Interferon-alpha 2b added to melphalan-prednisone for initial and maintenance therapy in multiple myeloma - A randomized, controlled trial

被引:73
作者
Hjorth, M
Westin, J
Dahl, IMS
Gimsing, P
Hippe, E
Holmberg, E
Lamvik, J
Nielsen, JL
Lofvenberg, E
Palva, IP
Rodjer, S
Talstad, I
Turesson, I
Wisloff, F
Zador, G
AmslerNordin, S
Polgary, M
Oden, A
Wallgren, A
Wilhelmsen, L
Hellqvist, L
Hasselblom, S
Carneskog, J
Lindqvist, O
Hoffman, P
Olsson, K
Tholen, A
Stolt, CM
Rindner, A
Svensson, R
Vaart, J
Hansen, S
Engqvist, L
Lannemyr, O
Nilsson, PG
Linne, I
Lilja, G
Tallroth, G
Hallgren, J
Andersson, B
Billstrom, R
Persson, S
Samuelsson, T
Odeberg, H
Adriansson, M
Tove, H
Stobeus, N
Habberstad, J
End, T
Dahlen, M
机构
[1] UNIV TROMSO HOSP, N-9012 TROMSO, NORWAY
[2] RIGSHOSP, COPENHAGEN, DENMARK
[3] UNIV TRONDHEIM HOSP, TRONDHEIM, NORWAY
[4] TAMPERE UNIV HOSP, TAMPERE, FINLAND
[5] HAUKELAND HOSP, N-5021 BERGEN, NORWAY
[6] UNIV LUND HOSP, DEPT MED, S-22185 LUND, SWEDEN
[7] RIGSHOSP, MED HAEMATOL AFDELING L, DK-2100 COPENHAGEN O, DENMARK
[8] UNIV COPENHAGEN HOSP, MED HAEMATOL AFDELING L, DK-2730 HERLEV, DENMARK
[9] SAHLGRENS UNIV HOSP, CTR ONCOL, S-41345 GOTHENBURG, SWEDEN
[10] AARHUS UNIV HOSP, MED HAEMATOL AFDELING, DK-8000 AARHUS C, DENMARK
[11] NORRLAND UNIV HOSP, DEPT MED, S-90185 UMEA, SWEDEN
[12] OSTRA UNIV HOSP, DEPT MED, S-41685 GOTHENBURG, SWEDEN
[13] MALMO UNIV HOSP, DEPT MED, S-20401 MALMO, SWEDEN
[14] ULLEVAL HOSP, N-0407 OSLO 4, NORWAY
[15] SCHERING PLOUGH AB, S-10252 STOCKHOLM, SWEDEN
关键词
multiple myeloma; melphalan; prednisone; interferon alfa-2b; dose-response relationship; drug;
D O I
10.7326/0003-4819-124-2-199601150-00004
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Objective: To evaluate the addition of low-dose interferon-alpha 2b to standard melphalan-prednisone therapy in patients with multiple myeloma. Design: Randomized, multicenter, phase III study. Setting: 15 university hospitals and 92 county hospitals in Sweden, Norway, Denmark, Finland, and Iceland. Patients: 583 patients with symptomatic multiple myeloma. Intervention: All patients received melphalan-prednisone every 6 weeks. Melphalan-prednisone therapy was interrupted after at least 8 courses in responding patients who achieved a plateau phase, and it was reinstituted at time of relapse. Patients randomly assigned to receive melphalan-prednisone and interferon also received interferon, 5 MU three times weekly, from the start of treatment through response, plateau phase, and relapse, until definitive failure of melphalan-prednisone occurred. Measurements: Survival was the main outcome measure. Secondary measures were response rate, response and plateau phase duration, and toxicity. All analyses were done according to the principle of intention-to-treat. Results: 45% of patients receiving melphalan-prednisone and 44% of patients receiving melphalan-prednisone and interferon achieved at least a partial response. Response duration and plateau phase duration were longer for patients receiving melphalan-prednisone and interferon than for patients receiving melphalan-prednisone alone (P < 0.05); the difference in median duration was 5 to 6 months. Toxicity was higher with melphalan-prednisone and interferon, and this led to premature discontinuation of interferon therapy in one third of patients and to a reduced overall dose intensity for melphalan. The median survival time was 29 months for patients receiving melphalan-prednisone and 32 months for patients receiving melphalan-prednisone and interferon. The risk ratio for death for patients receiving melphalan-prednisone compared with patients receiving melphalan-prednisone and interferon was 1.02 (95% CI, 0.89 to 1.40). Conclusions: Adding continuous low-dose interferon to standard melphalan-prednisone therapy does not improve response rate or survival. However, response duration and plateau phase duration are prolonged by maintenance therapy with interferon.
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页码:212 / +
页数:1
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