Interferon-α 2b Added to Melphalan-Prednisone for Initial and Maintenance Therapy in Multiple Myeloma

A Randomized, Controlled Trial

  1. Martin Hjorth, MD, PhD;
  2. Jan Westin, MD, PhD;
  3. Inger Marie S. Dahl, MD, PhD;
  4. Peter Gimsing, MD, PhD;
  5. Erik Hippe, MD, PhD;
  6. Erik Holmberg, MSc;
  7. Jon Lamvik, MD, PhD;
  8. Johan Lanng Nielsen, MD, PhD;
  9. Eva Lofvenberg, MD, PhD;
  10. Ilmari P. Palva, MD, PhD;
  11. Stig Rodjer, MD, PhD;
  12. Ingebrigt Talstad, MD, PhD;
  13. Ingemar Turesson, MD, PhD;
  14. Finn Wisloff, MD, PhD; and
  15. Goran Zador, MD, PhD
  1. The Nordic Myeloma Study Group* Grant Support: In part by Schering-Plough, Sweden, Norway, and Denmark. Requests for Reprints: Martin Hjorth, MD, PhD, Department of Medicine, Lidkoping Hospital, S-53185 Lidkoping, Sweden. Current Author Addresses: Dr. Hjorth: Department of Medicine, Lidkoping Hospital, S-53185 Lidkoping, Sweden.

    Abstract

    Objective: To evaluate the addition of low-dose interferon-α2b 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.

    *For a listing of members of the Nordic Myeloma Study Group, see the Appendix.

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    1. Ann Intern Med January 15, 1996 vol. 124 no. 2 212-222
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