Abstract
Bortezomib (btz) has established efficacy in relapsed/refractory multiple myeloma (MM) patients (pts). Combinations of btz and other agents can produce even higher response rates. We have reported that oral cyclophosphamide (CY) + prednisone (P) produced partial remissions (PR) in 41% and a median progression free survival (PFS) of 18.6 mos in MM pts who had progressed after ASCT. We now report a phase I trial adding btz to CY + P in 27 patients with relapsed/refractory MM. CY was given p.o. once weekly on days 1, 8, 15, and 22 of a 28 day cycle while P 100 mg was given every other morning. CY was given before btz on appropriate days. A total of 8 cycles was planned.
The median age was 59 yrs (48–74); 16 were male. Ig subtypes were: IgG (19 pts), IgA (4 pts), kappa light chain (4 pts). The median number of prior regimens was 2 (1–6); all had undergone prior ASCT and 59% had received thalidomide and/or lenalidomide. The median pretreatment β2-microglobulin was 228 nm/L (114–875), albumin 38 g/L (30–46) and creatinine 86 nmol/L (58–153).
The dose escalation scheme and toxicity with cycle 1 is shown below:
Dose levels and toxicity
| Dose Level . | N . | CY dose (mg/m2) . | Btz dose (mg/m2) . | Gr 3–4 Toxicity (cycle 1) . |
|---|---|---|---|---|
| *Community acquired pneumonia without neutropenia; ** protocol amended to exclude G-CSF for 2 weeks before study entry. | ||||
| 1 | 6 | 150 | 0.7 d 1,8,15 | 2 CAP* |
| 2 | 3 | 300 | 0.7 d 1,8,15 | 0 |
| 3 | 3 | 300 | 1.0 d 1,8,15 | 1 ↓ PO4 |
| 4 | 6 | 300 | 1.0 d 1,4,8,11 | 1 ↓ANC**; 1 ↑ AST/ALT |
| 5 | 6 | 300 | 1.3 d 1,4,8,11 | 1 N/V |
| 6 | 3 | 300 | 1.5 d 1,8,15 | 0 |
| Dose Level . | N . | CY dose (mg/m2) . | Btz dose (mg/m2) . | Gr 3–4 Toxicity (cycle 1) . |
|---|---|---|---|---|
| *Community acquired pneumonia without neutropenia; ** protocol amended to exclude G-CSF for 2 weeks before study entry. | ||||
| 1 | 6 | 150 | 0.7 d 1,8,15 | 2 CAP* |
| 2 | 3 | 300 | 0.7 d 1,8,15 | 0 |
| 3 | 3 | 300 | 1.0 d 1,8,15 | 1 ↓ PO4 |
| 4 | 6 | 300 | 1.0 d 1,4,8,11 | 1 ↓ANC**; 1 ↑ AST/ALT |
| 5 | 6 | 300 | 1.3 d 1,4,8,11 | 1 N/V |
| 6 | 3 | 300 | 1.5 d 1,8,15 | 0 |
All the above toxicities above were gr 3 except for 1 transient episode of gr 4 hypophosphatemia. Dose limiting toxicity was not seen. The median number of protocol cycles given per pt was 7 (1–8); 1 pt chose to continue therapy and has received 15 cycles. Toxicities in cycles 2–8 were generally mild. Episodes of infection included shingles (5), gr 3 respiratory infection (6) and febrile neutropenia (2). A total of 168 cycles have been administered; the dose of CY was reduced in 5 cycles due to neutropenia (↓ANC) (3), thrombocytopenia (1) or increased AST/ALT (1), while the btz dose was decreased in 4 cycles due to gr 2 peripheral neuropathy (PN) (1) or ↓ANC (3). 12 pts have completed all 8 cycles, 5 are on therapy and 7 have progressed after a median of cycles 3 (1–7). 3 stopped protocol therapy (physician choice in 1 pt with minimal response, gr 2 PN in 2 pts (after 7 cycles at dose levels 2 and 5) including the pt with prior btz dose reduction. 14/15 pts treated at dose levels 4–6 (effective btz doses) were evaluable for response after receiving at least 2 cycles. Best response was CR/nearCR in 6 (43%) and PR in 7 (50%) for an overall response rate of 93%. The median follow-up is 12 mos (1–20). 6 pts have progressed after stopping therapy. The median PFS is 11 mos, while the median overall survival (OS) has not been reached. The actuarial 1 year OS and PFS are 83% (95% CI 61–93%) and 47% (95% CI 24–68%), respectively.
7 of 10 planned additional pts have entered the phase II portion of the trial at dose level 6. 3 have completed at least 2 cycles; 2 are in CR/near CR while one is in PR.
We conclude:
Btz 1.5 mg/m2 can be given safely on a convenient weekly schedule days 1, 8 and 15 of a 28 day cycle in combination with full dose oral CY + P in relapsed/refractory MM pts;
preliminary response rates at this dose level include 4/6 (67%) CR/near CRs and 1/6 (17%) PR.
Disclosures: Bortezomib in combination with cyclophosphamide and prednisone.; Donna E Reece, MD--consultancy for development of research protocol for bortezomib in Primary amyloidosis for Johnson & Johnson; consultancy for Ortho Biotech Canada for analysis of financial impact of bortezomib in Ontario and for planning Canadian symposia on proteasome inhibition; Joseph R Mikhael, MD - consultancy for Ortho Biotech Canada; Keith Stewart, MD - consultancy for Ortho Biotech Canada and Millennium Pharmaceuticals, Inc.; Donna E Reece, MD -- research funding for bortezomib pharmacokinetics trial from Millennium Pharmaceuticals Inc.; research funding for phase I-II investigator initiated trial with bortezomib in relapsed/refractory myeloma from Ortho Biotech Canada (current study); research funding for phase II industry sponsored mulitcentre trial of bortezomib as induction therapy in myeloma from Ortho Biotech Canada; research funding for Canadian Expanded Access Program for bortezomib from Ortho Biotech Canada; research funding for international phase I–II trial of bortezomib in primary amyloidosis from Johnson & Johnson.; Keith Stewart, MD --research funding for clinical trials from Ortho Biotech Canada and Millennium Pharmaceuticals, Inc.; Donna E Reece, MD - honoraria for unrestricted educational lectures and Advisory Committee chair/moderator/speaker for Ortho Biotech Canada; Giovanni Piza MD - honorarium for development of case report forms for Ortho Biotech Canada; Joseph R Mikhael, MD - honoraria from Ortho Biotech; Keith Stewart, MD[ ndash] honoraria from Ortho Biotech Canada and Millennium Pharmaceuticals, Inc.; Donna E Reece - Advisory Committee chair/speaker for Ortho Biotech Canada; Joseph R Mikhael, MD - Advisory Board participant for Ortho Biotech Canada.; Donna E Reece, MD - one year funding for myeloma database entry person from Ortho Biotech Canada.
Author notes
Corresponding author
This feature is available to Subscribers Only
Sign In or Create an Account Close Modal