Descrizione riassuntiva della sperimentazione (Fonte di dati: BASEC)
Diese internationale Studie untersucht, ob das Studienmedikament MBG453 in Kombination mit Azacitidin sicher ist und für Patienten mit einem myelodysplastischem Syndrom mit mittelhohem, hohem oder sehr hohem Risiko oder mit chronischer myelomonozytischer Leukämie-2 im Vergleich zur Behandlung mit Azacitidin allein einen grösseren Nutzen bietet.
Ungefähr 500 Patientinnen und Patienten weltweit (2 in der Schweiz) werden an dieser Studie teilnehmen und in zwei Gruppen eingeteilt, Sie erhalten entweder Azacitidin + MBG453 oder Azacitidin + Placebo. Es wird zufällig bestimmt, ob Sie MBG453 oder Placebo bekommen.
Azacitidin ist die derzeit zugelassene Behandlung für Ihrer Erkrankung.
MBG453 handelt sich um ein in der Prüfung befindliches Medikament, das bisher noch in keinem Land zur Anwendung zugelassen wurde. MBG453 wird gegenwärtig in dieser Studie und in anderen Studien weltweit für die Behandlung von Patienten mit unterschiedlichen Formen von Blutkrebs geprüft. MBG453 blockiert ein Protein namens TIM-3, das auf Blutzellen namens T-Lymphozyten vorkommt. Indem es TIM-3 blockiert, erhöht MBG453 möglicherweise die Aktivität Ihrer T-Lymphozyten, damit diese den Krebs angreifen und vernichten.
Ihre Studienteilnahme kann bis zu ca. 5 Jahre dauern, je nachdem, an welchem Datum Sie in die Studie eintreten und wie gut Sie auf die Behandlung ansprechen. Zu Ihrer Studienteilnahme gehören regelmässige Spitalvisite, körperliche Untersuchungen, Fragebögen sowie Entnahme von Blut- und Knochenmarkproben.
Malattie studiate(Fonte di dati: BASEC)
Myelodysplastisches Syndrom mit mittelhohem, hohem oder sehr hohem Risiko gemäss IPSS-R, oder chronische myelomonozytische Leukämie-2
Health conditions
(Fonte di dati: WHO)
Myelodysplastic Syndromes;Leukemia, Myelomonocytic, Chronic
Malattia rara
(Fonte di dati: BASEC)
No
Interventi esaminati (p. es. medicamento, terapia, campagna)
(Fonte di dati: BASEC)
Azacitidin wird subkutan (unter die Haut) an den ersten sieben aufeinanderfolgenden Tagen in jedem 28 Tägigen Zyklus (von Tag 1 bis Tag 7) oder von Tag 1 bis Tag 5, gefolgt von einer Pause von zwei Tagen, und dann wieder an Tagen 8 und 9 jedes Zyklus subkutan verabreicht.
MBG453 bzw. das Placebo wird intravenös (direkt in eine Vene) an Tag 8 in jedem 28 Tägigen Zyklus verabreicht.
