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Optimal Use of Newly Approved Agents – Carfilzomib and Pomalidomide Lymphoma-Myeloma Symposium...
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Optimal Use of Newly Approved Agents – Carfilzomib and Pomalidomide Lymphoma-Myeloma Symposium October 2013 Scottsdale, Arizona Scottsdale, Arizona Rochester, Minnesota Rochester, Minnesota Jacksonville, Florida Jacksonville, Florida Joseph Mikhael, MD, MEd, FRCPC, FACP Staff Hematologist, Mayo Clinic Arizona
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Transcript of Optimal Use of Newly Approved Agents – Carfilzomib and Pomalidomide Lymphoma-Myeloma Symposium...
Optimal Use of Newly Approved Agents – Carfilzomib and Pomalidomide
Lymphoma-Myeloma Symposium
October 2013
Scottsdale, ArizonaScottsdale, Arizona Rochester, MinnesotaRochester, Minnesota Jacksonville, FloridaJacksonville, Florida
Joseph Mikhael, MD, MEd, FRCPC, FACPStaff Hematologist, Mayo Clinic Arizona
Disclosures
• I do not have any relevant financial relationships with any commercial interests.
Objectives
1. Review recent and critical data on the use of carfilzomib and pomalidomide
2. Provide practical advice as to the optimal use of these agents in clinical practice
Treatment sequence
Induction Consolidation
Front line treatment
Post consolidation
Maintenance
Rescue
Relapsed
OLD VADDEX
SCTNothing
PrednisoneThalidomide
Few options
NEW
Thal/Dex VD
Rev/DexCyBorD
VTDVRD
SCTVD/VRD
NothingThalidomide?Bortezomib?Lenalidomide
BortezomibLenalidomideThalidomideCarfilzomib
Pomalidomide
Carfilzomib: A Novel Agent Designed to Promote Selective and Sustained Proteasome Inhibition
• Carfilzomib is a next-generation, selective proteasome inhibitor• Potent and sustained target suppression• Improved antitumor activity• Minimal off-target activity with low neurotoxicity
5
HN
NH
O HN
O
O
NHO
NO O
O
EpoxyketoneTetrapeptide
Adapted from: Kuhn DJ, et al. Blood. 2007;110:3281-3290.
Neuropathy Was Infrequent and Not Dose LimitingPooled data from single-agent studies (003 / 004 / 005)
• Peripheral neuropathy occurred infrequently across all single-agent studies*
• Only 6 patients (1.2%) experienced a Grade 3 PN event
• No Grade 4 PN events
• Only 1 patient had drug discontinued for PN (study 004; BTZ-treated arm)
6Adapted from: Singhal S, et al. ASH 2010. Abstract 1954 (poster presentation).*Includes the terms peripheral neuropathy, neuropathy, peripheral sensory neuropathy, peripheral motor neuropathy
N=505
Did not experience peripheral neuropathy
Grade 3 PN (1.2%)
Grade 1/2 PN (13.4%)
Carfilzomib Single-Agent Activity
7
BTZ-naïve patients*
Response Rate 20/27 mg/m2 (N=53)*
CR 0%
VGPR 17%
PR 38%
MR 8%
SD 26%
PD 11%
ORR 55% CBR
62%
0.4%
5.1%
18.7%
10.1%
34.6%
26.8%
0
5
10
15
20
25
30
35
CR* (n=1)
VGPR (n=13)
PR (n=48)
MR (n=26)
SD (n=89)
PD (n=69)
Responses in Bortezomib-Refractory Immunomodulator-Exposed Patients (Response-
Evaluable Population, N=257)
ORR = 24%
CBR = 34%
DOR (≥ PR) and (≥ MR) = 8.3 mo
8
Phase III ASPIRE Trial
9
Randomized 1:1
N = 700
Stratification
• Prior bortezomib
• Prior lenalidomide
• β2m
Primary End Point: PFS
• Carfilzomib 27 mg/m2 IV Day 1, 2, 8, 9, 15, 16 (20 mg/m2 on Days 1, 2 of Cycle 1)
• Lenalidomide 25 mg PO Days 1–21
• Dexamethasone 40 mg PO or IV on Days 1, 8, 15, 22
• Lenalidomide 25 mg Days 1–21
• Dexamethasone 40 mg PO or IV on Days 1, 8, 15, 22
Cycle = 28 days
Cycle = 28 days
β2m = beta-2-microglobulin. US NIH, 2011.
