Post on 20-Feb-2019
Highlights from EHA 2014Myelodysplastic syndromes
Valeria Santini, M.D.Dept of Hematology AOU Careggi, University of FlorenceFlorence, Italy
-Sessione educativa
-2 sessioni simultanee
( 10 comunicazioni cliniche e
1 late breaking abs;
5 comunicazioni biologiche)
-3 sessioni poster
( 32 clinici e
19 biologici)
Scenario
1. Ciò su cui è importante essere aggiornati
(educativa)
2. Nuovi farmaci per MDS/AML refrattarie
3. Correlazione tra markers molecolari e
clinica
Punto 1
Sessione educativa: cosa dobbiamo sapere
su MDS nel 2014
The molecular basis of MDS
B. Ebert
Prognostic biomarkers in MDS
M. Cazzola
Clinical management of MDS
U. Platzbecker
PROGNOSTIC BIOMARKERS IN MYELODYSPLASTIC
SYNDROMES
MARIO CAZZOLA
Department of Molecular Medicine, University of Pavia, Pavia, Italy;
Department of Hematology Oncology, Fondazione Istituto di Ricovero e Cura a Carattere Scientifico Policlinico San Matteo, Pavia, Italy;
OUTLINE
• Importance of morphology in diagnosis and
prognostication of MDS
• Contribution of cytogenetics in diagnosis and
prognostication of MDS
• Current prognostic scoring systems based on
morphology and cytogenetics
• Emerging evidence that detection of somatic gene
mutations can improve both our understanding of MDS
and clinical decision making
Representative examples of morphologic abnormalities of myelodysplasia.
Cazzola M et al. Blood 2013;122:4021-4034
©2013 by American Society of Hematology
WHO 2008: Classificazione delleneoplasie mieloidi e leucemie acute
Sindromi mielodisplastiche WHO 2008
Citopenia refrattaria con displasia unilineare
- anemia refrattaria
- neutropenia refrattaria
- trombocitopenia refrattaria
Anemia refrattaria con sideroblasti ad anello
Citopenia refrattaria con displasia multilineare
Anemia refrattaria con eccesso di blasti
Sindrome mielodisplastica con isolata del(5q)
Sindrome mielodisplastica inclassificabile
Sindrome mielodisplastica dell’infanzia
Provisional entity: citopenia refrattaria dell’infanzia
Survival according to WPSS-R
at diagnosis
IPSS-R variables and weighted scores
* Regression analysis for survival and AML evolution.
ANC, absolute neutrophil count; BM bone marrow. Greenberg PL, et al. Blood. 2012;120:2454-65.
Cytogenetics
Score
Very good
0
Good
1
Intermediate
2
Poor
3
Very poor
4
BM blasts, %
Score
≤ 2
0
> 2–< 5
1
5–10
2
> 10
3
Hb, g/dL
Score
≥ 10
0
8–9.9
1
< 8
1.5
ANC, x 109/L
Score
≥ 0.8
0
< 0.8
0.5
Platelets, x 109/L
Score
≥ 100
0
50–99
0.5
< 50
1
Overall survival and leukemia-free survival of 1110 patients with MDS
Cazzola M et al. Blood 2013;122:4021-4034©2013 by American Society of Hematology
Della Porta M G et al. Blood 2014;123:2333-2342©2014 by American Society of Hematology
Patient-based and disease status–based risk stratification of outcome among MDS patients receiving allo HSCT.
Frequence of somatic mutations in MDS
Papaemmanuil et al, 2013 ; 122:3616
Frequence of somatic mutations in MDSNagata et al, Leukemia 2014
Nagata et al. Leukemia 2014
Survival and risk of leukemic evolution of patients with MDS classified according to the clusters resulting from the unsupervised analysis including WHO classification criteria and
mutation patterns.
Malcovati L et al. Blood 2014;124:1513-1521©2014 by American Society of Hematology
Authors’ Conclusions
• Clonal marker in 90% of patients (vs 505 of cytogenetic
abnormalities)
• Already established genotype/phenotype relationships
SF3B1 mutant MDS
TET2/SRSF2 comutant MDS/MPN (CMML)
• Prognostic relevance of somatic mutations of RNA
splicing and DNA methylation
SF3B1 mutation vs other mutation of the spliceosome (
SRSF2 and U2AF1)
Favorable outcome of pts without somatic muations of RNA
splicing and DNA methylation
Punto 2
Molti pazienti sia con alto che con basso
rischio MDS, dopo una prima risposta alla
terapia, “ricadono”.
