Obecabtagene autoleucel (obe-cel), a CD19-targeting Autologous Chimeric Antigen Receptor T-cell Therapy (CAR T) with a fast off-rate binding domain, in Patients (pts) with Severe, Refractory Systemic Lupus Erythematosus (srSLE): Preliminary Results from the Phase I CARLYSLE Study

Maria Leandro¹, Ruth Pepper², Ben Parker³, Eleni Tholouli⁴, David Jayne⁵, Ben Uttenthal⁶, Josefina Cortés-Hernández⁷, Pere Barba⁷, José Andrés Román Ivorra⁸, Yanqing Hu⁹, Wolfram Brugger¹⁰, Silvia Basilico¹¹, Davide Germano¹¹ and Claire Roddie¹, ¹University College London and University College London Hospital, London, United Kingdom, ²University College London, University College London Hospital and Royal Free Hospital NHS Trust, London, United Kingdom, ³NIHR Manchester CRF, Manchester Royal Infirmary, Manchester, United Kingdom, ⁴Manchester Royal Infirmary, Manchester, United Kingdom, ⁵University of Cambridge, Cambridge, United Kingdom, ⁶Cambridge University Hospitals NHS Foundation Trust, Cambridge, United Kingdom, ⁷Hospital Universitari Vall d’Hebron-Universitat Autónoma de Barcelona, Barcelona, Spain, ⁸Hospital Universitari i Politècnic La Fe, Valencia, Spain, ⁹Autolus Therapeutics, Rockville, MD, ¹⁰Autolus Therapeutics, Munich, Germany, ¹¹Autolus Therapeutics, Basel, Switzerland

Meeting: ACR Convergence 2025

Keywords: B-Cell Targets, clinical trial, gene therapy, Lupus nephritis, Systemic lupus erythematosus (SLE)

Session Information

Date: Tuesday, October 28, 2025

Title: (2437–2469) Systemic Lupus Erythematosus – Treatment Poster III

Session Type: Poster Session C

Session Time: 10:30AM-12:30PM

Background/Purpose: Pts with srSLE have limited remaining treatment options and represent a population with an unmet need. CD19 CAR Ts have potential for deep depletion of the B-cell lineage, including plasmablasts. Obe-cel is an autologous CD19-directed CAR T with a fast off-rate binding domain designed to reduce immunotoxicity, approved in adult relapsed/refractory B-cell acute lymphoblastic leukemia. We report initial safety and preliminary efficacy results from the single-arm, open-label, dose-finding, Phase I CARLYSLE study (NCT06333483).

Methods: Eligible pts (12–65 years old) had a diagnosis of SLE based on the 2019 EULAR/ACR criteria and a ≥8-point SLEDAI-2K score at screening with ≥1 major SLE-related organ involvement, and were refractory to multiple prior standard-of-care SLE medications. Immunosuppressants were tapered off prior to apheresis. Following lymphodepletion with fludarabine (3×25 mg/m2) and cyclophosphamide (1×1,000 mg/m2), obe-cel was administered as a single starting target dose of 50×106 (±20%) CAR T-cells. Primary endpoints: incidence of dose limiting toxicities (DLTs) within 28 days of infusion; frequency of adverse events. Secondary endpoints included: SLEDAI-2K; PGA; pharmacokinetics (PK); autoantibody and biomarker levels over time.

Results: As of 17 Mar 2025, seven pts had been enrolled and six had been infused with obe-cel with up to 8 months of follow up. At baseline, all infused pts had severe, refractory, active SLE (SLEDAI-2K score range: 15–28). All infused pts had class III or IV lupus nephritis; four also had class V. Four pts had elevated serum creatinine and an estimated glomerular filtration rate of < 60 mL/min/1.73m2; six pts had elevated urinary protein-creatinine ratio. Pts were refractory to B-cell targeting agents and immunosuppressants (median: 5 prior medicines; range: 5–6). No DLTs or immune effector cell-associated neurotoxicity syndrome (ICANS) were observed. Three pts experienced Grade (Gr) 1 cytokine release syndrome (CRS) with no Gr ≥2 CRS. Transient hypertension was observed in five pts. All pts had Gr ≥3 neutropenia. Infections were transient and manageable; no life-threatening infections were observed. A ≥10 point reduction in SLEDAI-2K scores was seen in the four pts who had ≥3 months of follow up and all non-renal manifestations completely resolved within 3 months. Steroid doses were tapered to ≤10mg/day post obe-cel infusion; no other SLE medications were administered. Three of six pts had a complete renal response (CRR) at last follow-up, one at Month 1 (M1) and two at M3. Complement C3 normalized and anti-double-stranded DNA antibody decreased in all six pts by M1 compared with baseline levels. PK data indicated robust CAR T-cell expansion; peak expansion was reached at a median of 10 days. Three pts had ongoing CAR T-cell persistence at last follow-up.

