Honing-in antigen-specific cells during antibody discovery: a user-friendly process to mine a deeper repertoire

Author:

Mahendra AnkitORCID,Haque Aftabul,Prabakaran PonrajORCID,Mackness Brian C.,Fuller Thomas P.,Liu Xiaohua,Kathuria Sagar V.ORCID,Wang Yui-Hsi,Amatya Nilesh,Yu Xiaocong,Hopke Joern,Hoffmann Dietmar,Bric-Furlong Eva,Zhang Ningning,Cho Hyun-Suk,Zhang RuijunORCID,Sancho Jose,Saleh Jacqueline,Rao Sambasiva P.,Wendt Maria,Chowdhury Partha S.ORCID

Abstract

AbstractImmunization based antibody discovery is plagued by the paucity of antigen-specific B cells. Identifying these cells is akin to finding needle in a haystack. Current and emerging technologies while effective, are limited in terms of capturing the antigen-specific repertoire. We report on the bulk purification of antigen-specific B-cells and the benefits it offers to various antibody discovery platforms. Using five different antigens, we show hit rates of 51–88%, compared to about 5% with conventional methods. We also show that this purification is highly efficient with loss of only about 2% antigen specific cells. Furthermore, we compared clones in which cognate chains are preserved with those from display libraries in which chains either from total B cells (TBC) or antigen-specific B cells (AgSC) underwent combinatorial pairing. We found that cognate chain paired clones and combinatorial clones from AgSC library had higher frequency of functional clones and showed greater diversity in sequence and paratope compared to clones from the TBC library. This antigen-specific B-cell selection technique exemplifies a process improvement with reduced cycle time and cost, by removing undesired clones prior to screening and increasing the chance of capturing desirable and rare functional clones in the repertoire.

Funder

Sanofi

Publisher

Springer Science and Business Media LLC

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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