23 results on '"Bahlis, N.J."'
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2. Sustained minimal residual disease negativity in newly diagnosed multiple myeloma and the impact of daratumumab in MAIA and ALCYONE
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San-Miguel, J. Avet-Loiseau, H. Paiva, B. Kumar, S. Dimopoulos, M.A. Facon, T. Mateos, M.-V. Touzeau, C. Jakubowiak, A. Usmani, S.Z. Cook, G. Cavo, M. Quach, H. Ukropec, J. Ramaswami, P. Pei, H. Qi, M. Sun, S. Wang, J. Krevvata, M. DeAngelis, N. Heuck, C. Van Rampelbergh, R. Kudva, A. Kobos, R. Qi, M. Bahlis, N.J.
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body regions ,hemic and lymphatic diseases - Abstract
In patients with transplant-ineligible newly diagnosed multiple myeloma (NDMM), daratumumab reduced the risk of disease progression or death by 44% in MAIA (daratumumab/lenalidomide/dexamethasone [D-Rd]) and 58% in ALCYONE (daratumumab/bortezomib/melphalan/prednisone [D-VMP]). Minimal residual disease (MRD) is a sensitive measure of disease and response to therapy. MRD-negativity status and durability were assessed in MAIA and ALCYONE. MRD assessments using next-generation sequencing (10−5) occurred for patients achieving complete response (CR) or better and after at least CR at 12, 18, 24, and 30 months from the first dose. Progression-free survival (PFS) by MRD status and sustained MRD negativity lasting ≥6 and ≥12 months were analyzed in the intent-to-treat population and among patients achieving at least CR. In MAIA (D-Rd, n = 368; lenalidomide and dexamethasone [Rd], n = 369) and ALCYONE (D-VMP, n = 350; bortezomib/melphalan/prednisone [VMP], n = 356), the median duration of follow-up was 36.4 and 40.1 months, respectively. MRD-negative status and sustained MRD negativity lasting ≥6 and ≥12 months were associated with improved PFS, regardless of treatment group. However, daratumumab-based therapy improved rates of MRD negativity lasting ≥6 months (D-Rd, 14.9% vs Rd, 4.3%; D-VMP, 15.7% vs VMP, 4.5%) and ≥12 months (D-Rd, 10.9% vs Rd, 2.4%; D-VMP, 14.0% vs VMP, 2.8%), both of which translated to improved PFS vs control groups. In a pooled analysis, patients who were MRD negative had improved PFS vs patients who were MRD positive. Patients with NDMM who achieved MRD-negative status or sustained MRD negativity had deep remission and improved clinical outcomes. These trials were registered at www.clinicaltrials.gov as #NCT02252172 (MAIA) and #NCT02195479 (ALCYONE). © 2022 American Society of Hematology
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- 2022
3. Prognostic value of minimal residual disease negativity in myeloma: combined analysis of POLLUX, CASTOR, ALCYONE, and MAIA
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Cavo, M. San-Miguel, J. Usmani, S.Z. Weisel, K. Dimopoulos, M.A. Avet-Loiseau, H. Paiva, B. Bahlis, N.J. Plesner, T. Hungria, V. Moreau, P. Mateos, M.-V. Perrot, A. Iida, S. Facon, T. Kumar, S. van de Donk, N.W.C.J. Sonneveld, P. Spencer, A. Krevvata, M. Heuck, C. Wang, J. Ukropec, J. Kobos, R. Sun, S. Qi, M. Munshi, N.
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hemic and lymphatic diseases - Abstract
We explored minimal residual disease (MRD) in relapsed/refractory multiple myeloma (RRMM) and transplant-ineligible (TIE) newly diagnosed multiple myeloma (NDMM) using data from 4 phase 3 studies (POLLUX, CASTOR, ALCYONE, and MAIA). Each study previously demonstrated that daratumumab-based therapies improved MRD negativity rates and reduced the risk of disease progression or death by approximately half vs standards of care. We conducted a large-scale pooled analysis for associations between patients achieving complete response or better (≥CR) with MRD-negative status and progression-free survival (PFS). MRD was assessed via next-generation sequencing (10−5 sensitivity threshold). Patient-level data were pooled from all 4 studies and for patients with TIE NDMM and patients with RRMM who received ≤2 prior lines of therapy (≤2 PL). PFS was evaluated by response and MRD status. Median follow-up (months) was 54.8 for POLLUX, 50.2 for CASTOR, 40.1 for ALCYONE, and 36.4 for MAIA. Patients who achieved ≥CR and MRD negativity had improved PFS vs those who failed to reach CR or were MRD positive (TIE NDMM and RRMM hazard ratio [HR] 0.20, P
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- 2022
4. Health-related quality of life in patients with relapsed or refractory multiple myeloma: treatment with daratumumab, lenalidomide, and dexamethasone in the phase 3 POLLUX trial
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Plesner, T. Dimopoulos, M.A. Oriol, A. San-Miguel, J. Bahlis, N.J. Rabin, N. Suzuki, K. Yoon, S.-S. Ben-Yehuda, D. Cook, G. Goldschmidt, H. Grosicki, S. Qin, X. Fastenau, J. Garvin, W. Carson, R. Renaud, T. Gries, K.S.
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humanities - Abstract
In the phase 3 POLLUX trial, daratumumab in combination with lenalidomide and dexamethasone (D-Rd) significantly improved progression-free survival in patients with relapsed/refractory multiple myeloma (RRMM) compared with lenalidomide and dexamethasone (Rd) alone. Here, we present patient-reported outcomes (PROs) from POLLUX, assessed using the validated European Organisation for Research and Treatment of Cancer Quality of Life Questionnaire Core 30-item (EORTC QLQ-C30) and the EuroQol 5-dimensional descriptive system (EQ-5D-5L) questionnaires. Changes from baseline are presented as least-squares mean changes with 95% confidence intervals (CIs) derived from a mixed-effects model. PRO assessment compliance rates were high and similar in both D-Rd and Rd groups through cycle 40 (week 156). In this on-treatment analysis, mean changes from baseline were significantly greater in EORTC QLQ-C30 global health status, physical functioning, and pain scores in the D-Rd group versus the Rd group at multiple time points; however, magnitude of changes was low, suggesting no meaningful impact on health-related quality of life (HRQoL). Subgroup results were similar to those in the overall population. In the POLLUX study, baseline HRQoL was maintained with prolonged D-Rd treatment. These findings complement the sustained and significant improvement in progression-free survival observed with D-Rd and supports its use in patients with RRMM. Clinical trial registration: NCT02076009. © 2021 British Society for Haematology and John Wiley & Sons Ltd.
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- 2021
5. Effect of prior treatments on selinexor, bortezomib, and dexamethasone in previously treated multiple myeloma
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Mateos, M.V. Gavriatopoulou, M. Facon, T. Auner, H.W. Leleu, X. Hájek, R. Dimopoulos, M.A. Delimpasi, S. Simonova, M. Špička, I. Pour, L. Kriachok, I. Pylypenko, H. Doronin, V. Usenko, G. Benjamin, R. Dolai, T.K. Sinha, D.K. Venner, C.P. Garg, M. Stevens, D.A. Quach, H. Jagannath, S. Moreau, P. Levy, M. Badros, A.Z. Anderson, L.D., Jr. Bahlis, N.J. Cavo, M. Chai, Y. Jeha, J. Arazy, M. Shah, J. Shacham, S. Kauffman, M.G. Richardson, P.G. Grosicki, S.
