Insulin Resistance Clinical Trial
Official title:
Does Modulating the Gut Hormones, Incretins, Modify Vascular Function, Thereby Reducing the Risk of Vascular Complications in Insulin Resistant Individuals?
Animal models have demonstrated that incretins have a glucose-independent effect on vascular
perfusion, and there is limited evidence that incretins may enhance endothelial function in
healthy subjects. Currently DPP-4 inhibition increases levels of the endogenous incretin
Glucagon-like Peptide 1 (GLP-1) and is licensed for the treatment of hyperglycaemia in type
2 diabetes. They are positioned as third or even fourth line therapy after metformin,
sulphonylureas ± glitazones, however recent analyses of cardiovascular outcomes in
glitazones and sulphonylureas suggest at best they do not reduce cardiovascular endpoints,
and may increase some outcomes. If the vascular benefits suggested in animal models are
realised in humans this should see the DPP-4 inhibitors moved to second line and possibly
1st line.
In order to realise the potential the investigators would like initially to demonstrate
increases in vascular perfusion and function in a placebo controlled trial using accurate
surrogates for vascular function in patients with insulin resistance and obesity.
The investigators hypothesis is that by increasing incretin activity in insulin resistant
states the investigators will lower capillary pressure and improve microvascular function,
which will be accompanied by a reduction in macular thickness (by reducing macular oedema)
and microalbuminuria, recognised surrogates for early diabetic retinopathy and renal failure
respectively.
After food intake, insulin secretion depends not only on the degree of glycemia, but also on
the secretion and insulinotropic effect of the gut hormones, gastric inhibitory polypeptide
(or glucose-dependent insulinotropic polypeptide; GIP) and glucagon-like polypeptide 1
(GLP-1), known as incretins. Normally, the incretins GLP-1 and GIP are responsible for as
much as half of the glucose-dependent insulin release after food ingestion. In obesity and
patients with insulin resistance the GIP and GLP-1 responses to a mixed meal are impaired
and in the latter case are related to the degree of insulin resistance[1, 2]. In subjects
with type 2 diabetes, the insulin releasing action of GIP is reduced, however GLP-1
responsiveness is normal [3]. This has resulted in the successful use of therapies either
increasing endogenous GLP-1 (by inhibiting its breakdown by dipeptidyl-peptidase IV; DPP-IV)
or administering synthetic GLP-1 in order to treat the hyperglycaemia of type 2 diabetes. It
is widely recognised, however, that diabetes and insulin resistance adversely impacts
vascular function, independently of hyperglycaemia, resulting in premature ischaemic heart
disease, stroke, retinopathy leading to blindness, renal failure and peripheral vascular
disease.
Dysfunction of the vasculature, both in macro- and microcirculation, is well described in
people with diabetes. Further, altered vascular function has been demonstrated in
individuals predisposed to diabetes, for example in subjects with fasting hyperglycaemia
[4], impaired glucose tolerance [5], in women with previous gestational diabetes [6], in
obese individuals [7, 8] and in 3 month old infants of low birth weight [9]. Unpublished
data from our own laboratory demonstrates capillary pressure is positively associated with
fovea (macular) thickness, the thickening of which is an early pre-clinical sign of macular
oedema, in healthy subjects with a wide range of body mass index (BMI) that varies from the
lean to the morbidly obese (20.0 - 46.6 m2/kg). In patients with established retinopathy
treatments that reduce fovea thickness are associated with improvements of visual acuity,
whereas increasing fovea thickness was associated with a trend towards poorer eyesight [10].
Microangiopathy appears to precede the development of cardiovascular events in those with
diabetes [11], and changes in microvascular function appear to precede this microangiopathy
[12, 13]. Therapies that improve clinically detectable evidence of microangiopathy, such as
microalbuminuria, have demonstrated improvements in cardiovascular outcomes independent of
their antihypertensive effect [14-16]. In the latter of these studies there was a linear
relationship between reduction in albumin excretion rate and cardiovascular outcome that was
independent of the intervention suggesting that microangiopathy is integral to the
aetiopathogenesis of cardiovascular disease. Thus it may be possible that by improving
vascular function, for example lowering capillary pressure, we may be able to prevent or
delay the progression of clinical vascular complications (eg macular oedema and increased
risk of cardiovascular disease) in individuals with or at risk of diabetes. In these cases
the administration of therapy that improves both glycaemic control and vascular function
will be of enormous health benefit.
