Regulatory Approved Monoclonal Antibodies Contain Framework Mutations Predicted From Human Antibody Repertoires

Regulatory Approved Monoclonal Antibodies Contain Framework Mutations Predicted From Human Antibody Repertoires

Monoclonal antibodies (mAbs) are an important class of therapeutics used to treat cancer, inflammation, and infectious diseases. Identifying highly developable mAb sequences in silico could greatly reduce the time and cost required for therapeutic mAb development. Here, we present position-specific...

Full description

Bibliographic Details
Main Authors: Brian M. Petersen, Sophia A. Ulmer, Emily R. Rhodes, Matias F. Gutierrez-Gonzalez, Brandon J. Dekosky, Kayla G. Sprenger, Timothy A. Whitehead
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-09-01
Series:Frontiers in Immunology
Subjects:
monoclonal antibodies
antibody therapeutics
antibody repertoires
deep sequencing
protein stability
affinity maturation
Online Access:https://www.frontiersin.org/articles/10.3389/fimmu.2021.728694/full
id doaj-10a36cfa20ad4ada87c052c6b7e5c904
record_format Article
spelling doaj-10a36cfa20ad4ada87c052c6b7e5c9042021-09-27T06:13:10ZengFrontiers Media S.A.Frontiers in Immunology1664-32242021-09-011210.3389/fimmu.2021.728694728694Regulatory Approved Monoclonal Antibodies Contain Framework Mutations Predicted From Human Antibody RepertoiresBrian M. Petersen0Sophia A. Ulmer1Emily R. Rhodes2Matias F. Gutierrez-Gonzalez3Brandon J. Dekosky4Brandon J. Dekosky5Kayla G. Sprenger6Timothy A. Whitehead7Department of Chemical and Biological Engineering, University of Colorado, Boulder, CO, United StatesDepartment of Chemical and Biological Engineering, University of Colorado, Boulder, CO, United StatesDepartment of Chemical and Biological Engineering, University of Colorado, Boulder, CO, United StatesDepartment of Pharmaceutical Chemistry, University of Kansas, Lawrence, KS, United StatesDepartment of Pharmaceutical Chemistry, University of Kansas, Lawrence, KS, United StatesDepartment of Chemical Engineering, University of Kansas, Lawrence, KS, United StatesDepartment of Chemical and Biological Engineering, University of Colorado, Boulder, CO, United StatesDepartment of Chemical and Biological Engineering, University of Colorado, Boulder, CO, United StatesMonoclonal antibodies (mAbs) are an important class of therapeutics used to treat cancer, inflammation, and infectious diseases. Identifying highly developable mAb sequences in silico could greatly reduce the time and cost required for therapeutic mAb development. Here, we present position-specific scoring matrices (PSSMs) for antibody framework mutations developed using baseline human antibody repertoire sequences. Our analysis shows that human antibody repertoire-based PSSMs are consistent across individuals and demonstrate high correlations between related germlines. We show that mutations in existing therapeutic antibodies can be accurately predicted solely from baseline human antibody sequence data. We find that mAbs developed using humanized mice had more human-like FR mutations than mAbs originally developed by hybridoma technology. A quantitative assessment of entire framework regions of therapeutic antibodies revealed that there may be potential for improving the properties of existing therapeutic antibodies by incorporating additional mutations of high frequency in baseline human antibody repertoires. In addition, high frequency mutations in baseline human antibody repertoires were predicted in silico to reduce immunogenicity in therapeutic mAbs due to the removal of T cell epitopes. Several therapeutic mAbs were identified to have common, universally high-scoring framework mutations, and molecular dynamics simulations revealed the mechanistic basis for the evolutionary selection of these mutations. Our results suggest that baseline human antibody repertoires may be useful as predictive tools to guide mAb development in the future.https://www.frontiersin.org/articles/10.3389/fimmu.2021.728694/fullmonoclonal antibodiesantibody therapeuticsantibody repertoiresdeep sequencingprotein stabilityaffinity maturation
collection DOAJ
language English
format Article
sources DOAJ
author Brian M. Petersen
Sophia A. Ulmer
Emily R. Rhodes
Matias F. Gutierrez-Gonzalez
Brandon J. Dekosky
Brandon J. Dekosky
Kayla G. Sprenger
