Table 3.

Comparison of anti-BCMA modalities

CAR-T cellsBispecific antibodiesADCs
Pros Unprecedented response rates, including MRD negativity in heavily pretreated patients Off the shelf Off the shelf 
One-time intervention; long chemotherapy holiday, resulting in median PFS ∼1 year Deep responses Encouraging response rates 
 Limited severe CRS; ? elderly 1-hour infusion every 3 weeks 
 Can be given in community settings No CRS 
  Can be given in community settings 
Cons Manufacturing time makes it impractical for patients with aggressive or rapidly progressing disease ? Need for admissions with initial doses until CRS risk is low Ocular toxicity; requires close collaboration with ophthalmology and may negatively impact quality of life 
Requires complex infrastructure, with a stem cell laboratory and nursing and ICU/ER training; thus restricted to accredited centers Limited data in triple class/pentarefractory Thrombocytopenia 
CRS; ? role in elderly and frail patients Dosing/schedule to be determined Need for continuous treatment until progression 
Impact of bridging chemotherapy on duration of remission Need for continuous treatment until progression Modest ORR and PFS in triple class/pentarefractory 
Cost, given relapses occur, even in MRD patients Toxicities require further study; neuropathy, infections  
Low white cells and platelets after CAR-T requiring ongoing/frequent monitoring and treatment   
Management of CAR-T relapses challenging, especially if soon after fludarabine/cyclophosphamide, given impact on T cells   
CAR-T cellsBispecific antibodiesADCs
Pros Unprecedented response rates, including MRD negativity in heavily pretreated patients Off the shelf Off the shelf 
One-time intervention; long chemotherapy holiday, resulting in median PFS ∼1 year Deep responses Encouraging response rates 
 Limited severe CRS; ? elderly 1-hour infusion every 3 weeks 
 Can be given in community settings No CRS 
  Can be given in community settings 
Cons Manufacturing time makes it impractical for patients with aggressive or rapidly progressing disease ? Need for admissions with initial doses until CRS risk is low Ocular toxicity; requires close collaboration with ophthalmology and may negatively impact quality of life 
Requires complex infrastructure, with a stem cell laboratory and nursing and ICU/ER training; thus restricted to accredited centers Limited data in triple class/pentarefractory Thrombocytopenia 
CRS; ? role in elderly and frail patients Dosing/schedule to be determined Need for continuous treatment until progression 
Impact of bridging chemotherapy on duration of remission Need for continuous treatment until progression Modest ORR and PFS in triple class/pentarefractory 
Cost, given relapses occur, even in MRD patients Toxicities require further study; neuropathy, infections  
Low white cells and platelets after CAR-T requiring ongoing/frequent monitoring and treatment   
Management of CAR-T relapses challenging, especially if soon after fludarabine/cyclophosphamide, given impact on T cells   

ICU/ER, intensive care unit/emergency room.

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