Interventions
(Fonte di dati: WHO)
Drug: Sabatolimab;Drug: Azacitidine;Drug: Placebo
Criteri per la partecipazione alla sperimentazione
(Fonte di dati: BASEC)
• Unterschriebene Studieneinwilligung
• Frauen und Männer ab 18 Jahren und ECOG Status 0-2, die an einem Mittelhoch- oder Hochrisiko myelodysplastischem Syndrom oder an chronischer myelomonozytischer Leukämie-2 leiden
• Patienten, die eine Indikation für die Behandlung mit Azacitidin aufweisen
• Patienten, die für eine Stammzelltransplantation oder intensive Chemotherapie nicht in Frage kommen
Criteri di esclusione
(Fonte di dati: BASEC)
• Vorherige Behandlung mit einer gegen TIM-3 gerichteten Therapie, Behandlung in den letzten 4 Monaten mit einem Checkpoint Inhibitor oder einer Krebsimpfung
• Vorherige Behandlung von Mittelhoch- oder Hochrisiko-MDS oder CMML-2 mit antineoplastischen Mitteln. Eine vorherige Behandlung mit Hydroxyurea oder einer Leukopherese zur Verringerung der Leukozytenzahl ist jedoch zulässig
• Frühere Organ- oder hämatopoetische Stammzelltransplantation
• Schwangere oder stillende Frauen, sowie gebärfähige Frauen, die keine hochwirksame Verhütung anwenden. Männliche Teilnehmer müssen ein Kondom verwenden
Inclusion/Exclusion Criteria
(Fonte di dati: WHO)
Gender: All
Maximum age: 100 Years
Minimum age: 18 Years
Inclusion Criteria:
- Signed informed consent must be obtained prior to participation in the study
- Age = 18 years at the date of signing the informed consent form
- Morphologically confirmed diagnosis of myelodysplastic syndrome (MDS) based on WHO
2016 classification (Arber et al 2016) by local investigator assessment with one of
the following Prognostic Risk Categories, based on the revised International
Prognostic Scoring System (IPSS-R):
- Very high (> 6 points)
- High (> 4.5 - = 6 points)
- Intermediate (> 3 - = 4.5 points) Or Morphologically confirmed diagnosis of
Chronic Myelomonocytic Leukemia -2 based on WHO 2016 classification (Arber et
al 2016, including persistent monocytosis) by local investigator assessment
with WBC < 13 x 109/L at time of initial diagnosis
- Indication for azacitidine treatment according to the investigator, based on local
standard medical practice and institutional guidelines for treatment decisions
- Not eligible at time of screening for intensive chemotherapy according to the
investigator, based on local standard medical practice and institutional guidelines
for treatment decisions, including assessment of individual clinical factors such as
age, comorbidities and performance status
- Not eligible at time of screening for hematopoietic stem cell transplantation (HSCT)
according to the investigator, based on local standard medical practice and
institutional guidelines for treatment decisions, including assessment of individual
clinical factors such as age, comorbidities, performance status, and donor
availability
- Eastern Cooperative Oncology Group (ECOG) performance status of 0, 1 or 2
Exclusion Criteria:
- Prior exposure to TIM-3 directed therapy at any time. Prior therapy with immune
checkpoint inhibitors (e.g, anti-CTLA4, anti-PD-1, anti-PD-L1, or anti-PD-L2),
cancer vaccines is allowed except if the drug was administered within 4 months prior
to randomization
- Previous first-line treatment for intermediate, high, very high risk myelodysplastic
syndromes (based on IPSS-R) or CMML with any antineoplastic agents including for
example chemotherapy, lenalidomide and hypomethylating agents (HMAs) such as
decitibine and azacitidine. However, previous treatment with hydroxyurea or
leukopheresis to reduce WBC count is allowed prior to randomization.
- Investigational treatment received within 4 weeks or 5 half-lives of this
investigational treatment, whatever is longer, prior to randomization. In case of a
checkpoint inhibitor: a minimal interval of 4 months prior to randomization is
necessary to allow randomization.
- Subjects with Myelodysplastic syndrome (MDS) based on 2016 WHO classification (Arber
et al 2016) with revised International Prognostic Scoring System (IPSS-R) = 3
- Diagnosis of acute myeloid leukemia (AML) including acute promyelocytic leukemia and
extra-medullary acute myeloid leukemia, primary or secondary myelofibrosis based on
WHO 2016 classification (Arber et al 2016)
- Diagnosis of therapy related myeloid neoplasms based on WHO 2016 classification
(Arber et al 2016)
- History of organ or allogeneic hematopoietic stem cell transplant
Other protocol-defined Inclusion/Exclusion Criteria may apply.
-
Altre informazioni sulla sperimentazione
Stato di reclutamento
Completed
Titolo scientifico
(Fonte di dati: WHO)
A Randomized, Double-blind, Placebo-controlled Phase III Multi-center Study of Azacitidine With or Without MBG453 for the Treatment of Patients With Intermediate, High or Very High Risk Myelodysplastic Syndrome (MDS) as Per IPSS-R, or Chronic Myelomonocytic Leukemia-2 (CMML-2)
Tipo di sperimentazione
(Fonte di dati: WHO)
Interventional
Disegno della sperimentazione
(Fonte di dati: WHO)
Allocation: Randomized. Intervention model: Parallel Assignment. Primary purpose: Treatment. Masking: Triple (Participant, Care Provider, Investigator).
