Venetoclax: A Game Changer in the Treatment of Younger AML Patients?
Abstract
:Simple Summary
Abstract
1. Introduction
2. Venetoclax Plus Intensive Chemotherapy in De Novo AML
2.1. Venetoclax in Combination with Daunorubicin and Cytarabine
2.2. Venetoclax Plus Purine-Analogue-Based Regimens
2.3. CPX-351 Plus Venetoclax
Trial/Reference | Design | Primary Endpoint | Number of Patients | Patients Enrolled | Response | Outcomes | Early Mortality |
---|---|---|---|---|---|---|---|
daunorubicin + cytarabine + venetoclax (DAV)/[17] | phase II | composite complete remission rate | 36 | patients aged 18–60 years | CRc 6 rate: 91% | estimated 1-year OS 11: 97% estimated 1-year EFS 12: 72% | 30-day mortality: 0% |
daunorubicin + cytarabine + venetoclax (DAV 2 + 6)/[18] | phase II | overall response rate | 42 | patients aged 16–60 years | ORR 7: 92.9%; 87.9% of the CR 8 patients with undetectable MRD 9 | estimated 12-month OS 11: 83.1% estimated 12-month EFS 12: 82.7% estimated 12-month DFS 13: 92% | 30-day mortality: 2.4% |
daunorubicin + cytarabine + venetoclax (5 + 2 + VEN)/[19] | phase Ib | optimal dose schedule of venetoclax with 5 + 2 | 69 | patients aged ≥65 years with de novo or s-AML 1 or t-AML 2 | overall response (CR 8/Cri 10) rate: 73% | median OS 11: 15.4 months | 30-day mortality: 6% |
daunorubicin + cytarabine + venetoclax (5 + 2 + VEN)/[20] | retrospective clinical trial | composite complete remission | 12 | patients aged ≥ 60 years | CR 8 rate: 91.7% All patients with poor-risk achieved CR 8 | estimated 1-year EFS 12: 75%. Estimated 1-year OS 11 rate: 100% | 30-day mortality: 0% |
cyclophosphamide + cytarabine + venetoclax (VCA)/[22] | pilot study | complete remission rate | 25 | adult AML 3 | CR 8/Cri 10: 92%; all these patients had undetectable MRD 9 | Estimated 12-month OS 11: 79.3%. | / |
fludarabine + cytarabine + idarubicin + filgastrim + venetoclax (FLAG-IDA + VEN)/[24] | phase Ib/II | overall response rate | 45 | patients aged ≥18 (including de novo, sAML 1, tAML 2, tsAML 4, or high-risk MDS 5) | ORR 7: 98%; among CR 8 patients, 93% MRD 9 negative | estimated 24-month EFS 12: 64% estimated 24-month OS 11: 76%, | 30-day mortality: 0% 60-day mortality: 0% |
fludarabine + cytarabine + idarubicin + venetoclax (V-FLAI)/[28] | phase I/II trial | complete remission rate | 57 | European LeukemiaNet intermediate- or high-risk adult AML 3 (median age 54 years; 18–65) | CR 8 rate: 84%; MRD 9 negative: 74% | probability of 12-month OS 11: 76% | 30-day mortality: 1.8% 60-day mortality 5.3% |
cladribine + cytarabine + idarubin + venetoclax (CLIA + VEN)/[29] | phase II | complete response rate | 67 | patients aged ≤65 years with newly diagnosed AML 3 or high-risk MDS 5 | CRc 7 rate: 96%; among CR 8 patients, 90% MRD 9 negative | estimated 12-month OS 11: 86.5% estimated 24-month OS 11: 86.5% estimated 12-month EFS 12: 71.8% estimated 24-month EFS 12: 69.7% | 30-day mortality: 2% 60-day mortality 3% |
CPX-351 + venetoclax (CPX-351 + VEN)/[31] | phase Ib/II | the safe dose and schedule | 5 | patients aged ≥ 18 years | CR 8/CRi 10: 80%; 75% MRD 9 negative | 1-year estimated OS 11: 75% | 30-day mortality: 0% 60-day mortality: 0% |
3. Venetoclax Plus Intensive Chemotherapy in Refractory/Resistant AML
4. Venetoclax Plus Intensive Chemotherapy in Pediatric AML
5. Molecular Markers Predicting the Response to Venetoclax and Chemotherapy-Based Regimens
6. Conclusions
Author Contributions
Funding
Conflicts of Interest
References
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Trial/Reference | Design | Primary Endpoint | Number of Patients | Patients Enrolled | Response | Outcomes | Early Mortality |
---|---|---|---|---|---|---|---|
