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Note: This record shows only 22 elements of the WHO Trial Registration Data Set. To view changes that have been made to the source record, or for additional information about this trial, click on the URL below to go to the source record in the primary register. |
Register:
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EUCTR |
Last refreshed on:
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19 March 2012 |
Main ID: |
EUCTR2006-000006-23-HU |
Date of registration:
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20/09/2006 |
Prospective Registration:
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Yes |
Primary sponsor: |
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Public title:
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A Multicenter, Randomized, Double-Blind, Active-Controlled, Phase 3 Trial to Evaluate
the Efficacy and Safety of Saxagliptin in Combination with Metformin IR as Initial Therapy Compared to Saxagliptin Monotherapy and to Metformin IR Monotherapy in
Subjects with Type 2 Diabetes Who Have Inadequate Glycemic Control.
Pharmacogenetics Blood Sample Amendment Number 01 - Site Specific
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Scientific title:
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A Multicenter, Randomized, Double-Blind, Active-Controlled, Phase 3 Trial to Evaluate
the Efficacy and Safety of Saxagliptin in Combination with Metformin IR as Initial Therapy Compared to Saxagliptin Monotherapy and to Metformin IR Monotherapy in
Subjects with Type 2 Diabetes Who Have Inadequate Glycemic Control.
Pharmacogenetics Blood Sample Amendment Number 01 - Site Specific |
Date of first enrolment:
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12/02/2007 |
Target sample size:
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2940 |
Recruitment status: |
Not Recruiting |
URL:
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https://www.clinicaltrialsregister.eu/ctr-search/search?query=eudract_number:2006-000006-23 |
Study type:
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Interventional clinical trial of medicinal product |
Study design:
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Controlled: yes
Randomised: yes
Open: no
Single blind: no
Double blind: yes
Parallel group: yes
Cross over: no
Other: no
If controlled, specify comparator, Other Medicinial Product: yes
Placebo: yes
Other: no
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Phase:
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Countries of recruitment
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Germany
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Hungary
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Italy
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Key inclusion & exclusion criteria
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Inclusion criteria: 1) Subjects must be willing and able to give written informed consent. 2) Subjects with a diagnosis of type 2 diabetes mellitus. 3) A1C = 8% but = 12% obtained at the screening visit. 4) Fasting C-peptide concentration = 1.0 ng/ml. 5) Subjects will be drug naïve. Drug naïve subjects are defined as subjects who have never received medical treatment for diabetes (insulin and/or oral hypoglycemic agents) or have received medical treatment for diabetes for less than a total of one month since original diagnosis. In addition, subjects should not have received any antihyperglycemic therapy for more than three consecutive days or a total of seven non-consecutive days during the 8 weeks prior to screening. The exceptions are for women who have received treatment for gestational diabetes during their pregnancy and are no longer receiving therapy or subjects who during a hospitalization received a short course of insulin treatment. 6) Body mass index = 40 kg/m2. 7) Men and women, ages 18 to 77. Women must be non-nursing and non-pregnant. Women of childbearing potential (WOCBP) must be using an adequate method of contraception to avoid pregnancy throughout the study and for up to 4 weeks after the study in such a manner that the risk of pregnancy is minimized. WOCBP must have a negative serum or urine pregnancy test (minimum sensitivity 25 IU/L or equivalent units of HCG) within 72 hours prior to the start of study medication. Are the trial subjects under 18? no Number of subjects for this age range: F.1.2 Adults (18-64 years) yes F.1.2.1 Number of subjects for this age range F.1.3 Elderly (>=65 years) yes F.1.3.1 Number of subjects for this age range
Exclusion criteria: 1) WOCBP who are unwilling or unable to use an acceptable method to avoid pregnancy for the entire study period and for up to 4 weeks after the study. 2) WOCBP using a prohibited contraceptive method. 3) Women who are pregnant or breastfeeding. 4) Women with a positive pregnancy test on enrollment or prior to study drug administration. 5) Symptoms of poorly controlled diabetes that would preclude participation in this active-controlled trial including but not limited to marked polyuria and polydipsia with greater than 10% weight loss during the last three months prior to screening or other signs and symptoms. 6) History of diabetic ketoacidosis or hyperosmolar nonketotic coma. 7) Insulin therapy within one year of screening (with the exception of insulin therapy during a hospitalization or use in gestational diabetes). 8) Significant cardiovascular history defined as: a/ History of myocardial infarction, coronary angioplasty or bypass graft(s), valvular disease or repair, unstable angina pectoris, transient ischemic attack, or cerebrovascular accidents within six months prior to entry into the study. or b/ Congestive heart failure defined as New York Heart Association (NYHA) stage III and IV (see Protocol Appendix 2) and/or known left ventricular ejection fraction of = 40%. 9) Chronic or repeated intermittent corticosteroid treatment (subjects receiving stable doses of replacement corticosteroid therapy may be enrolled). 10) History of unstable or rapidly progressing renal disease. 11) History of alcohol or drug abuse within the previous one year. 12) Unstable major psychiatric disorders. 13) Immunocompromised individuals such as subjects that have undergone organ transplantation or subjects diagnosed with human immunodeficiency virus. 