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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02182830
Other study ID # 1245.29
Secondary ID
Status Completed
Phase Phase 3
First received
Last updated
Start date July 25, 2014
Est. completion date May 18, 2017

Study information

Verified date June 2018
Source Boehringer Ingelheim
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This trial is designed to investigate the efficacy and safety of empagliflozin compared with placebo in hypertensive black/African Americans with type 2 Diabetes Mellitus. Since hyperglycaemia and hypertension are key risk factors for both micro- and macrovascular complications, assessment of both glucose and BP lowering effects of empagliflozin in hypertensive African American patients with type 2 Diabetes Mellitus could provide clinically highly relevant, new information for the use of empagliflozin.

Essential hypertension is four times more common in African Americans than in Caucasians.

One of the risk factors for hypertension is sodium sensitivity and approximately one third of the essential hypertensive population is responsive to sodium intake. There is a higher association of hypertension with sodium sensitivity in African American patients with type 2 Diabetes Mellitus.

The treatment duration of this trial (24 weeks) will enable assessment of the clinically relevant endpoint of a decrease in HbA1c, a well accepted measurement of chronic glycaemic control and the key secondary endpoints of decreases in systolic BP (SBP) and diastolic BP (DBP) at 12 and 24 weeks.


Recruitment information / eligibility

Status Completed
Enrollment 166
Est. completion date May 18, 2017
Est. primary completion date May 18, 2017
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion criteria:

- Diagnosis of Type 2 Diabetes Mellitus (T2DM) prior to informed consent.

- Male and female black/African American patients on diet and exercise regimen who are EITHER drug-naïve (defined as absence of any oral antidiabetic therapy, glucagon like peptide-1 (GLP-1) analog or insulin for 12 weeks, 16 weeks for pioglitazone prior to randomisation) OR pre-treated with stable dose of

- Metformin only, or

- Sulfonylurea only, or

- Dipeptidyl peptidase-4 (DPP-4) inhibitor only, or

- metformin plus sulfonylurea, or

- metformin plus DPP-4 inhibitor. Treatment has to be unchanged for a minimum of 12 weeks prior to randomization. Dose for metformin: maximum tolerated dose The maximum daily dose of Sulfonylurea (SU) or DPP-4 inhibitor should not exceed that stated in the local label.

- HbA1c of >= 7.0% (53 mmol/mol) and = 11.0% (97 mmol/mol) at Visit 1 (screening).

- Mean seated Systolic Blood Pressure (SBP) 140-180 mmHg at Visit 1 (screening).

- Successful completion of baseline Ambulatory Blood Pressure Monitor (ABPM) testing with a mean SBP 135-175 mmHg prior to randomisation.

- Treatment with stable doses of at least one but not more than 4 antihypertensive medication >= 4 weeks prior to randomisation.

- Age >= 18 years at Visit 1 (screening)

- Signed and dated written informed consent by date of Visit 1 in accordance with Good Clinical Practice (GCP) and local legislation

Exclusion criteria:

- Uncontrolled hyperglycemia with a glucose level >270 mg/dl (>15.0 mmol/L) after an overnight fast during placebo run-in (includes Visit 2.1) and confirmed by a second measurement (not on the same day).

- Exposure to any other antidiabetic medication within 12 weeks prior to randomisation other than metformin, sulfonylurea, Dipeptidyl peptidase-4 (DPP-4) inhibitor, metformin plus sulfonylurea or metformin plus DPP-4 inhibitor.

- Current hypertension treatment with oral Minoxidil (topical minoxidil for hair growth is allowed).

- Mean seated Systolic Blood Pressure (SBP) =181 mmHg during placebo run-in visit and confirmed by a second measurement (not on the same day) preferably within one day.

- Upper arm circumference that exceeds the upper circumference level of the cuff size of either Ambulatory Blood Pressure Monitor (ABPM) and/or (BP) measurement device used in the study.

- Night shift workers who routinely sleep during the daytime and/or whose work hours include midnight.

