From the Cover: Precise determination of the diversity of a combinatorial antibody library gives insight into the human immunoglobulin repertoire |
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Authors: | Jacob Glanville Wenwu Zhai Jan Berka Dilduz Telman Gabriella Huerta Gautam R. Mehta Irene Ni Li Mei Purnima D. Sundar Giles M. R. Day David Cox Arvind Rajpal Jaume Pons |
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Affiliation: | aResearch Informatics, Rinat-Pfizer Inc., 230 East Grand Avenue, South San Francisco, CA 94080; ;bProtein Engineering, Rinat-Pfizer Inc., 230 East Grand Avenue, South San Francisco, CA 94080; and ;cTarget Generation Unit, Pfizer Inc., 230 East Grand Avenue, South San Francisco, CA 94080 |
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Abstract: | Antibody repertoire diversity, potentially as high as 1011 unique molecules in a single individual, confounds characterization by conventional sequence analyses. In this study, we present a general method for assessing human antibody sequence diversity displayed on phage using massively parallel pyrosequencing, a novel application of Kabat column-labeled profile Hidden Markov Models, and translated complementarity determining region (CDR) capture-recapture analysis. Pyrosequencing of domain amplicon and RCA PCR products generated 1.5 × 106 reads, including more than 1.9 × 105 high quality, full-length sequences of antibody variable fragment (Fv) variable domains. Novel methods for germline and CDR classification and fine characterization of sequence diversity in the 6 CDRs are presented. Diverse germline contributions to the repertoire with random heavy and light chain pairing are observed. All germline families were found to be represented in 1.7 × 104 sequences obtained from repeated panning of the library. While the most variable CDR (CDR-H3) presents significant length and sequence variability, we find a substantial contribution to total diversity from somatically mutated germline encoded CDRs 1 and 2. Using a capture-recapture method, the total diversity of the antibody library obtained from a human donor Immunoglobulin M (IgM) pool was determined to be at least 3.5 × 1010. The results provide insights into the role of IgM diversification, display library construction, and productive germline usages in antibody libraries and the humoral repertoire. |
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Keywords: | HMM phage display pyrosequencing CDRs |
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