Addition of Rituximab to First-Line MCP (Mitoxantrone, Chlorambucil, Prednisolone) Chemotherapy Prolongs Survival in Advanced Follicular Lymphoma - 4 Year Follow-Up Results of a Phase III Trial of the East German Study Group Hematology and Oncology (OSHO#39).

Author:

Herold Michael1,Haas Antje2,Srock Stephanie3,Neser Sabine4,Al Ali Kathrin H.5,Neubauer Andreas6,Doelken Gottfried7,Naumann Ralph8,Fietz Thomas9,Freund Mathias10,Rohrberg Robert11,Hoeffken Klaus12,Franke Astrid13,Ittel Thomas H.14,Kettner Erika15

Affiliation:

1. Hematology/Oncology, Helios Klinikum, Erfurt, Germany

2. Klinikum Ernst von Bergmann, Potsdam, Germany

3. Rudolph Virchow Klinikum, Berlin, Germany

4. Klinikum, Chemnitz, Germany

5. Universitaetsklinikum, Leipzig, Germany

6. Philipps Universitaet, Marburg, Germany

7. Ernst Moritz Arndt Universitaet, Greifswald, Germany

8. Klinikum der Technischen Universitaet, Dresden, Germany

9. Klinikum Benjamin Franklin, Berlin, Germany

10. Klinikum der Universität, Rostock, Germany

11. Onkologische Schwerpunktpraxis, Halle, Germany

12. Universitaetsklinikum, Jena, Germany

13. Otto von Guericke Ubiversität, Magdeburg, Germany

14. Klinikum, Stralsund, Germany

15. Staedtisches Klinikum, Magdeburg, Germany

Abstract

Abstract Introduction: Rituximab plus chemotherapy has been proved to be the gold - standard in treating advanced follicular lymphoma. Here we report the 4-year-follow-up data of our phase III trial comparing MCP - chemotherapy vs rituximab + MCP both followed by interferon maintenance in advanced symptomatic follicular lymphoma. Methods: Previously untreated patients with advanced stage (III + IV) symptomatic CD 20-positive indolent NHL and mantle cell lymphoma (n=358) were randomized to receive either MCP-chemotherapy (mitoxantrone 8 mg/m² d1+2, chlorambucil 3x3 mg/m² d 1–5, prednisolone 25 mg/m² d 1–5 x 8 q 4 weeks) or MCP + rituximab (375 mg/m² d −1). Here we report the results of the ITT population of patients with follicular lymphoma (FL) (grade 1+2), who represented the majority of patients and for whom the sample size primarily was calculated, so this is not a subgroup analysis. Study endpoints included overall and complete response rate (RR + CR), progression free survival (PFS), event free survival (EFS), time to next treatment (TTNT), overall survival (OS) and toxicities. Results: with a median follow - up of nearly 4 years (47 months) we are able to provide relatively mature data. Concerning toxicities there was no striking difference, but there was a significantly increased risk to experience a CTC grade III or IV toxicity for leukocytes in the R-MCP arm, however this did not increase the risk of infections. For the FL - ITT population the results are given in the table. Conclusions: Concerning all end points rituximab plus MCP is significantly superior to MCP alone in the treatment of advanced follicular lymphoma. Special attention should be drawn to the fact, that after a median follow-up of 47 months we can demonstrate a clinically and statistically significant survival advantage for the immunochemotherapy. Results R-MCP (n=105) MCP (n=96) p-value Response rate 92,4% 75% .0004 Complete Response 49,5% 25% .0009 PFS median n.r. 29 months < .0001 PSF 4 years 71% 40% EFS median n.r. 26 months < .0001 EFS 4 years 69% 35,5% TTNT median n.r. 29,4 months .0002 OS median n.r. n.r. .0096 OS 4 years 87% 74%

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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