- Diagnosis of autoimmune diabetes/Type I diabetes mellitus, monogenic (neonatal or maturity onset diabetes of the young (MODY)) diabetes or Type I diabetes in adults/latent autoimmune diabetes of adults (LADA) per investigator or patient medical history at the time of Visit 1 (screening).

- Known or suspected secondary hypertension (e.g. renal artery stenosis,phaeochromocytoma, Cushing's disease).

- History or evidence of hypertensive retinopathy (Keith-Wagener grade III or IV) and/or hypertensive encephalopathy.

- Clinically significant valvular heart disease or severe aortic stenosis in the opinion of the investigator.

- Acute coronary syndrome (non- ST wave elevated myocardial infarction (STEMI), STEMI and unstable angina pectoris), stroke or transient ischemic attack within 3 months prior to informed consent.

- Indication of liver disease, defined by serum levels of either Alanine Aminotransferase (ALT) (Serum Glutamic Pyruvate Transaminase(SGPT)), Aspartate Aminotransferase (AST) (Serum Glutamic Oxaloacetic Transaminase (SGOT)), or alkaline phosphatase above 3 x upper limit of normal (ULN) as determined during screening and/or run-in phase.

- Impaired renal function, defined as Estimated Glomerular Filtration Rate (eGFR)< 45 ml/min/1.73m2 (moderate renal impairment, chronic kidney disease epidemiology collaboration Chronic Kidney Disease Epidemiology Collaboration (CKD-EPI) formula) as determined during screening and/or run-in phase.

- Bariatric surgery within the past two years and other gastrointestinal surgeries that induce chronic malabsorption.

- Medical history of cancer (except for basal cell carcinoma) and/or treatment for cancer within the last 5 years.

- Blood dyscrasias or any disorders causing hemolysis or unstable Red Blood Cells (e.g. malaria, babesiosis, haemolytic anaemia, thalassemia, sickle cell anaemia (sickle cell trait is allowed)).

- Medical history and signs and symptoms of diabetic autonomic neuropathy.

- Treatment with anti-obesity drugs 3 months prior to randomisation (i.e. surgery, aggressive diet regimen, etc.) leading to unstable body weight.

- Current treatment with systemic steroids at time of informed consent or change in dosage of thyroid hormones within 6 weeks prior to informed consent or any other uncontrolled endocrine disorder except Type 2 Diabetes Mellitus (T2DM) in the opinion of the investigator.

- Pre-menopausal women (last menstruation <=1 year prior to informed consent) who:

- are nursing or pregnant or

- are of child-bearing potential and are not practicing an acceptable method of birth control, or do not plan to continue using this method throughout the study and do not agree to submit to periodic pregnancy testing during participation in the trial. Acceptable methods of birth control include tubal ligation, transdermal patch, intra uterine devices/systems (IUDs/IUSs), oral, implantable or injectable contraceptives, complete sexual abstinence (if acceptable by local authorities), double barrier method and vasectomised partner.

- Alcohol, drug or confectionary liquorice abuse within the 3 months prior to informed consent that would interfere with trial participation or any ongoing condition leading to a decreased compliance to study procedures or study drug intake in the investigator's opinion.

- Intake of an investigational drug in another trial within 30 days prior to intake of study medication in this trial; or participating in another trial (involving an investigational drug and/or follow-up) after discontinuing medication in that trial.

- Any other clinical condition that would jeopardize patient's safety while participating in this clinical trial in the opinion of the investigator.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Empagliflozin low dose
starting dose 10mg; forced titration after 4 weeks 25mg dose
placebo
starting dose 10mg; forced titration after 4 weeks 25mg dose
Empagliflozin high dose
starting dose 10mg; forced titration after 4 weeks 25mg dose

