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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01903733
Other study ID # B1871040
Secondary ID 2013-000691-15
Status Completed
Phase N/A
First received
Last updated
Start date August 28, 2013
Est. completion date June 5, 2020

Study information

Verified date June 2022
Source Pfizer
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The objective of the study is to provide long term access to bosutinib treatment and assess long term safety, tolerability and duration of clinical benefit, without any formal hypothesis testing; therefore, there is no formal primary endpoint.


Recruitment information / eligibility

Status Completed
Enrollment 281
Est. completion date June 5, 2020
Est. primary completion date June 5, 2020
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: - Only subjects previously participating in two specific studies are eligible to enroll into this study. Enrollment is not open to subjects if not previously enrolled in studies B1871006 or B1871008. Exclusion Criteria: - All subjects are excluded unless previously participating in studies B1871006 or B1871008.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
bosutinib
The starting bosutinib dose is 500 mg once daily, however the dose can vary from 300 mg to 600 mg.

Locations

Country Name City State
Argentina Instituto Medico Especializado Alexander Fleming Cd. Autonoma De Buenos Aires Buenos Aires
Argentina Hospital Dr. Jose Ramon Vidal Corrientes
Argentina Hospital Italiano de la Plata La Plata Buenos Aires
Australia Royal Adelaide Hospital Adelaide South Australia
Australia Royal Brisbane & Women's Hospital Herston Queensland
Belgium GHDC (Grand Hopital de Charleroi) Charleroi
Brazil Universidade Estadual de Campinas / Centro de Hematologia e Hemoterapia Campinas SP
Brazil Faculdade de Medicina do ABC - Centro de Estudos e Pesquisa em Hematologia e Oncologia (CEPHO) Santo Andre SP
Canada Alberta Health Services - Department of Medical Oncology - Cross Cancer Institute Edmonton Alberta
Canada Sir Mortimer B. Davis-Jewish General Hospital Montreal Quebec
Canada Princess Margaret Cancer Centre Toronto Ontario
Canada Vancouver General Hospital Vancouver British Columbia
Chile Instituto Oncologico Renaca V Region
Chile Instituto Oncologico, Clinica Renaca Renaca V Region
China Chinese People's Liberation Army General Hospital Beijing
China Peking Union Medical College Hospital Beijing Beijing
China The First affiliated Hospital of College of Medicine, Zhejiang University Hangzhou Zhejiang
China Ruijin Hospital- Shanghai Jiaotong University School of Medicine Shanghai
China Blood Disease Hospital, Chinese Academy of Medical Science & Peking Union Medical College Tianjin
Colombia Fundacion Santa Fe de Bogota Bogota Cundinamarca
Finland Helsingin Yliopistollinen Keskussairaala, Hematologian poliklinikka Helsinki
France CHU de CAEN Caen Cedex 9
France CHU Hotel Dieu - Service Hematologie Nantes cedex 1
France CHU Poitiers Poitiers
France CHU de Poitiers Poitiers Cedex
France Strasbourg Oncologie Liberale -Centre de Radiotherapie, Clinique Ste Anne Strasbourg
Hong Kong Pamela Youde Nethersole Eastern Hospital Chai Wan
Hong Kong Department of Medicine & Therapeutics, Prince of Wales Hospital Shatin, New Territories
Hungary Egyesitett Szent Istvan es Szent Laszlo Korhaz-Rendelointezet Budapest
Hungary Somogy Megyei Kaposi Mor Oktato Korhaz, Belgyogyaszati Osztaly Kaposvar
India Christian Medical College. Vellore Vellore Tamil NADU
Italy A.O.U. Policlinico S.Orsola Malpighi Bologna BO
Italy ASST Monza - Ospedale san Gerardo Monza Monza AND Brianza
Italy A.O.U. San Luigi Gonzaga di Orbassano Orbassano TO
Italy Ospedale S. Eugenio - UOC Ematologia Roma
Japan Akita University Hospital Akita City Akita
Japan National Hospital Organization Kyushu Cancer Center Fukuoka-shi Fukuoka
Japan Hamamatsu University School of Medicine University Hospital Hamamatsu-shi Shizuoka
Japan Kanazawa University Hospital Kanazawa-shi Ishikawa
