Abstract
Abstract 3979
In recent years, proteasome inhibition with bortezomib (Bort) and immunomodulation with lenalidomide (Len) has resulted in improved outcomes of patients with multiple myeloma. However, neither of these treatment options offers a cure for patients, as they will eventually relapse and require alternate therapy. The optimal sequence of therapy with these two agents has yet to be established.
All adult patients with multiple myeloma who received both Bort and Len non-concurrently at our institution between January 2004 and August 2010 were included in this analysis. The primary endpoints were overall survival and response (partial response or better) to therapy among two groups of patients: Group A, those who received len-based therapy followed by bort-based therapy and, Group B, those who received bort-based therapy followed by len-based therapy.
208 patients were identified and divided into the two groups (97 in Group A, 111 in Group B). Baseline demographics are summarized in Table 1. Patients in Group B were younger (60 vs 57 years; p=0.03), had more bone disease (61% vs 77%; p=0.03), and were more likely to receive a stem cell transplant (57% vs 71%; p=0.04). The median overall survival was not statistically different between the 2 groups (Group A versus Group B: 78.5 vs. 74.0 months, respectively; p=0.62). The sequence of therapy was not predictive of overall survival within subgroups (including patients with poor risk cytogenetics, elevated beta2-microglobulin, presence of bone disease), with the exception of patients with a serum creatinine ≥2 mg/dl at diagnosis. In this case, Group B had a better median overall survival than Group A (24.1 vs 53.9 months, p=0.01). In addition, among patients who have received Len and Bort without intervening therapy (n= 158), no difference in overall survival was noted in Group A and B. There was also no statistically significant difference in response rates (partial response or better) to bort-based therapy between Group A and B (68.7% vs. 77.2% respectively, p= 0.265) nor to len-based therapy between Group A and B (60.4% vs. 73.6% respectively, p=0.168). Multivariable analysis identified baseline renal dysfunction and the presence of bone disease at diagnosis as predictors of worse outcomes however the sequence of therapy was not a predictor of outcome. ISS stage and b2m were not entered in the logistic regression model as these were only available on 30–40% of patients at baseline.
Characteristic . | Lenalidomide First . | Bortezomib First . |
---|---|---|
Group A (n=97) | Group B (n=111) | |
Mean Age, years ± SD | 60 ± 9.5 | 57 ± 9.8 |
Gender, % male | 56.0 | 62.2 |
Caucasian, n (%) | 76 (78.4) | 89 (80.2) |
MM Subtype, n (%) | ||
IgG | 56 (57.7) | 66 (59.5) |
IgA | 19 (19.6) | 26 (23.4) |
IgM | 1 (1.0) | 0 (0) |
Light Chain | 17 (17.5) | 17 (15.3) |
Non-Secretory | 4 (4.1) | 2 (1.8) |
ISS Stage, n (%)* | ||
I | 10 (25.6) | 12 (36.4) |
II | 16 (41.0) | 14 (41.2) |
III | 13 (33.3) | 8 (23.5) |
Total* | 39 (40.2) | 34 (30.6) |
Initial serum creatinine>2 mg/dl, n (%)* | 8 (9.8) | 15(15.3) |
Median β2M level, n (range) | 3.8 (1.2–16.6) | 3.5 (1–60) |
Presence of bone disease, n (%)* | 54 (61.4) | 75 (76.5) |
Received stem cell transplant, n (%) | 55 (56.7) | 79 (71.1) |
Poor-Risk FISH Abnormalities, n (%)** | 32 (33.3) | 44 (42.3) |
Characteristic . | Lenalidomide First . | Bortezomib First . |
---|---|---|
Group A (n=97) | Group B (n=111) | |
Mean Age, years ± SD | 60 ± 9.5 | 57 ± 9.8 |
Gender, % male | 56.0 | 62.2 |
Caucasian, n (%) | 76 (78.4) | 89 (80.2) |
MM Subtype, n (%) | ||
IgG | 56 (57.7) | 66 (59.5) |
IgA | 19 (19.6) | 26 (23.4) |
IgM | 1 (1.0) | 0 (0) |
Light Chain | 17 (17.5) | 17 (15.3) |
Non-Secretory | 4 (4.1) | 2 (1.8) |
ISS Stage, n (%)* | ||
I | 10 (25.6) | 12 (36.4) |
II | 16 (41.0) | 14 (41.2) |
III | 13 (33.3) | 8 (23.5) |
Total* | 39 (40.2) | 34 (30.6) |
Initial serum creatinine>2 mg/dl, n (%)* | 8 (9.8) | 15(15.3) |
Median β2M level, n (range) | 3.8 (1.2–16.6) | 3.5 (1–60) |
Presence of bone disease, n (%)* | 54 (61.4) | 75 (76.5) |
Received stem cell transplant, n (%) | 55 (56.7) | 79 (71.1) |
Poor-Risk FISH Abnormalities, n (%)** | 32 (33.3) | 44 (42.3) |
On available patients
Defined by presence of one or more of the following FISH abnormalities: del 13q, del 17 p, t(4;14) or t(14;16)
To our knowledge, this is the only study that has examined the impact of sequence of therapy with immunomodulators and proteasome inhibitors in myeloma. This data suggests that the sequence of therapy with these agents is only relevant in patients who have baseline renal insufficiency (≥2 mg/dl at diagnosis); therefore, a bort-based treatment should be considered as first-line therapy in these patients.
Alsina:Millennium: Consultancy, Membership on an entity's Board of Directors or advisory committees, Research Funding; Novartis: Consultancy, Membership on an entity's Board of Directors or advisory committees; Allergan: Research Funding. Djulbegovic:Millenium: Research Funding. Baz:Millenium: Research Funding, Speakers Bureau; Celgene: Research Funding.
Author notes
Asterisk with author names denotes non-ASH members.