Diabetes Mellitus, Type 2 Clinical Trial
Official title:
Effects of a Chronical Treatment With Benfotiamine in People With Type 2 Diabetes Mellitus on Pre- and Postprandial Endothelial Function, as Well as on the Function of the Autonomic Nervous System
An AGE-rich diet can induce after 2-6 weeks persistent increases in mediators linked to
vascular dysfunction (e.g. TNFα, VCAM-1) in people with type 2 diabetes mellitus (T2DM).
Benfotiamine (BT), the liposoluble derivative of vitamin B1, blocks several pathways common
to hyperglycaemia- and AGE-induced endothelial dysfunction. We have shown that advanced
glycation end products (AGE) of a regular mixed meal can acutely induce vascular dysfunction
in T2DM and that this effects can be prevented by a three days pretreatment with BT.
The hypotheses of this study are that chronical treatment with benfotiamine (900 mg/day for
6 weeks) in people with type 2 diabetes mellitus:
1. prevents postprandial impairment of endothelial function after a high-AGE meal.
2. Improves fasting endothelial function.
3. Improves parameters of autonomic function in fasting and postprandial state.
4. Improves insulin sensitivity and prevents postprandial increase in insulin resistance.
People with type 2 diabetes mellitus (T2DM) have a two to fivefold increase in
cardiovascular mortality compared to non-diabetic controls.
Endothelial dysfunction (ED) is an early messenger of atherosclerosis and is responsible for
increased vascular permeability, platelet aggregation and adhesion, leucocyte adhesion and
smooth muscle cell proliferation and favours a vasoconstrictive and pro-inflammatory state.
Postprandial ED occurs not only in patients with CV disease or diabetes, but even in healthy
subjects. Distinctive and cumulative effects of hyperglycemia and hypertriglyceridemia on
postprandial ED have been demonstrated. Since postprandial dysmetabolism was linked to CV
disease, the postprandial ED was proposed to be the mechanism connecting them. Considering
that the postprandial state covers most of our daytime, interventions targeting a reduction
in postprandial ED might play a decisive role in atherosclerosis prevention.
For the treatment of postprandial ED several therapeutical approaches have been suggested,
such as treatment with folic acid, tetrahydrobiopterin, vitamins C and E,statins etc.
These approaches aim at reducing postprandial oxidative stress (vitamins C and E, statins
and partly folic acid), postprandial hyperglycemia (insulin), postprandial
hypertriglyceridemia (statins) or have a direct effect on endothelial NO production (folic
acid, insulin and tetrahydrobiopterin).
Recent data suggests that advanced glycation endproducts (AGE) might also play a role in the
development of ED, leading to the long-term complications of diabetes and accelerated aging.
AGEs are a heterogeneous group of moieties, one of the most representative being
carboxymethyllysine (CML). Diet is a major source of exogenous AGEs and the food AGE content
is highly dependent on food nutrient composition, as well as on temperature, method and
duration of heat application during cooking. About 10% of ingested AGEs are rapidly absorbed
and partly retained into the body, where they exert different pathological effects including
binding with and activation of receptors for AGE (RAGE). AGE precursors such as
methylglyoxal (MG) can also activate RAGE. Endogenous MG synthesis increases in parallel
with hyperglycemia in vivo. Postprandially, the absorbed and endogenously generated AGEs and
MG act synergistically to decrease vascular function through direct NO scavenging or
increased oxidative stress. Part of these effects can be counteracted by benfotiamine (BT),
a liposoluble vitamin B1 derivative with much higher bioavailability than thiamine. BT,
commonly used in the treatment of diabetic neuropathy, is a transketolase activator that
directs glucose substrates to the pentose phosphate pathway. Thus, it blocks several
hyperglycemia-induced pathways, one of them being endogenous AGE and dicarbonyls formation.
We have recently shown that a three day pretreatment with benfotiamine can prevent
postprandial ED in T2DM (Stirban et al, Diabetes Care, 2006).
This study aims at investigating the effects of a chronical treatment with benfotiamine (900
mg/day for 6 weeks) on parameters of endothelial function and autonomic neuropathy in
fasting and postprandial state in people with T2DM.
We will therefore investigate 30 people with type 2 diabetes mellitus in a randomized,
cross-over, double blind, placebo-controlled design. Pre- and postprandial endothelial
dysfunction (flow mediated dilatation -ultrasound- and reactive hyperemia -laser-doppler-)
will be investigated before and after chronical treatment with benfotiamine. Investigations
will be performed in fasting state as well as 2,4 and 6 hours postprandially.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Prevention
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