Advanced hybridoma technology for selective production of high-affinity monoclonal antibodies through B-cell receptors

Kento Sakashita; Kanta Tsumoto; Masahiro Tomita

doi:10.1016/j.jim.2022.113384

Advanced hybridoma technology for selective production of high-affinity monoclonal antibodies through B-cell receptors

J Immunol Methods. 2022 Dec:511:113384. doi: 10.1016/j.jim.2022.113384. Epub 2022 Nov 11.

Authors

Kento Sakashita¹, Kanta Tsumoto², Masahiro Tomita³

Affiliations

¹ Division of Chemistry for Materials, Graduate School of Engineering, Mie University, 1577 Kurimamachiya-cho, Tsu Mie 514-8507, Japan; Denka Company Limited, 1359-1 Kagamida Kigoshi Gosen-city, Niigata 959-1695, Japan. Electronic address: s.kento0720@gmail.com.
² Division of Chemistry for Materials, Graduate School of Engineering, Mie University, 1577 Kurimamachiya-cho, Tsu Mie 514-8507, Japan.
³ Division of Chemistry for Materials, Graduate School of Engineering, Mie University, 1577 Kurimamachiya-cho, Tsu Mie 514-8507, Japan. Electronic address: tomita@chem.mie-u.ac.jp.

PMID: 36372268
DOI: 10.1016/j.jim.2022.113384

Abstract

In general, it is difficult to raise novel monoclonal antibodies against relatively low-molecular weight antigen, and particularly those with high homology for the mouse protein. The optimized B-cell targeting (BCT) technique can overcome this limitation. The point of this advanced technology is the selection of sensitized B lymphocytes by the antigen through B-cell receptors (BCRs). This strict selection by specific and strong interaction between antigen and antibody enables the efficient production of monoclonal antibodies with high specificity and affinity. It also offers the condensation of sensitized target B lymphocytes to selectively generate hybridoma cells secreting desired monoclonal antibodies. In this study, several kinds of biotinylated human myoglobin (hMyo) were prepared to select sensitized B lymphocytes via BCRs. Biotinylated hMyo prepared by a 3.75- and 7.5-fold molar excess of N-hydroxysuccinimide (NHS)-biotin provided high antigenicity of 68-88%. B lymphocytes selected by these biotinylated antigens had an ELISA-positive rate >17 times higher than that with usual biotinylated antigen. Monoclonal antibodies generated by the optimized BCT technology by preselecting sensitized B lymphocytes with the target antigen were identified to specifically recognize lower antigenic epitopes in hMyo with high affinity, while this would be impossible by the polyethylene glycol (PEG) method. Furthermore, combination of these high-affinity monoclonal antibodies gave the best binding rate in an epitope binning assay. These outcomes could be attributed to the unique characteristic that BCRs on sensitized B lymphocytes themselves can select the target epitopes in the antigen. The BCRs may act as a strict sensor of B lymphocytes to precisely select the target epitopes, even though the number of immunized B lymphocytes is low.

Keywords: Antigen-based selection; B-cell receptor (BCR); B-cell targeting; High-affinity monoclonal antibody; Lower antigenic sites; Target epitope.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Antibodies, Monoclonal*
Humans
Mice
Receptors, Antigen, B-Cell*
Technology

Substances

Antibodies, Monoclonal
Receptors, Antigen, B-Cell