Post on 05-Jun-2020
Has immunotherapykept its promises
in malignant lymphomas?
Franco Cavalli M.D., F.R.C.P.
President
Institute of Oncology Research (IOR)
President WOF and Scientific Committee ESO
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Lymphomas and immunotherapy
Notwithstanding the “natural correlation” for many
years only adoptive immunotherapy through allogeneic SCT was
“sometimes” efficacious.
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What do we mean today by ‘immunotherapy’?
• MONOCLONAL ANTIBODIES
– ‘Naked’
– Radio-immunotherapy
– Immuno-toxins
• ENGAGING T-CELLS
– Interferon
– Vaccination
– Immune checkpoint inhibition
– CAR T cells
– Bispecific antibodies
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Rituximab: mechanisms of action
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Patients usually respond to upfront R
Colombat 2001 (n= 50) 73%
Hainsworth 2002 (n= 60) 73%
Witzig 2005 (n= 37) 72%
Ghielmini 2005 (n= 202) 75%
Kimby 2008 (n= 123) 78%
Ardeshna 2010 (n= 192) 85%
RR of prolonged rituximab in first-line FL
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FL: the response to upfront rituximab (RR 70%) can be long lasting if maintained
1. Martinelli G, et al. J Clin Oncol 2010;28:4480–842. Taverna C, et al. ASH 2013; Abstract 508
PFS2
Median EFS = 4.4 years
Median EFS = 2.5 years
P=0.04
1 year
5 years
Years since start of treatment
0.0
0.4
0.6
0.8
1.0
0.2
2 4 6 8 101 3 5 7 9
p = 0.045
1 month
1 year
Prolonged
Standard
Time from randomisation (years)
0.0
0.4
0.6
0.8
1.0
0.2
2 4 6 8 91 3 5 70
Pro
bab
ility
EFS1
Median PFS = 7.4 years
Median PFS = 3.5 years
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R2 in FL patients in need of treatment
10% 13%25%
36%
35%
62% 36%
45%
0
10
20
30
40
50
60
70
80
90
Rituximab (N=77) Rituximab +Lenalidomide (N=77)
Rituximab (N=77) Rituximab +Lenalidomide (N=77)
PR
CR/CRu
Week 10 Week 23
45%
75%
61%
82%
Pro
po
rtio
n o
f p
atie
nts
(%
)
p<0.0001 p=0.002
Kimby E, et al. ASH 2014; Abstract 7995th
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RELEVANCE trial
Morschhauser F, et al.NEJM, 2018;379:934-947 5th
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Improvement in lymphoma treatment: DLBCL
1st phase
Chemo
Survival improvement
2nd phase
Some are cured
Doxo
3rd phase
More are cured
Rituximab
4th phase
New drugs?
All are cured, no side effects
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131I
Targeted irradiation: radio-immuno-therapy
Properties
90Yttrium
(Zevalin)
131Iodine
(Bexxar)
Half-life 64 hours 192 hours
Energy emitter Beta
(2.3 MeV)
Gamma (0.36 MeV)
Beta (0.6 MeV)
Path length 90 5 mm 90 0.8 mm
Urinary excretion Minimal
7% in 7 days
Extensive/variable
46 - 90% in 2 days
Dosing
Based on weight
and platelet
count
Clearance based dosing
using whole body
dosimetry
Administration Outpatient Inpatient or restrictions to
protect family/public
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Radio-immunotherapy as initial therapy for indolent NHL
GELF, Groupe d'Etude des Lymphomes Folliculaires1. Kaminski MS, et al. N Engl J Med 2005;352:441–49
2. Ibatici A, et al. Br J Haematol 2014;164:710–16
I-131 Tositumomab1
n=76 patients, 95% OR, 75% CR
90-Y Ibritumomab2
n=50 patients, 94% OR, 86% CR
Years after dosimetric dose
0
40
60
80
100
20
2 4 60 81 3 5 7
Progression-free survival
Overall survival
Su
rviv
al (%
)
0.0
0.4
0.6
0.8
1.0
0.2
24 48 8412 36 60 720
Progression-free survival (months)
Cu
mu
lati
ve
su
rviv
al
GELF criteria
GELF criteria not met
GELF criteria met
Global
Censored data
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Brentuximab vedotin (SGN35) Anti-CD30 conjugated to an antitubulin agent
MMAE – microtubule-disrupting agent
ADC binds to CD30
MMAE disruptsmicrotubule network