Carfilzomib - Upfront
1. Carfilzomib-Lenalidomide Dexamethasone (CRD) in newly diagnosed
2. Cyclophosphamide – Carfilzomib – Thalidomide – Dex (CYCLONE) in newly diagnosed
Stem cell collection
≥PR
CRd Cycles 9–24
CRdInduction
CRdMaintenance
CRd Cycles 1–4 CRd Cycles 5–8
ASCT
LEN Cycles 25+
Lenalidomide (off protocol)
Transplant-eligible
Transplant-eligible and --ineligible patients
•Assessments on D1 and 15 of C1 and D1 thereafter using modified IMWG Criteria with nCR•Cycles 1–8
• CFZ Days 1–2, 8–9, 15–16 at assigned doses1
• LEN 25 mg Days 1–21• DEX 40 mg weekly Cycles 1-4, 20 mg weekly Cycles 5–8
•Cycles 9–24• CFZ on Days 1–2 and 15–16 only• CFZ, LEN, DEX at last best tolerated doses•After Cycle 4, pts could undergo stem cell collection and then continue CRd with the
option to proceed to ASCT
Until disease progression or unacceptable toxicity
Treatment Schema
1. Jakubowiak AJ, et al. Blood. 2011;118: abstract 631. ASCO 2012 Slides courtesy of Dr. Jakubowiak
Responses
51%
Change from baseline
67%
81%
Pat
ien
ts (
%)
N= 53; median 12 cycles (range 1–25)
Initial Response Best Response
ASCO 2012 Slides courtesy of Dr. Jakubowiak
Results From the Phase II Dose Expansion of Cyclophosphamide, Carfilzomib, Thalidomide and
Dexamethasone (CYCLONE) in Patients with Newly Diagnosed Multiple Myeloma
#445
J. Mikhael, C. Reeder, E. Libby, L. Costa, A. Mayo, L. Bergsagel, F. Buadi, N. Pirooz, J. Lubben, AC. Dueck, AK. Stewart
Scottsdale, ArizonaScottsdale, Arizona Rochester, MinnesotaRochester, Minnesota Jacksonville, FloridaJacksonville, Florida
Newly Diagnosed: CYCLONE Phase I/II
Carfilzomib
Cyclophosphamide
Thalidomide
Dexamethasone
Newly Diagnosed MM
ResponsePFS
ToxicityStem cell harvest
ResponsePFS
ToxicityStem cell harvest
4%
26%
22%
48%
CRVGPRPRMR
Results Levels 0 and 1– Response n=27
• Overall Response 96%
CR 7 VGPR 13 PR
6MR 1
≥ VGPR 74%
Carfilzomib - Practical
• Highly effective and very well tolerated
• Beware of tumor lysis hence dosing schedule
• Cardiac issue present but mostly mitigated by fluid management
• Issues of weekly dosing being explored
• Lack of neuropathy very attractive
• Upfront uses increasing
Structurally similar, but functionally different both qualitatively and
quantitatively
Molecular Structure of Thalidomide, Lenalidomide and Pomalidomide
Molecular Structure of Thalidomide, Lenalidomide and Pomalidomide
Myeloma Pomalidomide Summary
18
Lacy Pom/Dex1-3 reg
Lacy Pom/DexLen ref
RichardsonPom+/- dex
MM-002
PR 63% 32% 28%
MR 82%* 47% 52%
Median 3 prior regimens
Median 4-6 prior regimens
Pomalidomide in 350 Relapsed Patients: Change in the Measurable Parameter From Baseline
19
MM-003 Design: POM + LoDEX vs. HiDEXRefractory MM Pts Who Have Failed BORT and LEN
(n = 302)
POM: 4 mg/day D1-21 +
LoDEX: 40 mg (≤ 75 yrs) 20 mg (> 75 yrs) D1, 8, 15, 22
Follow-Up for OS and SPM
Until 5 Years Post Enrollment
(n = 153)
HiDEX: 40 mg (≤ 75 yrs) 20 mg (> 75 yrs) D1-4, 9-12, 17-20
28-day cycles
PD* orintolerable AE