fludarabine + cytarabine + idarubicin + filgastrim + venetoclax (FLAG-IDA+ VEN)/[23] | phase Ib/II | overall response rate | 49 | patients aged ≥ 18 | CR 1/CRi 2 rate: 67% (69% were MRD 3-negative); 46% proceeded to HSCT 4 | estimated 1-year EFS 7: 41% estimated 1-year OS 8: 68% | 30-day mortality: 0% 60-day mortality: 4.4% |
fludarabine + cytarabine + idarubicin + filgastrim + venetoclax (FLAG-IDA + VEN)/[35] | real-life analysis | / | 24 | patients aged ≥ 18 | CRc 5: 72% for the entire cohort and 91% in patients treated for post-HCT 4 relapse | 12-month RFS 9: 67% 12-month OS 8: 50% | 30-day mortality: 12%; 60-day mortality: 48% |
fludarabine + cytarabine + idarubicin + venetoclax (FLAVIDA)/[36] | real-life analysis | / | 13 | patients aged ≥ 18 | ORR 6: 69%, with a median duration of CR 1/CRi 2 of 7.3 months | estimated 6-month EFS 7: 52% estimated 6-month OS 8: 76%, | / |
high-dose cytarabine + mitoxantrone + venetoclax (HAM + VEN)/[38] | phase I/II | dose-limiting toxicity | 12 | patients aged ≥ 18 | CR 1/CRi 2 rate: 92% (62.5% were MRD 3-negative); | / | 30-day mortality: 8.3% |
CPX-351 + venetoclax (CPX-351 + VEN)/[31] | phase Ib/II | the safe dose and schedule | 26 | patients aged ≥ 18 | CR 1/CRi 2 rate: 46% (78% were MRD 3-negative). | 1-year estimated OS 8: 39%; in responding patients, the median OS 8 was 26.9 months | 30-day mortality: 12% 60-day mortality: 19% |
+ cytarabine +/− idarubicin + venetoclax/[39] | phase Ib/II | the safe dose and schedule | 38 | patients between 2 and 22 years | ORR 6: 69%; 80% of patients who achieved a CR 1/CRi 2 proceeded to HSCT 4 | / | / |
Clinical Trial Gov. Identifier | Trial Phase | Combination Treatment | Treatment Status |
---|---|---|---|
NCT06068621 | 2 | CACAG 1 + venetoclax | Newly diagnosed AML 2 |
NCT05356169 | 2 | DA 3 “3 + 7” + venetoclax | Newly diagnosed AML 2 |
NCT05522192 | 1/2 | Mitoxantrone hydrochloride Liposome + venetoclax | Relapsed/Refractory AML 2 |
NCT06084819 | 2 | CACAG 1 + venetoclax | Relapsed/Refractory AML 2 |
NCT05918198 | 2 | CAG 4 + venetoclax | Relapsed/Refractory AML 2 |
NCT05807347 | 2 | Azacytidine + CAG 4 + venetoclax | Relapsed/Refractory AML 2 |
NCT03629171 | 2 | CPX351 + venetoclax | Newly diagnosed AML 2 and relapsed/refractory AML 2 |
NCT05780879 | 2 | FLAG 5 or CLAG 6 + venetoclax | Newly diagnosed AML 2 |
NCT05263284 | 1 | 8-Chloroadenosine + venetoclax | Relapsed/Refractory AML 2 |
NCT03709758 | 2 | DA 3 + venetoclax | Newly diagnosed AML 2 |
NCT05805098 | 2/3 | Homoharringtonine + cytarabine + venetoclax | Newly diagnosed AML 2 |
NCT03826992 | 1 | CPX351 + venetoclax | Relapsed/Refractory AML 2 |
NCT02115295 | 2 | CLIA + venetoclax | Newly diagnosed AML 2 and relapsed/refractory AML 2 |
NCT04797767 | 1 | CLAG-M 7 + venetoclax | Newly diagnosed AML 2 and relapsed/refractory AML 2 |
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Molica, M.; Perrone, S.; Federico, V.; Alati, C.; Molica, S.; Rossi, M. Venetoclax: A Game Changer in the Treatment of Younger AML Patients? Cancers 2024, 16, 73. https://doi.org/10.3390/cancers16010073
Molica M, Perrone S, Federico V, Alati C, Molica S, Rossi M. Venetoclax: A Game Changer in the Treatment of Younger AML Patients? Cancers. 2024; 16(1):73. https://doi.org/10.3390/cancers16010073
Chicago/Turabian StyleMolica, Matteo, Salvatore Perrone, Vincenzo Federico, Caterina Alati, Stefano Molica, and Marco Rossi. 2024. "Venetoclax: A Game Changer in the Treatment of Younger AML Patients?" Cancers 16, no. 1: 73. https://doi.org/10.3390/cancers16010073
APA StyleMolica, M., Perrone, S., Federico, V., Alati, C., Molica, S., & Rossi, M. (2024). Venetoclax: A Game Changer in the Treatment of Younger AML Patients? Cancers, 16(1), 73. https://doi.org/10.3390/cancers16010073