Diabetes Mellitus, Type 2 Clinical Trial
Official title:
Study ATG115317, a Comparison of Atorvastatin and Glimepiride Fixed Dose Combination and Atorvastatin and Glimepiride Loose Combination in the Treatment of Patients With Type 2 Diabetes Mellitus
The aim of this 20 week study is to show that glimepiride/atorvastatin fixed dose combination tablet is safe and as effective as atorvastatin + glimepiride combination taken as separate tablets, in improving glycaemic control (glycated haemoglobin, HbA1c) and cholesterol levels (Low-density lipoprotein, LDL) in diabetic subjects, who are inadequately controlled on a stable dose of metformin. Eight dose combinations will be included.
Patients diagnosed with Type 2 diabetes (T2D) are initially provided with lifestyle advice in
order to manage the condition by diet, exercise and weight reduction, followed by treatment
with metformin. However, many patients do not gain adequate control of fasting glucose by
these methods and other anti-diabetic agents are needed. Furthermore, these patients have an
increased cardiovascular risk compared with the general population. Approximately one half of
patients with T2D die prematurely of a cardiovascular cause and approximately 10% die of
renal failure.
Atherogenic dyslipidemia, which is defined as the triad of elevated triglycerides, low
high-density lipoprotein cholesterol (HDL-C), and small low-density lipoprotein cholesterol
(LDL-C) particles, is commonly found in individuals with T2D. In diabetic patients, the LDL
particles tend to be smaller, denser, and more atherogenic than in the general population. As
a result, in patients with diabetes, lowering LDL-C levels may lead to a greater benefit in
terms of Cardiovascular disease (CVD) risk reduction than in patients without diabetes.
Multiple clinical trials have demonstrated significant benefits of lipid-lowering (primarily
statin) therapy on CVD outcomes for primary and secondary prevention, irrespective of
baseline lipid levels. Hence, clinical treatment guidelines recommend that patients with T2D
should be treated with both an anti-diabetic agent and a statin.
Glimepiride is an established once-daily sulphonylurea for use as first-line therapy, and is
often used in patients who are metformin intolerant, or in those who are failing to achieve
glucose control on metformin monotherapy. Atorvastatin is an established statin that is
indicated for reducing the risk of cardiovascular events in diabetic patients, without
clinically evident coronary heart disease (CHD), irrespective of whether cholesterol is
raised. The risk:benefit of both glimepiride and atorvastatin is well established and
described in the approved product labels. There is widespread use of both glimepiride and
atorvastatin, prescribed separately, in the T2D population. The available literature
indicates that there is no drug-drug interaction risk associated with this combination
therapy and no clinical PK interactions between atorvastatin and glimepiride have been
recorded. A once-daily combination product which combines both glimepiride and atorvastatin
will fulfil an unmet clinical need in simplifying patient treatment regimens in a patient
population who have a significant disease burden. Providing concurrent access to a statin in
patients with T2D, in addition to medication to manage glucose levels, is a critical
requirement for ensuring appropriate management of cardio-metabolic risk.
In this study, subjects already on a stable dose of metformin will be randomised to either to
receive the glimepiride/atorvastatin fixed dose combination treatment or atorvastatin +
glimepiride combination taken as separate tablets. The starting dose for all subjects will be
1mg glimepiride and 10mg atorvastatin. The glimepiride dose will be titrated up if the
average fasting glucose is >7.0mmol/L. The atorvastatin dose will be titrated up if LDL is
>2.6mmol/L.
The purpose of the study is to demonstrate non-inferiority of the glimepiride/atorvastatin
fixed dose combination compared with glimepiride +atorvastatin taken as separate tablets in
reducing HbA1c and LDL.
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