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The Effects of Somatic Hypermutation on Neutralization and Binding in the PGT121 Family of Broadly Neutralizing HIV Antibodies

Broadly neutralizing HIV antibodies (bnAbs) are typically highly somatically mutated, raising doubts as to whether they can be elicited by vaccination. We used 454 sequencing and designed a novel phylogenetic method to model lineage evolution of the bnAbs PGT121–134 and found a positive correlation...

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Autores principales: Sok, Devin, Laserson, Uri, Laserson, Jonathan, Liu, Yi, Vigneault, Francois, Julien, Jean-Philippe, Briney, Bryan, Ramos, Alejandra, Saye, Karen F., Le, Khoa, Mahan, Alison, Wang, Shenshen, Kardar, Mehran, Yaari, Gur, Walker, Laura M., Simen, Birgitte B., St. John, Elizabeth P., Chan-Hui, Po-Ying, Swiderek, Kristine, Kleinstein, Stephen H., Alter, Galit, Seaman, Michael S., Chakraborty, Arup K., Koller, Daphne, Wilson, Ian A., Church, George M., Burton, Dennis R., Poignard, Pascal
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3836729/
https://www.ncbi.nlm.nih.gov/pubmed/24278016
http://dx.doi.org/10.1371/journal.ppat.1003754
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author Sok, Devin
Laserson, Uri
Laserson, Jonathan
Liu, Yi
Vigneault, Francois
Julien, Jean-Philippe
Briney, Bryan
Ramos, Alejandra
Saye, Karen F.
Le, Khoa
Mahan, Alison
Wang, Shenshen
Kardar, Mehran
Yaari, Gur
Walker, Laura M.
Simen, Birgitte B.
St. John, Elizabeth P.
Chan-Hui, Po-Ying
Swiderek, Kristine
Kleinstein, Stephen H.
Alter, Galit
Seaman, Michael S.
Chakraborty, Arup K.
Koller, Daphne
Wilson, Ian A.
Church, George M.
Burton, Dennis R.
Poignard, Pascal
author_facet Sok, Devin
Laserson, Uri
Laserson, Jonathan
Liu, Yi
Vigneault, Francois
Julien, Jean-Philippe
Briney, Bryan
Ramos, Alejandra
Saye, Karen F.
Le, Khoa
Mahan, Alison
Wang, Shenshen
Kardar, Mehran
Yaari, Gur
Walker, Laura M.
Simen, Birgitte B.
St. John, Elizabeth P.
Chan-Hui, Po-Ying
Swiderek, Kristine
Kleinstein, Stephen H.
Alter, Galit
Seaman, Michael S.
Chakraborty, Arup K.
Koller, Daphne
Wilson, Ian A.
Church, George M.
Burton, Dennis R.
Poignard, Pascal
author_sort Sok, Devin
collection PubMed
description Broadly neutralizing HIV antibodies (bnAbs) are typically highly somatically mutated, raising doubts as to whether they can be elicited by vaccination. We used 454 sequencing and designed a novel phylogenetic method to model lineage evolution of the bnAbs PGT121–134 and found a positive correlation between the level of somatic hypermutation (SHM) and the development of neutralization breadth and potency. Strikingly, putative intermediates were characterized that show approximately half the mutation level of PGT121–134 but were still capable of neutralizing roughly 40–80% of PGT121–134 sensitive viruses in a 74-virus panel at median titers between 15- and 3-fold higher than PGT121–134. Such antibodies with lower levels of SHM may be more amenable to elicitation through vaccination while still providing noteworthy coverage. Binding characterization indicated a preference of inferred intermediates for native Env binding over monomeric gp120, suggesting that the PGT121–134 lineage may have been selected for binding to native Env at some point during maturation. Analysis of glycan-dependent neutralization for inferred intermediates identified additional adjacent glycans that comprise the epitope and suggests changes in glycan dependency or recognition over the course of affinity maturation for this lineage. Finally, patterns of neutralization of inferred bnAb intermediates suggest hypotheses as to how SHM may lead to potent and broad HIV neutralization and provide important clues for immunogen design.
