Diabetes Clinical Trial
Official title:
A Prospective, Randomized, Probe Trial to Evaluate Whether, at Comparable Blood Pressure Control, Combined Therapy With the ACEI Benazepril and the ARB Valsartan, Reduces the Incidence of Microalbuminuria More Effectively Than BEN or VAL Alone in Hypertensive Patients With Type 2 Diabetes and High-normal Albuminuria
In people with type 2 diabetes, microalbuminuria is a strong, independent risk factor for
diabetic nephropathy and cardiovascular morbidity and mortality. ACE inhibitor therapy
decreased the risk of microalbuminuria in hypertensive subjects with type 2 diabetes and
normoalbuminuria by about 40%. Available data suggest that angiotensin II receptor blockers
(ARBs) might have a similar renoprotective effect and that this effect might be increased by
combined ACE inhibitor therapy.
The study will evaluate the effects, at similar blood pressure control (systolic/diastolic
<130/80 mmHg), for a period of three years, of dual renin-angiotensin-system (RAS) blockade
by benazepril and valsartan combination therapy as compared to single RAS blockade by
benazepril or valsartan alone on microalbuminuria and cardiovascular events in high-risk
patients with type 2 diabetes, creatinine <1.5 mg/dl, no evidence of microalbuminuria but at
high risk of renal disease, with hypertension and a urinary albumin excretion between 7 and
19 microgram/min. The relationship between albuminuria and cardiovascular outcomes will also
be evaluated.
The study is expected to show a more effective prevention of microalbuminuria and
cardiovascular events with combined than with single drug ACE inhibitor or ARB therapy. As
compared to ACE inhibitor, ARB therapy is expected to have a similar effect on
microalbuminuria, but an inferior cardioprotective effect. Applied to clinical practice, the
findings should help preventing renal and cardiovascular complications, and related treatment
costs, of type 2 diabetes.
Nephropathy of type 2 diabetes is the leading cause of end stage renal disease (ESRD) in the
world.According to the World Health Organization (WHO), diabetes affects over 170 million
people, and, due to progressive aging of the population, life-style modifications and
increasing burden of obesity, this number is expected to rise to 370 millions by 2030. About
one third of those affected will eventually have progressive deterioration of renal function
Untreated, these patients progress to ESRD within 10 years or die prematurely because of
cardiovascular complications (that are 10-fold more frequent in diabetics with nephropathy
than in those without and the general population). Costs for renal replacement therapy of
these patients - and for treatment of related complications - are also progressively
increasing.
Persistent microalbuminuria is the first clinical sign of renal dysfunction in diabetic
patients and progresses to overt proteinuria in 20 to 40 percent of cases. In 10 to 50
percent of patients with proteinuria, chronic kidney disease develops that ultimately
requires dialysis or transplantation. Of great concern, 40 to 50 percent of type 2 diabetic
patients with microalbuminuria eventually die of cardiovascular disease.Thus, preventing (or
delaying) the development of microalbuminuria is a key treatment goal for renoprotection and,
possibly, for cardioprotection.
A large scale randomized trial, the BErgamo NEphrologic DIabetes Complications Trial
(BENEDICT) found that treatment with the ACE-inhibitor trandolapril (either alone or combined
to the calcium channel blocker verapamil) significantly reduced the incidence of
microalbuminuria in 1204 patients with type 2 diabetes and hypertension, but normal urinary
albumin excretion, as compared with placebo. The effect of preventing microalbuminuria
exceeded expectations based on changes in blood pressure alone and was not enhanced by
combined calcium channel blocker therapy.
Studies in patients with type 2 diabetes and micro- or macro- albuminuria clearly show that
ARBs can have renoprotective effect but trials evaluating the effects of angiotensin receptor
blockers (ARBs) on the incidence of microalbuminuria in type 2 diabetic patients with normal
urinary albumin excretion rate are missing.
