Smoldering Myeloma: Leave them alone! -...

4/23/2012

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Smoldering Myeloma: Leave them alone!

D id H V l MD PhDDavid H. Vesole, MD, PhD

Co-Director, Myeloma Division

Director, Myeloma Research

John Theurer Cancer Center

Hackensack University Medical Center

Smoldering MM

• Prevalence• 1960‐2002

• 16% of MM (1000/6179)

• Progression rate• MGUS 1% per year

• SMM 10‐25% per year

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Progression to Symptomatic MM• MGUS: up to 2 percent of persons 50 years of age or older and about 3

percent of those older than 70 years

• For SMM, maximum risk in the first 5 years

• Risk factors: Higher M spike, higher plasma cell burden, type of M protein,Risk factors: Higher M spike, higher plasma cell burden, type of M protein, Abnormal free light chain ratio, circulating plasma cells

Kyle et al, NEJM, Volume 356:2582‐2590, June 21, 2007

Risk stratification based on bone marrow plasmacytosis, serum M protein, and serum immunoglobulin free‐light chain (FLC) ratio. Patients are assigned 1 point for meeting each of the following criteria: bone marrow clonal plasma cells 10%; serum M protein 3 g/dL; and serum immunoglobulin FLC ratio either less than 0.125 or > 8. The median times to progression for 1, 2, or 3 risk factors are 10, 5.1, and 1.9 years, respectively.

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Risk stratification schemes for SMM• Mayo Clinic for SMM patientsRisk factors: plasma cells >10%, M‐protein > 3 g/dL, FLC ratio < 0.125 or > 8N f i k f t N f ti t (%) 20 i % RRNo. of risk factors No. of patients (%) 20‐year progression, % RR

1 76 (28) 25 12 115 (42) 51 2.03 82 (30) 76 3.0Total 273 (100) 51 N/A

• Spanish study group for SMM patients• Spanish study group for SMM patientsRisk factors: 95% aPC, immunoparesis

0 28 (31) 4 11 22 (25) 46 11.52 39 (44) 72 18Total 89‡ (100) 46 N/A

Smoldering MM

Gr 1:TTP 1.9 y

Gr 2: TTP: 5 y

p < 0.001100

80 • PCsBM Infiltration ≥ 10%

No. of risk factors No. Rel risk

Gr 2: TTP: 5 y

Gr 3: TTP 10 y60

40

20

Pro

bab

ility

of

Pro

gre

ssio

n (

%)

• Serum M protein ≥ 3 g/dL

• Serum FLC ratio < 1/8 or > 8

Kyle RA, et al. N Engl J Med. 2007; 356:2582-90

Dispenzieri A, et al. Blood. 2008;111:785-9.

1 81 1

2 114 1.9 (1.2–2.9)

3 78 4.0 (2.6–6.1)00 5 10 15

Years

Mateos et al., Abstract #991

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Treatment of SMM

• Bisphosphonates

–Pamidronate (n =12) no direct anti‐tumor effect (Martin et al Br J Haematol 118:239–243, 2002)

–Pamidronate‐randomized triial: decrease SRE bu no prolongation of TTP or OS (Musto et

al Leukemia and Lymphoma 44:1545–1548, 2003)

Zoledronic acid randomized trial: decrease– Zoledronic acid‐randomized trial: decrease in SRE but no impact on TTP or OS (Musto et al

Cancer 113:1588–1595, 2008)

Treatment of SMM

• Alkylating Agents and Corticosteroids

– MP vs Obs (n = 50)‐no difference in response rate at time of PD, no difference in DOR or OS (Hjorth et a lEur J Haematol50:95–102, 1993)

– MP vs Obs (n = 44)‐median survival similar 54 vs 58 mo (Grignani et alBr J Cancer 73:1101–1107, 1996)( g , )

– MP vs Obs (n = 145)‐no difference in survival (Riccardi et al Br J Cancer 82:1254–1260, 2000)

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Treatment of SMM• Thalidomide

–Mayo Clinic (N =29): RR 34% (Rajkumar et al Leukemia

17:775–779, 2003))

Comparison (29 pts on thal study) with historical control (57 pts)• 2 year PFS: 47% (untreated) vs 63% (Thal)

–MD Anderson (n = 28): RR 36% (Weber et al J Clin Oncol21:16–19, 2003), )

– Arkansas (n = 74); RR42%, median time to progression 7 years; PN dose reduction 86%, DC’d 50% (200 mg/d) (Barlogie et al Blood 112:3122–3125, 2008)

63%(47% in historical controls)

Rajkumar SV. Leukemia 2003; 17:775-9

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Fig 3. (A) Event‐free survival was similar in patients with multiple myeloma (MM) evolved from monoclonal gammopathy of undetermined significance (MGUS)/SMM and other subgroups. (B) Overall survival was similar in patients with MM evolved from MGUS/SMM and other subgroups. Barlogie et al BJH 2007; 136: 393

Multivariate analysis of factors predicting for complete response, event‐free survival and overall survival – all patients

