Novel Therapies for Relapsed or Refractory Diffuse Large B-Cell Lymphoma
Abstract
:1. Introduction
2. Tafasitamab
3. Polatuzumab Vedotin
4. Selinexor
5. CAR T Cells
6. Sequencing Therapy
7. Future of DLBCL and Immunotherapy
8. Conclusions
Author Contributions
Funding
Conflicts of Interest
References
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Agent | Year of FDA Approval | Regimen | Population | Relapse < 1 year of DLBCL Diagnosis | Refractory to Last Regimen | DHL/THL | Efficacy Outcomes |
---|---|---|---|---|---|---|---|
Axicabtagene ciloleucel (axi-cel) | 2017 | Flu/Cy LD | R/R DLBCL refractory to 2 lines of therapy | 30% | 77% | NR | ORR 83% CR 58% mOS 24 mos |
Lisocabtagene maraleucel | Flu/Cy LD | R/R DLBCL refractory to 2 lines of therapy | NR | 44% | 13% | ORR 73% CR 53% mOS >12 mos | |
Tisagenlecleucel a | 2018 | Flu/Cy LD or Benda-Flu LD | R/R DLBCL refractory to 2 lines of therapy | NR | 40% | 27% | ORR 52 CR 40% mOS 12 mos |
Polatuzumab vedotin [20] | 2019 | Pola + BR | R/R DLBCL Ineligible for ASCT | 53% | 75% | 0% | CMR 40% mOS 12.4 mos |
Selinexor [21] | 2020 | Selinexor 60 mg po on days 1 and 3 of each week | R/R DLBCL | 33% §§ | 72% | 4% | ORR 28% CR 12% mOS 9.1 mos |
Tafasitamab [22] | 2020 | Tafa + LEN 25 mg | R/R DLBCL Ineligible for ASCT | 19% § | 44% | 0% | ORR 58% CR 33% mOS 22 mos |
Bispecific Abs | ||||
Epcoritamab (CD3/CD20) Flat dose Subcutaneous weekly Escalation study | Hutchings et al. [41] NCT03625037 | Phase 1/2 R/R DLBCL | N = 41 | Enrolling Median f/u 4.7 mo ORR 56% CR 44% No dose limiting toxicities |
Odronextamab REGN1979 (CD3/CD20) 18–320 mg doses | Bannerji et al. [42] NCT03888105 | Phase 1 R/R DLBCL | N = 19 | Enrolling phase 2 ORR 58% CR 37% |
Monsenetuzumab (CD3/CD20) | Schuster et al. [43] NCT03677154 | Phase 1/2 R/R DLBCL including p CAR-T | N = 119 | Enrolling phase 3 ORR 34.7% CR 18.6% |
Glofitamab RG6026 (CD3/CD20) | Morschhauser et al. [44] NCT03075696 | Phase 1/Ib R/R aggressive NHL +/− Obinituzumab | N = 21 | Enrolling Phase 1 ORR 38% CR 31% |
Monoclonal Abs | ||||
Tafasitamab (anti-CD19) (Fc-enhanced, humanized) +Lenolidomide | Nowakowski et al. [25] Maddocks et al. [45] NCT02399085 | Phase 1/2 R/R DLBCL Ineligible for ASCT Excluded double-hit | N = 81 | Enrolling phase 3 ORR 58% CR 33% Median OS 22 mos (95% CI: 18.6–NR) |
Magrolimab (5F9) (anti-CD47, promote phagocytosis) +Rituximab | Advani et al. [46] NCT02953509 | Phase 1b/2 R/R DLBCL | N = 15 | Enrolling, Preliminary results ORR 40% CR 27% On-target anemia primarily 1st dose |
Anti-PD-L1 Containing Regimens | ||||
Atezolizumab (anti-PDL1) +Obinituzumab (anti-CD20) +Venetoclax (BCL2 inhibitor) | Herbaux et al. [47] NCT03276468 | Phase 2 R/R DLBCL | N = 58 | Interim Results ORR 23.6% CMR 18% |
Mogamulizumab (anti-CCR4) +Pembrolizumab | Joffe et al. NCT03309878 | Phase 1b/2 R/R DLBCL Ineligible for ASCT | Enrolling | |
