JNJ-5322 Trispecific Antibody Achieves 100% Response Rate in Relapsed/Refractory Multiple Myeloma Phase 1 Trial

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Trispecific antibody JNJ-5322 achieves 100% response rate in R/R myeloma with improved oral toxicity vs current bispecifics.

JNJ-79635322, a trispecific antibody targeting BCMA, GPRC5D, and CD3, demonstrated 100% overall response rate at the recommended phase 2 dose (100 mg) in BCMA/GPRC5D-naïve relapsed/refractory multiple myeloma patients. The agent shows promise as a potential replacement for individual bispecific antibodies with superior oral toxicity profile and fixed-duration therapy option.

Study Design & Population

Phase 1 dose-escalation trial (NCT05652335)

Sample size: 76 patients across dose cohorts (50-300 mg)
Population: Relapsed/refractory multiple myeloma patients exposed to CD38 monoclonals, proteasome inhibitors, and immunomodulatory agents
Design: First-in-human, dose-escalation study with step-up dosing optimization
Primary endpoint: Safety, tolerability, and recommended phase 2 dose determination

Key Findings

Overall response rates by dose: 55.0% (50-300 mg mixed, n=20), 66.7% (50 mg, n=21), 100% (100 mg, n=27), 100% (300 mg, n=8)
Recommended phase 2 dose: 100 mg every 4 weeks with 5 mg step-up dose
BCMA/GPRC5D-naïve patients (85% of cohort): 100% ORR, 96.3% VGPR rate at RP2D
BCMA/GPRC5D-exposed patients: 55.0% ORR
12-month PFS rate: 95% at RP2D (limited by one treatment-related death)
CRS incidence: 56.5% overall; 69.2% without prophylactic tocilizumab vs 20.0% with prophylaxis
Improved oral toxicity profile: Lower dysgeusia rates (grade 1), no mucositis, dysphagia, or significant weight loss vs talquetamab

Clinical Implications

Dual targeting mechanism may overcome resistance to single bispecific antibodies while improving specificity
Prophylactic tocilizumab significantly reduces CRS rates, enabling outpatient dosing strategy
Fixed-duration therapy option (18 cycles) may improve patient quality of life compared to continuous bispecific therapy
Superior oral toxicity profile compared to GPRC5D-targeting agents like talquetamab may improve patient tolerance

Limitations

Early-phase data with small cohorts, particularly at higher doses
Short follow-up limits durability assessment and long-term safety profile
Single-arm design prevents direct comparison with existing bispecific antibodies
Limited data in heavily BCMA/GPRC5D-exposed population

Source: https://www.onclive.com/view/trispecific-antibody-jnj-5322-shows-potential-to-redefine-treatment-in-r-r-myeloma

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