Conclusion: Initial findings from the ongoing CARLYSLE study of obe-cel in srSLE show a manageable safety profile, with no DLTs, ICANS or Gr ≥2 CRS. SLEDAI-2K score reduction and clinical benefit were observed in all pts, including three pts who had a CRR. Despite the short follow up and small number of pts, initial findings are promising; further research is warranted. Updated data will be presented at the conference.

Disclosures: M. Leandro: Artiva, 12, PI for Clinical Trials on B cell targeting therapies:, Autolus Therapeutics, 12, PI for Clinical Trials on B cell targeting therapies:, BMS, 12, PI for Clinical Trials on B cell targeting therapies:, Fate Therapeutics, 12, PI for Clinical Trials on B cell targeting therapies:, Roche Basel, 12, PI for Clinical Trials on B cell targeting therapies:, Roche Basel (Co-PI in research grant paid to UCL), 5, Roche Basel/UCB - Advisory board September 2024, 1; R. Pepper: Autolus Therapeutics, 1, Roche (Lupus Nephritis) Advisory board, 1, Stada symposium, 6, Vifor (IgA) advisory board, 1; B. Parker: Autolus Therapeutics, 1, LUPUS UK, 5, Otsuka, 6, UCB, 12, Conference attendance; E. Tholouli: Autolus Therapeutics, 2, 5, Bristol-Myers Squibb(BMS), 2, Janssen, 2, Jazz Pharmaceuticals, 6, Kite/Gilead, 2, 5, 6, 12, Travel expenses, Pfizer, 6, Sobi, 6, Takeda, 6, Vertex, 2, 6; D. Jayne: Alentis, 2, 11, Amgen, 2, 6, AstraZeneca, 1, 2, 6, Aurinia, 1, 11, Boehringer-Ingelheim, 2, 6, Bristol-Myers Squibb(BMS), 2, 6, ChemoCentryx, 2, 6, Chinook, 1, Chugai, 2, 6, CSL Vifor, 2, 6, Fate, 2, GlaxoSmithKlein(GSK), 2, 6, GSK, 1, Hansa, 1, Novartis, 1, 2, 6, Otsuka, 2, Roche, 2, 6, Takeda, 1, 2, 6; B. Uttenthal: AbbVie, 12, Sponsorship to attend conference, Analog Devices, 2, Gilead, 12, Sponsorship to attend conference, Jazz, 12, Sponsorship to attend conference, Kite, 6, Kite/Gilead, 1, Kyverna, 1, 12, Sponsorship to attend conference, Novartis, 12, Sponsorship to attend conference, Sartorius, 2, Swarm Oncology, 2, Takeda, 12, Sponsorship to attend conference; J. Cortés-Hernández: AstraZeneca, 6, Bristol-Myers Squibb (BMS), 1, GlaxoSmithKline (GSK), 6, Novartis, 1, 5, 6; P. Barba: Allogene, 5, Amgen, 5, Bristol-Myers Squibb, 5, Gilead Sciences, 5, InCyte, 5, Jazz Pharmaceuticals, 5, Miltenyi Biomedicine, 5, Nektar, 5, Novartis, 5, Pfizer, 5, Pierre Fabre, 5; J. Andrés Román Ivorra: AstraZeneca, 6, GSK, 6, UCB, 6; Y. Hu: Autolus Therapeutics, 3, 11; W. Brugger: Autolus Therapeutics, 3, 11; S. Basilico: Autolus Therapeutics, 3, 11; D. Germano: Autolus Therapeutics, 3, 11; C. Roddie: Autolus Therapeutics, 2, 6, Bristol-Myers Squibb(BMS), 2, 6, Gilead, 2, 6, Janssen, 2.

To cite this abstract in AMA style:

Leandro M, Pepper R, Parker B, Tholouli E, Jayne D, Uttenthal B, Cortés-Hernández J, Barba P, Andrés Román Ivorra J, Hu Y, Brugger W, Basilico S, Germano D, Roddie C. Obecabtagene autoleucel (obe-cel), a CD19-targeting Autologous Chimeric Antigen Receptor T-cell Therapy (CAR T) with a fast off-rate binding domain, in Patients (pts) with Severe, Refractory Systemic Lupus Erythematosus (srSLE): Preliminary Results from the Phase I CARLYSLE Study [abstract]. Arthritis Rheumatol. 2025; 77 (suppl 9). https://acrabstracts.org/abstract/obecabtagene-autoleucel-obe-cel-a-cd19-targeting-autologous-chimeric-antigen-receptor-t-cell-therapy-car-t-with-a-fast-off-rate-binding-domain-in-patients-pts-with-severe-refractory-systemic/. Accessed .

« Back to ACR Convergence 2025

ACR Meeting Abstracts - https://acrabstracts.org/abstract/obecabtagene-autoleucel-obe-cel-a-cd19-targeting-autologous-chimeric-antigen-receptor-t-cell-therapy-car-t-with-a-fast-off-rate-binding-domain-in-patients-pts-with-severe-refractory-systemic/