Timothy A. Whitehead
spellingShingle Brian M. Petersen
Sophia A. Ulmer
Emily R. Rhodes
Matias F. Gutierrez-Gonzalez
Brandon J. Dekosky
Brandon J. Dekosky
Kayla G. Sprenger
Timothy A. Whitehead
Regulatory Approved Monoclonal Antibodies Contain Framework Mutations Predicted From Human Antibody Repertoires
Frontiers in Immunology
monoclonal antibodies
antibody therapeutics
antibody repertoires
deep sequencing
protein stability
affinity maturation
author_facet Brian M. Petersen
Sophia A. Ulmer
Emily R. Rhodes
Matias F. Gutierrez-Gonzalez
Brandon J. Dekosky
Brandon J. Dekosky
Kayla G. Sprenger
Timothy A. Whitehead
author_sort Brian M. Petersen
title Regulatory Approved Monoclonal Antibodies Contain Framework Mutations Predicted From Human Antibody Repertoires
title_short Regulatory Approved Monoclonal Antibodies Contain Framework Mutations Predicted From Human Antibody Repertoires
title_full Regulatory Approved Monoclonal Antibodies Contain Framework Mutations Predicted From Human Antibody Repertoires
title_fullStr Regulatory Approved Monoclonal Antibodies Contain Framework Mutations Predicted From Human Antibody Repertoires
title_full_unstemmed Regulatory Approved Monoclonal Antibodies Contain Framework Mutations Predicted From Human Antibody Repertoires
title_sort regulatory approved monoclonal antibodies contain framework mutations predicted from human antibody repertoires
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2021-09-01
description Monoclonal antibodies (mAbs) are an important class of therapeutics used to treat cancer, inflammation, and infectious diseases. Identifying highly developable mAb sequences in silico could greatly reduce the time and cost required for therapeutic mAb development. Here, we present position-specific scoring matrices (PSSMs) for antibody framework mutations developed using baseline human antibody repertoire sequences. Our analysis shows that human antibody repertoire-based PSSMs are consistent across individuals and demonstrate high correlations between related germlines. We show that mutations in existing therapeutic antibodies can be accurately predicted solely from baseline human antibody sequence data. We find that mAbs developed using humanized mice had more human-like FR mutations than mAbs originally developed by hybridoma technology. A quantitative assessment of entire framework regions of therapeutic antibodies revealed that there may be potential for improving the properties of existing therapeutic antibodies by incorporating additional mutations of high frequency in baseline human antibody repertoires. In addition, high frequency mutations in baseline human antibody repertoires were predicted in silico to reduce immunogenicity in therapeutic mAbs due to the removal of T cell epitopes. Several therapeutic mAbs were identified to have common, universally high-scoring framework mutations, and molecular dynamics simulations revealed the mechanistic basis for the evolutionary selection of these mutations. Our results suggest that baseline human antibody repertoires may be useful as predictive tools to guide mAb development in the future.
topic monoclonal antibodies
antibody therapeutics
antibody repertoires
deep sequencing
protein stability
affinity maturation
url https://www.frontiersin.org/articles/10.3389/fimmu.2021.728694/full
work_keys_str_mv AT brianmpetersen regulatoryapprovedmonoclonalantibodiescontainframeworkmutationspredictedfromhumanantibodyrepertoires
AT sophiaaulmer regulatoryapprovedmonoclonalantibodiescontainframeworkmutationspredictedfromhumanantibodyrepertoires
AT emilyrrhodes regulatoryapprovedmonoclonalantibodiescontainframeworkmutationspredictedfromhumanantibodyrepertoires
AT matiasfgutierrezgonzalez regulatoryapprovedmonoclonalantibodiescontainframeworkmutationspredictedfromhumanantibodyrepertoires
AT brandonjdekosky regulatoryapprovedmonoclonalantibodiescontainframeworkmutationspredictedfromhumanantibodyrepertoires
AT brandonjdekosky regulatoryapprovedmonoclonalantibodiescontainframeworkmutationspredictedfromhumanantibodyrepertoires
AT kaylagsprenger regulatoryapprovedmonoclonalantibodiescontainframeworkmutationspredictedfromhumanantibodyrepertoires
AT timothyawhitehead regulatoryapprovedmonoclonalantibodiescontainframeworkmutationspredictedfromhumanantibodyrepertoires
_version_ 1716867066095468544

Similar Items