- Abstract
Therapeutic regimens for previously treated multiple myeloma (MM) may not provide prolonged disease control and are often complicated by significant adverse events, including peripheral neuropathy. In patients with previously treated MM in the Phase 3 BOSTON study, once weekly selinexor, once weekly bortezomib, and 40 mg dexamethasone (XVd) demonstrated a significantly longer median progression-free survival (PFS), higher response rates, deeper responses, a trend to improved survival, and reduced incidence and severity of bortezomib-induced peripheral neuropathy when compared with standard twice weekly bortezomib and 80 mg dexamethasone (Vd). The pre-specified analyses described here evaluated the influence of the number of prior lines of therapy, prior treatment with lenalidomide, prior proteasome inhibitor (PI) therapy, prior immunomodulatory drug therapy, and prior autologous stem cell transplant (ASCT) on the efficacy and safety of XVd compared with Vd. In this 1:1 randomized study, enrolled patients were assigned to receive once weekly oral selinexor (100 mg) with once weekly subcutaneous bortezomib (1.3 mg/m2) and 40 mg per week dexamethasone (XVd) versus standard twice weekly bortezomib and 80 mg per week dexamethasone (Vd). XVd significantly improved PFS, overall response rate, time-to-next-treatment, and showed reduced all grade and grade ≥ 2 peripheral neuropathy compared with Vd regardless of prior treatments, but the benefits of XVd over Vd were more pronounced in patients treated earlier in their disease course who had either received only one prior therapy, had never been treated with a PI, or had prior ASCT. Treatment with XVd improved outcomes as compared to Vd regardless of prior therapies as well as manageable and generally reversible adverse events. XVd was associated with clinical benefit and reduced peripheral neuropathy compared to standard Vd in previously treated MM. These results suggest that the once weekly XVd regimen may be optimally administered to patients earlier in their course of disease, as their first bortezomib-containing regimen, and in those relapsing after ASCT. Trial registration: ClinicalTrials.gov (NCT03110562). Registered 12 April 2017. https://clinicaltrials.gov/ct2/show/NCT03110562. © 2021, The Author(s).
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- 2021
6. Selinexor, bortezomib, and dexamethasone versus bortezomib and dexamethasone in previously treated multiple myeloma: Outcomes by cytogenetic risk
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Richard, S. Chari, A. Delimpasi, S. Simonova, M. Spicka, I. Pour, L. Kriachok, I. Dimopoulos, M.A. Pylypenko, H. Auner, H.W. Leleu, X. Usenko, G. Hajek, R. Benjamin, R. Dolai, T.K. Sinha, D.K. Venner, C.P. Garg, M. Stevens, D.A. Quach, H. Jagannath, S. Moreau, P. Levy, M. Badros, A. Anderson, L.D., Jr. Bahlis, N.J. Facon, T. Mateos, M.V. Cavo, M. Chang, H. Landesman, Y. Chai, Y. Arazy, M. Shah, J. Shacham, S. Kauffman, M.G. Grosicki, S. Richardson, P.G.
- Abstract
In the phase 3 BOSTON study, patients with multiple myeloma (MM) after 1–3 prior regimens were randomized to once-weekly selinexor (an oral inhibitor of exportin 1 [XPO1]) plus bortezomib-dexamethasone (XVd) or twice-weekly bortezomib-dexamethasone (Vd). Compared with Vd, XVd was associated with significant improvements in median progression-free survival (PFS), overall response rate (ORR), and lower rates of peripheral neuropathy, with trends in overall survival (OS) favoring XVd. In BOSTON, 141 (35.1%) patients had MM with high-risk (presence of del[17p], t[4;14], t[14;16], or ≥4 copies of amp1q21) cytogenetics (XVd, n = 70; Vd, n = 71), and 261 (64.9%) exhibited standard-risk cytogenetics (XVd, n = 125; Vd, n = 136). Among patients with high-risk MM, median PFS was 12.91 months for XVd and 8.61 months for Vd (HR, 0.73 [95% CI, (0.4673, 1.1406)], p = 0.082), and ORRs were 78.6% and 57.7%, respectively (OR 2.68; p = 0.004). In the standard-risk subgroup, median PFS was 16.62 months for XVd and 9.46 months for Vd (HR 0.61; p = 0.004), and ORRs were 75.2% and 64.7%, respectively (OR 1.65; p = 0.033). The safety profiles of XVd and Vd in both subgroups were consistent with the overall population. These data suggest that selinexor can confer benefits to patients with MM regardless of cytogenetic risk. ClinicalTrials.gov identifier: NCT03110562. © 2021 The Authors. American Journal of Hematology published by Wiley Periodicals LLC.
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- 2021
7. Effect of age and frailty on the efficacy and tolerability of once-weekly selinexor, bortezomib, and dexamethasone in previously treated multiple myeloma
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Auner, H.W. Gavriatopoulou, M. Delimpasi, S. Simonova, M. Spicka, I. Pour, L. Dimopoulos, M.A. Kriachok, I. Pylypenko, H. Leleu, X. Doronin, V. Usenko, G. Hajek, R. Benjamin, R. Dolai, T.K. Sinha, D.K. Venner, C.P. Garg, M. Stevens, D.A. Quach, H. Jagannath, S. Moreau, P. Levy, M. Badros, A. Anderson, L.D., Jr. Bahlis, N.J. Facon, T. Mateos, M.V. Cavo, M. Chai, Y. Arazy, M. Shah, J. Shacham, S. Kauffman, M.G. Richardson, P.G. Grosicki, S.
- Abstract
Elderly and frail patients with multiple myeloma (MM) are more vulnerable to the toxicity of combination therapies, often resulting in treatment modifications and suboptimal outcomes. The phase 3 BOSTON study showed that once-weekly selinexor and bortezomib with low-dose dexamethasone (XVd) improved PFS and ORR compared with standard twice-weekly bortezomib and moderate-dose dexamethasone (Vd) in patients with previously treated MM. This is a retrospective subgroup analysis of the multicenter, prospective, randomized BOSTON trial. Post hoc analyses were performed to compare XVd versus Vd safety and efficacy according to age and frailty status (
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- 2021
8. Early M-Protein Dynamics Predicts Progression-Free Survival in Patients With Relapsed/Refractory Multiple Myeloma
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Yan, X. Xu, X.S. Weisel, K.C. Mateos, M.-V. Sonneveld, P. Dimopoulos, M.A. Usmani, S.Z. Bahlis, N.J. Puchalski, T. Ukropec, J. Bellew, K. Ming, Q. Sun, S. Zhou, H.
- Abstract
This study aimed to predict long-term progression-free survival (PFS) using early M-protein dynamic measurements in patients with relapsed/refractory multiple myeloma (MM). The PFS was modeled based on dynamic M-protein data from two phase III studies, POLLUX and CASTOR, which included 569 and 498 patients with relapsed/refractory MM, respectively. Both studies compared active controls (lenalidomide and dexamethasone, and bortezomib and dexamethasone, respectively) alone vs. in combination with daratumumab. Three M-protein dynamic features from the longitudinal M-protein data were evaluated up to different time cutoffs (1, 2, 3, and 6 months). The abilities of early M-protein dynamic measurements to predict the PFS were evaluated using Cox proportional hazards survival models. Both univariate and multivariable analyses suggest that maximum reduction of M-protein (i.e., depth of response) was the most predictive of PFS. Despite the statistical significance, the baseline covariates provided very limited predictive value regarding the treatment effect of daratumumab. However, M-protein dynamic features obtained within the first 2 months reasonably predicted PFS and the associated treatment effect of daratumumab. Specifically, the areas under the time-varying receiver operating characteristic curves for the model with the first 2 months of M-protein dynamic data were ~ 0.8 and 0.85 for POLLUX and CASTOR, respectively. Early M-protein data within the first 2 months can provide a prospective and reasonable prediction of future long-term clinical benefit for patients with MM. © 2020 The Authors. Clinical and Translational Science published by Wiley Periodicals LLC on behalf of the American Society for Clinical Pharmacology and Therapeutics.
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- 2020
9. Daratumumab plus lenalidomide and dexamethasone in relapsed/ refractory multiple myeloma: extended follow-up of POLLUX, a randomized, open-label, phase 3 study
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Bahlis, N.J. (Nizar J.), Dimopoulos, M.A. (Meletios A.), White, D.J. (Darrell J.), Benboubker, L. (Lotfi), Cook, G. (Gordon), Leiba, M. (Merav), Ho, P.J. (P. Joy), Kim, K. (Kihyun), Takezako, N. (Naoki), Moreau, P. (Philippe), Kaufman, J.L. (Jonathan L.), Krevvata, M. (Maria), Chiu, C. (Christopher), Qin, X. (Xiang), Okonkwo, L. (Linda), Trivedi, S. (Sonali), Ukropec, J. (Jon), Qi, M. (Ming), and San-Miguel, J.F. (Jesús F.)