Whether the beneficial effect against the development of microalbuminuria is enhanced when
ACE inhibitors and ARBs are given in combination is not established so far. However, finding
that combined ACE inhibitor and ARB therapy more effectively than single drug RAS blockade
reduced albuminuria or proteinuria in subjects with type 2 diabetes and slowed progression to
ESRD in those with non-diabetic chronic nephropathies, suggests that the renoprotective
effect of combined therapy could be superior to that of single drug blockade of the RAS also
in diabetic patients with no evidence of renal disease.
Post hoc analyses of the BENEDICT trial found that high-normal albuminuria at baseline
evaluation (defined as a urinary albumin excretion rate between 10 µg/min and the upper limit
for study entry: 19 µg/min) was the strongest baseline predictor of subsequent development of
microalbuminuria. Indeed, regardless of treatment randomization, 69 of 271 (25.5%) patients
with high-normal albuminuria (urinary albumin excretion >10µg/min) progressed to the end
point as compared to only 32 of 933 (3.4%) with low-normal albuminuria (<10%). Thus,
large-part of the excess risk for microalbuminuria observed in people with type 2 diabetes is
associated with high-normal albuminuria.
In addition, this clinical trial might have a clinical relevance for the Italian National
Health service (SSN): applied to clinical practice the results should help in reducing renal
and cardiovascular complications and related treatment costs, of type 2 diabetes.
Aims Primary To evaluate whether, at comparable blood pressure control, dual RAS blockade
with combined therapy with halved doses of benazepril (10 mg/day) and valsartan (160 mg/day)
reduces the incidence of microalbuminuria more effectively than single drug RAS blockade by
full doses of benazepril (20 mg/day) given alone in high-risk patients with type 2 diabetes,
hypertension and high normal albuminuria.
Secondary
- To evaluate whether, at comparable blood pressure control, dual RAS blockade with
combined therapy with halved doses of benazepril (10 mg/day) and valsartan (160 mg/day)
reduces the incidence of microalbuminuria more effectively than valsartan (320 mg/day)
given alone in high-risk patients with type 2 diabetes, hypertension and high normal
albuminuria.
- To evaluate whether, at comparable blood pressure control, the effects of benazepril and
valsartan therapy are similar or whether, alternatively, one of the two treatments offer
a superior protective effect against the development of microalbuminuria in the above
study population.
- To evaluate the effects of the three study treatments on the incidence of fatal and
non-fatal cardiovascular events, regression to low-normal albuminuria (urinary albumin
excretion <7 µg/min), albuminuria (considered as a continuous variable), serum
creatinine, lipid profile, and GFR (in a representative subgroup);
- To assess the relationships, in the study group as a whole and within each treatment
group, between renal outcome variables (including microalbuminuria and time-dependent
changes in albuminuria) and fatal and non-fatal cardiovascular events, between achieved
blood pressure or metabolic control and renal and/or cardiovascular outcome variables
and between achieved albuminuria reduction or residual follow-up albuminuria and renal
and/or cardiovascular outcome variables.
Design This will be a multicenter, Prospective, Randomized, Open label, Blinded End point
(PROBE) trial of 3-year treatment with halved doses of benazepril (10 mg/day) and valsartan
(160 mg/day) given in combination, or full doses of both benazepril (20 mg/day), or valsartan
(320 mg/day) given alone in 1020 consenting patients >40 year old, with type 2 diabetes (WHO
criteria), serum creatinine <1.5 mg/dl, high-normal albuminuria (UAE >7 and <20 µg/min in at
least 2 of 3 overnight urine collections), and no specific contraindications to the study
drugs. Primary outcome variable will be microalbuminuria (UAE > 20µg /min in at least 2 of 3
overnight urine collections in two consecutive visits 2 months apart) and primary comparison
will be between the combined benazepril plus valsartan and the benazepril alone groups. The
analysis will have an 80% power to detect (p=0.05, two-side test) a 40% difference in the
incidence of microalbuminuria.
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