All patients Factor % HR (95% CI) P-value

Complete response (n = 637) Prior MGUS/SMM 7 0·45 (0·25,0·81) 0·007

Thalidomide arm 49 1·54 (1·24,1·91) <0·001

LDH > upper normal limit 27 1 28 (1 00 1 62) 0 045LDH > upper normal limit 27 1·28 (1·00,1·62) 0·045

Event-free survival (n = 654) Prior MGUS/SMM 7 1·12 (0·71,1·76) 0·637

Thalidomide arm 49 0·75 (0·59,0·95) 0·016

LDH > upper normal limit 27 1·51 (1·17,1·96) 0·002

Cytogenetic abnormalities

30 1·55 (1·22,1·98) <0·001

Albumin < 35 g/l 18 1·52 (1·14,2·02) 0·004

B2M ≥ 35 mg/l 36 1·47 (1·14,1·88) 0·003

IgA isotype 24 1·45 (1·12,1·89) 0·006

CR (time dependent) 52 0·64 (0·49,0·83) 0·001

Overall survival (n = 654) Prior MGUS/SMM 7 1·04 (0·59,1·81) 0·900

LDH > upper normal limit 27 1·66 (1·22,2·25) 0·001

Cytogenetic abnormalities

30 1·88 (1·41,2·52) <0·001

Albumin < 35 g/l 18 1·85 (1·33,2·56) <0·001

CR (time dependent) 52 0·52 (0·37,0·72) <0·001

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QuiRedex: Study Design

• Multicenter, open‐label, randomized phase III trial– Evaluated new treatment regimen for smoldering MM vs currentEvaluated new treatment regimen for smoldering MM vs current

standard of care

Patients with high‐risk

smoldering MM

Lenalidomide 25 mg/day on Days 1‐21 +

Dexamethasone 20 mg/day on Days 1‐4, 12‐15

Lenalidomide10 mg/day on Days 1‐21(Low‐dose dexamethasone

added at time ofbiologic progression)

Induction9 x 28‐day cycles

Maintenance28‐day cycles

2 yrs

Mateos MV, et al. ASH 2011. Abstract 991.

smoldering MM

(N = 126)No Treatment No Treatment

Primary endpoint: TTP to symptomatic MMSecondary endpoints: response, duration of response, safety and tolerability, PFS, OS

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QuiRedex: Response• Majority of patients responded to lenalidomide plus

dexamethasone

– Responses improved with maintenance

Response, %

ITT Population With Median of 9 Induction Cycles

(Range: 1-9)(n = 57)

After Completion of

9 Induction Cycles(n = 51)

After Median of 15 Maintenance

Cycles(Range: 2-31)

(n = 50)

ORR 86 96 96

Stringent

• 12 of 14 patients either improved to PR or had SD after receiving low‐dose dexamethasone during lenalidomide maintenance


Stringent CR

7 8 16

CR 7 8 12

VGPR 11 12 16

PR 61 68 52

SD 14 4 4

QuiRedex: Safety• 3 cases of second primary malignancies reported in treatment arm

Adverse Event, % Lenalidomide + Dexamethasone(n = 57)

No Treatment(n = 62)

Grade 1/2 Grade 3 Grade 1/2

Anemia 28 2 --

Neutropenia 20 5 --

Thrombocytopenia 13 2 --

Asthenia 20 7 11

Constipation 18 -- 2


Diarrhea 24 2 4

Rash 33 4 --

Paresthesias 5 -- --

Tremor 13 -- 2

Infection 46 6 26

Deep vein thrombosis 5 --

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1 0

Len‐dex vs no treatment: TTP to active disease (n = 119)

ITT analysis

Median follow-up: 32 months (range 12–49)

Lenalidomide + dex

[Len 25*21 d + dex 20*4*2]q28 *9 then len 10 q21

1.0

0.8

0.6

0.4

Lenalidomide + dex

Median TTP: NR

9 Progressions (15%)

5 pts:early disc then DP

4 pts:symptomatic DP

No treatment

on of patients alive

454035302520151050

0.2

0.0

Median TTP: 23m

37 Progressions (59%)

20 patients: bone disease

7 patients: renal failure

HR: 6.0; 95% IC (2.9–12.6); p < 0.0001

Time from inclusion

Proportio


QuiRedex: TTP to Symptomatic MM and OS• Significant increase in TTP with vs without treatment

1 0

Median TTPLenalidomide + dexamethasone: NR

No treatment: 23 mosHR: 6.0 (95% CI: 2.9‐12.6; P < .0001)

Median follow‐up: 32 mos (range: 12‐49)

1.0

0.8

0.6

0.4

0.2

0

Proportion of

Patien

ts Alive

0 0 20 2 30 3 0

Lenalidomide + dexamethasoneNo treatment

• Significantly prolonged OS with vs without treatment

– Median 3‐yr OS (from study inclusion): 93% vs 76%; P = .04

– Median 5‐yr OS (from diagnosis): 94% vs 79%; P = .03


Mos From Inclusion

0 455 10 15 20 25 30 35 40

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Len‐dex vs no treatment: OS from inclusion(n = 119)

