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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00123474
Other study ID # CA180-034
Secondary ID
Status Completed
Phase Phase 3
First received July 21, 2005
Last updated July 29, 2015
Start date July 2005
Est. completion date July 2014

Study information

Verified date July 2015
Source Bristol-Myers Squibb
Contact n/a
Is FDA regulated No
Health authority United States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

This is a phase III study of BMS-354825 in subjects with chronic phase Philadelphia chromosome or BCR-ABL positive chronic myelogenous leukemia, who are resistant or intolerant to imatinib mesylate (Gleevec).


Recruitment information / eligibility

Status Completed
Enrollment 724
Est. completion date July 2014
Est. primary completion date September 2006
Accepts healthy volunteers No
Gender Both
Age group 18 Years to 90 Years
Eligibility For more information regarding BMS clinical trial participation, please visit www.BMSStudyConnect.com.

Inclusion Criteria:

- Subjects with Philadelphia chromosome positive (Ph+) (or BCR/ABL+) chronic phase chronic myeloid leukemia whose disease has primary or acquired hematologic resistance to imatinib mesylate or who are intolerant of imatinib mesylate.

- Men and women, 18 years or older

- Adequate hepatic function

- Adequate renal function

- Women of childbearing potential (WOCBP) must be using an adequate method of contraception to avoid pregnancy throughout the study and for a period of at least 1 month before and at least 3 months after the study in such a manner that the risk of pregnancy is minimized.

Exclusion Criteria:

- Women who are pregnant or breastfeeding

- Subjects who are eligible and willing to undergo transplantation during the screening period

- A serious uncontrolled medical disorder or active infection that would impair the ability of the subject to receive protocol therapy

- Uncontrolled or significant cardiovascular disease

- Medications that increase bleeding risk

- Medications that change heart rhythms

- Dementia or altered mental status that would prohibit the understanding or rendering of informed consent

- History of significant bleeding disorder unrelated to CML

- Concurrent incurable malignancy other than CML

- Evidence of organ dysfunction or digestive dysfunction that would prevent administration of study therapy

- Prisoners or subjects who are compulsorily detained (involuntarily incarcerated) for treatment of either a psychiatric or physical (e.g., infectious disease) illness must not be enrolled into this study

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
dasatinib
Tablets, Oral, 50 mg BID, indefinitely, survival study
dasatinib
Tablets, Oral, 70 mg BID, indefinitely, survival study
dasatinib
Tablets, Oral, 100 mg QD, indefinitely, survival study
dasatinib
Tablets, Oral, 140 mg QD, indefinitely, survival study

