Diabetes Mellitus Clinical Trial
Official title:
Effect of Rosuvastatin in the Mobilization of Endothelial Progenitor Cells and Graft Vascular Function Following Creation of Arteriovenous Fistula in Diabetic Patients With Chronic Renal Failure
Background Arteriovenous (AV) fistula is the most common vascular access for long-term
hemodialysis in the end-stage renal disease (ESRD) patients. About 25% of these patients are
diabetes mellitus. However, the effects of hyperglycemia on the vascular function of
arteriovenous fistula are still remained unclear. Studies have shown that blood flow in the
AV fistula is significantly reduced in patients with diabetes mellitus. Diabetic patients
also require a longer period of time for the maturation of AV fistula, and have slightly
higher complication rate than non-diabetic patients. Statins have been widely shown to
mediate several important pleiotropic effects in the improvement of vascular endothelial
dysfunction, attenuation of inflammatory responses, stabilization of atherosclerotic plaques,
inhibition of vascular smooth muscle proliferation, and modulation of procoagulant activity
and platelet function.Our experimental studies in diabetic animals demonstrate that
administration of a water-soluble statin rosuvastatin significantly improves the fistula
flow, vascular function and luminal dilatation of AV fistula in diabetic rats by suppression
of vascular oxidative stress and inflammatory load.
Study hypothesis The central hypothesis of this research project is rosuvastatin mediates
pleiotropic protective effect on vascular endothelial function and suppresses the regional
pro-inflammatory reaction in the vasculature, therefore administration of rosuvastatin during
the perioperative period of creation of native AV fistulas in diabetic patients with ESRD may
potentiate the vascular function and reduce the primary failure rate of AV fistulae.
Background In Taiwan, diabetic nephropathy is the second most common cause of end-stage renal
disease (ESRD), but diabetic patients engender 12% more expense for care of dialysis than
non-diabetic patients. ESRD patients with diabetes are also more frequently hospitalized due
to problems such as failure of vascular access. Hemodialysis necessitates the placement of an
arteriovenous (AV) fistula, which involves a direct anastomosis of the radial/brachial artery
and cephalic vein. In the United States, procedures for creating the AV fistula and treatment
of the related complication account for over 20% of hospitalizations of dialysis patients and
cost about US$100 million annually. Two major hurdles in establishing a useable and patent AV
fistula for dialysis are primary failure (failure of fistula to mature adequately for
dialysis) and long-term survival of the vascular access. The reported primary failure rate
varies from 20 to 50%. It has been shown that reduction of blood flow (>15% drop of flow over
time) is the most critical factor for premature failure of AV fistula. Although blood flow in
the venous site of AV fistula is also determined by the surrounding draining veins, blood
pumped from the arterial site is the most important factor in maintaining sufficient fistula
blood flow. However, very limited of studies have reported the effect of arterial blood flow
on the function and patency of AV fistula. More evidences have shown that progressive failure
of AV fistula after long-term use is due to the development of thrombosis (~80%) and stenosis
(~20%). The mechanisms that underlie the failure of AV fistula are still poorly understood
and there are very few, if any, specific therapeutic approaches that can increase the
lifespan of these fistulas. Therefore, there is the critical need for experimental studies
that seek to understand the basic mechanisms of primary failure and progressive failure of
the AV fistula in diabetes mellitus.
Creation of an AV fistula is the most common vascular access for ESRD patients, who require
long-term hemodialysis. In Taiwan, about 25% of these patients have underlying diabetes
mellitus. However, the effects of hyperglycemia on the vascular function of arteriovenous
fistula are still remained unclear. Studies have shown that blood flow in the AV fistula is
significantly reduced in patients with diabetes mellitus. Diabetic patients also require a
significantly longer period of time (2 more months) for the maturation of AV fistula, and
have slightly higher complication rate than non-diabetic patients. Diabetes mellitus has been
shown as an independent risk factor of reduced blood flow in the native vessel arteriovenous
fistula. Compared with patients without diabetes access blood flow was significantly lower in
patients with diabetes mellitus (788±580 vs 1054±681 ml/min, P = 0.002). Patients with
diabetes mellitus required a longer time until first use of their AV fistula than did
patients without diabetes (4.4±2.9 vs 2.9±1.6 months, respectively, P= 0.02). AV
access-related complications and need of re-intervention were higher in these patients. Most
recently, Previous study identified that risk for reduced primary patency of AV fistula was
increased by diabetes (Hazard Ratio, 1.54; 95% Confidence Interval, 1.14-2.07). Presence of
diabetes is also a strong independent predictive factor for reduced initial intra-access
blood flow within 6 months after creation of AV fistula (OR 3.5, P = 0.001). However, there
is currently very limited effective therapeutic strategy in the prevention of loss of primary
patency and improvement of life expectancy of AV access in patients with diabetes.
3-Hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase inhibitors (statins) are one of the
most commonly prescribed agents in controlling hyperlipidemia. Apart from their serum
lipid-lowering properties, statins have been widely shown to mediate several important
pleiotropic effects, such as improvement of vascular endothelial dysfunction, attenuation of
inflammatory responses, stabilization of atherosclerotic plaques, inhibition of vascular
smooth muscle proliferation, and modulation of procoagulant activity and platelet function.
