A novel co-infusion strategy employing both CD19– and BCMA-targetingโ CAR-T cells demonstrated promising initial results in a phase 1 trial for patients wiht treatment-refractory systemic lupus erythematosus (SLE), researchers report. The study,โค published in Nature Medicine, offers โฃa potential breakthrough for a challenging autoimmune disease where current therapies frequently enough fall short,โ and represents a significant โstep โคtoward precision cellular immunotherapy โfor SLE.
Systemic โคlupus erythematosus,a chronic autoimmune disease,affects an estimated 500,000 Americans,disproportionately impactingโข women and individuals of African,Hispanic,Asian,and Native โAmerican descent. Existing treatments, including immunosuppressants and corticosteroids, can have debilitatingโ side effects and frequently enough fail to achieve long-term remission. This new approach aims to selectively target and deplete autoreactive B cells-key players in SLE’s pathology-while concurrently โaddressing antibody-secreting plasma cells, offering a dual-pronged attack on the disease.
The โphase 1 trial โenrolled six patients with severe, treatment-refractory SLE. participants received aโ single infusion of CAR-T cells targeting both CD19, found on many B cells, and BCMA, expressed on plasma cells. Preliminary data โindicate โthe treatment was well-tolerated,โ with no dose-limiting toxicities observed. Cytokine releaseโฃ syndrome (CRS) and neurologic toxicity-potential complications of CAR-T therapy-whereโ managed using established protocols, guided by โฃASTCT consensus grading (Lee, D. W.โ et al.โข Biol.Blood Marrow Transpl. 25, 625-638 (2019)).
Notably, fourโฃ of the six patients achieved a โฃclinical response, defined asโค a reductionโฃ in SLE Disease โActivityโ Indexโ 2000 (SLEDAI) scores. Two patients experienced โฃcomplete remission,maintaining symptom control for at least six months following CAR-T cell infusion.โฃ B-cell depletionโ was observed in all patients, with varyingโฃ degrees ofโข reconstitution over time. Further examination into the durability ofโ these responses and the long-term safety profile isโ ongoing.
researchers acknowledgeโฃ the need for larger, randomized controlled trials to confirm these findings and optimize the CAR-T cell dosing and conditioning regimens.The safety and efficacyโข of autologous โand allogeneic humanized CD19-targeted CAR-T cell therapy for relapsed/refractory B-ALL has paved the way for this research (Song,C. J. Immunother. cancer 11 (2023)). This earlyโ success suggests โคthatโข co-targeting CD19 and BCMA may represent a viable therapeutic strategy for SLE patients who have exhausted conventional treatment options, potentially transforming โคthe landscape of autoimmune disease management.