Locations

Country Name City State
Argentina Local Institution Buenos Aires
Argentina Local Institution Capital Federal
Argentina Local Institution Cordoba
Argentina Local Institution La Plata Buenos Aires
Australia Local Institution Adelaide South Australia
Australia Local Institution Camperdown New South Wales
Australia Local Institution East Melbourne Victoria
Australia Local Institution Perth Western Australia
Australia Local Institution South Brisbane Queensland
Australia Local Institution St Leonards New South Wales
Austria Local Institution Wien
Belgium Local Institution B-leuven
Belgium Local Institution Brugge
Belgium Local Institution Bruxelles
Belgium Local Institution Charleroi
Belgium Local Institution Edegem
Belgium Local Institution Yvoir
Brazil Local Institution CEP - Campinas
Brazil Local Institution Curitiba Parana
Brazil Local Institution Rio de Janeiro
Brazil Local Institution San Paulo, Sp
Brazil Local Institution Sao Paulo
Canada Local Institution Edmonton Alberta
Canada Local Institution Hamilton Ontario
Canada Local Institution Montreal Quebec
Czech Republic Local Institution Brno
Czech Republic Local Institution Prague 2
Denmark Local Institution Aarhus C
Denmark Local Institution Herlev
Denmark Local Institution Odense C
Finland Local Institution Helsinki
France Local Institution Caen
France Local Institution Cedex Pierre Benite
France Local Institution Creteil Cedex
France Local Institution Grenoble Cedex 09
France Local Institution Lille Cedex
France Local Institution Marseille Cedex 9
France Local Institution Nantes
France Local Institution Paris Cedex 10
France Local Institution Poitiers Cedex
France Local Institution Strasbourg
France Local Institution Toulouse Cedex 9
Germany Local Institution Dresden
Germany Local Institution Frankfurt/main
Germany Local Institution Hamburg
Germany Local Institution Leipzig
Germany Local Institution Mainz
Germany Local Institution Mannheim
Hungary Local Institution Budapest
Ireland Local Institution Co Galway Galway
Ireland Local Institution Dublin
Israel Local Institution Ramat-gan
Italy Local Institution Bari
Italy Local Institution Monza (mi)
Italy Local Institution Napoli
Italy Local Institution Orbassano
Italy Local Institution Roma
Italy Local Institution Roma
Korea, Republic of Local Institution Jeollanam-do
Korea, Republic of Local Institution Kyunggi-do
Korea, Republic of Local Institution Seoul
Korea, Republic of Local Institution Seoul
Mexico Local Institution Distrito Federal
Netherlands Local Institution Nijmegen
Netherlands Local Institution Rotterdam
Norway Local Institution Trondheim
Peru Local Institution Jesus Maria Lima
Peru Local Institution Lima
Philippines Local Institution Quezon City
Poland Local Institution Gdansk
Poland Local Institution Katowice
Poland Local Institution Krakow
Poland Local Institution Lodz
Poland Local Institution Lublin
Poland Local Institution Warsaw
Russian Federation Local Institution Moscow
Russian Federation Local Institution St.petersburg
Singapore Local Institution Singapore
South Africa Local Institution Bloemfontein Free State
South Africa Local Institution Groenkloof Gauteng
South Africa Local Institution Observatory Western Cape
South Africa Local Institution Parktown Gauteng
South Africa Local Institution Soweto Gauteng
Spain Local Institution Madrid
Spain Local Institution Madrid
Spain Local Institution Pamplona
Sweden Local Institution Lund
Sweden Local Institution Uppsala
Switzerland Local Institution Basel
Taiwan Local Institution Taipei
Taiwan Local Institution Taoyuan County
United Kingdom Local Institution Birmingham West Midlands
United Kingdom Local Institution Cambridge Cambridgeshire
United Kingdom Local Institution Glasgow
United Kingdom Local Institution Liverpool Merseyside
United Kingdom Local Institution London Greater London
United Kingdom Local Institution Newcastle Tyne And Wear
United States Central Hematology Oncology Medical Group Inc. Alhambra California
United States Pacific Cancer Medical Center Inc Anaheim California
United States Emory University School Of Medicine Atlanta Georgia
United States Georgia Cancer Specialists Atlanta Georgia
United States University Of Maryland Baltimore Maryland
United States University Of Alabama At Birmingham Birmingham Alabama
United States Dana Faber Cancer Institute Boston Massachusetts
United States University Of North Carolina At Chapel Hill Chapel Hill North Carolina
United States Northwestern University Feinberg School Of Medicine Chicago Illinois
United States University Of Chicago Chicago Illinois
United States Cleveland Clinic Foundation Cleveland Ohio
United States Ut Southwestern Medical Center Dallas Texas
United States Karmanos Cancer Institute Detroit Michigan
United States University Of Florida Gainesville Florida
United States The Cancer Center At Hackensack University Medical Center Hackensack New Jersey
United States The University Of Texas Md Anderson Cancer Center Houston Texas
United States Indiana University Cancer Center Indianapolis Indiana
United States Nevada Cancer Institute Las Vegas Nevada
United States Gwinnett Hospital System Inc. Lawrenceville Georgia
United States University Of Kentucky Lexington Kentucky
United States Loma Linda University Cancer Center Loma Linda California
United States Pacific Shores Medical Group Long Beach California
United States Ucla Dept. Of Medicine Los Angeles California
United States University Of Miami Miami Florida
United States Sarah Cannon Research Institute Nashville Tennessee
United States The Cancer Institute Of New Jersey New Brunswick New Jersey
United States New York Presbyterian Hospital New York New York
United States Devetten, Marcel Omaha Nebraska
United States Nebraska Methodist Hospital Omaha Nebraska
United States Md Anderson Cancer Center Orlando Orlando Florida
United States Ventura County Hematology-Oncology Specialists Oxnard California
United States Oncology Hematology Associates Of Central Illinois, Pc Peoria Illinois
United States Western Pennsylvania Cancer Institute Pittsburgh Pennsylvania
United States Oregon Health & Science University Portland Oregon
United States Washington University School Of Medicine Saint Louis Missouri
United States Seattle Cancer Care Alliance Seattle Washington
United States Kaiser Permanente Medical Center Vallejo California
United States Georgetown University Med Ctr Washington District of Columbia
United States Washington Cancer Institute At Washington Hospital Center Washington District of Columbia
United States University Of Kansas Medical Center Westwood Kansas