Alcune opzioni terapeutiche di seconda linea
sono disponibili , ma c’è comunque
bisogno di identificare nuovi agenti
Abstract number: LB2434 Slides available on EHA website
IDH1/2 mutations in MDS
Present in ~4-12% of patients with MDS
Missense mutations: heterozygous; target highly conserved
Arginine residues
IDH1: R132H mutations
IDH2: R172K or R140Q mutations
All variants produce 2-hydroxyglutarate (2-HG)
Mutations in IDH1/2 are associated with increased 5-
methylcytosine
Initial reports: Unfavorable prognosis for IDH-mut MDS
Authors’ Conclusions
• Treatment with AG-221 leads to a
profound differentiation effect and is
associated with durable complete
remissions in patients who are extremely
ill and have limited treatment options
ACE-536 Increases HemoglobinLevels in Patients with Low or Int-1 Risk MDS:Preliminary Results From A Phase 2 Study
Uwe Platzbecker1, Ulrich Germing2, Aristoteles Giagounidis3, Katharina Götze4,
Philipp Kiewe5, Karin Mayer6, Oliver Ottmann7, Markus Radsak8, Thomas Wolff9,
Monty Hankin10, Dawn Wilson10, Matthew Sherman10, Kenneth Attie10
1Universitätsklinikum Carl Gustav Carus, Dresden, 2Universitätsklinikum Düsseldorf, 3Marien Hospital Düsseldorf, Düsseldorf, 4Technical University of Munich, Munich, 5Onkologischer Schwerpunkt am Oskar-Helene-Heim, Berlin, 6Universitätsklinikum
Bonn, Bonn, 7Klinikum der J.W. Goethe-Universität Frankfurt, Frankfurt/Main, 8University Medical Center – Johannes
Gutenberg-Universität, Mainz, 9OncoResearch Lerchenfeld UG, Hamburg, Germany, 10Acceleron Pharma, Cambridge, MA,
United States
Slides kindly provided by U. Platzbecker
Abstract number S1296
Therapeutic Options in MDS
Intensive CTx/allo TxFe-Chelation
Hypomethylating Agents
Registered
Lenalidomide (del 5q)
- 80–90% of MDS patients become dependent on RBC transfusions
- Ineffective erythropoiesis
- Many patients unresponsive/refractory to ESAs/HMT
Lower-risk Higher-risk
Stratification according to IPSS-(R)
ESA
ACE-536: Background
Suragani et al. Nature Medicine 2014
TGF-ß Superfamily
Signaling
ACE-536
Erythropoiesis
GDF11,Others
Modified Extracellular
Domain (ECD) of ActRIIB
Fc domain of human IgG1
Fusion protein containing modified activin receptor IIB (ActRIIB)
Phase 2, multicenter, open-label, dose-finding
IPSS Low/Int-1
Transfusion-dependent (TD), or
Non-transfusion dependent (NTD, Hgb <10 g/dL)
EPO >500 U/L or nonresponsive/refractory to ESAs
No prior azacitidine or decitabine
Schedule: ACE-536 SC every 3 weeks for 3 months (up to 5 doses)
Preliminary data as of 28 April 2014
ACE-536 PACE-MDS Study: Overview
ACE-536Treatment Period
Screening Period
-28 1 22 43 64 85 113 141 1
Follow-up Period
Study Day
Adverse Events in ≥ 10% of Patients Overall
• No drug-related serious adverse events
• Severity Grade 1 (mild) unless noted otherwise
Preferred Term
0.125
mg/kg
(N=3)
n
0.25
mg/kg
(N=3)
n
0.50
mg/kg
(N=3)
n
0.75
mg/kg
(N=6)
n
1.0
mg/kg
(N=3)
n
1.33
mg/kg
(N=3)
n
Overall
(N=21)
n
Diarrhoea - 1 11
Gr 2- 1 4
Bone Pain - -1
Gr 2-
2
Gr 1, Gr 2- 3
Fatigue - - - - - 3 3
Muscle Spasms - -2
Gr 1, Gr 2- 1 - 3
Myalgia - 1 1 - 1 - 3
Nasopharyngitis - 1 -2
Gr 1, Gr 2- - 3
Hemoglobin Responsein 2/5 pts non transfusion dependent
Patient ID
Dose Group (mg/kg)
Prior MDS Therapy
Hgb Increase≥ 1.5 g/dL for ≥
2 wks
Hgb Increase≥ 1.5 g/dL for ≥ 8
wks [IWG]
0103 0.125 No No No
0201 0.25 No No No
0404 0.75 ESA Yes No
0405 0.75 ESA No No
0406 0.75 ESA Yes Yes
NTD, non-transfusion dependent; ESA, erythropoiesis-stimulating agent
Maximum Hemoglobin Increase in NTD Patients
NTD, non-transfusion dependent
0,81,0
1,6
1,9
3,3
0,0
0,5
1,0
1,5
2,0
2,5
3,0
3,5
0.125mg/kg(n=1)
0.25mg/kg(n=1)
0.75mg/kg(n=3)
Ma
x.
Ch
an
ge
in
He
mo
glo
bin
(g
/d
L)
Patient
ID
Dose Group
(mg/kg)
Prior MDS
Therapy
% Change
RBC Units
≥4 Unit Decrease
/ 8 Weeks [IWG]
0101 0.125 LEN 0 No
0102 0.125 ESA -50% (42) No
0202 0.25 ESA -25% No
0203 0.25 -50% (42) No
0301 0.5 LEN -50% (84) Yes
0302 0.5 +25% No
0303 0.5 ESA 0 No
0401 0.75 ESA, LEN -100% (40) Yes
0402 0.75 ESA 0 No
0403 0.75 +50% No
0501 1.00 -33% No
0502 1.00 ESA, LEN -39% (138) Yes
0503 1.00 0 No
0601 1.33 0 No
0602 1.33 ESA 0 No
0603 1.33 -67% (62) Yes
Transfusion ResponseIn 6/16 transfusion dependent pts
TD, transfusion dependent; LEN, lenalidomide; ESA, erythropoiesis-stimulating agent
Authors’ Conclusions
• Treatment with ACE 536 is safe and well
tolerated
• Patients may obtain substantial Hb
increase
• Dosing every 3 weeks
• Required more studies with larger number
of patients
Punto 3
Esiste ormai ampia evidenza che
l’identificazione di mutazioni geniche
somatiche e di markers molecolari può
migliorare la qualità delle nostre decisioni
cliniche, assieme alla migliore
comprensione della patogenesi delle
MDS (M. Cazzola EHA 2014)
Abstract number P299 E-poster online EHA website
Baseline serum
levels of miRNA-21
Levels of miRNA 21 correlate with disease progression
in MDS treated with HMT
Authors’ Conclusions
• Serum microRNA 21 level is significantly
associated with the response to treatment
with azacitidine and decitabine
• miR-21 is a potential biomarker to be
further validated for prediction of response
to the most common agents used in MDS
therapy
Questions?