Preclinical Restenosis Models: Challenges and Successes

Touchard, Arturo García; Schwartz, Robert S.

doi:10.1080/01926230500499407

Cited by 50 publications

(36 citation statements)

References 89 publications

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“…Although the porcine coronary model seems to represent the human coronary artery response to stenting, mimicking several clinical conditions, including thrombosis and neointimal formation, 20 it does not precisely simulate human in-stent restenosis. 18,20 An important point in the present model is that stent implantation was performed in normal porcine coronary arteries, whereas in humans, much of the stent would be in contact with atheromatous plaque and not with media. Furthermore, in the present study the extent of in stent stenosis was examined only at 28 days after stent implantation; for example, longer follow-up should be performed to assess the effect of bindarit on arterial healing.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of In-Stent Stenosis by Oral Administration of Bindarit in Porcine Coronary Arteries

Ialenti

Grassia

Gordon

et al. 2011

ATVB

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Objective-We have previously demonstrated that bindarit, a selective inhibitor of monocyte chemotactic proteins (MCPs), is effective in reducing neointimal formation in rodent models of vascular injury by reducing smooth muscle cell proliferation and migration and neointimal macrophage content, effects associated with the inhibition of MCP-1/CCL2 production. The aim of the current study was to evaluate the efficacy of bindarit on in-stent stenosis in the preclinical porcine coronary stent model. Methods and Results-One or 2 bare metal stents (Multi-Link Vision, 3.5 mm) were deployed (1:1.2 oversize ratio) in the coronary arteries of 42 pigs (20 bindarit versus 22 controls). Bindarit (50 mg/kg per day) was administered orally from 2 days before stenting until the time of euthanasia at 7 and 28 days. Bindarit caused a significant reduction in neointimal area (39.4%, PϽ0.001, nϭ9 group), neointimal thickness (51%, PϽ0.001), stenosis area (37%, PϽ0.001), and inflammatory score (40%, PϽ0.001) compared with control animals, whereas there was no significant difference in the injury score between the 2 groups. Moreover, treatment with bindarit significantly reduced the number of proliferating cells (by 45%, PϽ0.05; nϭ6 group) and monocyte/macrophage content (by 55%, PϽ0.01; nϭ5-6 group) in stented arteries at day 7 and 28, respectively. These effects were associated with a significant (PϽ0.05) reduction of MCP-1 plasma levels at day 28. In vitro data showed that bindarit (10 -300 mol/L) reduced tumor necrosis factor-␣ (50 ng/mL)-induced pig coronary artery smooth muscle cell proliferation and inhibited MCP-1 production. Key Words: pharmacology Ⅲ restenosis Ⅲ stent Ⅲ bindarit I ncreasing evidence suggests that monocyte chemotactic protein (MCP)-1/CCL2 plays an early and important role in the formation of intimal hyperplasia and in-stent restenosis 1 by increasing macrophage accumulation and smooth muscle cell (SMC) proliferation and migration. 2,3 Deletion of the MCP-1 gene, blocking MCP-1 signaling or MCP-1 receptor CCR2 decreases neointimal hyperplasia after balloon-and stent-induced injury in several animal models. 4 -7 Similarly, catheter-based adenovirus-mediated antimonocyte chemoattractant gene therapy attenuates in-stent neointimal formation in monkeys. 8 These data suggest that an antiinflammatory/antiproliferative strategy targeting MCP-1 might be an appropriate and reasonable approach for the prevention of neointimal formation and in-stent restenosis. Conclusion-OurBindarit is a selective inhibitor of MCP-1/CCL2, MCP-3/ CCL7, and MCP-2/CCL8 synthesis 9 that shows potent antiinflammatory activity in a number of experimental models, including nephritis, arthritis, pancreatitis, and colitis, 10 -13 as well as reducing myocardial and renal dysfunction in swine renovascular hypertension. 14,15 Phase II clinical trials have shown that bindarit is well tolerated and significantly reduced urinary MCP-1 and albumin excretion in kidney disease. 10,16 Interestingly, we have already shown that oral administration of b...

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Section: Discussionmentioning

confidence: 99%

Inhibition of In-Stent Stenosis by Oral Administration of Bindarit in Porcine Coronary Arteries

Ialenti

Grassia

Gordon

et al. 2011

ATVB

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“…These approximations tend to be prolonged for drug-eluting stent systems and vary according to system design and elution or bioabsorption profiles. 160,186,199 atherosclerotic plaque is a contributory factor in vessel injury, given that compression and/or strut penetration of the plaque has been documented in up to 90% of angioplasties, which can further the potential for subsequent inflammation and cellular proliferation. 44,45 Concurrent with the initiating injury and in the following hours to days, thrombus formation occurs where there is endothelial denudation, exposed subintimal components, and exposed surfaces of the device.…”