Among these pleiotropic effects, the protective effects on vascular endothelial function have
mostly been highlighted. In clinical settings, statins improve cardiovascular outcomes of
patients with atherosclerosis even in the population of normal plasma cholesterol level. The
improvement in cardiovascular outcomes is well correlated with improved endothelial function
by upregulation of endothelial nitric oxide synthase (eNOS) expression and nitric oxide (NO)
bioavailability following treatment with statins. At subcellular levels, statins stabilize
the eNOS messenger ribonucleic acid (mRNA), enhance eNOS enzymatic activity via phosphatidyl
inositide (PI)3 kinase signaling pathway, reduce inflammatory responses in the vasculature,
inhibit Rho isoprenylation and suppress oxidized- LDL-induced endothelin-1 expression.
Statins have also been characterized to enhance re-endothelialization of damaged vascular
endothelium by stimulating pre-existing endothelial cells and by mobilizing bone
marrow-derived endothelial progenitor cells (EPCs). Collectively, stains restore vascular
endothelial function and mediate vascular protective effects that are independent from their
lipid-lowering effects. Although the beneficial pleiotropisms by statins are well documented
in a variety of endothelial dysfunctional disorders, their potential therapeutic effects in
maintaining a healthy, usable AV fistula in subjects with diabetes mellitus have been
previously demonstrated.
According to the knowledge of applicant, there was no published randomized control clinical
study prospectively investigated the vascular protective effect of statins on the
establishment of AV fistula in patients with chronic kidney disease (CKD) or ESRD. A
long-term (up to 987 days) case-control study suggested that patients receiving statin
therapy were associated with significantly higher overall primary patency rate of AV fistula
after 1 year (81.7 vs 66 %) and after 2 years (71.5 vs 39.1%).
During the past national science council (NSC)-funded years 2009-2011, the applicant
undertook experimental study in rats with streptozotocin-induced diabetes, in which an AV
fistula was created in each control and diabetic animals. The diabetic rats received either
placebo or rosuvastatin (10 mg/kg/d) in chow for a period 18 days (3 days before creation of
AV fistula and 14 after operation). Circulating cluster of differentiation (CD)133+/vascular
endothelial growth factor receptor (KDR)+ EPCs were determined 2 weeks after creation of AV
fistula using flow cytometry. Vascular function of AV fistula was assessed by isometric force
testing. The expression of pro-inflammatory genes (iNOS and NADPH oxidase) and generation of
superoxide anions in the fistula were examined. The results showed that number of EPCs was
reduced in diabetic rats, and rosuvastatin significantly increased numbers of circulating
EPC. Reduced blood flow and impaired endothelium-dependent relaxation in the AV fistula of
animals with diabetes was significantly potentiated following treatment with rosuvastatin.
Rosuvastatin also attenuated the expression of iNOS and NADPH oxidase, and generation of
superoxide anions in the fistula tissues isolated from diabetic rats. These findings provide
the first and very important evidence demonstrating that rosuvastatin improves blood flow and
endothelial function of AV fistula in subjects with diabetes mellitus by attenuating the
activity of pro-inflammatory genes and generation of superoxide anions in the remodeled
vasculature. Based on these fascinating and encouraging findings, the applicant proposes to
undertake clinical study in translating these experimental results to diabetic patients with
CKD, who are scheduled to creation of AV fistula for further hemodialysis.
Central Hypothesis and Specific Aims
The central hypothesis of this research project is rosuvastatin mediates pleiotropic
protective effect on vascular endothelial function and suppresses the regional
pro-inflammatory reaction in the vasculature, therefore administration of rosuvastatin during
the perioperative period of creation of native AV fistulas in diabetic patients with ESRD may
potentiate the vascular function and reduce the primary failure rate of AV fistulae. Here,
the applicant proposes to undertake a three-year research project investigating the
therapeutic potential of rosuvastatin in the establishment of AV fistula in patients with
diabetes mellitus. The applicant opts to test the proposed effect of rosuvastatin in diabetic
patients. The long-term aim of this project is to develop a clinical feasible,
endothelium-targeted therapeutic strategy for a durable AV fistula in human subjects
necessitates hemodialysis. To achieve these research goals the applicant proposes studies
with following specific aims:
1. Administration of rosuvastatin protects the endothelial function in the AV fistula and
restores the blood flow rate in the shunt of diabetic patients with ESRD, thereby
improves the primary patent rate and early maturation of these fistulas.
2. Administration of rosuvastatin improves the vascular function of AV fistulas in diabetic
patients with ESRD, therefore reduces the overall shunt-related complication rate and
the requirement for surgical re-interventions.
3. Administration of rosuvastatin is associated with reduction of the systemic
pro-inflammatory response and oxidative stress (levels of proinflammatory cytokines and
other mediators in the circulation) in diabetic patients with ESRD. On the other hand,
administration of rosuvastatin may mobilize the bone marrow-derived EPCs into systemic
circulation, and the number of these circulating endothelial progenitors may provide
prognostic value to the outcomes of AV fistula.
4. Administration of rosuvastatin reduces the overall perioperative cardiovascular and
other morbidities in diabetic patients with ESRD.
5. Administration of rosuvastatin does not increase the incidence of statin-related
complications (such as myopathy, abnormal liver function and neurologic deficit) in
diabetic patients with ESRD.
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