Sponsors (1)

Lead Sponsor Collaborator
Bristol-Myers Squibb

Countries where clinical trial is conducted

United States,  Argentina,  Australia,  Austria,  Belgium,  Brazil,  Canada,  Czech Republic,  Denmark,  Finland,  France,  Germany,  Hungary,  Ireland,  Israel,  Italy,  Korea, Republic of,  Mexico,  Netherlands,  Norway,  Peru,  Philippines,  Poland,  Russian Federation,  Singapore,  South Africa,  Spain,  Sweden,  Switzerland,  Taiwan,  United Kingdom, 

References & Publications (3)

Müller MC, Cortes JE, Kim DW, Druker BJ, Erben P, Pasquini R, Branford S, Hughes TP, Radich JP, Ploughman L, Mukhopadhyay J, Hochhaus A. Dasatinib treatment of chronic-phase chronic myeloid leukemia: analysis of responses according to preexisting BCR-ABL mutations. Blood. 2009 Dec 3;114(24):4944-53. doi: 10.1182/blood-2009-04-214221. Epub 2009 Sep 24. — View Citation

Porkka K, Khoury HJ, Paquette RL, Matloub Y, Sinha R, Cortes JE. Dasatinib 100 mg once daily minimizes the occurrence of pleural effusion in patients with chronic myeloid leukemia in chronic phase and efficacy is unaffected in patients who develop pleural effusion. Cancer. 2010 Jan 15;116(2):377-86. doi: 10.1002/cncr.24734. — View Citation