Internalised in lysosome
MMAE is released
anti-CD30 monoclonal antibody
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Brentuximab vedotin in HL
80% of patients respond to the treatment even in relapses after
autologous/allogeneic SCT
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Brentuximab vedotin within chemotherapy for stage III or IV Hodgkin’s lymphoma
N = 670 ABVD= 664 A-AVD
Fu = 25 months
A-AVD5% lower combined risk of PD, death or non-CR requiring alternative treatment
J.M. Connors et al. NEJM 2018; 378:331-3445th
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ECHELON-1 trial
HL Stage III-IV untreated
670 ABVDR
664 AVD + A (Adcetris = Brentuximab)
4.9% less modified PFS (including non CR requesting new treatment)
P = 0.04
J.M. Connors et al. NEJM 2018; 378:331-3445th
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NativeT cell
Malignant B Cell
PD1
PD-L1PD-L2
MHC I/II
TCRCD3
5.- BiTEEngineeredT Cell
1.- Cytokines2.- Tumor vaccines
3.- Immune checkpointinhibitors
TCR
4.- CAR
Batlevi C, Matsuki E, et al: Nature Rev Clin Oncol 2015 (Accepted)
Therapeutic strategies to overcome immune tolerance to cancer
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Interferon prolongs survival in FL
META-ANALYSIS10 randomised trials, 1922 patients
Survival benefit of 2 years (p=0.0008) if IFN given With (NOT after) intensive chemotherapy
At a dose of ≥ 5 million UI
At a cumulative dose of ≥ 36 million UI / month
Rohatiner AZS, et al. J Clin Oncol 2005;23:2215–235th
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Vaccines are directed against idiotypes
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Vaccinated patients developing anti-idiotype Ab have a longer response after chemotherapy
Analysis of 136 patients with FL receiving idiotype (Id) vaccinationHumoral represents patients with specific anti-Id Abs
Weng WK, et al. J Clin Oncol 2004;22:4717–24
Humoral
Other
HumoralOther
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Mitumprotimut-T vs placebo
Freedman A, et al. J Clin Oncol 2009;27:3036–43
Negative vaccine trial
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Analysis of patients with advanced stage previously untreated FL
Schuster SJ, et al. J Clin Oncol 2009;27:2
“Positive” vaccine trial
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Blockade of CTLA-4, PD-1, PD-L1 in tumour immunotherapy
Ribas A, N Engl J Med. 2012;366:2517–195th
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Armand P, et al. ASH 2014; Abstract 289
Nivolumab: RR 87%, CR 17%
Responses of HL to anti-PD1 in R/R HL
-100
-80
-60
-40
-20
0
20
40
60
80
100
Ch
ange
fro
m b
ase
line
, %
Moskowitz CH, et al. ASH 2014; Abstract 290
Pembrolizumab: RR 66%, CR 21%
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9p24.1Gene amplification
EBVInfection
JAK2
PDL1
Hodgkin and Reed Sternberg (HRS) Cells
CD30
HRS Cells Express High Levels of PDL-1
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Nivolumab
Abstr. 010
CHL (n = 23) ORR 87% CR 17%
B-NHL (n = 31) ORR 26% CR 10%
T – NHL (n = 23) ORR 17%
13-ICML 20155th
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PD-1 blockade by pidilizumab plus rituximab in relapsed FL
Westin JR, Lancet Oncol 2014;15:69–77
Efficacy Safety
n= 29 pts No gr 3–4 AEs
ORR 66% (CR 52%)
Median PFS 19 months
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Two strategies to engage T-cells against B-cell lymphoma
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Kochenderfer JN, Rosenberg SA. Nat Rev Clin Oncol 2013;10:267–76
CAR-T cells(Chimeric Antigen Receptor)
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*Any grade or no details of grade; **Total n=30
Summary of available data for CAR T cells in R/R ALL
19-28z(MSKCC/Juno;
n=39)1
CTL019(CHOP/UPenn/