- Abstract
In POLLUX, daratumumab (D) plus lenalidomide/dexamethasone (Rd) reduced the risk of disease progression or death by 63% and increased the overall response rate (ORR) versus Rd in relapsed/refractory multiple myeloma (RRMM). Updated efficacy and safety after >3 years of follow-up are presented. Patients (N = 569) with ≥1 prior line received Rd (lenalidomide, 25 mg, on Days 1–21 of each 28-day cycle; dexamethasone, 40 mg, weekly) ± daratumumab at the approved dosing schedule. Minimal residual disease (MRD) was assessed by next-generation sequencing. After 44.3 months median follow-up, D-Rd prolonged progression-free survival (PFS) in the intent-to-treat population (median 44.5 vs 17.5 months; HR, 0.44; 95% CI, 0.35–0.55; P
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- 2020
10. Once-per-week selinexor, bortezomib, and dexamethasone versus twice-per-week bortezomib and dexamethasone in patients with multiple myeloma (BOSTON): a randomised, open-label, phase 3 trial
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Grosicki, S. Simonova, M. Spicka, I. Pour, L. Kriachok, I. Gavriatopoulou, M. Pylypenko, H. Auner, H.W. Leleu, X. Doronin, V. Usenko, G. Bahlis, N.J. Hajek, R. Benjamin, R. Dolai, T.K. Sinha, D.K. Venner, C.P. Garg, M. Gironella, M. Jurczyszyn, A. Robak, P. Galli, M. Wallington-Beddoe, C. Radinoff, A. Salogub, G. Stevens, D.A. Basu, S. Liberati, A.M. Quach, H. Goranova-Marinova, V.S. Bila, J. Katodritou, E. Oliynyk, H. Korenkova, S. Kumar, J. Jagannath, S. Moreau, P. Levy, M. White, D. Gatt, M.E. Facon, T. Mateos, M.V. Cavo, M. Reece, D. Anderson, L.D., Jr Saint-Martin, J.-R. Jeha, J. Joshi, A.A. Chai, Y. Li, L. Peddagali, V. Arazy, M. Shah, J. Shacham, S. Kauffman, M.G. Dimopoulos, M.A. Richardson, P.G. Delimpasi, S.
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hemic and lymphatic diseases - Abstract
Background: Selinexor combined with dexamethasone has shown activity in patients with heavily pre-treated multiple myeloma. In a phase 1b/2 study, the combination of oral selinexor with bortezomib (a proteasome inhibitor) and dexamethasone induced high response rates with low rates of peripheral neuropathy, the main dose-limiting toxicity of bortezomib. We aimed to evaluate the clinical benefit of weekly selinexor, bortezomib, and dexamethasone versus standard bortezomib and dexamethasone in patients with previously treated multiple myeloma. Methods: This phase 3, randomised, open-label trial was done at 123 sites in 21 countries. Patients aged 18 years or older, who had multiple myeloma, and who had previously been treated with one to three lines of therapy, including proteasome inhibitors, were randomly allocated (1:1) to receive selinexor (100 mg once per week), bortezomib (1·3 mg/m2 once per week), and dexamethasone (20 mg twice per week), or bortezomib (1·3 mg/m2 twice per week for the first 24 weeks and once per week thereafter) and dexamethasone (20 mg four times per week for the first 24 weeks and twice per week thereafter). Randomisation was done using interactive response technology and stratified by previous proteasome inhibitor therapy, lines of treatment, and multiple myeloma stage. The primary endpoint was progression-free survival in the intention-to-treat population. Patients who received at least one dose of study treatment were included in the safety population. This trial is registered at ClinicalTrials.gov, NCT03110562. The trial is ongoing, with 55 patients remaining on randomised therapy as of Feb 20, 2020. Findings: Of 457 patients screened for eligibility, 402 were randomly allocated—195 (49%) to the selinexor, bortezomib, and dexamethasone group and 207 (51%) to the bortezomib and dexamethasone group—and the first dose of study medication was given between June 6, 2017, and Feb 5, 2019. Median follow-up durations were 13·2 months [IQR 6·2–19·8] for the selinexor, bortezomib, and dexamethasone group and 16·5 months [9·4–19·8] for the bortezomib and dexamethasone group. Median progression-free survival was 13·93 months (95% CI 11·73–not evaluable) with selinexor, bortezomib, and dexamethasone and 9·46 months (8·11–10·78) with bortezomib and dexamethasone (hazard ratio 0·70 [95% CI 0·53–0·93], p=0·0075). The most frequent grade 3–4 adverse events were thrombocytopenia (77 [39%] of 195 patients in the selinexor, bortezomib, and dexamethasone group vs 35 [17%] of 204 in the bortezomib and dexamethasone group), fatigue (26 [13%] vs two [1%]), anaemia (31 [16%] vs 20 [10%]), and pneumonia (22 [11%] vs 22 [11%]). Peripheral neuropathy of grade 2 or above was less frequent with selinexor, bortezomib, and dexamethasone (41 [21%] patients) than with bortezomib and dexamethasone (70 [34%] patients; odds ratio 0·50 [95% CI 0·32–0·79], p=0·0013). 47 (24%) patients in the selinexor, bortezomib, and dexamethasone group and 62 (30%) in the bortezomib and dexamethasone group died. Interpretation: A once-per-week regimen of selinexor, bortezomib, and dexamethasone is a novel, effective, and convenient treatment option for patients with multiple myeloma who have received one to three previous lines of therapy. Funding: Karyopharm Therapeutics. © 2020 Elsevier Ltd
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- 2020
11. Daratumumab, lenalidomide, and dexamethasone in relapsed/refractory myeloma: a cytogenetic subgroup analysis of POLLUX
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Kaufman, J.L. Dimopoulos, M.A. White, D. Benboubker, L. Cook, G. Leiba, M. Morton, J. Joy Ho, P. Kim, K. Takezako, N. Moreau, P. Sutherland, H.J. Magen, H. Iida, S. Kim, J.S. Miles Prince, H. Cochrane, T. Oriol, A. Bahlis, N.J. Chari, A. O’Rourke, L. Trivedi, S. Casneuf, T. Krevvata, M. Ukropec, J. Kobos, R. Avet-Loiseau, H. Usmani, S.Z. San-Miguel, J.
- Abstract
High cytogenetic risk abnormalities confer poor outcomes in multiple myeloma patients. In POLLUX, daratumumab/lenalidomide/dexamethasone (D-Rd) demonstrated significant clinical benefit versus lenalidomide/dexamethasone (Rd) in relapsed/refractory multiple myeloma (RRMM) patients. We report an updated subgroup analysis of POLLUX based on cytogenetic risk. The cytogenetic risk was determined using fluorescence in situ hybridization/karyotyping; patients with high cytogenetic risk had t(4;14), t(14;16), or del17p abnormalities. Minimal residual disease (MRD; 10–5) was assessed via the clonoSEQ® assay V2.0. 569 patients were randomized (D-Rd, n = 286; Rd, n = 283); 35 (12%) patients per group had high cytogenetic risk. After a median follow-up of 44.3 months, D-Rd prolonged progression-free survival (PFS) versus Rd in standard cytogenetic risk (median: not estimable vs 18.6 months; hazard ratio [HR], 0.43; P < 0.0001) and high cytogenetic risk (median: 26.8 vs 8.3 months; HR, 0.34; P = 0.0035) patients. Responses with D-Rd were deep, including higher MRD negativity and sustained MRD-negativity rates versus Rd, regardless of cytogenetic risk. PFS on subsequent line of therapy was improved with D-Rd versus Rd in both cytogenetic risk subgroups. The safety profile of D-Rd by cytogenetic risk was consistent with the overall population. These findings demonstrate the improved efficacy of daratumumab plus standard of care versus standard of care in RRMM, regardless of cytogenetic risk. © 2020, The Author(s).
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- 2020
12. Daratumumab plus lenalidomide and dexamethasone in relapsed/refractory multiple myeloma: extended follow-up of POLLUX, a randomized, open-label, phase 3 study
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Bahlis, N.J. Dimopoulos, M.A. White, D.J. Benboubker, L. Cook, G. Leiba, M. Ho, P.J. Kim, K. Takezako, N. Moreau, P. Kaufman, J.L. Krevvata, M. Chiu, C. Qin, X. Okonkwo, L. Trivedi, S. Ukropec, J. Qi, M. San-Miguel, J.
