Generation, diversity determination, and application to antibody selection of a human naive Fab library

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Title
Generation, diversity determination, and application to antibody selection of a human naive Fab library
Author(s)
S Kim; Insoo Park; S G Park; Seulki Cho; J H Kim; N S Ipper; S S Choi; E S Lee; H J Hong
Bibliographic Citation
Molecules and Cells, vol. 40, no. 9, pp. 655-666
Publication Year
2017
Abstract
We constructed a large naive human Fab library (3 × 1010 colonies) from the lymphocytes of 809 human donors, assessed available diversities of the heavy-chain variable (VH) and κ light-chain variable (VK) domain repertoires, and validated the library by selecting Fabs against 10 therapeutically relevant antigens by phage display. We obtained a database of unique 7,373 VH and 41,804 VK sequences by 454 pyrosequencing, and analyzed the repertoires. The distribution of VH and VK subfamilies and germline genes in our antibody repertoires slightly differed from those in earlier published natural antibody libraries. The frequency of somatic hypermutations (SHMs) in heavy-chain complementarity determining region (HCDR)1 and HCDR2 are higher compared with the natural IgM repertoire. Analysis of position-specific SHMs in CDRs indicates that asparagine, threonine, arginine, aspartate and phenylalanine are the most frequent non-germline residues on the antibody-antigen interface and are converted mostly from the germline residues, which are highly represented in germline SHM hotspots. The amino acid composition and length-dependent changes in amino acid frequencies of HCDR3 are similar to those in previous reports, except that frequencies of aspartate and phenylalanine are a little higher in our repertoire. Taken together, the results show that this antibody library shares common features of natural antibody repertoires and also has unique features. The antibody library will be useful in the generation of human antibodies against diverse antigens, and the information about the diversity of natural antibody repertoires will be valuable in the future design of synthetic human antibody libraries with high functional diversity.
Keyword
diversityhuman monoclonal antibodynaive antibody libraryphage displaysomatic hypermutation
ISSN
1016-8478
Publisher
Korea Soc-Assoc-Inst
Full Text Link
http://dx.doi.org/10.14348/molcells.2017.0106
Type
Article
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1. Journal Articles > Journal Articles
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