Management of Multiple Myeloma: The Changing Paradigm

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Management of Multiple Myeloma: The Changing Paradigm High-Dose Chemotherapy and Stem Cell Transplantation in the Era of Novel Therapies Larry Anderson, MD, PhD Multiple Myeloma and Stem Cell Transplant Program

Introduction: Example Patient Case RW is a 65 year old African American man with back pain, fatigue Workup showed lytic lesions in the spine, compression fracture in L1, anemia with Hgb 9.5, M-spike 3.1 g/dl, Kappa Light Chains 205 mg/l, Ca 11, 60% PCs on Bx He underwent Vertebroplasty to L1 and started monthly Zometa He was treated with 4 cycles of Velcade/Revlimid/Dex induction therapy He achieved a Near CR (M-spike now only Faint/Unquantifiable in serum and 24 hr urine, BMBx now clean He then underwent an autologous stem cell transplant (ASCT) as consolidation He had a fever and some mouth sores but engrafted day 11 and discharged day 12 without complications Day 90 restaging showed Stringent Complete Remission, then started on maintenance low dose Revlimid

High-Dose Chemotherapy and Stem Cell Transplantation Offers best chance for durable remission based on current data Outcomes improving with the use of newer drugs prior to transplantation New trials comparing novel drugs vs transplant (results so far still favor SCT in 1 st Remission) Can be done as part of frontline therapy or at relapse (or both) More patients considered candidates than in the past Based on overall health and age Criteria varies by cancer center Talk to your Dr to see if you qualify We transplant up to age ~ 75 at UTSW, Europe to 65

Types of Stem Cell Transplantation Transplant Type Autologous (ASCT)* Your own cells Allogeneic A donor s cells (requires a match) Stem Cell Source Peripheral Blood Bone Marrow Harvest (Not done for Myeloma) Transplant Process Single Auto (Most Common for Myeloma) Tandem Auto (only proven benefit if not in >90% Remission after 1 st Auto) Tandem Auto/ Mini Allo *Most common

Overview: ASCT 1. Induction therapy 2. Collection of stem cells from the bloodstream 3. Freezing of stem cells 4. High-dose chemotherapy (Consolidation) 5. Day of Rest 6. Thawing and infusion of stem cells ~3 6 cycles Stem cell mobilization Neupogen Neulasta Leukine Cytoxan Mozobil Melphalan

Novel Agents + ASCT ASCT

Should I Get a Transplant After Induction Therapy or Can I Wait Until After I Relapse? Ongoing Clinical Trial Initial therapy RVD: 3 cycles Group A: Early ASCT Stem cell collection/storge with Cytoxan Group B: ASCT at relapse High-dose chemotherapy + ASCT Continue RVD: 5 cycles Consolidation: RVD: 2 cycles Maintenance: Revlimid 12 months (Until PD in US) Maintenance: Revlimid 12 months (Until PD in US) ASCT at relapse RVD, Revlimid, Velcade, dexamethasone; Cytoxan, cyclophosphamide; Consolidation: Additional therapy post-asct

Should I Get a Transplant After Induction Therapy or Should I Wait Until After I Relapse? Initial Results of French Study Early ASCT conveys benefit in Progression Free Survival (PFS) but so far not in Overall Survival Early ASCT higher rate of Deep Remissions 1 year of maintenance therapy (per IFM study) conveys MRD negativity benefit but could longer maintenance overcome need for early ASCT? Continuous therapy with lenalidomide maintenance until progression to be addressed by US study. Attal M et al. Blood. 2015;126: Abstract 391. Avet-Loiseau H et al. Blood. 2015;126: Abstract 191.

Following Transplantation: Possible Consideration of Maintenance Therapy NINLARO Oral proteasome inhibitor What are the benefits vs risks? Who should get maintenance therapy? How long should patients get maintenance therapy? VELCADE-BASED TREATMENT Supported by several smaller studies Talk to your doctor about whether maintenance therapy is right for you. REVLIMID Reduction in myeloma progression (3 large studies) Improved survival (1 of 3 studies) Small risk of second cancers when used after melphalan

Mini (Nonmyeloablative) Allogeneic Transplantation Reduced-intensity allograft approach (Mini or RIC) Not a proven standard; experimental procedure Potential benefits: Lower toxicity than myeloablative Allo (10-15% instead of 40% treatment related death within 100 days) More candidates (elderly, comorbid conditions) Outpatient treatment possible Fast recovery, few complications, less infection Small subset with long term remission However, most still relapse and many get Graft vs Host Disease so new methods needed and should be done only on a clinical trial