Shah NP, Kantarjian HM, Kim DW, Réa D, Dorlhiac-Llacer PE, Milone JH, Vela-Ojeda J, Silver RT, Khoury HJ, Charbonnier A, Khoroshko N, Paquette RL, Deininger M, Collins RH, Otero I, Hughes T, Bleickardt E, Strauss L, Francis S, Hochhaus A. Intermittent target inhibition with dasatinib 100 mg once daily preserves efficacy and improves tolerability in imatinib-resistant and -intolerant chronic-phase chronic myeloid leukemia. J Clin Oncol. 2008 Jul 1;26(19):3204-12. doi: 10.1200/JCO.2007.14.9260. Epub 2008 Jun 9. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Percent of Participants With Major Cytogenetic Response (MCyR) After at Least 6 Months Follow-Up Cytogenetic response (CyR) was based on the number of Philadelphia chromosome positive (Ph+) metaphases among cells in metaphase on a Bone Marrow (BM) sample. The criteria for CyR were as follows: Complete cytogenetic response (CCyR): 0% Ph+ cells in metaphase in BM; Partial cytogenetic response (PCyR): >0 to 35% Ph+ cells in metaphase in BM; Minor cytogenetic response: >35 to 65% Ph+ cells in metaphase in BM; Minimal cytogenetic response: >65 to 95% Ph+ cells in metaphase in BM; No cytogenetic response: >95 to 100% Ph+ cells in metaphase in BM; Best CyR was defined as the best response obtained at any time during the study; MCyR was defined as a best CyR of complete cytogenetic response (CCyR) or partial cytogenetic response (PCyR). Baseline=closest to, but no later than, the first day of study drug for treated participants and closest to, but no later than, the date of randomization, for those who were randomized but who never received treatment, unless otherwise specified. Baseline and after at least 6 months follow-up No
Secondary Percent of Participants With MCyR At or Prior to 24 Months Follow-Up CyR was based on the number of Ph+ metaphases among cells in metaphase on a Bone Marrow (BM) sample. The criteria for CyR were as follows: CCyR: 0% Ph+ cells in metaphase in BM; PCyR: >0 to 35% Ph+ cells in metaphase in BM; Minor cytogenetic response: >35 to 65% Ph+ cells in metaphase in BM; Minimal cytogenetic response: >65 to 95% Ph+ cells in metaphase in BM; No cytogenetic response: >95 to 100% Ph+ cells in metaphase in BM; Best CyR was defined as the best response obtained at any time during the study; MCyR was defined as a best CyR of CCyR or PCyR. Baseline=closest to, but no later than, the first day of study drug for treated participants and closest to, but no later than, the date of randomization, for those who were randomized but who never received treatment, unless otherwise specified. Baseline and after at least 24 months follow-up No
Secondary Percent of Participants With Complete Hematologic Response (CHR) After at Least 6 and 24 Months Follow-Up A complete hematologic response (CHR) was obtained when all the following criteria were met: White Blood Cells (WBC) = institutional upper limit of normal (ULN); Platelets < 450,000/mm³; No blasts or promyelocytes in peripheral blood (PB); < 5% myelocytes plus metamyelocytes in PB; Basophils in PB < 20%; No extramedullary involvement (including no splenomegaly or hepatomegaly). Hematologic responses were counted anytime following 14 days after the dosing start date. Baseline and after at least 6 and 24 months follow-up No
Secondary Time to MCyR in Participants With MCyR After At Least 6 Months Follow-Up Time to MCyR was defined as the time from the first dosing date until criteria were first met for CCyR or PCyR, whichever occurred first. Non-responders were censored at the maximum time of all participants in their respective group (ie, maximum between time to MCyR response for responders and time to last cytogenetic assessment for non-responders). Baseline and after at least 6 months follow-up No
Secondary Time to CHR in Participants With CHR After at Least 6 Months Follow-Up Time to CHR was defined as the time from the first dosing date until criteria are first met for the response. Non-responders were censored at the maximum time of all participants in their respective group (ie, maximum between time to CHR response for responders and time to last hematologic assessment for non-responders). Baseline and after at least 6 months follow-up No
Secondary Time to MCyR in Participants With MCyR After at Least 24 Months Follow-Up Time to MCyR was defined as the time from the first dosing date until criteria were first met for CCyR or PCyR, whichever occurred first. Non-responders were censored at the maximum time of all participants in their respective group (ie, maximum between time to MCyR response for responders and time to last cytogenetic assessment for non-responders). Cytogenetic assessments were not done after the 2 Year Follow-up. Baseline and after at least 24 months follow-up No