Median follow-up: 32 months (range 12–49)

Lenalidomide + Dex1.0

No treatment

tion of patients alive

p=0.04

0.8

0.6

0.4

Lenalidomide + Dex: 93% at 3 yearsNo treatment: 76% at 3 years

Time from inclusion

Proport

50454035302520151050

0.2

0.0


QuiRedex: Conclusions• Improved outcomes with lenalidomide and dexamethasone induction

plus maintenance lenalidomide vs no treatment in smoldering MM[1]

– Significantly prolonged TTP OS– Significantly prolonged TTP, OS

• Addition of low‐dose dexamethasone to maintenance lenalidomide maintained disease stabilization in most cases of biologic progression[1]

• Well tolerated, with most adverse events grade 1/2[1]

– Drug‐related toxicities should be considered when evaluating risk/benefitrisk/benefit

• Question remains regarding effect of treatment at this disease stage

– Delay progression only or alter natural history also

• Ongoing phase II/III ECOG trial evaluating single‐agent lenalidomide vs observation in smoldering MM; suspended in December 2011[2]

1. Mateos MV, et al. ASH 2011. Abstract 991. 2. ClinicalTrials.gov. NCT01169337.

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E3A06: Eligibility

•Diagnosis asymptomatic high‐risk disease•No immediate need for chemotherapy

•No lytic lesions on skeletal surveys and no hypercalcemia (i e ≥ 11 mg/dL)No lytic lesions on skeletal surveys and no hypercalcemia (i.e., ≥ 11 mg/dL)

•Bone marrow plasmacytosis with ≥ 10% plasma cells or sheet of plasma cells by bone marrow aspiration and/or biopsy

•Abnormal serum free‐light chain (FLC) ratio (< 0.125 or > 8.0) bby serum FLC assay

•Measurable monoclonal protein in the serum ≥ 1.0 g/dL or urine ≥ 200 mg/24 hrs

E3A06: Objectives

Primary• Study the risk of grade 3‐4 non‐hematologic adverse events in patients with asymptomatic high‐risk

smoldering multiple myeloma treated with lenalidomide. (Phase II)• Compare the progression‐free survival (PFS) of patients with asymptomatic high‐risk smoldering

multiple myeloma treated with lenalidomide versus observation alone. (Phase III)

Secondary• Assess the response of patients treated with lenalidomide. (Phase II) • Describe the gene expression profile (GEP) and cytogenetic risk classification and evaluate baseline

immune and MRI parameters in these patients. (Phase II)• Determine and compare the response rate, time to progression, 1‐year PFS probability, and the

overall survival of patients treated with lenalidomide versus observation alone. (Phase III)• Estimate the incidence of adverse events of these regimens in these patients. (Phase III)• Evaluate the impact of therapy within GEP‐defined risk groups and GEP as a prognostic marker.

(Phase III)• Study the effects of lenalidomide on laboratory markers of immune function. (Phase III)• Study the prognostic value of MRI‐detected asymptomatic bone disease on clinical outcome. (Phase

III)• Evaluate the prognostic effect of baseline high‐risk cytogenetic abnormalities on clinical outcome.

(Phase III)• Compare the quality of life of patients treated with these regimens. (Phase III)

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Diagnosis & Managementof High‐Risk SMM

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What are the best risk factors today toidentify patients with high risk SMM?

Goal

• To identify patients with high‐risk SMM with ≥ 90%

chance to develop symptomatic MM at 2 years in order to:

• ‐ prevent end‐organ damagep g g

• ‐ possibly extend survival

• ‐ avoid unnecessary treatment in low‐risk SMM

What are potential new risk factors that weshould look for?

• Bone imaging (wbMRI, PET‐CT)

• Changes in dFLC and e GFR

• Total concentration FLC (i.e. > 1000 mg/L)

• BMPCs (i.e.≥ 60%)

• Number of circulating plasma cells

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Should we treat some patients with SMM?

• Len‐dex is a promising and attractive option

• All efforts to plan an early treatment in asymptomatic MM patients should be focused on high‐risk patients

• Long term follow‐up is required to actually confirm the benefit, especially in OS

• Results of other trials that they are being conducted are needed

In the near future, we could offer early treatment to a selected high‐risk of patients with the confidence that they are going to obtain a significant benefit

Does the survival benefit seen in the Spanish trialoutweigh the risks? Should we change practice?

• The present data of the QuiRedex trial do not support change of practice!

• High risk patients are encouraged to enroll into clinical trials

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Conclusions

• Treatment of SMM should only be considered in the context of a clinical

Consensus opinion of IMWG– Consensus opinion of IMWG

• No proven survival advantage with conventional Rx OR transplant

• Short and Long‐term toxicities need to be delineated

• ? Second malignancies

• We need to better define ‘High Risk’ SMM

• The use of bisphosphonates is not clear, especially in light of the MRC data

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