Single-dose intramuscular administration of sustained-release Angiopeptin reduces neointimal hyperplasia in a porcine coronary in-stent restenosis model

M K Hong; K M Kent; F O Tio; M Foegh; R Kornowski; O Bramwell; S S Cathapermal; M B Leon

doi:10.1097/00019501-199702000-00006

Single-dose intramuscular administration of sustained-release Angiopeptin reduces neointimal hyperplasia in a porcine coronary in-stent restenosis model

Coron Artery Dis. 1997 Feb;8(2):101-4. doi: 10.1097/00019501-199702000-00006.

Authors

M K Hong¹, K M Kent, F O Tio, M Foegh, R Kornowski, O Bramwell, S S Cathapermal, M B Leon

Affiliation

¹ Department of Internal Medicine (Cardiology Division), Washington Hospital Center, Washington, District of Columbia, USA.

PMID: 9211050
DOI: 10.1097/00019501-199702000-00006

Abstract

Background: In-stent restenosis results primarily from neointimal hyperplasia. In a previous study we showed that continuous subcutaneous Angiopeptin infusion for 1 week significantly reduces neointimal hyperplasia in a porcine coronary overstretch in-stent restenosis model. The present study evaluated the relative efficacy of immediate-release and sustained-release Angiopeptin in the same model.

Methods: Thirty pigs (n = 10 in each group) were randomly assigned to three groups: controls receiving no Angiopeptin (Group 1); a sustained-release treatment group receiving one time intramuscular administration of 20 mg of Angiopeptin (Group 2); and a systemic treatment group receiving continuous Angiopeptin over a 1-week period via a subcutaneous osmotic pump (200 micrograms/kg total dose) (Group 3). One oversized Palmaz-Schatz stent (mean stent/artery = 1.25) was subsequently implanted in the left anterior descending coronary artery. The degree of neointimal reaction was evaluated 4 weeks later by angiography (maximal per cent diameter stenosis) and histology (maximal neointimal area corrected for injury score).

Results: A trend towards a reduction in diameter stenosis was observed by angiography, despite a similar degree of injury (25 +/- 17% in Group 1, 13 +/- 8% in Group 2, and 14 +/- 9% in Group 3; P = 0.072 by ANOVA). Histology demonstrated that both Angiopeptin treatment strategies significantly reduced in-stent neointimal area compared with the control group (1.65 +/- 0.97 mm2 in Group 1 versus 0.93 +/- 0.41 mm2 in Group 2 versus 0.85 +/- 0.28 mm2 in Group 3; P = 0.016 by ANOVA). Measurement of plasma Angiopeptin levels revealed comparable levels in both treatment groups, which persisted for up to 2 weeks.

Conclusions: This study shows that single-dose intramuscular administration of sustained-release Angiopeptin reduces in-stent restenosis as effectively as the prolonged systemic treatment requiring a subcutaneous pump. Thus, a practical, effective, pharmacologic therapy for preventing in-stent restenosis may be available and should be evaluated in patients.

Publication types

Comparative Study

MeSH terms

Animals
Cardiovascular Agents / administration & dosage*
Cardiovascular Agents / pharmacokinetics
Coronary Angiography
Coronary Disease / blood
Coronary Disease / diagnostic imaging
Coronary Disease / surgery*
Coronary Vessels / drug effects*
Coronary Vessels / pathology
Hyperplasia / drug therapy
Injections, Intramuscular
Oligopeptides / administration & dosage*
Oligopeptides / pharmacokinetics
Peptides, Cyclic
Radioimmunoassay
Random Allocation
Somatostatin / administration & dosage
Somatostatin / analogs & derivatives*
Somatostatin / pharmacokinetics
Stents
Swine
Tunica Intima / drug effects*
Tunica Intima / pathology

Substances

Cardiovascular Agents
Oligopeptides
Peptides, Cyclic
lanreotide
Somatostatin