14) History of hemoglobinopathies (sickle cell anemia or thalassemias, sideroblastic anemia). 15) Donation of blood or plasma to a blood bank within three months of screening. 16) Administration of any other investigational drug or participation in a clinical research trial within 30 days of planned enrollment to this study (or a longer period of duration if dictated by local regulatory guidelines). 17) Any condition which in the Investigator’s opinion may render the subject unable to complete the study or which may pose significant risk to the subject. 18) Physical and Laboratory Test Findings 19) Active liver disease and/or significant abnormal liver function defined as AST > 2x ULN and/or ALT > 2x ULN and /or serum total bilirubin > 2.0 mg/dL. 20) History of positive serologic evidence of current infectious liver disease including anti-HAV (IgM), HbsAg, or anti-HCV. Subjects who may have isolated positive anti HBs may be included. 21) Serum creatinine (Scr) = 1.5 mg/dL (132.6 µmol/L) for males and = 1.4 mg/dL (123.8µmol/L) for females. 22) Creatine Kinase = 3x ULN. 23) Anemia, of any etiology defined as hemoglobin = 12.0 g/dL (120 g/L) for men andhemoglobin = 11.0 g/dL (110 g/L) for women. 24) Absolute lymphocyte count less than 1000 cells/mm³. 25) Platelet count < 140,000 cells/µL. 26) Subjects that have an abnormal TSH value at screening will be further evaluated by free T4. Subjects with an abnormal free T4 will be excluded. 27) Subjects who have contraindications to therapy as outlined in the Saxagliptin Investigator Brochure, metformin package insert, or pioglitazone package insert. 28) History of administration of any antihyperglycemic therapy for a total of one month or for more than three cons
Age minimum:
Age maximum:
Gender:
Female: yes Male: yes
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Health Condition(s) or Problem(s) studied
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Type 2 Diabetes Mellitus
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Intervention(s)
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Product Name: Saxagliptin Product Code: BMS-477118-11 Pharmaceutical Form: Film-coated tablet INN or Proposed INN: Saxagliptin CAS Number: 361442-04-8 Current Sponsor code: BMS-477118-11 Concentration unit: mg milligram(s) Concentration type: equal Concentration number: 5- Pharmaceutical form of the placebo: Film-coated tablet Route of administration of the placebo: Oral use
Product Name: Saxagliptin Product Code: BMS-477118-11 Pharmaceutical Form: Film-coated tablet INN or Proposed INN: Saxagliptin CAS Number: 361442-04-8 Current Sponsor code: BMS-477118-11 Concentration unit: mg milligram(s) Concentration type: equal Concentration number: 10- Pharmaceutical form of the placebo: Film-coated tablet Route of administration of the placebo: Oral use
Trade Name: Glucophage Product Name: metformin IR Pharmaceutical Form: Film-coated tablet INN or Proposed INN: metformin hydrochloride CAS Number: 657-24-9 Concentration unit: mg milligram(s) Concentration type: equal Concentration number: 500- Pharmaceutical form of the placebo: Film-coated tablet Route of administration of the placebo: Oral use
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Primary Outcome(s)
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Main Objective: To compare, after 24 weeks of oral administration of double-blind treatment, the change from baseline in A1C level achieved with each dose of saxagliptin plus metformin IR compared to saxagliptin plus placebo and to metformin IR plus placebo in treatment-naïve subjects with type 2 diabetes who have inadequate glycemic control defined as A1C = 8% but = 12%.
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Secondary Objective: -Compare each dose of saxagliptin plus metformin IR versus saxagliptin plus placebo and metformin IR plus placebo after 24 weeks of oral administration of double-blind therapy for: 1/change from baseline in fasting plasma glucose 2/proportion of subjects achieving a therapeutic glycemic response defined as A1C<7.0% 3/proportion of subjects achieving a therapeutic glycemic response defined as A1C=6.5% 4/change from baseline in the area under the curve (AUC) from 0 to 180 minutes for postprandial glucose response to an oral glucose tolerance test 5/proportion of subjects requiring rescue for failing to achieve pre-specified glycemic targets or discontinuing for lack of efficacy within 24 week, short-term, double-blind phase
-Assess safety and tolerability of each dose of saxagliptin plus metformin IR, saxagliptin plus placebo and metformin IR plus placebo when administered: 1/for up to 24 weeks of short-term double-blind phase 2/in long-term extension phase
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Primary end point(s): Primary efficacy endpoint: To compare, after 24 weeks of oral administration of double-blind treatment, the change from baseline in A1C level achieved with saxagliptin plus metformin IR compared to saxagliptin plus placebo and to metformin IR plus placebo in treatment-naïve subjects with type 2 diabetes who have inadequate glycemic control defined as A1C = 8% but = 12%.
Secondary efficacy endpoints: To compare saxagliptin plus metformin IR versus saxagliptin plus placebo and metformin IR plus placebo after 24 weeks of oral administration of double-blind therapy for the following: 1) The change from baseline in fasting plasma glucose (FPG). 2) The proportion of subjects achieving a therapeutic glycemic response defined as A1C < 7.0%. 3) The proportion of subjects achieving a therapeutic glycemic response defined as A1C = 6.5%. 4) The change from baseline in the area under the curve (AUC) from 0 to 180 minutes for postprandial glucose (PPG) response to an oral glucose tolerance test (OGTT). 5) The proportion of subjects requiring rescue for failing to achieve pre-specified glycemic targets or discontinuing for lack of efficacy within the 24 week, short-term, double-blind treatment phase.
Primary safety measure: The incidence of adverse events and of marked abnormalities in clinical laboratory tests.
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Source(s) of Monetary Support
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Results
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Results available:
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