- Abstract
In POLLUX, daratumumab (D) plus lenalidomide/dexamethasone (Rd) reduced the risk of disease progression or death by 63% and increased the overall response rate (ORR) versus Rd in relapsed/refractory multiple myeloma (RRMM). Updated efficacy and safety after >3 years of follow-up are presented. Patients (N = 569) with ≥1 prior line received Rd (lenalidomide, 25 mg, on Days 1–21 of each 28-day cycle; dexamethasone, 40 mg, weekly) ± daratumumab at the approved dosing schedule. Minimal residual disease (MRD) was assessed by next-generation sequencing. After 44.3 months median follow-up, D-Rd prolonged progression-free survival (PFS) in the intent-to-treat population (median 44.5 vs 17.5 months; HR, 0.44; 95% CI, 0.35–0.55; P < 0.0001) and in patient subgroups. D-Rd demonstrated higher ORR (92.9 vs 76.4%; P < 0.0001) and deeper responses, including complete response or better (56.6 vs 23.2%; P < 0.0001) and MRD negativity (10–5; 30.4 vs 5.3%; P < 0.0001). Median time to next therapy was prolonged with D-Rd (50.6 vs 23.1 months; HR, 0.39; 95% CI, 0.31–0.50; P < 0.0001). Median PFS on subsequent line of therapy (PFS2) was not reached with D-Rd versus 31.7 months with Rd (HR, 0.53; 95% CI, 0.42–0.68; P < 0.0001). No new safety concerns were reported. These data support using D-Rd in patients with RRMM after first relapse. © 2020, The Author(s).
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- 2020
13. Daratumumab plus lenalidomide and dexamethasone versus lenalidomide and dexamethasone in relapsed or refractory multiple myeloma: Updated analysis of POLLUX
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Dimopoulos, M.A. San-Miguel, J. Belch, A. White, D. Benboubker, L. Cook, G. Leiba, M. Morton, J. Joy Ho, P. Kim, K. Takezako, N. Moreau, P. Kaufman, J.L. Sutherland, H.J. Lalancette, M. Magen, H. Iida, S. Kim, J.S. Miles Prince, H. Cochrane, T. Oriol, A. Bahlis, N.J. Chari, A. O’Rourke, L. Wu, K. Schecter, J.M. Casneuf, T. Chiu, C. Soong, D. Kate Sasser, A. Khokhar, N.Z. Avet-Loiseau, H. Usmani, S.Z.
- Abstract
In the POLLUX study, daratumumab plus lenalidomide/dexamethasone significantly reduced risk of progression/death versus lenalidomide/ dexamethasone alone in relapsed/refractory multiple myeloma. We provide one additional year of follow up and include the effect on minimal residual disease and in clinically relevant subgroups. After 25.4 months of follow up, daratumumab plus lenalidomide/dexamethasone prolonged progression-free survival versus lenalidomide/dexamethasone alone (median not reached vs. 17.5 months; hazard ratio, 0.41; 95% confidence interval, 0.31-0.53; P12 and ≤12 months and >6 and ≤6 months. No new safety signals were observed. In relapsed/refractory multiple myeloma patients, daratumumab plus lenalidomide/dexamethasone continued to improve progression-free survival and deepen responses versus lenalidomide/dexamethasone. © 2018 Ferrata Storti Foundation.
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- 2018
14. Final analysis of survival outcomes in the phase 3 FIRST trial of up-front treatment for multiple myeloma
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Facon, T. Dimopoulos, M.A. Dispenzieri, A. Catalano, J.V. Belch, A. Cavo, M. Pinto, A. Weisel, K. Ludwig, H. Bahlis, N.J. Banos, A. Tiab, M. Delforge, M. Cavenagh, J.D. Geraldes, C. Lee, J.-J. Chen, C. Oriol, A. De La Rubia, J. White, D. Binder, D. Lu, J. Anderson, K.C. Moreau, P. Attal, M. Perrot, A. Arnulf, B. Qiu, L. Roussel, M. Boyle, E. Manier, S. Mohty, M. Avet-Loiseau, H. Leleu, X. Ervin-Haynes, A. Chen, G. Houck, V. Benboubker, L. Hulin, C.
- Abstract
This FIRST trial final analysis examined survival outcomes in patients with transplant-ineligible newly diagnosed multiple myeloma (NDMM) treated with lenalidomide and low-dose dexamethasone until disease progression (Rd continuous), Rd for 72 weeks (18 cycles; Rd18), or melphalan, prednisone, and thalidomide (MPT; 72 weeks). The primary endpoint was progression-free survival (PFS; primary comparison: Rd continuous vs MPT). Overall survival (OS) was a key secondary endpoint (final analysis prespecified ‡60 months’ follow-up). Patients were randomized to Rd continuous (n 5 535), Rd18 (n 5 541), or MPT (n 5 547). At a median follow-up of 67 months, PFS was significantly longer with Rd continuous vs MPT (hazard ratio [HR], 0.69; 95% confidence interval [CI], 0.59-0.79; P < .00001) and was similarly extended vs Rd18. Median OS was 10 months longer with Rd continuous vs MPT (59.1 vs 49.1 months; HR, 0.78; 95% CI, 0.67-0.92; P 5 .0023), and similar with Rd18 (62.3 months). In patients achieving complete or very good partial responses, Rd continuous had an 30-month longer median time to next treatment vs Rd18 (69.5 vs 39.9 months). Over half of all patients who received second-line treatment were given a bortezomib-based therapy. Second-line outcomes were improved in patients receiving bortezomib after Rd continuous and Rd18 vs after MPT. No new safety concerns, including risk for secondary malignancies, were observed. Treatment with Rd continuous significantly improved survival outcomes vs MPT, supporting Rd continuous as a standard of care for patients with transplant-ineligible NDMM. This trial was registered at www.clinicaltrials.gov as #NCT00689936 and EudraCT as 2007-004823-39. © 2018 by The American Society of Hematology.
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- 2018
15. Daratumumab, lenalidomide, and dexamethasone for multiple myeloma
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Dimopoulos, M.A. Oriol, A. Nahi, H. San-Miguel, J. Bahlis, N.J. Usmani, S.Z. Rabin, N. Orlowski, R.Z. Komarnicki, M. Suzuki, K. Plesner, T. Yoon, S.-S. Ben Yehuda, D. Richardson, P.G. Goldschmidt, H. Reece, D. Lisby, S. Khokhar, N.Z. O'Rourke, L. Chiu, C. Qin, X. Guckert, M. Ahmadi, T. Moreau, P. POLLUX Investigators
- Abstract
BACKGROUND: Daratumumab showed promising efficacy alone and with lenalidomide and dexamethasone in a phase 1-2 study involving patients with relapsed or refractory multiple myeloma. METHODS: In this phase 3 trial, we randomly assigned 569 patients with multiple myeloma who had received one or more previous lines of therapy to receive lenalidomide and dexamethasone either alone (control group) or in combination with daratumumab (daratumumab group). The primary end point was progression-free survival. RESULTS: At a median follow-up of 13.5 months in a protocol-specified interim analysis, 169 events of disease progression or death were observed (in 53 of 286 patients [18.5%] in the daratumumab group vs. 116 of 283 [41.0%] in the control group; hazard ratio, 0.37; 95% confidence interval [CI], 0.27 to 0.52; P
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- 2016
16. International myeloma working group recommendations for the diagnosis and management of myeloma-related renal impairment