Secondary Time to CHR in Participants With CHR After at Least 24 Months Follow-Up Time to CHR was defined as the time from the first dosing date until criteria are first met for the response. Non-responders were censored at the maximum time of all participants in their respective group (ie, maximum between time to CHR response for responders and time to last hematologic assessment for non-responders). Cytogenetic assessments were not done after the 2 Year Follow-up. Baseline and after at least 24 months follow-up No
Secondary Number of Participants With MCyR Whose Disease Progressed Progression in a participant=participant achieved a CHR and no longer met the criteria consistently over consecutive 2-weeks after starting their maximum dose; had no CHR after receiving their maximum dose and had an increase in white blood count (WBC) defined as a doubling of the count from the lowest value to >20,000/mm^3 or an increase by > 50,000/mm^3 on two assessments performed at least 2 weeks apart; participant met criteria of accelerated or blast phase CML at any time; had a MCyR and subsequently no longer met the criteria for MCyR after starting their maximum dose; had a = 30% absolute increase in the number of Ph+ metaphases. Although a related secondary endpoint was estimated duration of MCyR, medium duration of MCyR could not be estimated because the majority of participants with MCyR continued to respond, or could not be reliably estimated because of the large number of censored participants. Cytogenetic assessments were not done after the 24 month follow-up. Baseline and after at least 24 months follow-up No
Secondary Number of Participants With CHR Whose Disease Progressed Progression in a participant=achieved a CHR and subsequently no longer met the criteria consistently over a consecutive 2-week period after starting their maximum dose; had no CHR after receiving their maximum dose and had an increase in white blood count (WBC) defined as a doubling of the count from the lowest value to >20,000/mm^3 or an increase by > 50,000/mm^3 on two assessments performed at least 2 weeks apart; met the criteria of accelerated or blast phase CML at any time; had a MCyR and subsequently no longer met the criteria for MCyR after starting their maximum dose; had a = 30% absolute increase in the number of Ph+ metaphases. Although a related secondary endpoint was estimated duration of CHR, medium duration of CHR could not be estimated because the majority of participants with CHR continued to respond, or could not be reliably estimated because of the large number of censored participants. Baseline and after at least 24 months follow-up No
Secondary Number of Participants With MCyR and Baseline BCR-ABL Gene Mutation - All Treated Participants BCR-ABL mutations were assessed in participants prior to the start of study drug (baseline) and at the time of disease progression or at end of therapy. Quantification of BCR-ABL transcripts in peripheral blood was evaluated using quantitative reverse transcriptase polymerase chain reaction (Q-RT-PCR, RT-PCR). Baseline to Year 2 No
Secondary Percent of Imatinib-Resistant Participants With Progression Free Survival (PFS) After at Least 24, 36, 48, 60, 72, and 84 Months Follow-Up PFS= time from randomization until: CHR achieved and participant subsequently no longer met criteria for CHR over 2 weeks; no CHR after receiving maximum dose and an increase in WBC (ie, doubling of the count from the lowest value to > 20,000/mm^3 or an increase by > 50,000/mm^3 on 2 assessments performed 2 weeks apart); participant met criteria of accelerated phase or blast phase CML; participant had MCyR and subsequently no longer met criteria for MCyR after starting maximum dose; participant had a = 30% absolute increase in number of Ph+ metaphases. Deaths without a reported prior progression were considered to have progressed on the date of death; those who neither progressed nor died were censored on the date of their last cytogenetic or hematologic assessment. When first progression reported during follow-up, it was censored at last on-study assessment. If the first progression reported during follow-up was death, participant considered to have progressed at date of death. Baseline and after 84 months follow-up No
Secondary Percent of Imatinib-Resistant Participants With Overall Survival (OS) After at Least 24, 36, 48, 60, 72, and 84 Months Follow-Up Overall survival (OS) was defined as the time from randomization until death. Survival data were collected for up to 5 years on participants who had discontinued dasatinib treatment. Participants who did not die or who were lost to follow-up were censored on the last date the participant was known to be alive. Baseline and after 84 months follow-up No
