Coronary Artery Disease Clinical Trial
Official title:
A Phase 1b, Randomized, Single Blind Study Evaluating RESTEN-MP in Subjects With Focal de Novo Stenosis
The process of re-narrowing of a coronary artery following a revascularization procedure
such as angioplasty, begins at the time of the procedure. Restenosis has long been
considered a major problem for effective long-term interventional success. This often
results in repeated procedures to deal with recurrent stenosis (or restenosis) of the
original targeted vessel.
There is a substantial body of literature suggesting that local MYC protein production in
the injured coronary artery is a major stimulus and potential cause of restenosis that
appears after stent placement. This study is based upon the hypothesis that stopping MYC
protein production in the vessel has will help reduce restenosis (vessel re-narrowing).
AVI BioPharma Inc., has utilized its proprietary antisense chemistry to design a drug that
interferes with MYC production.
This study will evaluate the safety, pharmacokinetics and potential effectiveness of a
single intravenous slow-push dose of RESTEN-MP at the time of stent placement to reduce
in-stent restenosis following balloon angioplasty and stent placement. The post-dose
follow-up period is up to six-months.
The process of restenosis following a revascularization procedure, begins at the time of
percutaneous coronary intervention (PCI). Restenosis has long been seen a major impediment
of effective long-term interventional cardiology, necessitating repeated procedures to deal
with in situ recurrent stenosis of the original targeted vessel. The restenosis rates are
between 30 to 50% of patients treated with balloon angioplasty and between 15 to 30% of
patients treated with bare metal stents. There is currently high enthusiasm for drug-eluting
stents already approved for the market and which have an overall restenosis rate of <3% as
reported in published reports for most clinical trial patient populations. However, there
are subsets of patients (e.g., diabetic patients and patients with diffuse small vessel
disease) that have restenosis rates around 10% despite the use of drug-eluting stents. It is
probably too early to conclude that the currently approved drug-eluting stents are a panacea
to relieve coronary arterial obstruction due to atherosclerotic heart disease. In fact, with
the increased usage of the current drug-eluting stents on the market, there are reports of
problems such as late stent malposition, subacute and late thromboses, and aneurysm
formations due to the vessel toxicity associated with this method of treatment. There
remains a definite need for a simple, safe and durable solution to restenosis.
The development of devices such as intravascular ultrasound has led to a greater
understanding of restenosis mechanisms, especially after coronary artery stenting. It is
presumed that the pathogenesis of coronary artery restenosis after a revascularization
procedure entails two major processes. The first component (viz., recoil and remodeling)
involves the mechanical collapse and constriction of the treated vessel; however, coronary
stents provide luminal scaffolding that eliminates recoil and remodeling. The second
component of coronary artery restenosis after a revascularization procedure is the
endothelial response to injury. Whereas, the former focus in modulating the
pathophysiological mechanisms involved in restenosis centered mainly on inhibition of
platelet aggregation and function, current targets of pharmaceutical agents for this
condition have shifted to inhibitors of the cell cycle, smooth muscle cell proliferation and
migration, synthesis of extra-cellular matrix, and inflammatory mediators. Many different
agents are currently being evaluated in pre-clinical and clinical studies.
AVI-4126, the active ingredient of RESTEN-MP, is a proprietary antisense drug designed to
interfere with the ability of human <c-myc> gene to translate mRNA into MYC protein.
Slow-push intravenous administration of RESTEN-MP in pharmacological doses in the restenosis
porcine model prevented subsequent in-stent stenosis.
In addition to the standard safety assessments, assessments of the potential therapeutic
value of RESTEN-MP as a neointimal hyperplasia inhibitor include late loss between the time
of stent placement and 6 months thereafter.
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Allocation: Randomized, Endpoint Classification: Safety Study, Intervention Model: Single Group Assignment, Masking: Single Blind, Primary Purpose: Treatment
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