Oral Everolimus Inhibits In-Stent Neointimal Growth

Farb, Andrew; John, Michael C.; Acampado, Eduardo; Kolodgie, Frank D.; Prescott, Margaret F.; Virmani, Renu

doi:10.1161/01.cir.0000033973.06059.04

Cited by 153 publications

(101 citation statements)

References 27 publications

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“…LBS and PES are the two most common DES in clinical practice. As mentioned before, the neointimal proliferation pharmacological mechanisms differ significantly between LBS and PES [8][9][10]. Thus, it is reasonable to hypothesize that LBS and PES would have different clinical outcomes, especially over a long period of time.…”

Section: Discussionmentioning

confidence: 91%

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Long time clinical outcomes of limus-eluting stent versus paclitaxel-eluting stent in patients undergoing percutaneous coronary artery intervention: A meta-analysis of randomized controlled clinical trials

2014

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Background: The meta-analysis was aimed to compare the long time (> 2 year) clinical outcomes of limus-based stents (LBS) and paclitaxel-eluting stents (PES). LBS and PES are two kinds of most common coronary artery stents in clinics. Methods: Electronic data bases of PubMed, Cochrane, and EMBASE were searched. We included randomized controlled clinical trials (RCT) comparing LBS and PES with long time clinical outcomes. Methodological quality of eligible trials was assessed using "risk of bias" tool. The efficacy endpoints included target lesion revascularization (TLR), target vessel revascularization (TVR), and stent thrombosis (ST), and the safety endpoints included all cause death, cardiac death, and myocardial infarction (MI). Odds ratios (OR) and OR = 0.59, TVR: OR = 0.63, ST: OR = 0.55,) and a lower rate of MI (OR = 0.67, . Subgroup analysis showed that both everolimus-eluting stents and sirolimus--eluting stents had better clinical outcomes compared with PES. The comparisons of 3, 4 and 5 year follow-up results revealed that the clinical outcomes of PES were non-inferior to those of LBS but LBS was associated with reduced risk of MI and ST at 3 years. Conclusions: LBS is associated with better clinical outcomes at 2 years. Both LBS and PESshowed similar efficacy and safety at long time period. (Cardiol J 2014; 21, 3: 211-219)

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Section: Discussionmentioning

confidence: 91%

“…Sirolimus is a potent immunosuppressant agent, which induces expression of the cyclin-dependent kinase inhibitor, p27 kip1, blocks the cell cycle at the G1 to S phase [9]. Everolimus can also exert anti-proliferative effect by inhibiting cell proliferation and inducing cell cycle arrest in the late G1 stage [10].…”

Section: Introductionmentioning

confidence: 99%

Long time clinical outcomes of limus-eluting stent versus paclitaxel-eluting stent in patients undergoing percutaneous coronary artery intervention: A meta-analysis of randomized controlled clinical trials

2014

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“…Small-scale neointimal formation is also reported in normocholesterolemic rabbits (0.1370.03 mm). 29 This difference might be because hypercholesterolemic animals were used in the present study. Although the appropriate animal model for evaluation of experimental in-stent restenosis is uncertain, the hypercholesterolemic non-human primate model might have an advantage over normocholesterolemic nonprimate animal models, because (1) adequate degrees of neointimal hyperplasia develop after stenting and (2) vascular inflammatory and proliferative responses to injury in non-human primates are presumed to be closer to those in humans than other nonprimate models.…”

Section: Discussionmentioning

confidence: 92%

Antimonocyte chemoattractant protein-1 gene therapy reduces experimental in-stent restenosis in hypercholesterolemic rabbits and monkeys

et al. 2004

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In-stent restenosis results exclusively from neointimal hyperplasia due to mechanical injury and a foreign body response to the prosthesis. Inflammation mediated by monocyte chemoattractant protein-1 (MCP-1) might therefore underlie in-stent restenosis. We recently devised a new strategy for anti-MCP-1 gene therapy by transfecting an Nterminal deletion mutant of the MCP-1 gene into skeletal muscles. We used this strategy to investigate the role of MCP-1 in experimental in-stent restenosis in hypercholesterolemic rabbits and monkeys. Transfection of the mutant MCP-1 gene suppressed monocyte infiltration/activation in the stented arterial wall and markedly reduced the development of neointimal hyperplasia. This strategy also suppressed local expression of MCP-1 and inflammatory cytokines. Therefore, inhibition of MCP-1-mediated inflammation is effective in reducing experimental in-stent restenosis. This strategy might be a useful form of gene therapy against human in-stent restenosis.