There is growing evidence that GLP-1 may have such favourable effects on vascular function,
independent of its glucose lowering effects. GLP-1 administration in animal models has been
shown to mediate endothelial dependent relaxation in the rat pulmonary artery [17, 18],
which was attenuated in the presence of a nitric oxide synthase blocker suggesting the
involvement of nitric oxide (NO) in mediating its vascular effects. This is supported by
observations that GLP-1 promotes NO-dependent relaxation of mouse mesenteric arteries [19].
This does vary by vascular bed, causing endothelial independent relaxation, via the GLP-1
receptor, in femoral arteries [20] but has no impact on rat aorta isolates [17]. GLP-1 is
also protective against ischaemia-reperfusion injury in isolated rat hearts [19, 21-24] and
has renoprotective (reducing proteinuria and microalbuminuria) effects, in addition, to the
cardio protective effects in Dahl salt sensitive hypertensive rats [25]. Whether these
effects are mediated directly via the GLP-1 receptor is unclear, as the vasodilatory effects
have been observed to be both dependent[20] and independent [19] of the GLP-1 receptor. In
the latter of these studies GLP-1(9-36), which is the product from the degradation of GLP-1
by dipeptidyl peptidase-IV (DPP-IV), mediated relaxation of mouse mesenteric arteries [19].
Thus it is clearly evident that GLP-1 acts as a vasodilator and has cardio protective
properties.
Work in humans is still at a more embryonic stage, although the literature looks similarly
promising. Acute administration of GLP-1 increases flow mediated dilatation (endothelial
dependent) in type 2 diabetic male subjects with coronary artery disease but had no
significant effect on young healthy, lean male subjects[26]. In a broader general population
sample aged 18-50, GLP-1 does improve forearm blood flow (approx 30% increase) and augments
endothelial dependent forearm blood flow response to acetylcholine (approx 40% increase)
[27]. Conversely, endothelial independent function is not influenced by the acute
administration of GLP-1 in either diabetic or healthy individuals [26, 27]. GLP-1 infusions
have also been shown to improve regional and global left ventricular function when
administered within 6 hours of an acute myocardial infarction and improve systolic function
after successful primary angioplasty in those with severe left ventricular dysfunction [28].
Much work has been completed using direct administration of a GLP-1 mimetic, however, in
clinical practice, patient tolerability of repeated subcutaneous injections limits
utilisation in the early stages of diabetes. There is little work to date exploring the role
of DPP-IV inhibition on vascular function. It is reasonable to assume that the effects of
DPP-IV inhibitors (the "gliptins") will not be as impressive as direct GLP-1 administration,
as lower levels of GLP-1 are achieved, however longer term therapy is more tolerable and
acceptable, due to their simple oral administration and good side-effect profile. It is
crucial, therefore, to determine whether these agents prompt clinically relevant
improvements in vascular function and thereby attenuate the inevitable cardiovascular
decline observed in insulin resistance, and this would necessarily alter current prescribing
pathways and guidelines.
Study Question
This study aims to explore the effects of the DPP-IV inhibitor, vildagliptin, on a range of
macro- and microvascular parameters. Specific hypotheses to be tested include:
1. increased incretin activity by administration of the DPP-IV inhibitor vildagliptin will
lower capillary pressure and improve microvascular function (skin maximum microvascular
blood flow, endothelial dependent and independent function) in insulin resistant
individuals.
2. improved microvascular function will which will be accompanied by a reduction in
macular thickness (by reducing macular oedema) and microalbuminuria, recognised
surrogates for early diabetic retinopathy and renal failure respectively.
3. administration of vildagliptin will improve macrovascular function (flow mediated
dilatation and arterial stiffness) in insulin resistant individuals.
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