Locations

Country Name City State
United States Lovelace Scientific Resources, Inc. Albuquerque New Mexico
United States Millennium Clinical Trials LLC Arlington Virginia
United States Atlanta Center Atlanta Georgia
United States Atlanta Clinical Research Centers Atlanta Georgia
United States Grady Memorial Hospital Atlanta Georgia
United States Morehouse School of Medicine Atlanta Georgia
United States American Institute of Research Studies Baltimore Maryland
United States University of Maryland School of Medicine Baltimore Maryland
United States Clinical Research Advantage, Inc./Rita B. Chuang, MD, LLC Birmingham Alabama
United States University of Alabama at Birmingham Birmingham Alabama
United States Healthwise Medical Associates Brooklyn New York
United States Modern Medical Brooklyn New York
United States Offic of Dr. Eric Cheng Brooklyn New York
United States Investigators Research Group, LLC Brownsburg Indiana
United States Erie County Medical Center Buffalo New York
United States Medical Research South Charleston South Carolina
United States Metrolina Internal Medicine, PA Charlotte North Carolina
United States Cedar Crosse Research Center Chicago Illinois
United States John H. Stroger Jr. Hospital of Cook Country Chicago Illinois
United States University of Chicago Chicago Illinois
United States eStudySite Chula Vista California
United States Amistad Clinical Research Center Columbia South Carolina
United States TLM Medical Services, LLC Columbia South Carolina
United States Hometown Urgent Care Columbus Ohio
United States Dayton Clinical Research Dayton Ohio
United States Lynn Institute of Denver Denver Colorado
United States Albert F. Johary MD, PC Dunwoody Georgia
United States PhysiqueMed Clinical Trials Greensboro North Carolina
United States Triad Clinical Trials Greensboro North Carolina
United States Greenville Pharmaceutical Rsch Greenville South Carolina
United States Mountain View Clinical Research Greer South Carolina
United States High Point Clinical Trials Center High Point North Carolina
United States Peters Medical Research High Point North Carolina
United States Pines Clinical Research Inc. Hollywood Florida
United States Centex Studies, Inc. Houston Texas
United States Cullen Family Practice, PLLC Houston Texas
United States Diagnostic Clinic of Houston Houston Texas
United States Kelsey-Seybold Clinic Houston Texas
United States Texas Center for Drug Development, Inc. Houston Texas
United States Longwood Research Huntsville Alabama
United States Phillips Medical Services, PLLC Jackson Mississippi
United States Care Partners Clinical Research LLC Jacksonville Florida
United States UF Health Jacksonville Jacksonville Florida
United States Centex Studies, Inc. Lake Charles Louisiana
United States Accent Clinical Trials Las Vegas Nevada
United States Scott Research, Inc. Laurelton New York
United States Cardiology and Medicine Clinic Little Rock Arkansas
United States Larry Watkins, M .D. Little Rock Arkansas
United States Torrance Clinical Research Institute Inc. Lomita California
United States Long Beach Center for Clinical Research Long Beach California
United States MD Clinical Trials Los Angeles California
United States Office of Dr. Alexander Ford, M.D. Los Angeles California
United States Clinical Research Advantage, Inc./Rita B. Chuang, MD, LLC Marietta Georgia
United States Sestron Clinical Research Marietta Georgia
United States Suburban Research Associates Media Pennsylvania
United States Memphis Veterans Affairs Medical Center Memphis Tennessee
United States Southwind Medical Specialists Memphis Tennessee
United States The Green Clinic PC Memphis Tennessee
United States University of Tennessee Memphis Tennessee
United States Gulf Regional Research and Education Services, LLC Metairie Louisiana
United States Family Medical Clinic Milwaukee Wisconsin
United States Internal Medicine Center, LLC Mobile Alabama
United States Mobile Medical and Diagnostic Center Mobile Alabama
United States University of South Alabama Mobile Alabama
United States Berkley Family Practice Moncks Corner South Carolina
United States Coastal Carolina Health Care, P.A. New Bern North Carolina
United States New Orleans Center for Clinical Research New Orleans Louisiana
United States Medex Healthcare Research, Inc. New York New York
United States York Clinical Research, LLC Norfolk Virginia
United States Today Clinical Research, Oklahoma City Oklahoma City Oklahoma
United States Quality Clinical Research Inc Omaha Nebraska
United States Sunshine Research Center Opa-locka Florida
United States Diabetes Associates Medical Group Orange California
United States Central Florida Internist Orlando Florida
United States Temple University School of Medicine Philadelphia Pennsylvania
United States Accord Clinical Research, LLC Port Orange Florida
United States Clinical Research Partners, LLC Richmond Virginia
United States Dominion Medical Associates, Inc. Richmond Virginia
United States Integrated Research Group, Inc. Riverside California
United States Carolina Cardiology Clinical Research Institute, LLC Rock Hill South Carolina
United States Laurelton Heart Specialist, PC Rosedale New York
United States Clinical Trials Research Sacramento California
United States Alternative Solutions Medical Research and Prevention Center Saint Petersburg Florida
United States Meridien Research Saint Petersburg Florida
United States WR-Mount Vernon Clinical Research, LLC Sandy Springs Georgia
United States International Clinical Research - US, LLC Sanford Florida
United States Eagle's Landing Diabetes and Endocrinology Stockbridge Georgia
United States Meridien Research Tampa Florida
United States Orange County Research Center Tustin California
United States Community Research Partners, Inc Varnville South Carolina
United States Hillcrest Family Health Center Waco Texas
United States Mercy Research Washington Missouri

