Type 2 Diabetes Mellitus Clinical Trial
Official title:
CSP #465 - Glycemic Control and Complications in Diabetes Mellitus Type 2 (VADT)
This study is a prospective, 2-arm, randomized controlled trial to determine whether glycemic control, achieved through intensification of treatment, is effective in preventing clinical macrovascular complications in patients with type 2 DM who are no longer responsive to oral agents alone. The study consists of a two-year accrual period and five years of follow-up (7 years total) of 1700 patients across 20 centers. We have powered the study to detect a 21% reduction in the primary event rate. Additional study goals are to determine whether the expenditures, discomfort, and adverse effects associated with intensive intervention are justified in terms of their clinical benefits, considering both macrovascular and microvascular complications.
Primary Hypothesis: Intensive glycemic control reduces major macrovascular morbidity and
mortality compared to standard glycemic control in type 2 diabetics who have failed simple
therapy.
Secondary Hypotheses: Intensive glycemic control, compared to standard glycemic control,
reduces other macrovascular morbidity and total mortality.
Intervention: The intervention is tight glycemic control, aiming at normalization of HbA1c.
This will be achieved through stepped care therapy, using all categories of tools available
to most diabetologists. These categories include: patient education of diabetes control
(e.g. diet, exercise, etc.), oral diabetes medications, and insulin. All drugs to be used
are approved. Specific agents will be used within the different classes to promote
consistency across sites.
The comparison is standard control, aiming at HbA1c of 8 - 9%. The same agents will be used,
but at reduced doses.
The general approach to the stepped care treatment protocol is to treat both groups with the
same agents, but at different intensities (doses) (taking into account
intolerance/contraindications). The sequence of steps is shown below.
STEP 1: Either Metformin (obese) or Glimepiride (lean)in combination with Rosiglitazone STEP
2: Insulin STEP 3: Increase doses in STEPS 1,2 in the Standard group. Since the Intensive
group is already at maximal doses of oral agents, they will intensify insulin and may add
Acarbose/Miglitol.
STEP 4: For standard, proceed as in STEP 3 for Intensive; Intensives will use multiple daily
injection (MDI) of insulin STEP 5: "Tool Box": Miscellaneous agents, tailored to the
individual patient.
Primary Outcomes: Time to one of the following major macrovascular events: myocardial
infarction, stroke, new or worsening congestive heart failure, amputation for ischemic
gangrene, invasive intervention for coronary artery or peripheral vascular disease,
inoperable coronary artery disease, or cardiovascular death.
Secondary Outcomes: Angina, transient ischemic attack, intermittent claudication, critical
limb ischemia, and total mortality.
Study Abstract: A quarter of the patients treated by the Department of Veterans Affairs (VA)
Health Administration have type 2 diabetes mellitus (DM). The costs of care for the
treatment of patients with type 2 DM are extremely high, both in treatment expenditures for
the metabolic disorder and for the care of end-organ complications. Although patients
initially respond to diet and oral agent treatment, most eventually need insulin to
near-normalize their glucose level, as the disease is characterized by progressive loss of
insulin secretory capacity.
After several clinical trials in both type 1 and type 2 DM, there is a reasonable certainty
that about half of the incidence and rate of progression of indicators of microvascular
complications (retinopathy, nephropathy, and neuropathy) can be prevented or delayed by
achieving and maintaining near-normalization of glycemic levels. Consequently, there has
been a uniform trend in recent guidelines to advise a near-normalization of glycemic levels
in both type 1 and type 2 DM. Note, however, that the clinical consequences of microvascular
deterioration are dependent not only on glycemic levels but also on the duration of the
disease. With the early onset of diabetes typical in type 1 patients, there is sufficient
time for development of clinical microvascular complications, and prevention of these
complications is a goal of treatment in type 1 diabetics. In contrast, the prevalence of
hard clinical endpoints indicative of microangiopathy, such as renal failure or blindness,
is very low in patients in whom the disease is diagnosed after the 5th decade, the greatest
age of prevalence of patients with type 2 DM in this country. Furthermore, microvascular
complications can be minimized by the well-established benefits of blood pressure and lipid
control, as well as by therapeutic intervention (photocoagulation, cataract extraction).
Since the costs and efforts necessary to reach near-normal levels of glycemia are very high,
there is a need to determine the cost/benefit ratios of such expenditures in the population
subject to type 2 diabetes, namely patients in their 6th to 8th decades of life.
In contrast with the late and relatively infrequent appearance of clinical endpoints of
microangiopathy, macrovascular complications (i.e., coronary heart disease and peripheral
vascular disease) are responsible for the overwhelming majority of the mortality, morbidity
and treatment costs in the American population of type 2 diabetics, even more so in the
older VA diabetic population. In the recently concluded United Kingdom Prospective Diabetes
Study (UKPDS) on type 2 DM, macrovascular mortality was 70 times higher than that of
microvascular mortality. Intervention studies to determine the effect of rigorous glycemic
control on these macrovascular events are inconclusive and contradictory. Intensive
treatment in patients who are newly diagnosed has failed to demonstrate a beneficial effect
of tight control on cardiovascular complications. The few studies conducted in later stages
of the disease (i.e., in patients requiring insulin treatment, alone or in combination with
oral agents) have been conflicting and indeterminate.
The decision on intensity of treatment is further compromised by current recommendations to
attenuate glycemic control goals, especially when usage of insulin is required, both in
patients with the common comorbidities of overweight or preexisting cardiovascular disease,
and in those in the later decades of life. These concerns are based on fears that intensive
insulin treatment might be associated with weight gain, increased cardiovascular risk
factors (hypertriglyceridemia, dyslipidemia, hyperinsulinemia, and insulin resistance), and
adverse effects of recurrent hypoglycemic events. The prevalent level of glycemic control in
insulin-treated type 2 diabetics is relatively poor, likely due to a combination of
practical difficulties and the uncertainties of what are the safe and effective glycemic
goals. There is no long-term study currently being done in the high-risk population typical
of the patient population in the VA. Before the Department of Veterans Affairs devotes
considerable resources to a widespread intervention (a quarter of patients) that may be of
little value, and might even be counterproductive, a trial to determine the value of the
intervention is mandated. It is expected that CSP #465 will provide the scientific data on
which the VA can base clinical treatment of Type II diabetes.
CSP #465 is a prospective, 2-arm, randomized controlled trial to determine whether glycemic
control, achieved through intensification of treatment, is effective in preventing clinical
macrovascular complications in patients with type 2 DM who are no longer responsive to oral
agents alone. The study consists of a two-year accrual period and five years of follow-up (7
years total) of 1700 patients across 20 centers. We have powered the study to detect a 25%
reduction in the primary event rate. Additional study goals are to determine whether the
expenditures, discomfort, and adverse effects associated with intensive intervention are
justified in terms of their clinical benefits, considering both macrovascular and
microvascular complications.
Main Manuscript:Duckworth W, Abraira C, Moritz T, Reda D, Emanuele N et al., VADT
investigators: Glucose Control and Complications in the VA Diabetes Trial (VADT). N Eng J of
Med 360:129-139, 2009.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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