Japan Kindai University Hospital Osakasayama-city Osaka
Japan Osaka University Hospital Suita-city Osaka
Japan Tokyo Metropolitan Cancer and Infectious diseases Center Komagome Hospital Tokyo
Japan Toyohashi Municipal Hospital Toyohashi Aichi
Korea, Republic of The Catholic University of Korea, Seoul St. Mary's Hospital Seoul
Latvia Riga East Clinical University Hospital Riga
Netherlands VU University Medical Center Amsterdam
Netherlands University Medical Center Groningen, Department of Hematology Groningen
Peru Unidad de Investigacion de Hematologia - Hospital Nacional Edgardo Rebagliati Martins Lima
Poland Uniwersyteckie Centrum Kliniczne Gdansk
Poland Uniwersyteckie Centrum Kliniczne Gdansk
Poland SP ZOZ Szpital Uniwersytecki w Krakowie Krakow
Poland Samodzielny Publiczny Szpital Kliniczny nr 1 w Lublinie Lublin
Russian Federation State Budgetary Institution of Healthcare of Sverdlovsk Region Ekaterinburg Sverdlovsk Region
Russian Federation Federal State-Funded Institution National Research Center of Hematology of the Ministry of Moscow
Russian Federation State Budgetary Educational Institution of Higher Professional Education Rostov-on-Don
Russian Federation State Budgetary Institution of Rostov Region - Rostov Regional Clinical Hospital Rostov-on-Don
Russian Federation Clinic "Institute of Pediatric Oncology, Hematology and Transplantation n.a. R.M. Gorbachova" Saint Petersburg
Russian Federation Federal State Budgetary Institution "Federal Almazov Medical Research Centre" Saint Petersburg
Russian Federation State Budgetary Institution of Healthcare - Leningrad Regional Clinical Hospital Saint Petersburg
Russian Federation State Budgetary Institution of Healthcare Samara Regional Clinical Hospital n.a. V.D. Seredavin Samara
Singapore Singapore General Hospital Singapore
South Africa Wits Clinical Research-Chris Hani Baragwanath Hospital Soweto Gauteng
Spain Hospital Clinic Barcelona Barcelona
Spain Hospital Universitario La Paz Madrid
Spain Hospital Universitario La Princesa Madrid
Spain Hospital Universitario Madrid Sanchinarro, Centro Integral Oncologico Clara Campal Madrid
Spain Hospital Virgen de la Salud Toledo
Spain Hospital Clinico Universitario De Valencia (CHUV) Valencia
Thailand Division of Hematology, Department of Medicine, Faculty of Medicine, Siriraj Hospital, Bangkok
Turkey Hacettepe Universitesi Tip Fakultesi Ankara
Turkey Gaziantep Universitesi Tip Fakultesi Sahinbey Uygulama ve Arastirma Hastanesi Gaziantep Sehit Kamil
Ukraine Municipal Institution "Cherkasy Regional Oncology Dispensary" Cherkasy
Ukraine MI "Dnipropetrovsk City Multi-field Clinical Hospital #4" of DRC Hematology Center Dnipropetrovsk
Ukraine Kyiv City Clinical Hospital #9, SI "Institute of Hematology and Transfusiology of NAMS of Ukraine" Kyiv
Ukraine State Institution "National Research Center for Radiation Medicine of the National Academy of Kyiv
Ukraine State Institution "Institute of Blood Pathology and Transfusion Medicine of Lviv
United Kingdom Freeman Hospital Newcastle Upon Tyne
United Kingdom Nottingham University Hospitals NHS Trust Nottinhgam
United States Emory University Hospital Atlanta Georgia
United States Northside Hospital Inc., - GCS/Northside Atlanta Georgia
United States Northside Hospital, Inc. - Central Research Department Atlanta Georgia
United States The Emory Clinic Atlanta Georgia
United States Winship Cancer Institute, Emory University Atlanta Georgia
United States Rcca Md,Llc Bethesda Maryland
United States Hudson Valley Hematology and Oncology Associates Hawthorne New York
United States Penn State Milton S. Hershey Medical Center Hershey Pennsylvania
United States The University of Texas MD Anderson Cancer Center Houston Texas
United States The University of Texas, MD Anderson Cancer Center Houston Texas
United States Indiana Blood and Marrow Transplantation Indianapolis Indiana
United States Orlando Health, Inc Orlando Florida
United States Siouxland Hematology-Oncology Associates, LLP Sioux City Iowa

Sponsors (1)