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spelling pubmed-38367292013-11-25 The Effects of Somatic Hypermutation on Neutralization and Binding in the PGT121 Family of Broadly Neutralizing HIV Antibodies Sok, Devin Laserson, Uri Laserson, Jonathan Liu, Yi Vigneault, Francois Julien, Jean-Philippe Briney, Bryan Ramos, Alejandra Saye, Karen F. Le, Khoa Mahan, Alison Wang, Shenshen Kardar, Mehran Yaari, Gur Walker, Laura M. Simen, Birgitte B. St. John, Elizabeth P. Chan-Hui, Po-Ying Swiderek, Kristine Kleinstein, Stephen H. Alter, Galit Seaman, Michael S. Chakraborty, Arup K. Koller, Daphne Wilson, Ian A. Church, George M. Burton, Dennis R. Poignard, Pascal PLoS Pathog Research Article Broadly neutralizing HIV antibodies (bnAbs) are typically highly somatically mutated, raising doubts as to whether they can be elicited by vaccination. We used 454 sequencing and designed a novel phylogenetic method to model lineage evolution of the bnAbs PGT121–134 and found a positive correlation between the level of somatic hypermutation (SHM) and the development of neutralization breadth and potency. Strikingly, putative intermediates were characterized that show approximately half the mutation level of PGT121–134 but were still capable of neutralizing roughly 40–80% of PGT121–134 sensitive viruses in a 74-virus panel at median titers between 15- and 3-fold higher than PGT121–134. Such antibodies with lower levels of SHM may be more amenable to elicitation through vaccination while still providing noteworthy coverage. Binding characterization indicated a preference of inferred intermediates for native Env binding over monomeric gp120, suggesting that the PGT121–134 lineage may have been selected for binding to native Env at some point during maturation. Analysis of glycan-dependent neutralization for inferred intermediates identified additional adjacent glycans that comprise the epitope and suggests changes in glycan dependency or recognition over the course of affinity maturation for this lineage. Finally, patterns of neutralization of inferred bnAb intermediates suggest hypotheses as to how SHM may lead to potent and broad HIV neutralization and provide important clues for immunogen design. Public Library of Science 2013-11-21 /pmc/articles/PMC3836729/ /pubmed/24278016 http://dx.doi.org/10.1371/journal.ppat.1003754 Text en © 2013 Sok et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Sok, Devin
Laserson, Uri
Laserson, Jonathan
Liu, Yi
Vigneault, Francois
Julien, Jean-Philippe
Briney, Bryan
Ramos, Alejandra
Saye, Karen F.
Le, Khoa
Mahan, Alison
Wang, Shenshen
Kardar, Mehran
Yaari, Gur
Walker, Laura M.
Simen, Birgitte B.
St. John, Elizabeth P.
Chan-Hui, Po-Ying
Swiderek, Kristine
Kleinstein, Stephen H.
Alter, Galit
Seaman, Michael S.
Chakraborty, Arup K.
Koller, Daphne
Wilson, Ian A.
Church, George M.
Burton, Dennis R.
Poignard, Pascal
The Effects of Somatic Hypermutation on Neutralization and Binding in the PGT121 Family of Broadly Neutralizing HIV Antibodies
title The Effects of Somatic Hypermutation on Neutralization and Binding in the PGT121 Family of Broadly Neutralizing HIV Antibodies
title_full The Effects of Somatic Hypermutation on Neutralization and Binding in the PGT121 Family of Broadly Neutralizing HIV Antibodies
title_fullStr The Effects of Somatic Hypermutation on Neutralization and Binding in the PGT121 Family of Broadly Neutralizing HIV Antibodies
title_full_unstemmed The Effects of Somatic Hypermutation on Neutralization and Binding in the PGT121 Family of Broadly Neutralizing HIV Antibodies
title_short The Effects of Somatic Hypermutation on Neutralization and Binding in the PGT121 Family of Broadly Neutralizing HIV Antibodies
title_sort effects of somatic hypermutation on neutralization and binding in the pgt121 family of broadly neutralizing hiv antibodies
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3836729/
https://www.ncbi.nlm.nih.gov/pubmed/24278016
http://dx.doi.org/10.1371/journal.ppat.1003754
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