Primary therapy of Waldenstrom macroglobulinemia (WM) with weekly bortezomib, low-dose dexamethasone, and rituximab (BDR): long-term results of a phase 2 study of the European Myeloma Network (EMN).

[waldenstrÃ¶m macroglobulinemia]

In this phase 2 multicenter trial , we evaluated the activity of bortezomib , dexamethasone , and rituximab (BDR ) combination in previously untreated symptomatic patients with WaldenstrÃ¶m macroglobulinemia (WM ). To prevent immunoglobulin M (IgM ) "flare ," single agent bortezomib (1 .3 mg /m (2 ) IV days 1 , 4 , 8 , and 11 ; 21 -day cycle ), was followed by weekly IV bortezomib (1 .6 mg /m (2 ) days 1 , 8 , 15 , and 22 ) every 35 days for 4 additional cycles , followed by IV dexamethasone (40 mg ) and IV rituximab (375 mg /m (2 )) in cycles 2 and 5 . Fifty -nine patients were treated ; 45 .5 % and 40 % were high and intermediate risk per the International Prognostic Scoring System for WM . On intent to treat , 85 % responded (3 % complete response , 7 % very good partial response , 58 % partial response [PR ]). In 11 % of patients , an increase of IgM â‰¥25 % was observed after rituximab ; no patient required plasmapheresis . After a minimum follow-up of 32 months , median progression-free survival was 42 months , 3 -year duration of response for patients with â‰¥PR was 70 %, and 3 -year survival was 81 %. Peripheral neuropathy occurred in 46 % (grade â‰¥3 in 7 %); only 8 % discontinued bortezomib due to neuropathy . BDR is rapidly acting , well tolerated , and nonmyelotoxic , inducing durable responses in previously untreated WM .

Diseases
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Diseases presenting "very good partial response" symptom

waldenstrÃ¶m macroglobulinemia

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