Stability-Diversity Tradeoffs Impose Fundamental Constraints on Selection of Synthetic Human V(H)/V(L) Single-Domain Antibodies from In Vitro Display Libraries

Human autonomous V(H)/V(L) single-domain antibodies (sdAbs) are attractive therapeutic molecules, but often suffer from suboptimal stability, solubility and affinity for cognate antigens. Most commonly, human sdAbs have been isolated from in vitro display libraries constructed via synthetic randomiz...

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Autores principales: Henry, Kevin A., Kim, Dae Young, Kandalaft, Hiba, Lowden, Michael J., Yang, Qingling, Schrag, Joseph D., Hussack, Greg, MacKenzie, C. Roger, Tanha, Jamshid
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2017
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5763143/
https://www.ncbi.nlm.nih.gov/pubmed/29375542
http://dx.doi.org/10.3389/fimmu.2017.01759
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author Henry, Kevin A.
Kim, Dae Young
Kandalaft, Hiba
Lowden, Michael J.
Yang, Qingling
Schrag, Joseph D.
Hussack, Greg
MacKenzie, C. Roger
Tanha, Jamshid
author_facet Henry, Kevin A.
Kim, Dae Young
Kandalaft, Hiba
Lowden, Michael J.
Yang, Qingling
Schrag, Joseph D.
Hussack, Greg
MacKenzie, C. Roger
Tanha, Jamshid
author_sort Henry, Kevin A.
collection PubMed
description Human autonomous V(H)/V(L) single-domain antibodies (sdAbs) are attractive therapeutic molecules, but often suffer from suboptimal stability, solubility and affinity for cognate antigens. Most commonly, human sdAbs have been isolated from in vitro display libraries constructed via synthetic randomization of rearranged V(H)/V(L) domains. Here, we describe the design and characterization of three novel human V(H)/V(L) sdAb libraries through a process of: (i) exhaustive biophysical characterization of 20 potential V(H)/V(L) sdAb library scaffolds, including assessment of expression yield, aggregation resistance, thermostability and tolerance to complementarity-determining region (CDR) substitutions; (ii) in vitro randomization of the CDRs of three V(H)/V(L) sdAb scaffolds, with tailored amino acid representation designed to promote solubility and expressibility; and (iii) systematic benchmarking of the three V(H)/V(L) libraries by panning against five model antigens. We isolated ≥1 antigen-specific human sdAb against four of five targets (13 V(H)s and 7 V(L)s in total); these were predominantly monomeric, had antigen-binding affinities ranging from 5 nM to 12 µM (average: 2–3 µM), but had highly variable expression yields (range: 0.1–19 mg/L). Despite our efforts to identify the most stable V(H)/V(L) scaffolds, selection of antigen-specific binders from these libraries was unpredictable (overall success rate for all library-target screens: ~53%) with a high attrition rate of sdAbs exhibiting false positive binding by ELISA. By analyzing V(H)/V(L) sdAb library sequence composition following selection for monomeric antibody expression (binding to protein A/L followed by amplification in bacterial cells), we found that some V(H)/V(L) sdAbs had marked growth advantages over others, and that the amino acid composition of the CDRs of this set of sdAbs was dramatically restricted (bias toward Asp and His and away from aromatic and hydrophobic residues). Thus, CDR sequence clearly dramatically impacts the stability of human autonomous V(H)/V(L) immunoglobulin domain folds, and sequence-stability tradeoffs must be taken into account during the design of such libraries.