Secondary Percent of Participants Intolerant to Imatinib With MCyR After at Least 6 Months and After at Least 24 Months Follow-Up, by QD and BID Schedules and by Total Daily Dose CyR was based on the number of Ph+ metaphases among cells in metaphase on a BM sample. The criteria for CyR were as follows: complete cytogenetic response (CCyR): 0% Ph+ cells in metaphase in BM; PCyR: >0 to 35% Ph+ cells in metaphase in BM; Minor cytogenetic response: >35 to 65% Ph+ cells in metaphase in BM; Minimal cytogenetic response: >65 to 95% Ph+ cells in metaphase in BM; No cytogenetic response: >95 to 100% Ph+ cells in metaphase in BM; Best CyR was defined as the best response obtained at any time during the study; MCyR was defined as a best CyR of CCyR or PCyR. Baseline and after at Least 6 Months and 24 Months Follow-Up No
Secondary Percent of Participants Intolerant to Imatinib With CHR After at Least 6 Months and After at Least 24 Months Follow-Up A CHR was obtained when all the following criteria were met: White Blood Cells (WBC) = institutional upper limit of normal (ULN); Platelets < 450,000/mm³; No blasts or promyelocytes in peripheral blood (PB); < 5% myelocytes plus metamyelocytes in PB; Basophils in PB < 20%; No extramedullary involvement (including no splenomegaly or hepatomegaly). Hematologic responses were counted anytime following 14 days after the dosing start date. Baseline and after at Least 6 Months and 24 Months Follow Up No
Secondary Percent of Imatinib Intolerant Participants With Progression Free Survival After 24, 36, 48, 60, 72, and 84 Months of Follow-Up PFS= time from randomization until: CHR achieved and participant subsequently no longer met criteria for CHR over 2 weeks; no CHR after receiving maximum dose and an increase in WBC (ie, doubling of the count from the lowest value to > 20,000/mm^3 or an increase by > 50,000/mm^3 on 2 assessments performed 2 weeks apart); participant met criteria of accelerated phase or blast phase CML; participant had MCyR and subsequently no longer met criteria for MCyR after starting maximum dose; participant had a = 30% absolute increase in number of Ph+ metaphases. Deaths without a reported prior progression were considered to have progressed on the date of death; those who neither progressed nor died were censored on the date of their last cytogenetic or hematologic assessment. When first progression reported during follow-up, it was censored at last on-study assessment. If the first progression reported during follow-up was death, participant considered to have progressed at date of death. Baseline and after 84 months follow-up No
Secondary Percent of Imatinib Intolerant Participants With Overall Survival After 24, 36, 48, 60, 72, and 84 Months of Follow-up Overall survival (OS) was defined as the time from randomization until death. Survival data were collected for up to 5 years on participants who had discontinued dasatinib treatment. Participants who did not die or who were lost to follow-up were censored on the last date the participant was known to be alive. Baseline and after 84 months follow-up No
Secondary Percent of All Randomized Participants With Cytogenic and Hematologic Response by Dosing Schedule (QD or BID) and by Total Daily Dose (100 mg or 140 mg) After at Least 6 Months Follow-Up Complete cytogenetic response (CCyR): 0% Ph+ cells in metaphase in BM. Partial cytogenetic response (PCyR): >0 to 35% Ph+ cells in metaphase in BM. MCyR: best cytogenetic response of CCyR or PCyR. A complete hematologic response (CHR) was obtained when all the following criteria were met: White Blood Cells (WBC) = institutional upper limit of normal (ULN); Platelets < 450,000/mm³; No blasts or promyelocytes in peripheral blood (PB); < 5% myelocytes plus metamyelocytes in PB; Basophils in PB < 20%; No extramedullary involvement (including no splenomegaly or hepatomegaly). Hematologic responses were counted anytime following 14 days after the dosing start date. Baseline and after at least 6 months follow-up No
Secondary Percent of All Randomized Participants With Cytogenic and Hematologic Response by Dosing Schedule (QD or BID) and by Total Daily Dose (100 mg or 140 mg) After at Least 24 Months Follow-Up Complete cytogenetic response (CCyR): 0% Ph+ cells in metaphase in BM. Partial cytogenetic response (PCyR): >0 to 35% Ph+ cells in metaphase in BM. MCyR: best cytogenetic response of CCyR or PCyR. A complete hematologic response (CHR) was obtained when all the following criteria were met: White Blood Cells (WBC) = institutional upper limit of normal (ULN); Platelets < 450,000/mm³; No blasts or promyelocytes in peripheral blood (PB); < 5% myelocytes plus metamyelocytes in PB; Basophils in PB < 20%; No extramedullary involvement (including no splenomegaly or hepatomegaly). Hematologic responses were counted anytime following 14 days after the dosing start date. No cytogenic assessments were made after 2 years of follow-up. Baseline and after at least 24 months follow-up No