Avelumab (anti-PD-L1) +/− Utomilumab (4-1BB agonist) +/− Rituximab +/− Bendamustine or Azacitidine | Chen et al. [48] NCT02951156 | Phase 1b/3 R/R DLBCL Ineligible for ASCT ECOG ≤ 1 | Enrolling | |
Bispecific CAR T Cell Therapies | ||||
AUTO3 (CD19/CD22) Dual targeted +Pembrolizumab | Osborne et al. NCT03287817 | Phase 1/2 R/R DLBCL | N = 11 | ORR 64%CRR 55% |
LV20.19CAR (CD19/CD20) Dual targeted Lentiviral | Shah et al. [49] NCT03019055 | Phase 1 R/R NHL 45% DLBCL | Enrolling in expansion phase ORR 82% CR 54.5% No grade 3–4 CRS or NTX in first 11 pts. | |
Antibody-Drug Conjugates | ||||
Polatuzumab vedotin (anti-CD79b/MMAE) added to BR | Sehn et al. [20] Lu et al. [28] NCT02257567 | Phase 2 R/R DLBCL Ineligible for ASCT | N = 80 | CMR 40% Median OS 12.4 mos |
Polatuzumab vedotin (anti-CD79b/MMAE) added to Gem-Ox | Haioun et al. [31] NCT04182204 | Phase 3 R/R DLBCL | Enrolling | |
Engineered Toxin Bodies | ||||
MT-3724 (CD20/ SLT-I A1) | Fanale et al. [50] Duque et al. [51] NCT02361346 | Phase 1 Relapsed B-NHL after anti-CD20 and CT | N = 100 | Safety and efficacy assessment of 50 mcg/kg/dose ongoing. |
PI3K Inhibitor | ||||
Parsaclisib 20 mg po daily | Coleman et al. [52,53] NCT02998476 | Phase 2 R/R DLBCL | N = 60 | Interim Results ORR 25% CMR 12.5% |
Buparlisib 80 mg po daily +Ibrutinib | Batlevi et al. [54] NCT02756247 | Phase 1/2 R/R DLBCL, Mantle Cell, Follicular | N = 37 | Interim Results ORR 31% CMR 23% |
BTK Inhibitors | ||||
Acalabrutinib 100 mg po BID +Pembrolizumab | Witzig et al. [55] NCT02362035 | Phase 1/2 R/R DLBCL | N = 61 | ORR 26% CR 7% |
Zanubrutinib 160 mg po BID | Yang et al. [56] NCT03145064 | Phase 2 R/R Non-GBC DLBCL Ineligible for ASCT | N = 41 | ORR 29.3% CR 17.1% Median OS 8.4 mos |
Immunomodulators | ||||
R2-GDP Lenalidomide 10 mg po d1-14 + R-GDP | Merino et al. [57] EudraCT 2014-001620-29 | Phase 2 R/R DLBCL Ineligible for ASCT | N = 79 | Enrolling ORR 59% CR 32% Median OS 12 mos |
R2-ICE Lenalidomide 20 mg po d1-14 + RICE | Guerra-Bauman et al. [58] NCT02628405 | Phase 1/2 R/R DLBCL Candidates for ASCT | Enrolling |
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Harris, L.J.; Patel, K.; Martin, M. Novel Therapies for Relapsed or Refractory Diffuse Large B-Cell Lymphoma. Int. J. Mol. Sci. 2020, 21, 8553. https://doi.org/10.3390/ijms21228553
Harris LJ, Patel K, Martin M. Novel Therapies for Relapsed or Refractory Diffuse Large B-Cell Lymphoma. International Journal of Molecular Sciences. 2020; 21(22):8553. https://doi.org/10.3390/ijms21228553
Chicago/Turabian StyleHarris, Leonard Jeff, Kruti Patel, and Michael Martin. 2020. "Novel Therapies for Relapsed or Refractory Diffuse Large B-Cell Lymphoma" International Journal of Molecular Sciences 21, no. 22: 8553. https://doi.org/10.3390/ijms21228553