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Dimopoulos, M.A. Sonneveld, P. Leung, N. Merlini, G. Ludwig, H. Kastritis, E. Goldschmidt, H. Joshua, D. Orlowski, R.Z. Powles, R. Vesole, D.H. Garderet, L. Einsele, H. Palumbo, A. Cavo, M. Richardson, P.G. Moreau, P. Miguel, J.S. Vincent Rajkumar, S. Durie, B.G.M. Terpos, E. Abildgaard, N. Abonour, R. Alsina, M. Anderson, K.C. Attal, M. Avet-Loiseau, H. Badros, A. Bahlis, N.J. Barlogie, B. Bataille, R. Beksaç, M. Belch, A. Ben-Yehuda, D. Bensinger, B. Leif Bergsagel, P. Bhutani, M. Bird, J. Bladé, J. Broijl, A. Boccadoro, M. Caers, J. Chanan-Khan, A. Chari, A. Chen, W.M. Chesi, M. Anthony Child, J. Chim, C.S. Chng, W.-J. Comenzo, R. Cook, G. Crowley, J. Crusoe, E. Dalton, W. Lee Moffitt, H. Davies, F. de la Rubia, J. de Souza, C. Delforge, M. Dhodapkar, M. Dispenzieri, A. Drach, J. Drake, M. Du, J. Dytfeld, D. Facon, T. Fantl, D. Fermand, J.-P. Fernández de Larrea, C. Fonseca, R. Gahrton, G. Garćia-Sanz, R. Gasparetto, C. Gertz, M. Ghobrial, I. Gibson, J. Gimsing, P. Giralt, S. Gu, J. Hajek, R. Hardan, I. Hari, P. Hata, H. Hattori, Y. Heffner, T. Hillengass, J. Ho, J. Hoering, A. Hoffman, J.E. Hou, J. Huang, J. Hungria, V. Ida, S. Jagannath, S. Jakubowiak, A.J. Johnsen, H.E. Jurczyszyn, A. Kaiser, M. Kaufman, J. Kawano, M. Korde, N. Kovacs, E. Krishnan, A. Kristinsson, S. Kröger, N. Kumar, S. Kyle, R.A. Kyriacou, C. Lacy, M. Lahuerta, J.J. Landgren, O. Larocca, A. Laubach, J. da Costa, F.L. Lee, J.-H. Leiba, M. Leleu, X. Lentzsch, S. Lokhorst, H. Lonial, S. Lu, J. Mahindra, A. Maiolino, A. Manasanch, E.E. Mark, T. Mateos, M.-V. Mazumder, A. McCarthy, P. Mehta, J. Mellqvist, U.-H. Mikhael, J. Morgan, G. Munshi, N. Nahi, H. Nawarawong, W. Niesvizky, R. Nouel, A. Novis, Y. Ocio, E. O'Dwyer, M. O'Gorman, P. Orfao, A. Otero, P.R. Paiva, B. Pavlovsky, S. Pilarski, L. Pratt, G. Qui, L. Raje, N. Reece, D. Reiman, A. Remaggi, G. Richter, J. Serra, E.R. Morales, A.R. Romeril, K.R. Roodman, D. Rosiñol, L. Rossi, A. Roussel, M. Russell, S. Schjesvold, F. Schots, R. Sevcikova, S. Sezer, O. Shah, J.J. Shimizu, K. Shustik, C. Siegel, D. Singhal, S. Spencer, A. Stadtmauer, E. Stewart, K. Tan, D. Terragna, C. Tosi, P. Tricot, G. Turesson, I. Usmani, S. Van Camp, B. Van de Donk, N. Van Ness, B. Van Riet, I. Broek, I.V. Vanderkerken, K. Vescio, R. Vij, R. Voorhees, P. Waage, A. Wang, M. Weber, D. Weiss, B.M. Westin, J. Wheatley, K. Zamagni, E. Zonder, J. Zweegman, S.
- Abstract
Purpose: The aim of the International Myeloma Working Group was to develop practical recommendations for the diagnosis and management of multiple myeloma–related renal impairment (RI). Methods: Recommendations were based on published data through December 2015, and were developed using the system developed by the Grading of Recommendation, Assessment, Development, and Evaluation Working Group. Recommendations: All patients with myeloma at diagnosis and at disease assessment should have serum creatinine, estimated glomerular filtration rate, and electrolytes measurements as well as free light chain, if available, and urine electrophoresis of a sample from a 24-hour urine collection (grade A). The Chronic Kidney Disease Epidemiology Collaboration, preferably, or the Modification of Diet in Renal Disease formula should be used for the evaluation of estimated glomerular filtration rate in patients with stabilized serum creatinine (grade A). International Myeloma Working Group criteria for renal reversibility should be used (grade B). For the management of RI in patients with multiple myeloma, high fluid intake is indicated along with antimyeloma therapy (grade B). The use of high-cutoff hemodialysis membranes in combination with antimyeloma therapy can be considered (grade B). Bortezomib-based regimens remain the cornerstone of the management of myeloma-related RI (grade A). High-dose dexamethasone should be administered at least for the first month of therapy (grade B). Thalidomide is effective in patients with myeloma with RI, and no dose modifications are needed (grade B). Lenalidomide is effective and safe, mainly in patients with mild to moderate RI (grade B); for patients with severe RI or on dialysis, lena-lidomide should be given with close monitoring for hematologic toxicity (grade B) with dose reduction as needed. High-dose therapy with autologous stem cell transplantation (with melphalan 100 mg/m2 to 140 mg/m2) is feasible in patients with RI (grade C). Carfilzomib can be safely administered to patients with creatinine clearance > 15 mL/min, whereas ixazomib in combination with lenalidomide and dex-amethasone can be safely administered to patients with creatinine clearance > 30 mL/min (grade A). © 2016 by American Society of Clinical Oncology.
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- 2016
17. Effect of prior treatments on selinexor, bortezomib, and dexamethasone in previously treated multiple myeloma
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Ashraf Badros, Nizar J. Bahlis, Roman Hájek, Larry D. Anderson, Vadim A Doronin, Meletios A. Dimopoulos, Jacqueline Jeha, Halyna Pylypenko, Jatin P. Shah, Reuben Benjamin, Sebastian Grosicki, Maria Gavriatopoulou, Dinesh Kumar Sinha, Xavier Leleu, Thierry Facon, Tuphan Kanti Dolai, Michele Cavo, Don A. Stevens, Moshe Yair Levy, Iryna Kriachok, Sundar Jagannath, L. Pour, Paul G. Richardson, Holger W. Auner, Maria V. Mateos, Sharon Shacham, Sosana Delimpasi, Hang Quach, Yi Chai, Mamta Garg, Michael Kauffman, Ivan Spicka, Maryana Simonova, Philippe Moreau, Christopher P. Venner, Ganna Usenko, Melina Arazy, Karyopharm, Mateos M.V., Gavriatopoulou M., Facon T., Auner H.W., Leleu X., Hajek R., Dimopoulos M.A., Delimpasi S., Simonova M., Spicka I., Pour L., Kriachok I., Pylypenko H., Doronin V., Usenko G., Benjamin R., Dolai T.K., Sinha D.K., Venner C.P., Garg M., Stevens D.A., Quach H., Jagannath S., Moreau P., Levy M., Badros A.Z., Anderson L.D., Bahlis N.J., Cavo M., Chai Y., Jeha J., Arazy M., Shah J., Shacham S., Kauffman M.G., Richardson P.G., and Grosicki S.
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0301 basic medicine ,Oncology ,Male ,Cancer Research ,medicine.medical_specialty ,SINE compound ,Selinexor ,Dexamethasone ,Bortezomib ,03 medical and health sciences ,0302 clinical medicine ,Multiple myeloma ,Internal medicine ,Antineoplastic Combined Chemotherapy Protocols ,medicine ,Hydrazine ,Humans ,Diseases of the blood and blood-forming organs ,1112 Oncology and Carcinogenesis ,Adverse effect ,Molecular Biology ,Letter to the Editor ,1102 Cardiorespiratory Medicine and Haematology ,RC254-282 ,Lenalidomide ,Antineoplastic Combined Chemotherapy Protocol ,Science & Technology ,business.industry ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,Exportin-1 ,Hematology ,Triazoles ,medicine.disease ,Regimen ,030104 developmental biology ,Prior Therapy ,Hydrazines ,030220 oncology & carcinogenesis ,Proteasome inhibitor ,Female ,RC633-647.5 ,business ,Life Sciences & Biomedicine ,medicine.drug ,Human - Abstract
Therapeutic regimens for previously treated multiple myeloma (MM) may not provide prolonged disease control and are often complicated by significant adverse events, including peripheral neuropathy. In patients with previously treated MM in the Phase 3 BOSTON study, once weekly selinexor, once weekly bortezomib, and 40 mg dexamethasone (XVd) demonstrated a significantly longer median progression-free survival (PFS), higher response rates, deeper responses, a trend to improved survival, and reduced incidence and severity of bortezomib-induced peripheral neuropathy when compared with standard twice weekly bortezomib and 80 mg dexamethasone (Vd). The pre-specified analyses described here evaluated the influence of the number of prior lines of therapy, prior treatment with lenalidomide, prior proteasome inhibitor (PI) therapy, prior immunomodulatory drug therapy, and prior autologous stem cell transplant (ASCT) on the efficacy and safety of XVd compared with Vd. In this 1:1 randomized study, enrolled patients were assigned to receive once weekly oral selinexor (100 mg) with once weekly subcutaneous bortezomib (1.3 mg/m2) and 40 mg per week dexamethasone (XVd) versus standard twice weekly bortezomib and 80 mg per week dexamethasone (Vd). XVd significantly improved PFS, overall response rate, time-to-next-treatment, and showed reduced all grade and grade ≥ 2 peripheral neuropathy compared with Vd regardless of prior treatments, but the benefits of XVd over Vd were more pronounced in patients treated earlier in their disease course who had either received only one prior therapy, had never been treated with a PI, or had prior ASCT. Treatment with XVd improved outcomes as compared to Vd regardless of prior therapies as well as manageable and generally reversible adverse events. XVd was associated with clinical benefit and reduced peripheral neuropathy compared to standard Vd in previously treated MM. These results suggest that the once weekly XVd regimen may be optimally administered to patients earlier in their course of disease, as their first bortezomib-containing regimen, and in those relapsing after ASCT.Trial registration: ClinicalTrials.gov (NCT03110562). Registered 12 April 2017. https://clinicaltrials.gov/ct2/show/NCT03110562.