Secondary Percent of Participants With Progression Free Survival (PFS) at 24, 36, 48, 60, 72, and 84 Months Follow-Up by Dose Schedule and Total Daily Dose - All Randomized Participants PFS= time from randomization until: CHR achieved and participant subsequently no longer met criteria for CHR over 2 weeks; no CHR after receiving maximum dose and an increase in WBC (ie, doubling of the count from the lowest value to > 20,000/mm^3 or an increase by > 50,000/mm^3 on 2 assessments performed 2 weeks apart); participant met criteria of accelerated phase or blast phase CML; participant had MCyR and subsequently no longer met criteria for MCyR after starting maximum dose; participant had a = 30% absolute increase in number of Ph+ metaphases. Deaths without a reported prior progression were considered to have progressed on the date of death; those who neither progressed nor died were censored on the date of their last cytogenetic or hematologic assessment. When first progression reported during follow-up, it was censored at last on-study assessment. If the first progression reported during follow-up was death, participant considered to have progressed at date of death. Baseline and after 84 Months Follow-up No
Secondary Percent of Participants Overall Survival at 24, 36, 48, 60, 72, and 84 Months Follow-Up - All Randomized Participants Overall survival (OS) was defined as the time from randomization until death. Survival data were collected for up to 5 years on participants who had discontinued dasatinib treatment. Participants who did not die or who were lost to follow-up were censored on the last date the participant was known to be alive. Baseline up to 84 Months Follow-up No
Secondary Baseline and After 2 Years Follow-Up: Number of Participants With Death, Serious Adverse Events (SAEs), Adverse Events (AEs) That Led to Treatment Discontinuation AE=any new unfavorable symptom, sign, or disease or worsening of a preexisting condition that may not have a causal relationship with treatment. SAE=a medical event that at any dose results in death, persistent or significant disability/incapacity, or drug dependency/abuse; is life-threatening, an important medical event, or a congenital anomaly/birth defect; or requires or prolongs hospitalization. Treatment-related=having certain, probable, possible, or missing relationship to study drug. Baseline=closest to, but no later than, the first day of study drug for treated participants. Baseline and after 2 Years Follow-Up Yes
Secondary Baseline and After 7 Years Follow-Up and Study Closure: Number of Participants With Death, Serious Adverse Events (SAEs), Adverse Events (AEs) That Led toTreatment Discontinuation AE=any new unfavorable symptom, sign, or disease or worsening of a preexisting condition that may not have a causal relationship with treatment. SAE=a medical event that at any dose results in death, persistent or significant disability/incapacity, or drug dependency/abuse; is life-threatening, an important medical event, or a congenital anomaly/birth defect; or requires or prolongs hospitalization. Treatment-related=having certain, probable, possible, or missing relationship to study drug. Baseline=closest to, but no later than, the first day of study drug for treated participants. After the 2-year analysis and Protocol Amendment 02, those on a BID dosing schedule were allowed to switch to a QD dosing schedule. Due to the large number of participants switching from BID dosing to QD dosing, the abbreviated dosing data collection method incorporated in Amendment 03, the overall safety data are presented for the 100 mg QD group and combined for the other treatment groups. Baseline to 30 days post last dose;7 years follow up; study closure July 2014 Yes
See also
  Status Clinical Trial Phase
Completed NCT02348957 - Treating Patients With Chronic Myeloid Leukemia (CML) in Chronic Phase (CP) With Dasatinib
Terminated NCT00114959 - Homoharringtonine With Oral Gleevec in Chronic, Accelerated and Blast Phase Chronic Myeloid Leukemia (CML) Phase 2
Completed NCT00510926 - Exploratory Study of IMATINIB High Dose in Intermediate Risk Chronic Myeloid Leukemia in Chronic Phase Phase 2
Withdrawn NCT00324077 - Phase I Study of Dasatinib (BMS-354825) and Imatinib in Subjects With Chronic Myeloid Leukemia in Chronic Phase Phase 1