Cardiovascular Diseases Clinical Trial
Official title:
Bypass Angioplasty Revascularization Investigation in Type 2 Diabetes
The BARI 2D trial is a multicenter study that uses a 2x2 factorial design, with 2400
patients being assigned at random to initial elective revascularization with aggressive
medical therapy or aggressive medical therapy alone with equal probability, and
simultaneously being assigned at random to an insulin providing or insulin sensitizing
strategy of glycemic control (with a target value for HbA1c of less than 7.0% for all
patients).
SPECIFIC AIMS
A. Primary Aim
The primary aim of the BARI 2D trial is to test the following two hypotheses of treatment
efficacy in 2400 patients with Type 2 diabetes mellitus and documented stable CAD, in the
setting of uniform glycemic control and intensive management of all other risk factors
including dyslipidemia, hypertension, smoking, and obesity:
1. Coronary Revascularization Hypothesis: a strategy of initial elective revascularization
of choice (surgical or catheter-based) combined with aggressive medical therapy results
in lower 5-year mortality compared to a strategy of aggressive medical therapy alone;
2. Method of Glycemic Control Hypothesis: with a target HbA1c level of less than 7.0%, a
strategy of hyperglycemia management directed at insulin sensitization results in lower
5-year mortality compared to a strategy of insulin provision.
B. Secondary Aims
The secondary aims of the BARI 2D trial include: a) comparing the death, myocardial
infarction or stroke combined endpoint event rate between the revascularization versus
medical therapy groups and between the insulin sensitization versus insulin provision
groups; b) comparing rates of myocardial infarction, other ischemic events, angina and
quality of life associated with each revascularization and hyperglycemia management
strategy; c) evaluating the relative economic costs associated with the trial treatment
strategies, d) exploring the effect of glycemic control strategy on the progression and
mechanism of vasculopathy including changes in PAI-1 gene expression.
BACKGROUND:
Type 2 diabetes mellitus, which is becoming more prevalent in our society as the population
ages, is one of the strongest risk factors for coronary artery disease (CAD) and consequent
mortality. In addition to generating an enormous toll in human suffering, diabetes places an
economic burden approaching 100 billion dollars annually on the U.S. health care system.
Despite the well known dismal prognosis of diabetes complicated by angiographically
documented CAD, the optimal treatment paradigm for this large group of patients has not been
studied. Coronary revascularization, while increasingly used, has not been directly shown to
be of additional benefit to simultaneous intensive medical management of CAD along with
management of hyperglycemia, hypertension, dyslipidemia, and other risk factors. Moreover,
while intensive efforts to lower HbA1c have been demonstrated to favorably affect the
clinical course of Type 2 diabetes mellitus in terms of microvascular complications, the
optimal hyperglycemia management strategy with regard to macrovascular outcome is not known.
These critical treatment dilemmas have motivated the development of BARI 2D, a multicenter
randomized trial designed to determine in patients with Type 2 diabetes and stable CAD: 1)
the efficacy of initial elective coronary revascularization combined with aggressive medical
therapy, compared to an initial strategy of aggressive medical therapy alone; and 2) the
efficacy of a strategy of providing more insulin (endogenous or exogenous), versus a
strategy of increasing sensitivity to insulin (reducing insulin resistance), in the
management of hyperglycemia, with a target HbA1c level of less than 7.0% for each strategy.
DESIGN NARRATIVE:
The BARI 2D trial is a multicenter study that uses a 2x2 factorial design, with 2400
patients being assigned at random to initial elective revascularization with aggressive
medical therapy or aggressive medical therapy alone with equal probability, and
simultaneously being assigned at random to an insulin providing or insulin sensitizing
strategy of glycemic control (with a target value for HbA1c of less than 7.0% for all
patients). Following confirmation of patient eligibility and provision of written consent,
patients were randomized as shown below:
Number of Patients Per Treatment Assignment (N=2400 patients in total)
Stable Ischemic Heart Disease Treatment Strategy and Glycemic Control Strategy:
Revascularization and Insulin Providing (IP) N=600; Revascularization and Insulin
Sensitizing (IS) N=600; Medical and Insulin Providing (IP) N=600; Medical and and Insulin
Sensitizing (IS) N=600.
;
Allocation: Randomized, Intervention Model: Factorial Assignment, Masking: Open Label, Primary Purpose: Treatment
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