Reprogramming human B cells with custom heavy chain antibodies

Author:

Rogers Geoffrey L.ORCID,Huang Chun,Mathur Atishay,Huang Xiaoli,Chen Hsu-Yu,Stanten Kalya,Morales Heidy,Chang Chan-Hua,Kezirian Eric J.,Cannon Paula M.ORCID

Abstract

AbstractWe describe a genome editing strategy to reprogram the immunoglobulin heavy chain (IgH) locus of human B cells to express custom molecules that respond to immunization. These heavy chain antibodies (HCAbs) comprise a custom antigen-recognition domain linked to an Fc domain derived from the IgH locus and can be differentially spliced to express either B cell receptor (BCR) or secreted antibody isoforms. The HCAb editing platform is highly flexible, supporting antigen-binding domains based on both antibody and non-antibody components, and also allowing alterations in the Fc domain. Using HIV Env protein as a model antigen, we show that B cells edited to express anti-Env HCAbs support the regulated expression of both BCRs and antibodies, and respond to Env antigen in a tonsil organoid model of immunization. In this way, human B cells can be reprogrammed to produce customized therapeutic molecules with the potential forin vivoamplification.

Publisher

Cold Spring Harbor Laboratory

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