Fase
(Fonte di dati: WHO)
Phase 3
Punti finali primari
(Fonte di dati: WHO)
Overall Survival
Punti finali secondari
(Fonte di dati: WHO)
Key secondary endpoint 1: Time to definitive deterioration of fatigue using Functional Assessment of Cancer Therapy (FACIT)-Fatigue score;Key secondary endpoint 2: Red Blood Cell transfusion-free intervals;Key secondary endpoint: Percent of subjects with at least 3 point confirmed improvement from baseline in FACIT-fatigue scoresscore;Key secondary endpoint 4: Percent of subjects with at least 10 point confirmed improvement from baseline in physical functioning using European Or ganization for Research and Treatment of Cancer's Core Quality of Life Questionnaire (EORTC QLQ-C30);Key secondary endpoint 5: Percent of subjects with at least 10 point confirmed improvement from baseline in emotional functioning using EORTC-QLQ-C30;Percentage of subjects with either CR, or mCR, or PR, or HI in each treatment arm according to International Working Group for MDS (IWG-MDS) as per investigator assessment;Percentage of subjects with SD in each treatment arm according to International Working Group for MDS (IWG-MDS) as per investigator assessment;Progression Free Survival (PFS);Leukemia-free survival;Number of transfusion dependent subjects at baseline who become Red Blood Cells/platelets transfusion independent after randomization;Percentage of transfusion dependent subjects at baseline who become Red Blood Cells/platelets transfusion independent after randomization;Pharmacokinetics of MBG453 (parameter Cmax);Pharmacokinetics of MBG453 (parameter AUC);Anti-drug Antibody (ADA) prevalence at baseline and ADA incidence on-treatment;Change from baseline in the European Quality of Life (EuroQol) - 5 Dimensions, 5 Level Questionnaire (EQ-5D-5L) score over time;Change from baseline in the European Quality of Life (EuroQoL) - 5 Dimensions, 5 Level Questionnaire (EQ-5D-5L) Visual Analogue Scale over time;Change from baseline to C12D1 of Global Health Status/Quality of Life scores using European Organization for Research and Treatment of Cancer's Core Quality of Life Questionnaire (EORTC-QLQ-C30)
Contatto per informazioni
(Fonte di dati: WHO)
Please refer to primary and secondary sponsors
Risultati della sperimentazione
(Fonte di dati: WHO)
Sintesi dei risultati
ancora nessuna informazione disponibile
Collegamento ai risultati nel registro primario
ancora nessuna informazione disponibile
Informazioni sulla disponibilità dei dati dei singoli partecipanti
ancora nessuna informazione disponibile
Siti di esecuzione della sperimentazione
Siti di esecuzione in Svizzera
(Fonte di dati: BASEC)
Zurigo
Paesi di esecuzione
(Fonte di dati: WHO)
Argentina, Australia, Austria, Belgium, Brazil, Canada, Chile, China, Colombia, Czechia, Finland, France, Germany, Greece, India, Israel, Italy, Japan, Korea, Lebanon, Lithuania, Malaysia, Mexico, Netherlands, Oman, Portugal, Republic of, Russian Federation, Saudi Arabia, Singapore, Spain, Switzerland, Taiwan, Thailand, Turkey, United Kingdom, United States
Contatto per maggiori informazioni sulla sperimentazione
Dati della persona di contatto in Svizzera
(Fonte di dati: BASEC)
Patrick Grabher
+41 79 330 70 18
patrick.grabher@novartis.com
Contatto per informazioni generali
(Fonte di dati: WHO)
Novartis Pharmaceuticals
Novartis Pharmaceuticals
Contatto per informazioni scientifiche
(Fonte di dati: WHO)
Novartis Pharmaceuticals
Novartis Pharmaceuticals
Autorizzazione da parte della commissione d’etica (Fonte di dati: BASEC)
Nome della commissione d’etica che rilascia l’autorizzazione (nel caso di studi multicentrici solo la commissione direttiva)
Kantonale
Ethikkommission Zürich
Data di autorizzazione da parte della commissione d’etica
23.04.2020
Altri numeri di identificazione delle sperimentazioni
Numero di identificazione della sperimentazione della commissione d’etica (BASEC-ID)
(Fonte di dati: BASEC)
2020-00463
Secondary ID (Fonte di dati: WHO)
2019-002089-11
CMBG453B12301
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