Lead Sponsor Collaborator
Pfizer

Countries where clinical trial is conducted

United States,  Argentina,  Australia,  Belgium,  Brazil,  Canada,  Chile,  China,  Colombia,  Finland,  France,  Hong Kong,  Hungary,  India,  Italy,  Japan,  Korea, Republic of,  Latvia,  Netherlands,  Peru,  Poland,  Russian Federation,  Singapore,  South Africa,  Spain,  Thailand,  Turkey,  Ukraine,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Number of Participants With Treatment-Emergent Adverse Events (AEs) and Serious Adverse Events (SAEs) Based on National Cancer Institute Common Terminology Criteria for AEs (NCI CTCAE) (Version 3.0) An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. SAE was any untoward medical occurrence at any dose that: resulted in death, was life threatening (immediate risk of death), required inpatient hospitalization or prolongation of existing hospitalization, resulted in persistent or significant disability/incapacity (substantial disruption of the ability to conduct normal life functions), resulted in congenital anomaly/birth defect. Treatment-emergent adverse events were defined as any event increasing in severity from baseline or any new event started during bosutinib therapy or within 30 days of the last dose of study drug. From first dose of drug up to 30 days after last dose (up to approximately 14 years)
Primary Number of Participants With Grade 3 or 4 Treatment-Emergent Adverse Events (AEs) Based on National Cancer Institute Common Terminology Criteria for AEs (NCI CTCAE) (Version 3.0) An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. AEs were assessed according to severity grading based on NCI CTCAE version 3.0. Grade 1 =mild; Grade 2 =moderate; Grade 3 =severe or medically significant but not immediately life-threatening, hospitalization or prolongation of hospitalization indicated; Grade 4 =life-threatening or disabling, urgent intervention indicated; Grade 5 =death. Treatment-emergent adverse events were defined as any event increasing in severity from baseline or any new event started during bosutinib therapy or within 30 days of the last dose of study drug. From first dose of drug up to 30 days after last dose (up to approximately 14 years)
Primary Number of Participants With Treatment-Emergent Treatment Related Adverse Events (AEs) Based on National Cancer Institute Common Terminology Criteria for AEs (NCI CTCAE) (Version 3.0) An AE was any untoward medical occurrence in a participant who received study drug. Treatment-emergent adverse events were defined as any event increasing in severity from baseline or any new event started during bosutinib therapy or within 30 days of the last dose of study drug. Related TEAEs were those AEs who were related to the study treatment as judged by the investigator. From first dose of drug up to 30 days after last dose (up to approximately 14 years)
Primary Number of Participants With Laboratory Test Abnormalities Based on National Cancer Institute Common Terminology Criteria for AEs (NCI CTCAE) (Version 4.03) Laboratory parameters included Chemistry: high alkaline phosphatase; high alanine aminotransferase; high aspartate aminotransferase; high blood bilirubin; high creatinine. Hematology: absolute neutrophils count decreased; anemia; platelet count decreased; white blood cells (WBC) decreased. Abnormalities in laboratory tests were graded per NCI CTCAE version 4.03 as Grade 1= mild; Grade 2= moderate; Grade 3= severe and Grade 4= life-threatening or disabling. From first dose of drug up to 30 days after last dose (up to approximately 14 years)
Primary Number of Participants With Adverse Events as Reason for Treatment Discontinuation An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. From first dose of drug up to 30 days after last dose (up to approximately 14 years)
Primary Number of Participants With Diarrhea After Switch From Bosutinib Clinical Formulation to Bosutinib Commercial Formulation The incidence of diarrhea was collected and analyzed before and after the switch from the clinical formulation of bosutinib to the commercial formulation of bosutinib. Last 6 months on clinical formulation and first 6 months on commercial formulation
Primary Number of Participants With Breakpoint Cluster Region Abelson Protooncogene (BCR-ABL) Mutations Present at Time of Bosutinib Treatment Discontinuation BCR-ABL is a gene resulting from the 9:22 chromosomal translocation (Philadelphia chromosome). In this outcome measure, the number of participants who had emergent mutation or new BCR-ABL mutations (participants who had a post-baseline mutation which was not present at baseline) were reported. Post-baseline on Day 1 (maximum up to 14 years)
Primary Overall Survival (OS) Rate at Year 10 OS was defined as the time from randomization (B1871008) and time from first dose (B1871006) to the occurrence of death due to any cause or censoring. Kaplan-Meier analysis was used for determination of OS. Percentage of participants who were alive were estimated in this outcome measure. Year 10