Novartis; n=39)2,3
CD19-CAR(NCI/Kite; n=20)4
Population Adults >18 years Children (age not specified)2
Children/youngadults (1–30 yr)
Status after conditioning chemotherapy, prior to CAR T-cell treatment
MRD+ CR (<5% BMB)MRD- (<0.01% BMB)
46%0%
23%2
15%225%0%
Status after conditioning chemotherapy and CAR T-cell treatment
CR/CRi 87% 92% 70%
MRD- (in evaluable patients) 81% 82% 60%
Clinically significant/severe CRS
23% 27**3 29
Neurotoxicity (%)* 28 (Grade 3/4) 43**3 29
1. Park JH, et al. Oral presentation at ASCO 2015. Abstract 7010; 2. Grupp S, et al. Oral presentation at ASH 2014. Abstract 380
3. Maude SL, et al. N Engl J Med 2014;371:1507–17; 4. Lee DW, et al. Lancet 2015;385:517–285th
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Car T-cell therapy in refractory large B-cell lymphoma
S.S Neelapu et al. NEJM 2017; 377:2531
N = 111 pts 77 DLBCL(101 administered) 24 PMBCL or tranformed FL
Most resistant to at least second-line therapy
OR = 82%CR = 54%FU (15 months) = 48% still in responseCytokine release Sy (≥ grade 3): 13%Neurologic events: 28%
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Car T-cell therapyin refractory B-cell lymphoma
S. J Schuster et al. NEJM. 2017; 377:2545
N = 28 enrolled, 28 treated (insufficient T-cell, PD)
14 FL 89% response, CR 71%14 DLBCL 86% response, CR 43%
Severe cytokine release Sy (18%)Serious encephalopathy (13 %)
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Conclusions on CAR T cell therapy
• Unprecedented activity in R/R DLBCL• Toxic so far manageable only in specialised centres• Possibly practice changing treatment
Pending issues:• Longer follow-up needed• Ideal timing for CAR T treatment yet to be determined• Logistics are complex and restrictive• Financial limitations (USD 300’000 to 500’000 per
treatment)
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Bi-specific antibodies
Frankel SR, Baeuerle PA. Curr Opin Chem Biol 2013;17:385–92
Design and mode of action of bispecific T-cell engager (BiTE®) antibody constructs
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CR after Blinatumomab in ALL patientsrefractory or relapsed after allotransplant
Topp MS, et al. Lancet Oncol 2015;16:57–66;Topp MS, et al. EHA 2014, Abstract S722 and oral presentation
All responders
Sex FemaleMale
Age 18 to <3535 to <5555 to <65≥65
Prior Salvage 012≥3
Primary refractory Yes
Prior SCT Yes
Bone marrow blasts <50%≥50%
0 20 40 60 80 100
189 43
4641
43
443646
50
343647
3843
4542
2973
70119
16173
64125
90462825
38774232
59130
No
No
CR/CRh rate, %
36–50
34–5832–51
33–54
24–6519–5631–61
33–67
19–5322–5235–58
15–6536–51
33–5833–51
22–3860–84
N
CR/CRh
% 95% CI
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PD-L1 blockade: rejuvenating T cells in CLL
CLL prime example of tumourinteracting with microenvironment.
T-cell defects in murine CLL point to a possible huge therapeutic role of
immune checkpoint blockade.
Mc Clanahel et. al. Blood 2015; 126:203-211Blood 2015; 126:212-221 5t
h ESO-E
SMO L
atin
Amer
ican
Mas
terc
lass i
n Clin
ical O
ncolo
gy
Immunotherapy in Multiple Myeloma
• Allogenic: limited results• Car-T cells: in China ↑↑↑• Checkpoint inhibitors:
alone −+ IMID + but too toxic
• Anti CD38 (Daratumumab): Breakthrough!!!
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Conclusions (for lymphomas)
• Chemotherapy is not likely to obtain more in B-cell malignancies
• Future progress most likely to be obtained by targeted drugs and immunotherapy
• Possibly enhancement activity of IT through radiotherapy (NK/T cell!)
• One avenue of success may be the engagement of T cells against malignant B cells
• Long-term toxicity still unclear
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THANKS FOR YOUR ATTENTION!
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