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- 2021
18. Peripheral neuropathy symptoms, pain, and functioning in previously treated multiple myeloma patients treated with selinexor, bortezomib, and dexamethasone
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Michele Cavo, Sundar Jagannath, Reuben Benjamin, Ganna Usenko, Sebastian Grosicki, Maryana Simonova, Xavier Leleu, Larry D. Anderson, Moshe Yair Levy, Hang Quach, Sosana Delimpasi, Ivan Spicka, Mamta Garg, Thomas Illmer, L. Pour, Paul G. Richardson, Nizar J. Bahlis, Hailin Yu, Jatin P. Shah, Shijie Tang, Christopher P. Venner, Hoyee Leong, Meletios A. Dimopoulos, Larysa Sanchez, Jennifer L. Beaumont, Don A. Stevens, Sharon Shacham, Iryna Kriachok, Thierry Facon, Yi Chai, Michael Kauffman, Holger W. Auner, Roman Hájek, Dinesh Kumar Sinha, Xiwen Ma, Stacie Hudgens, Sanchez L., Leleu X., Beaumont J.L., Yu H., Hudgens S., Simonova M., Auner H.W., Quach H., Delimpasi S., Spicka I., Pour L., Kriachok I., Dimopoulos M.A., Usenko G., Hajek R., Benjamin R., Sinha D.K., Venner C., Illmer T., Garg M.K., Stevens D.A., Jagannath S., Levy M., Anderson L.D., Bahlis N.J., Facon T., Cavo M., Chai Y., Ma X., Tang S., Leong H., Shah J., Shacham S., Kauffman M., Richardson P., Grosicki S., and Karyopharm
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Oncology ,Male ,medicine.medical_specialty ,Immunology ,Pain ,Dexamethasone ,Bortezomib ,Internal medicine ,Antineoplastic Combined Chemotherapy Protocols ,medicine ,Hydrazine ,Humans ,1102 Cardiorespiratory Medicine and Haematology ,Multiple myeloma ,Aged ,Science & Technology ,Antineoplastic Combined Chemotherapy Protocol ,business.industry ,Peripheral Nervous System Diseases ,Hematology ,Triazoles ,medicine.disease ,Hydrazines ,Peripheral neuropathy ,Female ,Peripheral Nervous System Disease ,business ,Previously treated ,Multiple Myeloma ,Life Sciences & Biomedicine ,medicine.drug ,Human - Abstract
NA
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- 2021
19. Effect of age and frailty on the efficacy and tolerability of once-weekly selinexor, bortezomib, and dexamethasone in previously treated multiple myeloma
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P. Moreau, Maria Gavriatopoulou, Reuben Benjamin, Tuphan Kanti Dolai, Moshe Yair Levy, Vadim A Doronin, Paul G. Richardson, Hang Quach, Maryana Simonova, Ludek Pour, Don A. Stevens, Halyna Pylypenko, Thierry Facon, Xavier Leleu, Melina Arazy, Christopher P. Venner, Larry D. Anderson, Ashraf Z. Badros, Dinesh Kumar Sinha, Nizar J. Bahlis, Maria-Victoria Mateos, Jatin P. Shah, Sebastian Grosicki, Michele Cavo, Ganna Usenko, Yi Chai, Ivan Spicka, Sundar Jagannath, Roman Hájek, Meletios A. Dimopoulos, Michael Kauffman, Iryna Kriachok, Mamta Garg, Sharon Shacham, Holger W. Auner, Sosana Delimpasi, Auner H.W., Gavriatopoulou M., Delimpasi S., Simonova M., Spicka I., Pour L., Dimopoulos M.A., Kriachok I., Pylypenko H., Leleu X., Doronin V., Usenko G., Hajek R., Benjamin R., Dolai T.K., Sinha D.K., Venner C.P., Garg M., Stevens D.A., Quach H., Jagannath S., Moreau P., Levy M., Badros A., Anderson L.D., Bahlis N.J., Facon T., Mateos M.V., Cavo M., Chai Y., Arazy M., Shah J., Shacham S., Kauffman M.G., Richardson P.G., and Grosicki S.
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Oncology ,Male ,Gastrointestinal Diseases ,Kaplan-Meier Estimate ,Severity of Illness Index ,Dexamethasone ,Bortezomib ,0302 clinical medicine ,Retrospective Studie ,Antineoplastic Combined Chemotherapy Protocols ,Hydrazine ,Multicenter Studies as Topic ,Age Factor ,Multiple myeloma ,Randomized Controlled Trials as Topic ,Aged, 80 and over ,Frailty ,Age Factors ,Peripheral Nervous System Diseases ,Hematology ,Middle Aged ,Progression-Free Survival ,Hydrazines ,Tolerability ,030220 oncology & carcinogenesis ,Female ,Multiple Myeloma ,medicine.drug ,Human ,Adult ,medicine.medical_specialty ,Gastrointestinal Disease ,Subgroup analysis ,Drug Administration Schedule ,03 medical and health sciences ,Internal medicine ,Severity of illness ,medicine ,Humans ,Progression-free survival ,Lenalidomide ,Retrospective Studies ,Aged ,Antineoplastic Combined Chemotherapy Protocol ,business.industry ,Hematologic Disease ,Triazoles ,medicine.disease ,Hematologic Diseases ,Clinical Trials, Phase III as Topic ,Peripheral Nervous System Disease ,business ,030215 immunology - Abstract
Elderly and frail patients with multiple myeloma (MM) are more vulnerable to the toxicity of combination therapies, often resulting in treatment modifications and suboptimal outcomes. The phase 3 BOSTON study showed that once-weekly selinexor and bortezomib with low-dose dexamethasone (XVd) improved PFS and ORR compared with standard twice-weekly bortezomib and moderate-dose dexamethasone (Vd) in patients with previously treated MM. This is a retrospective subgroup analysis of the multicenter, prospective, randomized BOSTON trial. Post hoc analyses were performed to compare XVd versus Vd safety and efficacy according to age and frailty status (
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- 2021
20. Final Overall Survival Analysis of the TOURMALINE-MM1 Phase III Trial of Ixazomib, Lenalidomide, and Dexamethasone in Patients With Relapsed or Refractory Multiple Myeloma
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Richard Labotka, Nizar J. Bahlis, Philippe Moreau, Jacob P. Laubach, Peter Ganly, Cyrille Touzeau, Michele Cavo, Mohamed Darif, Anne-Marie Stoppa, Peter Gimsing, Tamás Masszi, Markus Hansson, Irwindeep Sandhu, Norbert Grzasko, Laurent Garderet, Shaji Kumar, Paul G. Richardson, Sharon Jackson, Deborah Berg, Luděk Pour, Bartrum W Baker, Francis K. Buadi, Richardson P.G., Kumar S.K., Masszi T., Grzasko N., Bahlis N.J., Hansson M., Pour L., Sandhu I., Ganly P., Baker B.W., Jackson S.R., Stoppa A.-M., Gimsing P., Garderet L., Touzeau C., Buadi F.K., Laubach J.P., Cavo M., Darif M., Labotka R., Berg D., and Moreau P.
