity and crosslinking-functional groups. Conjugates coupled with different degrees of multimerization and peptide-to-rTTHC stoichiometry, but all were well recognized by HIV-fusion-peptide-directed antibodies VRC34.01, VRC34.05, PGT151, and ACS202 except for the conjugate with the longest linker (24-PEGylated SMCC; SM(PEG)24), which had lower affinity for ACS202, as did the conjugate with the shortest linker (succinimidyl iodoacetate; SIA), which also had the lowest peptide-to-rTTHC stoichiometry. Murine immunizations testing seven FP8-rTTHC conjugates elicited fusion-peptide-directed antibody responses, with SIA- and SM(PEG)24-linked conjugates eliciting lower responses than the other five conjugates. After boosting with prefusion-closed envelope trimers from strains BG505 clade A and consensus clade C, trimer-directed antibody-binding responses were lower for the SIA-linked conjugate; elicited neutralizing responses were similar, however, though statistically lower for the SM(PEG)24-linked conjugate, when tested against a strain especially sensitive to fusion-peptide-directed responses. Overall, correlation analyses revealed the immunogenicity of FP8-rTTHC conjugates to be negatively impacted by hydrophilicity and extremes of length or low peptide-carrier stoichiometry, but robust to other linker parameters, with several commonly used crosslinkers yielding statistically indistinguishable serological results. MDPI 2022-11-12 /pmc/articles/PMC9698951/ /pubmed/36423012 http://dx.doi.org/10.3390/vaccines10111916 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Ou, Li
Gulla, Krishana
Biju, Andrea
Biner, Daniel W.
Bylund, Tatsiana
Changela, Anita
Chen, Steven J.
Zheng, Cheng-Yan
Cibelli, Nicole
Corrigan, Angela R.
Duan, Hongying
Gonelli, Christopher A.
Kong, Wing-Pui
Cheng, Cheng
O’Dell, Sijy
Sarfo, Edward K.
Shaddeau, Andrew
Wang, Shuishu
Vinitsky, Alison
Yang, Yanhong
Zhang, Baoshan
Zhang, Yaqiu
Koup, Richard A.
Doria-Rose, Nicole A.
Gall, Jason G.
Mascola, John R.
Kwong, Peter D.
Assessment of Crosslinkers between Peptide Antigen and Carrier Protein for Fusion Peptide-Directed Vaccines against HIV-1
title Assessment of Crosslinkers between Peptide Antigen and Carrier Protein for Fusion Peptide-Directed Vaccines against HIV-1
title_full Assessment of Crosslinkers between Peptide Antigen and Carrier Protein for Fusion Peptide-Directed Vaccines against HIV-1
title_fullStr Assessment of Crosslinkers between Peptide Antigen and Carrier Protein for Fusion Peptide-Directed Vaccines against HIV-1
title_full_unstemmed Assessment of Crosslinkers between Peptide Antigen and Carrier Protein for Fusion Peptide-Directed Vaccines against HIV-1
title_short Assessment of Crosslinkers between Peptide Antigen and Carrier Protein for Fusion Peptide-Directed Vaccines against HIV-1
title_sort assessment of crosslinkers between peptide antigen and carrier protein for fusion peptide-directed vaccines against hiv-1
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9698951/
https://www.ncbi.nlm.nih.gov/pubmed/36423012
http://dx.doi.org/10.3390/vaccines10111916
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