A Novel Immunosuppressive Compound (79-6) That Targets Bcl6 Prevents the Humoral Alloresponse

R. Kraaijeveld, D. A. Hesselink, C. C. Baan

Internal medicine - Nephrology and Transplantation, Erasmus Medical Center, Rotterdam, Netherlands

Meeting: 2022 American Transplant Congress

Abstract number: 1282

Keywords: B cells, IgG, Immunosuppression, Transcription factors

Topic: Basic Science » Basic Science » 12 - Immunosuppression & Tolerance: Preclinical & Translational Studies

Session Information

Session Name: Immunosuppression & Tolerance: Preclinical & Translational Studies

Session Type: Poster Abstract

Date: Monday, June 6, 2022

Session Time: 7:00pm-8:00pm

Presentation Time: 7:00pm-8:00pm

Location: Hynes Halls C & D

*Purpose: BCL6, is a transcription factor involved in B cell activation and differentiation. BCL6-expressing B cells play a crucial role in the development and maintenance of germinal centers, which are essential for the development of a humoral response. Targeting BCL6-mediated responses has the potential to prevent humoral alloreactivity. Here, a small molecule BCL6 inhibitor named 79-6 was tested in vitro and its effect on plasma blast formation and IgG production was investigated.

*Methods: The following experiments were performed in the presence and absence of the small molecule BCL-6 inhibitor 76-9 (range 25-100 µg/mL): (1) Polyclonally-activated B cells (anti-IgM/anti-CD40 and IL-21) from healthy controls were studied for differentiation, plasma cell formation and IgG-production. (2) To study 79-6’s inhibitory effect on B cell differentiation stages, circulating TfH cells and B cells were stimulated with alloantigen, and 79-6 was added at different time points (day 0, 3, and 7).

*Results: After polyclonal stimulation, a median of 7.4% of the B cells differentiated into plasmablasts. In the presence of 79-6, plasmablast formation was significantly inhibited by 91% and the proportion of class switched memory B cells dropped by 22%, both p<0.01). Production of IgGs was measured in culture supernatants (median of 600 ng/ml), After inhibition by 79-6, IgG-concentrations were significantly reduced (91%, p <0.01). After stimulation with alloantigen, B cells successfully differentiated into plasma blasts (median 9.8%). Early addition of 79-6 (day 0, day 3) resulted in inhibition of plasma blast formation (median inhibition: 97% and 73%, respectively), while addition of 79-7 at day 7, when B cells have differentiated into plasmablast, did not result in significant inhibition of plasma blast formation.

*Conclusions: 79-6 effectively inhibits differentiation of B lymphocytes into immunoglobulin-producing plasmablasts, whereas it does not inhibit Ig production once plasmablast formation is established. This implies that the timing of 79-6 administration in clinical practice is crucial.

To cite this abstract in AMA style:

Kraaijeveld R, Hesselink DA, Baan CC. A Novel Immunosuppressive Compound (79-6) That Targets Bcl6 Prevents the Humoral Alloresponse [abstract]. Am J Transplant. 2022; 22 (suppl 3). https://atcmeetingabstracts.com/abstract/a-novel-immunosuppressive-compound-79-6-that-targets-bcl6-prevents-the-humoral-alloresponse/. Accessed May 18, 2025.

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