Background: Single autologous stem cell transplant (ASCT) is considered the standard of care for younger multiple myeloma (MM) patients (pts). However, it is not curative and virtually all patients will ultimately relapse. As more options, such as biological therapy, are available to treat relapsed disease, the role of a second ASCT as salvage therapy is unclear.

Method: Retrospective review of all MM pts who received a 2nd ASCT as salvage therapy at Princess Margaret Hospital.

Results: Between February 1997 and June 2007, 61 MM pts received a second ASCT for relapsed MM at our institution. Median age was 56 yrs (range 35–71) at second transplant. 37 pts (61%) were male. Immunoglobulin subtype included IgG (36), IgA (14), light chain (6), nonsecretory (3), IgM(1) and IgD (1). Transplant conditioning regimen for first transplant was high dose melphalan (MEL) 140–200 mg/m2 in 51, MEL/etoposide(E)/TBI in 4, and MELl/TBI in 2. 2nd ASCT conditioning consisted of MEL + TBI +/− E in 2, MEL alone in 58 and Busulfan/Cyclophosphomide in 1. The median time from diagnosis to first transplant was 9.7 months (2.0–74.2). The median time to relapse after the first transplant was 32.6 months (9.7–85.6), with a median interval between transplants of 45.1 months (19.7– 115). Two transplant-related deaths occurred (3%). Response to first transplant was 4 CR (8%), 34 PR (68%), 2 MR (4%) and 10 SD (20%). Nineteen pts went on to maintenance therapy between transplants. Response to second transplant was 4 CR (8%), 41 PR (80%), 5 SD (10%) and 1 PD (2%). Median progression-free survival (PFS) was 15.8 months (0–63.8) while median overall survival (OS) was 4.2 years (0–7.0) after 2nd ASCT. The relationship between progression-free interval after 1st ASCT and the outcome of the 2nd ASCT is summarized Table 1. Patients can be stratified into two groups, those with a disease free interval of less than or greater than 24 months. The use of maintenance therapy did not differ between the two groups, 6 (40%) in patients with PFS ≤24 months and 13 (28%) in patients with PFS >24 months.

Conclusions:

  1. 2nd ASCT is a feasible and safe salvage therapy in patients with relapsed MM.

  2. 2nd ASCT is effective in providing a median progression free survival of 1.25 years and median overall survival of 4.2 years after 2nd ASCT - results that compare favourably with other salvage approaches.

  3. Patients with a longer disease free interval after 1st ASCT experience a better progression free survival and overall survival after 2nd ASCT.

  4. It is reasonable, therefore, to consider a 2nd ASCT if the time to progression is greater than 2 years after first ASCT.

Outcomes Based on Time to Progression Post 1st ASCT

PFS post 1st ASCT# of ptsmedian PFS post 2nd ASCTPFS post 2nd ASCT1Median OS post 2nd ASCTOS post 2nd ASCT2
1 p< 0.005, 2 p< 0.05 
≤24 months 15 12.7 months 1 year: 46% 3.5 years 1 year: 85% 
   2 year: 11%  2 years: 76% 
   3 years 0%  3 years: 63% 
     4 years: 31% 
> 24 months 46 19.8 months 1 year: 74% 5.9 years 1 year: 91% 
   2 year: 45%  2 years: 82% 
   3 year: 31%  3 years: 65% 
     4 years: 55% 
PFS post 1st ASCT# of ptsmedian PFS post 2nd ASCTPFS post 2nd ASCT1Median OS post 2nd ASCTOS post 2nd ASCT2
1 p< 0.005, 2 p< 0.05 
≤24 months 15 12.7 months 1 year: 46% 3.5 years 1 year: 85% 
   2 year: 11%  2 years: 76% 
   3 years 0%  3 years: 63% 
     4 years: 31% 
> 24 months 46 19.8 months 1 year: 74% 5.9 years 1 year: 91% 
   2 year: 45%  2 years: 82% 
   3 year: 31%  3 years: 65% 
     4 years: 55% 

Author notes

Disclosure: No relevant conflicts of interest to declare.

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