Primary Plasma Steady-State Trough Concentrations (Ctrough) of Bosutinib Ctrough refers to plasma concentration of bosutinib observed just before treatment administration. One pre-dose sample was collected at the first scheduled visit (after approval and implementation of protocol amendment 1) following at least 2 weeks of uninterrupted dosing at the same dose level
Primary Kaplan-Meier Estimate of Probability of Maintaining Major Cytogenetic Response (MCyR) at Year 10: B1871006 Participants Cytogenetic response (CyR) is based on prevalence of Ph+ cells. Duration for MCyR: time from first response to confirmed loss, progression of disease, or on-treatment death due to any cause, or censoring analyzed for responders only. Confirmed loss was defined as 2 consecutive non-responses at least 28 days apart. MCyR was categorized as either complete cytogenetic response (CCyR) or partial cytogenetic response (PCyR). Response was achieved when there was 0% (CCyR) or 1-35% (PCyR) Ph+ cells analyzed from conventional cytogenetics based on the analysis of 20 to 100 metaphases or <1% (CCyR) or 1-35% (PCyR) Ph+ cells analyzed from fluorescence in-situ hybridization (FISH) based on analysis of at least 200 nuclei. CCyR may be imputed on a specific date if an MMR or better is achieved and denoted on the CRF on that date for B1871040 study visits. The Kaplan-Meier analysis was used to analyze percentage of participants maintaining MCyR at Year 10. Year 10
Primary Kaplan-Meier Estimate of Probability of Maintaining Complete Cytogenetic Response (CCyR) at Year 10: B1871006 Participants Duration for CCyR was defined as time from first response to confirmed loss, progression of disease, or on-treatment death due to any cause, or censoring analyzed for responders only. Confirmed loss was defined as 2 consecutive assessments with >0 Ph+ metaphases or >=1% positive cells from FISH at least 28 days apart or progression or death. CCyR was achieved when there was 0% Ph+ cells analysed from conventional cytogenetics with 20 to 100 metaphases or <1% Ph+ cells analysed from FISH with at least 200 nuclei. CCyR may be imputed on a specific date if MMR or better is achieved and denoted on the CRF on that date for B1871040 study visits. The Kaplan-Meier analysis was used to analyze percentage of participants maintaining CCyR at Year 10. Year 10
Primary Kaplan-Meier Estimate of Probability of Maintaining Complete Hematologic Response (CHR) at Year 10: B1871006 Participants Duration for CHR was defined as time from first response to confirmed loss, progression of disease, or on-treatment death due to any cause, or censoring analyzed for responders only. Confirmed loss was defined as 2 consecutive non-responses at least 14 days apart. Complete hematologic response was considered when participants met all of the following criteria: White blood cells equal to or less than (<=) institutional upper limit of normal (ULN), no blasts or promyelocytes in blood, <20% basophils in blood, no extramedullary involvement (including hepatomegaly or splenomegaly), myelocytes and metamyelocytes <5% in blood, platelets <450*10^9 per liter (/L). The following were applicable only to advanced phase: <=5% bone marrow blasts, absolute neutrophil count >=1.0*10^9/L, platelets >=100*10^9/L. The Kaplan-Meier analysis was used to analyze percentage of participants maintaining CHR at Year 10. Year 10
Primary Cumulative Incidence of Progression/Death Events at Year 10: B1871006 Participants Progression free survival (PFS):interval from date of first dose of bosutinib in parent study until earlier date of progression or death from any cause. Participants without events censored at last evaluation date. PD:evolution from CP (or return to CP for ADV participants) to AP or BP (on 2 consecutive assessments at least 1 week apart), evolution from AP to BP (on 2 consecutive assessments at least 1 week apart) and one of following conditions occurred after dose escalation or presence of AEs prohibiting dose escalation: for 2nd or later line, loss of MCyR (need at least 30% increase); for all lines of treatment, loss of CHR confirmed by 2 assessments >=2 weeks apart; for all lines of treatment, increasing WBC defined as doubling of WBC over a period of >=1 month with second WBC >20*10^9/L confirmed at least 1 week later. Percentage of participants with PFS/death events based on cumulative incidence method adjusting for competing event of treatment discontinuation without event. Year 10
Primary Cumulative Incidence of Rate of Transformation to Accelerated Phase (AP) or Blast Phase (BP) at Year 10: B1871006 Participants Time to transformation was defined as the time from first dose in the parent study to the first date of confirmed transformation to AP or BP. Confirmed transformation was defined as 2 consecutive assessments at least 1 week apart or 1 assessment confirmed by progression of disease or death. For participants without transformation, censorship was at the last evaluation date. Percentage of participants with time to transformation to AP/BP was reported based on cumulative incidence method adjusting for the competing risk of treatment discontinuation without the event. Year 10
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