Immune Cell Therapy and Vaccines in Development Type Trial Patient Types CAR T MILs DLI Vaccine CAR-T for multiple myeloma (BCMA or CD19) Tadalafil and lenalidomide maintenance with or without activated marrow infiltrating lymphocytes (MILs) in high-risk myeloma Adoptive immunotherapy with activated MILs and cyclophosphamide graft-versus-host disease prophylaxis in patients with relapse of hematologic malignancies after allogeneic hematopoietic cell transplantation CD3/CD28 activated Id-KLH primed autologous lymphocytes Dendritic cell fusion vaccine + CT-011 (monoclonal antibody) Salvage ASCT after early relapse following first ASCT Newly diagnosed; relapsed (without prior ASCT) Relapsed/ refractory after allosct Study Phase 1 2 1 Site(s) University of Pennsylvania NIH Dana Farber Sidney Kimmel Comprehensive Cancer Center Sidney Kimmel Comprehensive Cancer Center Post-transplant 2 University of Pennsylvania Post-transplant 2 Beth Israel Deaconess Medical Center/ Dana-Farber Hiltonol (MAGE-A3 vaccine Poly-ICLC) Post-transplant 2 University of Pennsylvania PVX-410 Post-transplant 2 Emory University Dendritic Cell /Myeloma Fusions Post-transplant 2 BMT CTN

CAR-BCMA T Cell Therapy in MM: Study Design First-in-human phase I trial BCMA = B Cell Maturation Antigen = Plasma Cell Specific Pts with advanced R/R MM; 3 prior lines of therapy; normal organ function; clear BCMA expression (N = 12) Cyclophosphamide 300 mg/m 2 Fludarabine 30 mg/m 2 QD for 3 days CAR-BCMA T cells* Single infusion *Dose escalation of CAR+ T cells/kg 0.3 x 10 6 1.0 x 10 6 3.0 x 10 6 9.0 x 10 6 CAR-BCMA expression determined by flow cytometry Ali SA, et al. ASH 2015. Abstract LBA-1.

CAR-BCMA T Cells in MM: Response Pt Myeloma Type Ali SA, et al. ASH 2015. Abstract LBA-1. CAR-BCMA Dose (T cells/kg) Response Response Duration, Wks 1 κ light chain only 0.3 x 10 6 PR 2 2 IgA λ 0.3 x 10 6 SD 6 3 κ light chain only 0.3 x 10 6 SD 6 4 κ light chain only 1.0 x 10 6 SD 12 5 IgG κ 1.0 x 10 6 SD 4 6 IgG λ 1.0 x 10 6 SD 2 7 IgG λ 3.0 x 10 6 SD 7 8 κ light chain only 3.0 x 10 6 VGPR 8 9 κ light chain only 3.0 x 10 6 SD 16 10 IgA λ 9.0 x 10 6 scr 12+ 11 IgG λ 9.0 x 10 6 PR 6+ 12 IgA λ 3.0 x 10 6 SD 2

CAR-BCMA T Cells in MM: Pt 10 Pt 10: chemotherapy-resistant IgA MM with 3 prior lines of therapy Relapse 3 mos after ASCT with 90% bone marrow plasma cells BCMA expression on pt s myeloma cells was uniform but dim After CAR-BCMA T-cell infusion, the pt experienced cytokine release syndrome (including fever, hypotension, tachycardia, high creatinine kinase, liver enzymes) which resolved within 2 wks ANC < 500/µL at time of infusion and for 40 days after Pt was platelet transfusion dependent for 9 wks after infusion Pt achieved ongoing scr after CAR-BCMA T-cell infusion Serum, urine immunofixation negative at 14 wks post infusion Bone marrow negative by flow cytometry 14 wks post induction MM eliminated from bone marrow cells after infusion with CAR-BCMA Eliminates Plasma Cells so will likely need lifelong IVIG Ali SA, et al. ASH 2015. Abstract LBA-1.

Questions To Ask Your Doctor Am I a candidate for high-dose chemotherapy and stem cell transplantation? What are the pros and cons of stem cell transplantation in my case? When is the best time for me to undergo transplantation? Does your center do stem cell transplants? How many transplants has your center performed in multiple myeloma in the last year? Is procedure performed as an inpatient or outpatient? How long will I be in the hospital? What is the recovery period? What kind of changes in my lifestyle will I need to make? When do I go back to you for follow-up?

Conclusion: Example Patient Case Our patient RW started Maintenance Revlimid after day 90 He has continued to remain in stringent Complete Remission for 4 years after Transplant Working Full Time and tolerating low dose Revlimid 10 mg well (I give 3 weeks on and 1 week off) Plan on continuing until relapse or as long as tolerating Monthly labs and checkup to watch for low blood counts or relapse Doses can be increased from 10 to 15 mg in those not in CR and decreased to 5 to 10 mg in those with low Neutrophils or diarrhea Modifying dose and staying on therapy is Key

Summary: High-Dose Chemotherapy and Stem Cell Transplantation Offers best chance for long-term remission for eligible patients based on current data Research questions: Given the availability of the novel agents, can we delay high-dose chemotherapy and stem cell transplantation until relapse? Which patients achieve the greatest benefit? What is the role of maintenance therapy? How long should patients remain on maintenance therapy? Does MRD Testing affect need for maintenance?