Antibody variable domain interface and framework sequence requirements for stability and function by high-throughput experiments

Hung Ju Hsu; Kuo Hao Lee; Jhih Wei Jian; Hung Ju Chang; Chung Ming Yu; Yu Ching Lee; Ing Chien Chen; Hung Pin Peng; Chih Yuan Wu; Yu Feng Huang; Chih Yun Shao; Kuo Ping Chiu; An Suei Yang

doi:10.1016/j.str.2013.10.006

Antibody variable domain interface and framework sequence requirements for stability and function by high-throughput experiments

Hung Ju Hsu, Kuo Hao Lee, Jhih Wei Jian, Hung Ju Chang, Chung Ming Yu, Yu Ching Lee, Ing Chien Chen, Hung Pin Peng, Chih Yuan Wu, Yu Feng Huang, Chih Yun Shao, Kuo Ping Chiu, An Suei Yang

Research output: Contribution to journal › Article › peer-review

21 Citations (Scopus)

Abstract

Protein structural stability and biological functionality are dictated by the formation of intradomain cores and interdomain interfaces, but the intricate sequence-structure-function interrelationships in the packing of protein cores and interfaces remain difficult to elucidate due to the intractability of enumerating all packing possibilities and assessing the consequences of all the variations. In this work, groups of β strand residues of model antibody variable domains were randomized with saturated mutagenesis and the functional variants were selected for high-throughput sequencing and high-throughput thermal stability measurements. The results show that the sequence preferences of the intradomain hydrophobic core residues are strikingly flexible among hydrophobic residues, implying that these residues are coupled indirectly with antigen binding through energetic stabilization of the protein structures. By contrast, the interdomain interface residues are directly coupled with antigen binding. The interdomain interface should be treated as an integral part of the antigen-binding site.

Original language	English
Pages (from-to)	22-34
Number of pages	13
Journal	Structure
Volume	22
Issue number	1
DOIs	https://doi.org/10.1016/j.str.2013.10.006
Publication status	Published - Jan 7 2014
Externally published	Yes

ASJC Scopus subject areas

Molecular Biology
Structural Biology

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10.1016/j.str.2013.10.006

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title = "Antibody variable domain interface and framework sequence requirements for stability and function by high-throughput experiments",

abstract = "Protein structural stability and biological functionality are dictated by the formation of intradomain cores and interdomain interfaces, but the intricate sequence-structure-function interrelationships in the packing of protein cores and interfaces remain difficult to elucidate due to the intractability of enumerating all packing possibilities and assessing the consequences of all the variations. In this work, groups of β strand residues of model antibody variable domains were randomized with saturated mutagenesis and the functional variants were selected for high-throughput sequencing and high-throughput thermal stability measurements. The results show that the sequence preferences of the intradomain hydrophobic core residues are strikingly flexible among hydrophobic residues, implying that these residues are coupled indirectly with antigen binding through energetic stabilization of the protein structures. By contrast, the interdomain interface residues are directly coupled with antigen binding. The interdomain interface should be treated as an integral part of the antigen-binding site.",

author = "Hsu, {Hung Ju} and Lee, {Kuo Hao} and Jian, {Jhih Wei} and Chang, {Hung Ju} and Yu, {Chung Ming} and Lee, {Yu Ching} and Chen, {Ing Chien} and Peng, {Hung Pin} and Wu, {Chih Yuan} and Huang, {Yu Feng} and Shao, {Chih Yun} and Chiu, {Kuo Ping} and Yang, {An Suei}",

note = "Funding Information: This work was supported by the National Science Council (NSC 100IDP006-3 and NSC 99-2311-B-001-014-MY3) and the Genomics Research Center at Academia Sinica (AS-100-TP2-B01). We thank the Sequencing Core Facility, Scientific Instrument Center at Academia Sinica for DNA sequencing and the Biophysics Core Facility, Scientific Instrument Center at Academia Sinica for the DSC experiment. ",

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doi = "10.1016/j.str.2013.10.006",

language = "English",

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T1 - Antibody variable domain interface and framework sequence requirements for stability and function by high-throughput experiments

AU - Hsu, Hung Ju

AU - Lee, Kuo Hao

AU - Jian, Jhih Wei

AU - Chang, Hung Ju

AU - Yu, Chung Ming

AU - Lee, Yu Ching

AU - Chen, Ing Chien

AU - Peng, Hung Pin

AU - Wu, Chih Yuan

AU - Huang, Yu Feng

AU - Shao, Chih Yun

AU - Chiu, Kuo Ping

AU - Yang, An Suei

N1 - Funding Information: This work was supported by the National Science Council (NSC 100IDP006-3 and NSC 99-2311-B-001-014-MY3) and the Genomics Research Center at Academia Sinica (AS-100-TP2-B01). We thank the Sequencing Core Facility, Scientific Instrument Center at Academia Sinica for DNA sequencing and the Biophysics Core Facility, Scientific Instrument Center at Academia Sinica for the DSC experiment.

PY - 2014/1/7

Y1 - 2014/1/7

N2 - Protein structural stability and biological functionality are dictated by the formation of intradomain cores and interdomain interfaces, but the intricate sequence-structure-function interrelationships in the packing of protein cores and interfaces remain difficult to elucidate due to the intractability of enumerating all packing possibilities and assessing the consequences of all the variations. In this work, groups of β strand residues of model antibody variable domains were randomized with saturated mutagenesis and the functional variants were selected for high-throughput sequencing and high-throughput thermal stability measurements. The results show that the sequence preferences of the intradomain hydrophobic core residues are strikingly flexible among hydrophobic residues, implying that these residues are coupled indirectly with antigen binding through energetic stabilization of the protein structures. By contrast, the interdomain interface residues are directly coupled with antigen binding. The interdomain interface should be treated as an integral part of the antigen-binding site.

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Antibody variable domain interface and framework sequence requirements for stability and function by high-throughput experiments

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