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spelling pubmed-57631432018-01-26 Stability-Diversity Tradeoffs Impose Fundamental Constraints on Selection of Synthetic Human V(H)/V(L) Single-Domain Antibodies from In Vitro Display Libraries Henry, Kevin A. Kim, Dae Young Kandalaft, Hiba Lowden, Michael J. Yang, Qingling Schrag, Joseph D. Hussack, Greg MacKenzie, C. Roger Tanha, Jamshid Front Immunol Immunology Human autonomous V(H)/V(L) single-domain antibodies (sdAbs) are attractive therapeutic molecules, but often suffer from suboptimal stability, solubility and affinity for cognate antigens. Most commonly, human sdAbs have been isolated from in vitro display libraries constructed via synthetic randomization of rearranged V(H)/V(L) domains. Here, we describe the design and characterization of three novel human V(H)/V(L) sdAb libraries through a process of: (i) exhaustive biophysical characterization of 20 potential V(H)/V(L) sdAb library scaffolds, including assessment of expression yield, aggregation resistance, thermostability and tolerance to complementarity-determining region (CDR) substitutions; (ii) in vitro randomization of the CDRs of three V(H)/V(L) sdAb scaffolds, with tailored amino acid representation designed to promote solubility and expressibility; and (iii) systematic benchmarking of the three V(H)/V(L) libraries by panning against five model antigens. We isolated ≥1 antigen-specific human sdAb against four of five targets (13 V(H)s and 7 V(L)s in total); these were predominantly monomeric, had antigen-binding affinities ranging from 5 nM to 12 µM (average: 2–3 µM), but had highly variable expression yields (range: 0.1–19 mg/L). Despite our efforts to identify the most stable V(H)/V(L) scaffolds, selection of antigen-specific binders from these libraries was unpredictable (overall success rate for all library-target screens: ~53%) with a high attrition rate of sdAbs exhibiting false positive binding by ELISA. By analyzing V(H)/V(L) sdAb library sequence composition following selection for monomeric antibody expression (binding to protein A/L followed by amplification in bacterial cells), we found that some V(H)/V(L) sdAbs had marked growth advantages over others, and that the amino acid composition of the CDRs of this set of sdAbs was dramatically restricted (bias toward Asp and His and away from aromatic and hydrophobic residues). Thus, CDR sequence clearly dramatically impacts the stability of human autonomous V(H)/V(L) immunoglobulin domain folds, and sequence-stability tradeoffs must be taken into account during the design of such libraries. Frontiers Media S.A. 2017-12-12 /pmc/articles/PMC5763143/ /pubmed/29375542 http://dx.doi.org/10.3389/fimmu.2017.01759 Text en Copyright © 2015 Her Majesty the Queen in Right of Canada. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Henry, Kevin A.
Kim, Dae Young
Kandalaft, Hiba
Lowden, Michael J.
Yang, Qingling
Schrag, Joseph D.
Hussack, Greg
MacKenzie, C. Roger
Tanha, Jamshid
Stability-Diversity Tradeoffs Impose Fundamental Constraints on Selection of Synthetic Human V(H)/V(L) Single-Domain Antibodies from In Vitro Display Libraries
title Stability-Diversity Tradeoffs Impose Fundamental Constraints on Selection of Synthetic Human V(H)/V(L) Single-Domain Antibodies from In Vitro Display Libraries
title_full Stability-Diversity Tradeoffs Impose Fundamental Constraints on Selection of Synthetic Human V(H)/V(L) Single-Domain Antibodies from In Vitro Display Libraries
title_fullStr Stability-Diversity Tradeoffs Impose Fundamental Constraints on Selection of Synthetic Human V(H)/V(L) Single-Domain Antibodies from In Vitro Display Libraries
title_full_unstemmed Stability-Diversity Tradeoffs Impose Fundamental Constraints on Selection of Synthetic Human V(H)/V(L) Single-Domain Antibodies from In Vitro Display Libraries
title_short Stability-Diversity Tradeoffs Impose Fundamental Constraints on Selection of Synthetic Human V(H)/V(L) Single-Domain Antibodies from In Vitro Display Libraries
title_sort stability-diversity tradeoffs impose fundamental constraints on selection of synthetic human v(h)/v(l) single-domain antibodies from in vitro display libraries
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5763143/
https://www.ncbi.nlm.nih.gov/pubmed/29375542
http://dx.doi.org/10.3389/fimmu.2017.01759
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