Section: Pathophysiology Of Isr: Preclinical Clinical and The Influmentioning

confidence: 99%

“…Atherosclerotic and diabetic models are on the forefront of development, becoming more desirable for evaluating DES performance, although their standardization is lacking. Despite the inherent lesion variability that occurs with these models, 140,186 it is of value to evaluate DESs in an environment in which the primary cause for the vascular intervention, the underlying atherosclerotic lesion, is present. Furthermore, DES systems may affect not only the development of ISR but they also may impact the formation or progression of the local atherosclerotic lesion and, thereby, long-term device efficacy.…”

Section: Current Generation Des: Correlating Preclinical Studies and mentioning

confidence: 99%

“…75,79,133 The rates of vascular healing in rat carotid arterial and aortic models appear to parallel those of models utilizing larger species qualitatively; however, the vascular response in the rat has similar salient features as mice, including only sparse thrombus formation and fibrin deposition, minimal inflammation, and a lack of remodeling. 11,77,104,105,186 Murine models have promise for elucidating pathophysiologic mechanisms related to atherosclerosis and ISR; nonetheless, the cumulative shortcomings of these models warrant their careful application and critical interpretation. First, murine arteries suitable for the evaluation of ISR are mostly elastic, which are less prone to injury and have only modest neointimal responses following vascular injury when compared to muscular arteries.…”

Section: Rodentsmentioning

confidence: 99%

“…30,57,192 Nonetheless, the paucity of studies in nonhuman primate models utilizing either balloon angioplasty or stent implantation and the relative inconsistencies among studies are further shortcomings. 64,186 Model Selection, Application, and Limitations Each preclinical model of ISR has a unique set of attributes, assumptions, and limitations. Given that there is no single model that serves as a blanket ideal for investigations into ISR and drugs or devices designed for its treatment, each model discussed herein is appropriate in its own right for application to answer targeted questions relative to ISR.…”

Section: Swinementioning

confidence: 99%

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Preclinical Models of Restenosis and Their Application in the Evaluation of Drug-Eluting Stent Systems

Perkins

2010

Vet Pathol

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Coronary arterial disease (CAD) is the leading cause of death in the United States, the European Union, and Canada. Percutaneous coronary intervention (PCI) has revolutionized the treatment of CAD, and it is the advent of drug-eluting stent (DES) systems that has effectively allayed much of the challenge of restenosis that has plagued the success of PCI through its 30-year history. However, DES systems have not been a panacea: There yet remain the challenges associated with interventions involving bare metallic stents as well as newly arisen concerns related to the application of DES systems. To effectively address these novel and ongoing issues, animal models are relied on both to project the safety and efficacy of endovascular devices and to provide insight into the pathophysiology underlying the vascular response to injury and mechanisms of restenosis. In this review, preclinical models of restenosis are presented, and their application and limitation in the evaluation of device-based interventional technologies for the treatment of CAD are discussed.Keywords restenosis, stent, animal models, coronary artery disease Coronary artery disease (CAD) is the progressive accumulation of atherosclerotic plaque within the lumen of a coronary artery, with the typical result being luminal narrowing, reduced compliance of the vessel wall, and either a gradual reduction or a dramatic and sudden loss of blood supply to the myocardium. It is the leading cause of death in the United States, the European Union, and Canada, singly accounting for the death of 1 in 5 Americans. 117,185 In treatment options for symptomatic CAD, percutaneous coronary intervention (PCI) is the foremost modality, being based on the nonsurgical placement of a bare metallic scaffold, or stent, to prop open the artery to regain patency. However, there are drawbacks to coronary stenting, with restenosis being the Achilles' heel, accounting for a rate of failure up to 15 to 25%.18,124 Drug-eluting stents (DESs) have revolutionized PCI by effectively reducing restenosis rates to the single digits over standard bare metallic stents.DES systems combine mechanical and pharmacological approaches to assuage one or more events in the cascade that results in restenosis. These combination products consist of an intravascular scaffolding device that presents or releases single or multiple bioactive agents or pharmaceuticals into the bloodstream and arterial wall. Traditional DESs have consisted of a platform (stent), a carrier (usually a polymer), and an antirestenotic agent that is delivered locally to avert the need for high, systemically administered doses. The fundamental goal of the DES is to restore lumen patency while curtailing the diseased vessel's innate and often exuberant response to the implanted foreign material (stent) and to stent-induced injury. Despite the success of current DESs at achieving these goals, concerns have surfaced with their accruing clinical use. Such concerns pertain to vascular healing and late stent thrombosis, biocompat...

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Cardiovascular Toxicology and Its Evaluation

Gad

2015

Mammalian Toxicology

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Preclinical Restenosis Models: Challenges and Successes

Cited by 50 publications

References 89 publications

Inhibition of In-Stent Stenosis by Oral Administration of Bindarit in Porcine Coronary Arteries

Inhibition of In-Stent Stenosis by Oral Administration of Bindarit in Porcine Coronary Arteries

Preclinical Models of Restenosis and Their Application in the Evaluation of Drug-Eluting Stent Systems

Cardiovascular Toxicology and Its Evaluation

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