Sponsors (2)

Lead Sponsor Collaborator
Boehringer Ingelheim Eli Lilly and Company

Country where clinical trial is conducted

United States, 

Outcome

Type Measure Description Time frame Safety issue
Primary Change From Baseline in Glycated Haemoglobin (HbA1c) (%) at 24 Weeks Change from baseline in HbA1c (%) at 24 weeks is presented. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means. Restricted maximum likelihood (REML)-based mixed model repeated measures (MMRM) model is used in the statistical analysis.
baseline and 24 weeks
Secondary Change From Baseline in Mean 24-hour Ambulatory Systolic Blood Pressure (SBP) at Week 12 Change from baseline in mean 24-hour ambulatory Systolic blood pressure SBP at Week 12 is presented. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means. This is a key secondary endpoint
baseline and 12 weeks
Secondary Changes From Baseline in Trough Mean Ambulatory SBP at Week 12 Changes from baseline in trough mean ambulatory SBP at Week 12 is presented. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means. This is a key secondary endpoint
baseline and 12 weeks
Secondary Change From Baseline in Body Weight at Week 24 Changes from baseline in body weight at Week 24 is presented. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means. This is a key secondary endpoint
baseline and 24 weeks
Secondary Change From Baseline in Trough Seated SBP at Week 12 Change from baseline in trough seated SBP (mmHg) at Week 12 is presented. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means. This is a key secondary endpoint
baseline and 12 weeks
Secondary Change From Baseline in Mean 24-hour Ambulatory SBP (mmHg) at Week 24 Change from baseline in mean 24-hour ambulatory SBP (mmHg) at Week 24 is secondary endpoint. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means.
baseline and 24 weeks
Secondary Change From Baseline in Mean 24-hour Ambulatory Diastolic Blood Pressure (DBP) at Week 12 Change from baseline in mean 24-hour ambulatory DBP (mmHg) at Week 12. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means.
baseline and 12 weeks
Secondary Change From Baseline in Mean 24-hour Ambulatory DBP (mmHg) at Week 24 Change from baseline in mean 24-hour ambulatory DBP (mmHg) at Week 24 is secondary endpoint. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means.
baseline and 24 weeks
Secondary Change From Baseline in Trough Seated SBP (mmHg) at Week 24 Change from baseline in trough seated SBP (mmHg) at Week 24 is secondary endpoint. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means.
baseline and 24 weeks
Secondary Change From Baseline in Trough Seated DBP (mmHg) at Week 12 Change from baseline in trough seated DBP (mmHg) at Week 12 is secondary endpoint. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means.
baseline and 12 weeks
Secondary Change From Baseline in Trough Seated DBP (mmHg) at Week 24 Change from baseline in trough seated DBP (mmHg) at Week 24 is secondary endpoint. The term "baseline" refers to the last observation prior to randomisation of the patient.
Means presented are the adjusted means.
baseline and 24 weeks
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