Type 2 Diabetes Mellitus Clinical Trial
Official title:
Effect of Normalization of Fasting Glucose by Intensified Insulin Therapy on the Incidence of Restenosis After Peripheral Angioplasty in Patients With Type 2 Diabetes.
Primary objective of the study is to test whether an intensified insulin therapy
incorporating the target of normal fasting glucose (<5.5 mmol/L) and glycated hemoglobin
<6.5% is able to halve the incidence of angiographic restenosis at 6 months (expected rate
45%, to be reduced at 15%) after peripheral angioplasty compared with standard care to
achieve a glycated hemoglobin <7.0% in patients with type 2 diabetes and limb ischemia.
Secondary objectives include the identification of markers associated with, and predictive
of, restenosis and the investigation of the underlying pathophysiological background, with
specific focus on the role of nitric oxide (NO), mechanisms of endothelial
activation/apoptosis, inflammation and matrix remodeling risk profiles, candidate gene
polymorphisms and endothelial progenitor cells evaluation.
Methodology: This is a randomized, open-label, clinical trial comparing two regimens of
insulin therapy having as an outcome measure the incidence of angiographic restenosis at 6
months after peripheral angioplasty. Seventy consecutive patients with type 2 diabetes and
peripheral arterial disease undergoing peripheral angiography and subsequent angioplastic
procedure will be studied. Patients will be treated by intensive insulin therapy, based on
three pre-prandial administrations of regular insulin or short acting insulin analogues
combined with the long-acting insulin analogue glargine or standard care based on once-daily
insulin and oral antidiabetics agents. Patients randomized to the intensive insulin therapy
arm will be educated and followed up with daily measurements of fasting glucose and weekly
phone contacts with the target of fasting glucose <5.5 mmol/L (99 mg/dl) to obtain glycated
hemoglobin <6.5%. The control arm will be followed to achieve a target of glycated
hemoglobin <7.0%. Life style recommendations, including diet and physical activity program,
will be the same for the two arms. All patients will undergo three visits with physical
examination and blood sampling, at baseline and at 2, 4 and 6 months after angioplasty.
Moreover, patients on normal fasting glucose arm will be monitored by phone on weekly basis
in order to test their adherence to therapeutic target.
The principal objectives of this project are:
Objectives Primary Objectives
To determine the role of fasting normoglycemia achieved with long term (6 months)
intensified insulin therapy in:
- Reduction of angiographic restenosis (> or=50%) after peripheral angioplasty
- Increase in the rate of primary clinical success at follow-up defined as continued
relief of ischemic rest pain, reduction in severity of claudication with persistent
hemodynamic success and/or symptomatic improvement of at least one category according
to Rutherford criteria, healing of ulceration, and freedom from unplanned surgical
amputation or bypass surgery
- Definition of the beneficial effect of normoglycemia in insulin mediated nitric oxide
(NO) modulation of neointima formation through its action on inflammation and/or matrix
remodelling Secondary Objectives
- To determine whether fasting normoglycemia achieved with intensified insulin therapy is
able to reduce or avoid planned or unplanned major amputation as limb loss above the
metatarsal level and minor amputation, as transmetatarsal amputation or removal of more
distal parts of the lower extremity and/or the performance of less extensive amputation
than initially intended through 6 months
- To evaluate the reduction of Major Adverse Cardiovascular Event (MACE) defined as the
occurrence of death, or repeat target vessel revascularization
- To find new risk profiles of systematically detectable indices able to define the
patients at the highest risk to develop restenosis
- To correlate angiographic and clinical indices of restenosis with endothelial
activation/apoptosis, inflammation and matrix remodelling risk profiles
- To define the association of candidate genes variants and the degree of restenosis
- To understand the impact of fasting normoglycemia achieved with intensified insulin
therapy on endothelial progenitor cells isolation and gene expression involved in the
process of vascular repair and in the inhibition of neointimal hyperplasia
This is a randomized, open-label, clinical trial comparing two regimens of insulin therapy
(intensified insulin therapy vs standard care) to determine if fasting normoglycemia
achieved with intensified insulin therapy is able to reduce the incidence of angiographic
restenosis at 6 months after peripheral angioplasty.
Seventy consecutive patients with type 2 diabetes mellitus and peripheral arterial disease
(PAD) defined at angiographic evaluation and/or clinical manifestations, will be admitted to
our Institute to undergo PTA procedure. After the procedure, suitable patients will be
screened to enter the study.