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“…33 Previous studies of rapamycin-or everolimusimpregnated stents in animal models have shown that, compared to controls, local drug delivery inhibited within-stent stenosis or intimal hyperplasia by approximately 50%, but not much more. [34][35][36] Clinical trials with rapamycin-impregnated coronary stents have found within-stent restenosis to be nearly completely eliminated, indicating that atherosclerotic lesions may be more sensitive to rapamycin than normal animal arteries. 37 Human leukocytes are more sensitive to the antiproliferative effect of rapamycin than porcine leukocytes, 38 and the clearance of systemic rapamycin is slower in humans than in other species.…”

Section: Discussionmentioning

confidence: 99%

Dose-dependent Inhibition of Myointimal Hyperplasia by Orally Administered Rapamycin

Uchimura

Perera

Fujitani

et al. 2004

Annals of Vascular Surgery

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Myointimal hyperplasia (MIH) after vascular intervention is a major problem. Recent reports describing elimination of within-stent restenosis by means of rapamycin-eluting stents prompted us to examine the effect of systemic oral rapamycin on MIH induced by arterial trauma. We studied the effect of oral rapamycin on MIH after rabbit aorta balloon injury. Thirty-five New Zealand white rabbits (2.5-3 kg) had aortic injury and were given either no rapamycin (control), 0.1 (low dose) rapamycin mg/kg/day, or 0.4 mg/kg/day (high dose). Rapamycin was started 1 week before injury and continued for 3 (4 weeks total) or 6 weeks (7 weeks total) post-injury. Sections were analyzed to measure aortic intima/media area ratios (I:M) at either 3 or 6 weeks. At 3 weeks, the I:M (mean ± SD) for controls was 0.53 ± 0.1; for low dose, 0.17 ± 0.13; and for high dose, 0.24 ± 0.07 (p < 0.001 vs. control). At 6 weeks, the I:M for controls was 0.52 ± 0.12; for low dose-4 weeks, 0.29 ± 0.15; low dose-7 weeks, 0.33 ± 0.07; and high dose-4 weeks, 0.47 ± 0.16. At 6 weeks only the difference between the low dose-4 weeks and control I:M ratios was significant (p = 0.018). The results confirm earlier studies showing that systemic rapamycin inhibits MIH after arterial injury when drug therapy is started before injury. Therapy for 3 or 6 weeks after injury yields similar inhibition, indicating that exposure to the drug early in the response to injury is more important than prolonged exposure. We observed a paradoxical relation between dose and degree of MIH inhibition, with the low dose being more effective than the high dose at both time intervals studied. Overall, the results suggest that oral rapamycin therapy might be a useful adjunct to clinical interventions at risk for development of MIH.

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Oral Everolimus Inhibits In-Stent Neointimal Growth

Cited by 153 publications

References 27 publications

Long time clinical outcomes of limus-eluting stent versus paclitaxel-eluting stent in patients undergoing percutaneous coronary artery intervention: A meta-analysis of randomized controlled clinical trials

Long time clinical outcomes of limus-eluting stent versus paclitaxel-eluting stent in patients undergoing percutaneous coronary artery intervention: A meta-analysis of randomized controlled clinical trials

Antimonocyte chemoattractant protein-1 gene therapy reduces experimental in-stent restenosis in hypercholesterolemic rabbits and monkeys

Dose-dependent Inhibition of Myointimal Hyperplasia by Orally Administered Rapamycin

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