The investigators will assess whether the DPP-inhibitor sitagliptin will ameliorate glucocorticoid-induced impairment of glucose metabolism and beta-cell dysfunction and thus could be used as a prophylaxis for glucocorticoid-induced diabetes. Therefore the investigators will administer in males with the metabolic syndrome 30 mg prednisolone daily for two weeks and give simultaneously sitagliptin 100 mg daily. Subjects will undergo at baseline and after two weeks of treatment several tests to assess changes in glucose metabolism.
The investigators will conduct a randomized, placebo-controlled, double-blind, 2x2 factorial-designed intervention trial. The pharmacological intervention for prednisolone/prednisolone-placebo is 14 days and for sitagliptin/sitagliptin-placebo 28 days. Subjects fulfilling the IDF criteria26 for the metabolic syndrome (aged 35-65; n=60) will be randomized to one of four groups: I) prednisolone 30 mg and sitagliptin 100 mg daily; II) prednisolone 30 mg and sitagliptin-placebo daily; III) prednisolone-placebo and sitagliptin 100 mg daily; IV) prednisolone-placebo and sitagliptin-placebo daily. Before and at day 14 of treatment subjects will undergo a standardized mixed-meal test in order to assess glucose disposal and beta-cell function (by modeling analysis). During these meal tests, plasma concentrations of (total and active) GLP-1, GIP, glucagon and additional biomarkers will be assessed. A combined hyperglycemic-euglycemic clamp will be performed at baseline and at day 13 of treatment to assess insulin sensitivity and insulin secretion. During the euglycemic clamp adipose tissue and muscle biopsies will be obtained, both in fasting and under hyperinsulinemic conditions. At baseline and at day 28 of treatment, a 7-point OGTT will be performed to assess time to restoration of glycemic control. Body composition, body fat distribution and liver fat content, measured by respectively bio-impedance analysis and magnetic resonance imaging/spectroscopy (MRI/MRS), will be assessed at baseline and after 28 days of treatment. Blood pressure will be assessed at baseline and after two weeks of treatment. Microvascular function will be assessed with capillary videomicroscopy both at baseline and after two weeks of treatment.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
PREVENTION
Masking
TRIPLE
Enrollment
82
28 days administration of 100 mg daily
14 days administration of 30 mg daily
28 days administration once daily
14 days administration once daily
VUmc Diabetes Center
Amsterdam, North Holland, Netherlands
Glucose tolerance as assessed by the area under the curve for glucose (AUCgluc) during a standardized meal test.
Time frame: 14 days
Incretin secretion during standardized meal test
Time frame: 14 days
Insulin sensitivity
Time frame: 14 days
Microvascular function: fasting and postprandial
Time frame: 14 days
Body composition, body fat distribution and intra organ fat accumulation
Time frame: 28 days
Molecular mechanisms in subcutaneous adipose tissue
Time frame: 14 days
Blood pressure and hemodynamic parameters
Time frame: 28 days
Biomarkers such as lipoproteins, adipocytokines, and markers of systemic inflammation
Time frame: 14 days
Time to recovery after cessation of the two-week prednisolone treatment
Time frame: 28 days
Beta-cell function as determined by hyperglycemic clamp tests and modeling analysis from mixed-meal tests.
Time frame: 14 days
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