Rapid, Site-specific Labeling of "off-the-shelf" and Native Serum Autoantibodies with T Cell-redirecting Domains

Overview

Journal Sci Adv

Specialties Biology
Science

Date 2022 May 6

PMID 35522741

Authors

Fabiana Zappala

Elizabeth Higbee-Dempsey

Bian Jang

Joann Miller

Lesan Yan

Nicholas G Minutolo

Gabriela T Rosado Gonzalez

Andrew Tsourkas

Burcin Altun Ozdemir

Affiliations

Soon will be listed here.

Abstract

Extensive antibody engineering and cloning is typically required to generate new bispecific antibodies. Made-to-order genes, advanced expression systems, and high-efficiency cloning can simplify and accelerate this process, but it still can take months before a functional product is realized. We developed a simple method to site-specifically and covalently attach a T cell-redirecting domain to any off-the-shelf, human immunoglobulin G (IgG) or native IgG isolated from serum. No antibody engineering, cloning, or knowledge of the antibody sequence is required. Bispecific antibodies are generated in just hours. By labeling antibodies isolated from tumor-bearing mice, including two syngeneic models, we generated T cell-redirecting autoantibodies (TRAAbs) that act as an effective therapeutic. TRAAbs preferentially bind tumor tissue over healthy tissue, indicating a previously unexplored therapeutic window. The use of autoantibodies to direct the tumor targeting of bispecific antibodies represents a new paradigm in personalized medicine that eliminates the need to identify tumor biomarkers.

Citing Articles

A simplified function-first method for the discovery and optimization of bispecific immune engaging antibodies.

Shepherd A, Bennychen B, Marcil A, Bloemberg D, Pon R, Weeratna R PLoS One. 2023; 18(6):e0273884.

PMID: 37347762 PMC: 10286961. DOI: 10.1371/journal.pone.0273884.

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