One week following hospital discharge after PTA procedure, patients will return to the
Diabetology Outpatients Clinic to be randomly assigned to receive intensified insulin
therapy or standard care. Prestudy treatments could be diet alone, oral antidiabetic agents,
or once-daily insulin and oral antidiabetic agents.
Two groups will be evaluated
- Intensified insulin therapy: three administrations of regular insulin or short acting
insulin analogues before meals combined with long-acting insulin analogue glargine in
the evening. The treatment goal will be a fasting blood glucose level of 5.5 mmol/L (99
mg/dl) and a HbA1c<6.5% at the end of the follow-up.
- Standard care: treatment will be once-daily long-acting insulin and oral antidiabetic
agents to achieve HbA1c levels of < 7.0% at the end of the follow-up.
Routine visits will be scheduled after 1, 2, 4 weeks and then at 2, 4 and 6 months.
All patients will be asked to monitor blood glucose levels each morning and document
hypoglycemia and 1-day six point glucose profiles (before and 2 h after breakfast, lunch and
dinner) before each clinic visit.
In the intensified insulin therapy arm, patients will be contacted by telephone every week
to target fasting glucose levels at 5.5 mmol/L through a titrated regimen.
The following titration regimen will be followed, according with (48):
Mean of self-monitored FPG values Increase of long-acting insulin dosage (UI) >180 mg/dl
(>10 mmol/l) 8 140-180 mg/dl (7.8-10 mmol/l) 6 120-140 mg/dl (6.7-7.8 mmol/l) 4 100-120
mg/dl (5.6-6.7 mmol/l) 2 72-100 mg/dl ( 4.0-5.6 mmol/l) no changes <72 mg/dl (<4.0 mmol/l)
decrease 2 Ethics Approval The protocol is in accordance with the guidelines contained in
the "Declaration of Helsinki 2" and with the current national legislation.
The protocol, the site's informed consent form and any other written information provided to
the patients prior to any enrollment will be approved by the local Ethics Committee and the
principal investigator will take responsibility to ensure that this procedure will be
followed. If, during the study, it is necessary to amend the informed consent form, the
investigator will be responsible for ensuring the local Ethics Committees reviews and
approves these amended documents before to enter new subjects into the study.
Discomforts of patients included in the studies are in all cases mild and temporary. Risks
involved in participating in all the studies are limited. Considering the potential benefits
related to preventing restenosis after peripheral angioplasty in diabetic patients, we
believe that these investigations are justified.
Utilization of drugs in this project will be subject to Institutional and National Safety
Regulations to ensure the safety of workers and to prevent damage to the environment and
community.
Experimental design During the hospitalization period, before procedure, from patients
suitable to enter into the study, blood samples will be drawn before breakfast for
evaluation of plasma glucose, serum insulin and plasma FFA. Samples will be drawn to
evaluate gene polymorphisms, circulating endothelial progenitor cells isolation and to study
insulin-mediated nitric oxide signalling pathway.
At the time of angiographic and angioplastic procedure, blood samples will be drawn from
femoral arterial and venous districts for the evaluation of indices of endothelial
activation/apoptosis, inflammation and matrix remodelling. A venous sample will be taken for
endothelial progenitor cells isolation and gene expression evaluation.
After the procedure of peripheral angiography and angioplasty, in Outpatient Clinic, before
randomisation, all patients will perform a baseline physical examination and blood samples
to evaluate both the metabolic parameters to define the degree of glucose control and
indices of endothelial activation/apoptosis, inflammation and matrix remodelling and DNA
isolation.
At the time of this visit, patients will be randomly assigned to intensive insulin treatment
for 6 months or to standard care for glycemic control, added to their usual cardiovascular
treatment. A similar diet and physical activity program will be planned for both groups. At
2, 4 and 6 months, a physical examination and blood samples to evaluate both the metabolic
parameters to define the degree of glucose control and indices of endothelial
activation/apoptosis, inflammation and matrix remodelling will be repeated. Samples will be
drawn to evaluate circulating endothelial progenitor cells and to study insulin-mediated
nitric oxide signalling pathway and its modulation by prolonged strict fasting
normoglycemia.
After 6 months or before in the presence of symptoms, they will perform an angiographic
control and evaluated for the presence of restenosis. At this time, blood samples will be
drawn from femoral arterial and venous districts for the evaluation of indices of
endothelial activation/apoptosis, inflammation and matrix remodelling. A venous sample will
be taken for endothelial progenitor cells isolation and gene expression evaluation. During
the hospitalization period,blood samples will be drawn before breakfast for evaluation of
plasma glucose, serum insulin and plasma FFA.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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