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Efficacy and safety of melphalan, arsenic trioxide and ascorbic acid combination therapy in patients with relapsed or refractory multiple myeloma: a prospective, multicentre, phase II, single-arm study

  1. James R. Berenson1,2,
  2. Ralph Boccia3,
  3. David Siegel4,
  4. Marek Bozdech5,
  5. Alberto Bessudo6,†,
  6. Edward Stadtmauer7,
  7. J. Talisman Pomeroy8,
  8. Ronald Steis9,
  9. Marshall Flam10,
  10. Jose Lutzky11,
  11. Syed Jilani12,
  12. Joseph Volk13,
  13. Siu-Fun Wong14,
  14. Robert Moss15,
  15. Ravi Patel16,
  16. Delina Ferretti2,
  17. Kit Russell2,
  18. Robert Louie17,‡,
  19. Howard S. Yeh1,2,
  20. Regina A. Swift1

Article first published online: 8 SEP 2006

DOI: 10.1111/j.1365-2141.2006.06280.x

Issue

British Journal of Haematology

British Journal of Haematology

Volume 135, Issue 2, pages 174–183, October 2006

Additional Information

How to Cite

Berenson, J. R., Boccia, R., Siegel, D., Bozdech, M., Bessudo, A., Stadtmauer, E., Talisman Pomeroy, J., Steis, R., Flam, M., Lutzky, J., Jilani, S., Volk, J., Wong, S.-F., Moss, R., Patel, R., Ferretti, D., Russell, K., Louie, R., Yeh, H. S. and Swift, R. A. (2006), Efficacy and safety of melphalan, arsenic trioxide and ascorbic acid combination therapy in patients with relapsed or refractory multiple myeloma: a prospective, multicentre, phase II, single-arm study. British Journal of Haematology, 135: 174–183. doi: 10.1111/j.1365-2141.2006.06280.x

Author Information

  1. 1

    Institute for Myeloma and Bone Cancer Research

  2. 2

    Oncotherapeutics, Inc., West Hollywood, CA

  3. 3

    Center for Cancer and Blood Disorders, Bethesda, MD

  4. 4

    Hackensack Medical Cancer Center, Hackensack, NJ

  5. 5

    Redwood Regional Oncology Center, Santa Rosa, CA

  6. 6

    San Diego Cancer Center, Vista, CA

  7. 7

    Department of Medicine, University of Pennsylvania, Philadelphia, PA

  8. 8

    Cancer Research and Prevention Center, Soquel, CA

  9. 9

    Atlanta Cancer Care, Atlanta, GA

  10. 10

    Hematology–Oncology Medical Group, Fresno, CA

  11. 11

    Mt Sinai Comprehensive Cancer Center, Miami Beach, FL

  12. 12

    Cancer Care Associates, Torrance, CA

  13. 13

    Palo Verde Hematology/Oncology Center, Glendale, AZ

  14. 14

    Hematology–Oncology Medical Group, Orange, CA

  15. 15

    Private practice, Fountain Valley, CA

  16. 16

    Comprehensive Blood and Cancer Center, Bakersfield, CA

  17. 17

    Cell Therapeutics, Inc., Seattle, WA, USA

  1. Present addresses: Alberto Bessudo, Pacific Oncology & Hematology, Encinitas, CA, USA.

  2. Robert Louie, Onyx Pharmaceuticals, Inc., Emeryville, CA, USA.

*James R. Berenson, Institute for Myeloma & Bone Cancer Research, 9201 W. Sunset Blvd., Suite 300, West Hollywood, CA 90069, USA. E-mail: jberenson@imbcr.org

Publication History

  1. Issue published online: 18 SEP 2006
  2. Article first published online: 8 SEP 2006
  3. Received 30 March 2006; accepted for publication 12 July 2006
Corrected by:

Erratum

Vol. 136, Issue 1, 173–174, Article first published online: 23 NOV 2006

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Keywords:

  • melphalan;
  • arsenic trioxide;
  • ascorbic acid;
  • multiple myeloma;
  • phase II trial

Summary

We assessed the safety and efficacy of melphalan, arsenic trioxide (ATO) and ascorbic acid (AA) (MAC) combination therapy for patients with multiple myeloma (MM) who failed more than two different prior regimens. Patients received melphalan (0·1 mg/kg p.o.), ATO (0·25 mg/kg i.v.) and AA (1 g i.v) on days 1–4 of week 1, ATO and AA twice weekly during weeks 2–5 and no treatment during week 6 of cycle 1; during cycles 2–6, the schedule remained the same except ATO and AA were given twice weekly in week 1. Objective responses occurred in 31 of 65 (48%) patients, including two complete, 15 partial and 14 minor responses. Median progression-free survival and overall survival were 7 and 19 months respectively. Twenty-two patients had elevated serum creatinine levels (SCr) at baseline, and 18 of 22 (82%) showed decreased SCr levels during treatment. Specific grade 3/4 haematological (3%) or cardiac adverse events occurred infrequently. Frequent grade 3/4 non-haematological adverse events included fever/chills (15%), pain (8%) and fatigue (6%). This steroid-free regimen was effective and well tolerated in this heavily pretreated group. These results indicate that the MAC regimen is a new therapeutic option for patients with relapsed or refractory MM.

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