Clinical development of gene edited tacrolimus-resistant Treg (FKBP12 KO -Treg) to enable simultaneous immunosuppression and support of immune regulation
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OA: closed
Abstract
Background: Unwanted immune responses play a central role in the pathogenesis of solid organ allograft rejection. These are managed by life-long immunosuppression with considerable burden for the patient and society. Adoptive therapy with regulatory T-cells (Treg) is a promising approach to restore sustainable immune balance and avoid long-term adverse effects of immunosuppression. While Treg effectively inhibit activation of unwanted immune responses, they are less effective in controlling pre-existing/activated memory effector T-cells (Teff). Thus, co-administration of Treg with immunosuppressants is required to achieve a sustainable organ acceptance. Calcineurin inhibitors (CNI) are powerful in controlling de novo generated and preformed Teff. However, CNI also dampen Treg immunoregulatory function. Thus, we hypothesize improved results of adoptive Treg therapy in immunosuppressed patients applying tacrolimus-resistant Treg. Methods: : While retaining CNI modulation of Teff with tacrolimus, we knocked-out FKBP12 in Treg (FKBP12 KO -Treg) by gene-editing using ribonucleoprotein-based CRISPR/Cas9 technology to generate tacrolimus-resistant Treg and characterised them using flow cytometry, functional assays and in-depth phenotyping. Results: : This detailed in vitro analysis showed FKBP12 KO -Treg were comparable to non-gene edited Treg and impervious to tacrolimus while maintaining immunoregulatory function and sensitivity to alternative CNIs raising no safety concerns. Furthermore, we aligned our methodology to achieve GMP compliance laying the basis for a manufacturing license in preparation of a clinical trial. Conclusion: Based on the presented preclinical dataset implying safety and efficacy of FKBP12 KO -Treg, we are now seeking to undertake a proof-of-concept clinical trial to evaluate the co-administrationof FKBP12 KO -Treg and tacrolimus to enhance the management of living donor kidney transplant recipients.
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- europepmc
- last seen: 2026-05-20T01:45:00.602351+00:00