Literature DB >> 32418062

ModiBodies: A computational method for modifying nanobodies in nanobody-antigen complexes to improve binding affinity and specificity.

Aysima Hacisuleyman1, Burak Erman2.   

Abstract

Nanobodies are special derivatives of antibodies, which consist of single domain fragments. They have become of considerable interest as next-generation biotechnological tools for antigen recognition. They can be easily engineered due to their high stability and compact size. Nanobodies have three complementarity-determining regions, CDRs, which are enlarged to provide a similar binding surface to that of human immunoglobulins. Here, we propose a benchmark testing algorithm that uses 3D structures of already existing protein-nanobody complexes as initial structures followed by successive mutations on the CDR domains. The aim is to find optimum binding amino acids for hypervariable residues of CDRs. We use molecular dynamics simulations to compare the binding energies of the resulting complexes with that of the known complex and accept those that are improved by mutations. We use the MDM4-VH9 complex, (PDB id 2VYR), fructose-bisphosphate aldolase from Trypanosoma congolense (PDB id 5O0W) and human lysozyme (PDB id 4I0C) as benchmark complexes. By using this algorithm, better binding nanobodies can be generated in a short amount of time. We suggest that this method can complement existing immune and synthetic library-based methods, without a need for extensive experimentation or large libraries.

Entities:  

Keywords:  CDR; Fructose-bisphosphate aldolase; Human lysozyme; MDM4; Molecular dynamics; Nanobody design; Steered molecular dynamics

Mesh:

Substances:

Year:  2020        PMID: 32418062      PMCID: PMC7334311          DOI: 10.1007/s10867-020-09548-3

Source DB:  PubMed          Journal:  J Biol Phys        ISSN: 0092-0606            Impact factor:   1.365


  35 in total

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Journal:  ACS Synth Biol       Date:  2018-11-16       Impact factor: 5.110

6.  A nanobody binding to non-amyloidogenic regions of the protein human lysozyme enhances partial unfolding but inhibits amyloid fibril formation.

Authors:  Erwin De Genst; Pak-Ho Chan; Els Pardon; Shang-Te D Hsu; Janet R Kumita; John Christodoulou; Linda Menzer; Dimitri Y Chirgadze; Carol V Robinson; Serge Muyldermans; André Matagne; Lode Wyns; Christopher M Dobson; Mireille Dumoulin
Journal:  J Phys Chem B       Date:  2013-09-24       Impact factor: 2.991

7.  Yeast surface display platform for rapid discovery of conformationally selective nanobodies.

Authors:  Conor McMahon; Alexander S Baier; Roberta Pascolutti; Marcin Wegrecki; Sanduo Zheng; Janice X Ong; Sarah C Erlandson; Daniel Hilger; Søren G F Rasmussen; Aaron M Ring; Aashish Manglik; Andrew C Kruse
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8.  Institute collection and analysis of Nanobodies (iCAN): a comprehensive database and analysis platform for nanobodies.

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Journal:  BMC Genomics       Date:  2017-10-17       Impact factor: 3.969

9.  An improved yeast surface display platform for the screening of nanobody immune libraries.

Authors:  Tomasz Uchański; Thomas Zögg; Jie Yin; Daopeng Yuan; Alexandre Wohlkönig; Baptiste Fischer; Daniel M Rosenbaum; Brian K Kobilka; Els Pardon; Jan Steyaert
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10.  Computational approaches to therapeutic antibody design: established methods and emerging trends.

Authors:  Richard A Norman; Francesco Ambrosetti; Alexandre M J J Bonvin; Lucy J Colwell; Sebastian Kelm; Sandeep Kumar; Konrad Krawczyk
Journal:  Brief Bioinform       Date:  2020-09-25       Impact factor: 11.622

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1.  INDI-integrated nanobody database for immunoinformatics.

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Review 2.  Engineered NK Cells Against Cancer and Their Potential Applications Beyond.

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