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Oncology ,Male ,Cancer Research ,medicine.medical_specialty ,Glycine ,Dexamethasone ,Ixazomib ,Follow-Up Studie ,chemistry.chemical_compound ,Text mining ,Double-Blind Method ,Internal medicine ,Overall survival ,Medicine ,In patient ,Lenalidomide ,Aged ,Neoplasm Staging ,Antineoplastic Combined Chemotherapy Protocol ,Boron Compound ,business.industry ,Refractory Multiple Myeloma ,Middle Aged ,Survival Analysis ,chemistry ,Quality of Life ,Female ,business ,Multiple Myeloma ,medicine.drug ,Human - Abstract
PURPOSE The double-blind, placebo-controlled, phase III TOURMALINE-MM1 study demonstrated a statistically significant improvement in progression-free survival with ixazomib-lenalidomide-dexamethasone (ixazomib-Rd) versus placebo-Rd in patients with relapsed or refractory multiple myeloma. We report the final analyses for overall survival (OS). PATIENTS AND METHODS Patients were randomly assigned to ixazomib-Rd (n = 360) or placebo-Rd (n = 362), stratified by number of prior therapies (1 v 2 or 3), previous proteasome inhibitor (PI) exposure (yes v no), and International Staging System disease stage (I or II v III). OS (intent-to-treat population) was a key secondary end point. RESULTS With a median follow-up of 85 months, median OS with ixazomib-Rd versus placebo-Rd was 53.6 versus 51.6 months (hazard ratio, 0.939; P = .495). Lower hazard ratios, indicating larger magnitude of OS benefit with ixazomib-Rd versus placebo-Rd, were seen in predefined subgroups: refractory to any (0.794) or last (0.742) treatment line; age > 65-75 years (0.757); International Staging System stage III (0.779); 2/3 prior therapies (0.845); high-risk cytogenetics (0.870); and high-risk cytogenetics and/or 1q21 amplification (0.862). Following ixazomib-Rd versus placebo-Rd, 71.7% versus 69.9% of patients received ≥ 1 anticancer therapy, of whom 24.7% versus 33.9% received daratumumab and 71.8% versus 76.9% received PIs (next-line therapy: 47.5% v 55.8%). Rates of new primary malignancies were similar with ixazomib-Rd (10.3%) and placebo-Rd (11.9%). There were no new or additional safety concerns. CONCLUSION Median OS values in both arms were the longest reported in phase III studies of Rd-based triplets in relapsed or refractory multiple myeloma at the time of this analysis; progression-free survival benefit with ixazomib-Rd versus placebo-Rd did not translate into a statistically significant OS benefit on intent-to-treat analysis. OS benefit was greater in subgroups with adverse prognostic factors. OS interpretation was confounded by imbalances in subsequent therapies received, especially PIs and daratumumab.
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- 2021
21. Selinexor, bortezomib, and dexamethasone versus bortezomib and dexamethasone in previously treated multiple myeloma: Outcomes by cytogenetic risk
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Hua Chang, Nizar J. Bahlis, Jatin P. Shah, Yi Chai, Shambavi Richard, Sosana Delimpasi, Ganna Usenko, Halyna Pylypenko, Meletios A. Dimopoulos, Holger W. Auner, Don A. Stevens, Ajai Chari, Reuben Benjamin, Melina Arazy, Moshe Yair Levy, Tuphan Kanti Dolai, Ivan Spicka, Hang Quach, Larry D. Anderson, Paul G. Richardson, Xavier Leleu, Maria-Victoria Mateos, Ashraf Z. Badros, Sharon Shacham, Iryna Kriachok, Thierry Facon, Roman Hájek, Sebastian Grosicki, Maryana Simonova, Ludek Pour, Yosef Landesman, Christopher P. Venner, Mamta Garg, Michael Kauffman, Dinesh Kumar Sinha, P. Moreau, Michele Cavo, Sundar Jagannath, Richard S., Chari A., Delimpasi S., Simonova M., Spicka I., Pour L., Kriachok I., Dimopoulos M.A., Pylypenko H., Auner H.W., Leleu X., Usenko G., Hajek R., Benjamin R., Dolai T.K., Sinha D.K., Venner C.P., Garg M., Stevens D.A., Quach H., Jagannath S., Moreau P., Levy M., Badros A., Anderson L.D., Bahlis N.J., Facon T., Mateos M.V., Cavo M., Chang H., Landesman Y., Chai Y., Arazy M., Shah J., Shacham S., Kauffman M.G., Grosicki S., and Richardson P.G.
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Adult ,Male ,medicine.medical_specialty ,Population ,Antineoplastic Agents ,Gastroenterology ,Dexamethasone ,Antineoplastic Agent ,Bortezomib ,Young Adult ,Internal medicine ,Antineoplastic Combined Chemotherapy Protocols ,medicine ,Hydrazine ,Humans ,Progression-free survival ,Young adult ,education ,Multiple myeloma ,Research Articles ,Aged ,education.field_of_study ,Hematology ,Antineoplastic Combined Chemotherapy Protocol ,business.industry ,Cytogenetic Analysi ,Triazoles ,Middle Aged ,medicine.disease ,Progression-Free Survival ,Peripheral neuropathy ,Hydrazines ,Treatment Outcome ,Cytogenetic Analysis ,Female ,Triazole ,business ,Multiple Myeloma ,medicine.drug ,Research Article ,Human - Abstract
In the phase 3 BOSTON study, patients with multiple myeloma (MM) after 1–3 prior regimens were randomized to once-weekly selinexor (an oral inhibitor of exportin 1 [XPO1]) plus bortezomib-dexamethasone (XVd) or twice-weekly bortezomib-dexamethasone (Vd). Compared with Vd, XVd was associated with significant improvements in median progression-free survival (PFS), overall response rate (ORR), and lower rates of peripheral neuropathy, with trends in overall survival (OS) favoring XVd. In BOSTON, 141 (35.1%) patients had MM with high-risk (presence of del[17p], t[4;14], t[14;16], or ≥4 copies of amp1q21) cytogenetics (XVd, n=70; Vd, n=71), and 261 (64.9%) exhibited standard-risk cytogenetics (XVd, n=125; Vd, n=136). Among patients with high-risk MM, median PFS was 12.91 months for XVd and 8.61 months for Vd (HR, 0.73 [95% CI, (0.4673, 1.1406)], p=0.082), and ORRs were 78.6% and 57.7%, respectively (OR 2.68; p= 0.004). In the standard-risk subgroup, median PFS was 16.62 months for XVd and 9.46 months for Vd (HR 0.61; p=0.004), and ORRs were 75.2% and 64.7%, respectively (OR 1.65; p=0.033). The safety profiles of XVd and Vd in both subgroups were consistent with the overall population. These data suggest that selinexor can confer benefits to patients with MM regardless of cytogenetic risk. ClinicalTrials.gov identifier: NCT03110562.
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- 2021
22. Once-per-week selinexor, bortezomib, and dexamethasone versus twice-per-week bortezomib and dexamethasone in patients with multiple myeloma (BOSTON): a randomised, open-label, phase 3 trial
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Vesselina Goranova-Marinova, Eirini Katodritou, Mamta Garg, Michael G. Kauffman, Paul G. Richardson, Lingling Li, Monica Galli, Sosana Delimpasi, Sebastian Grosicki, Jelena Bila, Galina Salogub, Dinesh Kumar Sinha, Holger W. Auner, Larry D. Anderson, Sybiryna Korenkova, Don A. Stevens, Melina Arazy, Reuben Benjamin, Supratik Basu, Jacqueline Jeha, Moshe Yair Levy, Artur Jurczyszyn, Nizar J. Bahlis, Jean Richard Saint-Martin, Jatin P. Shah, Hang Quach, Anna M. Liberati, Tuphan Kanti Dolai, Iryrna Kriachok, Roman Hájek, Anita A. Joshi, Darrell White, Michele Cavo, Sundar Jagannath, Meletios A. Dimopoulos, Xavier Leleu, Hanna Oliynyk, Pawel Robak, Maryana Simonova, Ganna Usenko, Ludek Pour, Maria V. Mateos, Ivan Spicka, Moshe E. Gatt, Atanas Radinoff, Craig T. Wallington-Beddoe, Jeevan Kumar, Vishnuvardhan Peddagali, Halyna Pylypenko, Thierry Facon, Christopher P. Venner, Donna E. Reece, Sharon Shacham, Maria Gavriatopoulou, Yi Chai, Mercedes Gironella, Vadim A Doronin, P. Moreau, Karyopharm, Grosicki S., Simonova M., Spicka I., Pour L., Kriachok I., Gavriatopoulou M., Pylypenko H., Auner H.W., Leleu X., Doronin V., Usenko G., Bahlis N.J., Hajek R., Benjamin R., Dolai T.K., Sinha D.K., Venner C.P., Garg M., Gironella M., Jurczyszyn A., Robak P., Galli M., Wallington-Beddoe C., Radinoff A., Salogub G., Stevens D.A., Basu S., Liberati A.M., Quach H., Goranova-Marinova V.S., Bila J., Katodritou E., Oliynyk H., Korenkova S., Kumar J., Jagannath S., Moreau P., Levy M., White D., Gatt M.E., Facon T., Mateos M.V., Cavo M., Reece D., Anderson L.D., Saint-Martin J.-R., Jeha J., Joshi A.A., Chai Y., Li L., Peddagali V., Arazy M., Shah J., Shacham S., Kauffman M.G., Dimopoulos M.A., Richardson P.G., and Delimpasi S.
