Type 2 Diabetes Clinical Trial
Official title:
L-Arginine and Endothelial Dysfunction in Type 2 Diabetic Patients
Patients with diabetes have dysfunction of the lining of the arteries which lead to impaired circulation in the small blood vessels. This is thought to be secondary to reduced chemicals in the blood viz: nitric oxide. This chemical is derived from an amino acid (protein) L-arginine. Therefore, the researchers investigated whether giving patients L-arginine (versus dummy powder) would improve the blood flow in the small blood vessels in the lower limbs of patients with damage to their nerves (neuropathy).
Peripheral neuropathy is one of the most common complications of diabetes mellitus (DM) with
a prevalence of around 30 - 45%. In addition, diabetic patients are at increased risk of
macrovascular disease, as well as other complications such as retinopathy and nephropathy.
The majority of patients will have developed peripheral neuropathy 10-20 years after the
onset of diabetes, which is an important cause of foot ulceration, Charcot joints,
amputation and increased morbidity and mortality. In view of this the cost to the National
Health Service in 1987 was a staggering £13.5 million. Therefore there is an urgent need for
prevention of diabetic neuropathy and its sequelae.
The exact pathogenesis of diabetic neuropathy is unclear, with both metabolic and vascular
factors having been implicated. Microvascular disease is possibly the initial event in the
development of diabetic complications. Microvascular disease may play an important role in
the causation and exacerbation of diabetic neuropathy. Histopathological studies have shown
thickening of vessel walls, hyperplasia of capillary endothelial cells and increased
plugging of vessels in neuropathic patients. Endothelial dysfunction is thought to be an
important initiating factor for the development of these complications. Endothelial
dysfunction is thought to develop as a consequence of changes in nitric oxide and cell
adhesion molecules in the plasma of diabetic patients. L-arginine is an amino acid, which is
the only source of NO in the body.
We therefore propose to study the efficacy of arginine supplementation ( this is available
over the counter as a food supplement) on endothelial function and other biomarkers of
impaired endothelial function. We hope with this study to demonstrate that L-arginine
supplementation will enhance nitric oxide availability, thereby improve the microcirculation
and subsequently improve peripheral nerve function. We will use surrogate markers to assess
the efficacy of L-arginine supplementation to show an improvement in diabetic complications
such as microalbuminuria in the urine, and TcPO2 in the skin of the lower limbs. In addition
microcirculation will be assessed using the Moor Laser Doppler flow machine and the
Radiometer TcPO2 device. Endothelial function will also be assessed indirectly by measuring
the cell adhesion molecules ICAM-1, VCAM-1, P-selectin and E-selectin. This will be
performed using standard ELISA techniques.
A total of 40 patients will be recruited for the study. Half will be randomised to taking
the food supplement L-arginine and half to placebo. At baseline all patient will have a
clinical assessment of their neuropathy status in the lower limb, blood pressure and BMI.
Fasting bloods for glucose, lipids profile, U&E's, FBC, CRP, cell adhesion molecules and
nitric oxide will be done at baseline and three months later at the end of the study. The
TcPO2 and micro-circulation will be assessed at baseline and also at three month.
Each of the twenty patients that is randomised to L-arginine will be given a tin containing
1 kilogram of the food supplement L-arginine. They are to take a spoonful (three grams) of
the L-arginine and dissolve it in a glass of sugar free cold drink of their choice such as
orange or lemon squash. They are to take it before food three times a day. The twenty
patient randomised to placebo will receive a tin containing one kilogram of placebo and the
instruction is as for the L-arginine group.
20 patients will receive L-arginine powder (3G TDS) and 20 patients will receive placebo,
lactose powder (3G TDS)
Clinical examination as part of routine care:
1. BMI, BMI will be calculated by weight/height (kg/m2).
2. Lying and standing blood pressure will be measured twice, in the right arm using
Dinamap™ (Critikon, UK), after resting for 10 minutes. Hypertension will be defined
according to WHO criteria (systolic blood pressure (sBP) >140 mm Hg and/or diastolic
blood pressure (dBP) >90 mm Hg or if the patient is on current antihypertensive
treatment.
3. Overnight microalbumin excretion rate.
4. Neuropathic Disability Score and Vibration Perception threshold.
Additional examination:
1. TcPO2 of the right foot.
2. Micro-circulation of the right foot using Moore Laser Doppler iontophoresis.
Blood from an antecubital vein will be collected after an overnight fast and after resting
for fifteen minutes in the supine position for:
1. as part of routine care - FBC, U&E's, fasting glucose, glycated haemoglobin, fasting
lipid profile
2. additional blood test - CRP, cell adhesion molecules, nitric oxide
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
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