PD* Companion trialMM-003C
POM 21/28 days
Stratification•Age (≤ 75 vs. > 75 yrs)
•Number of prior Tx ( 2 vs. > 2)
•Disease population
Thromboprophylaxis was indicated for those receiving POM or with DVT history
*Progression of disease was independently adjudicated in real-timeDimopoulos Blood 2012, 120(21): LBA-6
MM-003: Key Eligibility Criteria• All pts had to be refractory to last therapy
• At least 2 prior therapies• ≥ 2 consecutive cycles of LEN and BORT (alone or in combination)
• Adequate prior alkylator therapy (SCT or ≥ 6 cycles or PD following ≥ 2 cycles)
• All pts must have failed LEN and BORT • Pt progressed on or within 60 days
• Pt with PR must have progressed within 6 months
• Intolerant to BORT
• Refractory or relapsed and refractory disease• Primary refractory: never achieved > PD to any therapy
• Relapsed and refractory: relapsed after having achieved ≥ SD for ≥ 2 cycles of Tx to at least one prior regimen and then developed PD ≤ 60 days of completing their last therapy
Dimopoulos Blood 2012, 120(21): LBA-6
MM-003: Patient Disposition*
*As of final PFS analysis, Sept 7, 2012.
POM + LoDEX(n = 302)
RANDOMIZATION 2:1
(N = 455)
HiDEX(n = 153)
PD
Discontinued 75% PD: 49%AE: 6%Death: 10%Withdrawal: 3%Lost to follow-up: 1%Other: 6%
25%Ongoing Tx
Discontinued 55%PD: 35%AE: 7%Death: 6%Withdrawal: 2%Lost to follow-up: 1%Other: 4%
45%Ongoing Tx
29% Pts received POM
after PD on HiDEX
Dimopoulos Blood 2012, 120(21): LBA-6
Based on adjudicated data; IMWG criteria
MM-003: Progression-Free Survival ITT Population
0 4 8 12 160.0
0.2
0.4
0.6
0.8
1.0
Progression-Free Survival (months)
Pro
po
rtio
n o
f P
atie
nts
Median PFS
POM + LoDEX (n = 302) 3.6 months
HiDEX (n = 153) 1.8 months
HR = 0.45P < .001
Dimopoulos Blood 2012, 120(21): LBA-6
MM-003: Overall SurvivalITT Population
NE, not estimable
Overall Survival (months)
0.0
0.2
0.4
0.6
0.8
1.0
0 4 8 12 16
Pro
po
rtio
n o
f P
atie
nts
Median OS (95% CI)
POM + LoDEX (n = 302) Not Reached (11.1-NE)
HiDEX (n = 153) 7.8 months (5.4-9.2)
HR = 0.53P < .001
29% of pts received POM after progression on HiDEX
Dimopoulos Blood 2012, 120(21): LBA-6
MM-003: Ongoing Evaluation of Response ITT Population
Response based on IMWG criteria, except for MR (based on EBMT criteria)* KM median, patients with ≥ PR onlyNE, not estimated due to too few responders
Response, % POM + LoDEX (n=302)
HiDEX (n=153)
P value
ORR (≥ PR) 21 3 < .001
VGPR 3 1 —
≥ MR 37 8 —
≥ SD 81 60 —
Median DOR*, m (95% CI)10.1
(6.2 – 12.1)NE —
As of Nov 9, 2012• PFS of ≥ MR in POM + LoDEX: 8.5 months
Dimopoulos Blood 2012, 120(21): LBA-6
Pomalidomide - Practical
• Similar to lenalidomide with slightly less myelotoxicity and fatigue
• Dosing range 2-4mg
• Thromboprophylaxis necessary
• Feasible in combination
Selecting Therapy
• Both are highly active agents
• Class switch a consideration
• Useful even when progressing on same class agent
• Convenience and toxicity is important
• Most MM patients will ultimately see both drugs