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Male ,medicine.medical_treatment ,Kaplan-Meier Estimate ,030204 cardiovascular system & hematology ,Gastroenterology ,Dexamethasone ,multiple myeloma, Selinexor, dexamethasone ,Bortezomib ,0302 clinical medicine ,hemic and lymphatic diseases ,Antineoplastic Combined Chemotherapy Protocols ,030212 general & internal medicine ,Multiple myeloma ,11 Medical and Health Sciences ,education.field_of_study ,General Medicine ,Middle Aged ,Progression-Free Survival ,Hydrazines ,XPO1 ,Female ,Multiple Myeloma ,Life Sciences & Biomedicine ,medicine.drug ,Adult ,medicine.medical_specialty ,Adolescent ,Population ,Antineoplastic Agents ,Drug Administration Schedule ,03 medical and health sciences ,Medicine, General & Internal ,Internal medicine ,General & Internal Medicine ,medicine ,Humans ,Progression-free survival ,education ,Aged ,Chemotherapy ,Science & Technology ,business.industry ,Triazoles ,medicine.disease ,EFFICACY ,Regimen ,Proteasome inhibitor ,business ,PERIPHERAL NEUROPATHY - Abstract
Summary Background Selinexor combined with dexamethasone has shown activity in patients with heavily pre-treated multiple myeloma. In a phase 1b/2 study, the combination of oral selinexor with bortezomib (a proteasome inhibitor) and dexamethasone induced high response rates with low rates of peripheral neuropathy, the main dose-limiting toxicity of bortezomib. We aimed to evaluate the clinical benefit of weekly selinexor, bortezomib, and dexamethasone versus standard bortezomib and dexamethasone in patients with previously treated multiple myeloma. Methods This phase 3, randomised, open-label trial was done at 123 sites in 21 countries. Patients aged 18 years or older, who had multiple myeloma, and who had previously been treated with one to three lines of therapy, including proteasome inhibitors, were randomly allocated (1:1) to receive selinexor (100 mg once per week), bortezomib (1·3 mg/m2 once per week), and dexamethasone (20 mg twice per week), or bortezomib (1·3 mg/m2 twice per week for the first 24 weeks and once per week thereafter) and dexamethasone (20 mg four times per week for the first 24 weeks and twice per week thereafter). Randomisation was done using interactive response technology and stratified by previous proteasome inhibitor therapy, lines of treatment, and multiple myeloma stage. The primary endpoint was progression-free survival in the intention-to-treat population. Patients who received at least one dose of study treatment were included in the safety population. This trial is registered at ClinicalTrials.gov , NCT03110562 . The trial is ongoing, with 55 patients remaining on randomised therapy as of Feb 20, 2020. Findings Of 457 patients screened for eligibility, 402 were randomly allocated—195 (49%) to the selinexor, bortezomib, and dexamethasone group and 207 (51%) to the bortezomib and dexamethasone group—and the first dose of study medication was given between June 6, 2017, and Feb 5, 2019. Median follow-up durations were 13·2 months [IQR 6·2–19·8] for the selinexor, bortezomib, and dexamethasone group and 16·5 months [9·4–19·8] for the bortezomib and dexamethasone group. Median progression-free survival was 13·93 months (95% CI 11·73–not evaluable) with selinexor, bortezomib, and dexamethasone and 9·46 months (8·11–10·78) with bortezomib and dexamethasone (hazard ratio 0·70 [95% CI 0·53–0·93], p=0·0075). The most frequent grade 3–4 adverse events were thrombocytopenia (77 [39%] of 195 patients in the selinexor, bortezomib, and dexamethasone group vs 35 [17%] of 204 in the bortezomib and dexamethasone group), fatigue (26 [13%] vs two [1%]), anaemia (31 [16%] vs 20 [10%]), and pneumonia (22 [11%] vs 22 [11%]). Peripheral neuropathy of grade 2 or above was less frequent with selinexor, bortezomib, and dexamethasone (41 [21%] patients) than with bortezomib and dexamethasone (70 [34%] patients; odds ratio 0·50 [95% CI 0·32–0·79], p=0·0013). 47 (24%) patients in the selinexor, bortezomib, and dexamethasone group and 62 (30%) in the bortezomib and dexamethasone group died. Interpretation A once-per-week regimen of selinexor, bortezomib, and dexamethasone is a novel, effective, and convenient treatment option for patients with multiple myeloma who have received one to three previous lines of therapy. Funding Karyopharm Therapeutics.
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- 2020
23. c-MYC expression and maturity phenotypes are associated with outcome benefit from addition of ixazomib to lenalidomide-dexamethasone in myeloma
- Author
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Katarina Luptakova, Dixie Lee Esseltine, Jacob Zhang, Sunita Badola, Michele Cavo, Tamás Masszi, Jianchang Lin, Nizar J. Bahlis, Jonathan J Keats, Christian Langer, Shaji Kumar, Luisa Viterbo, Hervé Avet-Loiseau, Peter Ganly, Paul G. Richardson, Deborah Berg, Helgi van de Velde, Philippe Moreau, Nikhil C. Munshi, Ludek Pour, Alessandra Di Bacco, S. Vincent Rajkumar, Bin Li, Lei Shen, Di Bacco A., Bahlis N.J., Munshi N.C., Avet-Loiseau H., Masszi T., Viterbo L., Pour L., Ganly P., Cavo M., Langer C., Kumar S.K., Rajkumar S.V., Keats J.J., Berg D., Lin J., Li B., Badola S., Shen L., Zhang J., Esseltine D.-L., Luptakova K., van de Velde H., Richardson P.G., and Moreau P.
- Subjects
Oncology ,Male ,Gene Expression ,Dexamethasone ,Ixazomib ,chemistry.chemical_compound ,0302 clinical medicine ,Antineoplastic Combined Chemotherapy Protocols ,Lenalidomide ,Multiple myeloma ,Aged, 80 and over ,Hazard ratio ,RNA sequencing ,Hematology ,General Medicine ,Middle Aged ,Prognosis ,multiple myeloma ,Prior Therapy ,Treatment Outcome ,030220 oncology & carcinogenesis ,Female ,Original Article ,c‐myc Proto‐Oncogenes ,medicine.drug ,Boron Compounds ,medicine.medical_specialty ,Glycine ,Proto-Oncogene Proteins c-myc ,03 medical and health sciences ,Internal medicine ,medicine ,Biomarkers, Tumor ,Humans ,c-myc Proto-Oncogene ,Progression-free survival ,Aged ,Neoplasm Staging ,business.industry ,Gene Expression Profiling ,progression‐free survival ,Original Articles ,medicine.disease ,Transplantation ,chemistry ,Neoplasm Grading ,mutation ,business ,progression-free survival ,030215 immunology - Abstract
Objectives: In the TOURMALINE-MM1 phase 3 trial in relapsed/refractory multiple myeloma, ixazomib-lenalidomide-dexamethasone (IRd) showed different magnitudes of progression-free survival (PFS) benefit vs placebo-Rd according to number and type of prior therapies, with greater benefit seen in patients with >1 prior line of therapy or 1 prior line of therapy without stem cell transplantation (SCT). Methods: RNA sequencing data were used to investigate the basis of these differences. Results: The PFS benefit of IRd vs placebo-Rd was greater in patients with tumors expressing high c-MYC levels (median not reached vs 11.3months; hazard ratio [HR] 0.42; 95% CI, 0.26, 0.66; P 
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- 2020
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