| Literature DB >> 24752517 |
Lidia Gil1, Maciej Kazmierczak, Renata Kroll-Balcerzak, Mieczyslaw Komarnicki.
Abstract
Recently, bendamustine has become an important agent in the treatment for patients with lymphoid malignancies. Although the drug has received approval for second-line therapy in indolent lymphoma, a growing body of evidence suggests its efficacy and safety in first-line use. The results of randomised and observational studies with bendamustine as front-line therapy in non-Hodgkin lymphoma (NHL) with emphasis on efficacy and toxicity are presented. Furthermore, completed and ongoing clinical trials evaluating upfront bendamustine effectiveness in combination with other agents are discussed. The review refers mainly to indolent lymphoma, mantle cell lymphoma and aggressive lymphoma, as the most commonly diagnosed NHL types. Finally, we elaborated on the safety profile of bendamustine and the perspectives of using the drug as a first-line therapy.Entities:
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Year: 2014 PMID: 24752517 PMCID: PMC4006123 DOI: 10.1007/s12032-014-0944-1
Source DB: PubMed Journal: Med Oncol ISSN: 1357-0560 Impact factor: 3.064
Bendamustine in first-line treatment for indolent or mantle cell lymphoma—prospective studies
| Study | Patients ( | Diagnosis | ORR % | CR % | PFS | Ref |
|---|---|---|---|---|---|---|
BOP versus COP prospective phase III Herold 2006 | 164 | FL, LPL, MCL | 66 versus 76 | 22 versus 20 | 5 yrs: 59 % versus 46 % |
|
BR versus CHOPR prospective phase III Rummel 2013 StiL study | 549 | FL, MCL, LPL, MZL, SLL | 93 versus 91 | 40 versus 30 | 69.5 versus 31.2 months |
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BR versus CVPR or CHOPR prospective phase III Flinn 2012 BRIGHT study | 436 | Indolent, MCL | 94 versus 84 | 31 versus 25 |
| |
BR prospective phase II Luminari 2013 | 69 | MZL, SLL, LPL | 84 | 58 | 1 yrs: 90 % |
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BR + cytarabine prospective phase II Visco 2013 | 20 | MCL | 100 | 95 | 2 yrs: 95 % |
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RiBVD (BR + bortezomib + dexamethasone) prospective phase II Gressin 2013 LYSA study | 76 elderly | MCL | 87 | 60 |
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BR + lenalidomide prospective phase I–II Jerkeman 2013 | 51 | MCL | 97 | 79 | Not reached in 18-month follow-up |
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BR + R maintenance prospective phase II Rummel 2012 | 162 | LPL | 86 |
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BR prospective phase II Salar 2012 | 60 | MALT | 100 | 98 |
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B + ofatumumab prospective phase II Fowler 2012 | 49 | Indolent | 98 | 60 |
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BR + mitoxantrone prospective phase II Boccomini 2012 | 76 elderly | FL | 96 | 75 |
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BR + bortezomib prospective phase II Flinn 2012 | 55 | Indolent | 89 | 47 |
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B + ofatumumab + dexamethasone prospective II phase Magni 2012 | 19 elderly | MCL | 94 | 89 |
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B; bendamustine, BR; bendamustine + rituximab, BOP; bendamustine + vincristine + prednisone, COP; cyclophosphamide + vincristine + prednisone, CVPR; cyclophosphamide + vincristine + prednisone + rituximab, CHOPR; cyclophosphamide + doxorubicin + vincristine + prednisone + rituximab, RiBVD; rituximab + bendamustine + bortezomib + dexamethasone, FL; follicular lymphoma, LPL; lymphoplasmacytic lymphoma, MCL; mantle cell lymphoma, MZL; marginal zone lymphoma, SLL; small lymphocytic lymphoma, MALT; mucosa-associated lymphoid tissue, ORR; overall response rate, CR; complete remission, PFS; progression-free survival, Ref; reference, yrs; years
Bendamustine in first-line treatment for aggressive lymphoma
| Study | Patients (n), diagnosis | ORR % | CR % | PFS months | OS months | Ref |
|---|---|---|---|---|---|---|
BR, retrospective Horn 2012 | 20, DLBCL, elderly | 55 | 20 | 8.3 | 19.4 |
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BR, retrospective Kuntz 2010 | 15, DLBCL | 46 | 33 | 14.1 | 23.1 |
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BR, retrospective Hammersen 2013 | 21 DLBCL MCL | 91 | 14 | 8 | 24 |
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BR, retrospective Walter 2012 | 15, DLBCL | 62 | 38 | 6 | 9 |
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BR, prospective phase II Weidmann 2011 | 14, DLBCL, MCL elderly | 69 | 54 | 7.7 | 7.7 |
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BR prospective phase II Park 2013 | 23, DLBCL, elderly | 93 | 60 | 9.9 |
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BR; bendamustine + rituximab, DLBCL; diffuse large B-cell lymphoma, MCL; mantle cell lymphoma, ORR; overall response rate, CR; complete remission, PFS; progression-free survival, OS; overall survival, Ref; reference
Haematological and non-haematological toxicity of bendamustine-based regimens
| Study | Patients diagnosis | Haematological toxicity % grade 3–4 | Non-haematological toxicity % grade 3–4 | Ref | ||
|---|---|---|---|---|---|---|
BOP versus COP prospective phase III Herold 2006 | 164 | Anaemia | 10 versus 13 | Alopecia | 4 versus 48 |
|
| FL, LPL | Thrombocytopenia | 19 versus 34 | Vomiting | 0 versus 1 | ||
| MCL | Leucopenia | 4 versus 1 | Neuropathy | 1 versus 0 | ||
BR versus CHOPR prospective phase III Rummel 2013 StiL study | 549 | Anaemia | 3 versus 5 | Alopecia* | 0 versus 100 |
|
| FL, LPL | Leucopenia | 37 versus 72 | Neuropathy* | 7 versus 29 | ||
| MZL, SLL, MCL | Thrombocytopenia | 5 versus 6 | Infection* | 37 versus 50 | ||
BR versus CVPR or CHOPR prospective phase III Flinn 2012 BRIGHT study | 436 | Anaemia* | 5 versus 5 | Alopecia* | 4 versus 51 |
|
| Indolent | Leucopenia* | 39 versus 87 | Vomiting* | 29 versus 13 | ||
| MCL | Thrombocytopenia* | 10 versus 12 | Neuropathy* | 14 versus 44 | ||
| Infection* | 55 versus 57 | |||||
RiBVD prospective phase II Gressin 2013 | 76 | Anaemia | 2 | Fatigue | 5 |
|
| MCL | Neutropenia | 21 | Diarrhoea | 8 | ||
| Elderly | Thrombocytopenia | 15 | Neuropathy | 4 | ||
* All grades