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Intramural Delivery of Recombinant
Apolipoprotein A-I Milano
/Phospholipid
Complex (ETC-216) Inhibits In-stent
Stenosis in Porcine Coronary Arteries
Sanjay Kaul, Vladimir Rukshin, Raul Santos, Babak Azarbal,
*Charles L. Bisgaier, *Jan Johansson, Vivian T. Tsang, Kuang-Yuh
Chyu, James Mirocha, Bojan Cercek, Prediman K. Shah
Atherosclerosis Research Center, Cedars-Sinai Burns & Allen
Research Institute, Division of Cardiology, Cedars-Sinai Medical Center
and *Esperion Therapeutics
• Mutant Apo A-I
• Arginine to cysteine substitution at 173 position
• Transmitted as an autosomal dominant trait by a
single mating couple in Italy in the 18th century
• Confers protection from vascular disease despite
elevated triglycerides and low HDL levels
• Associated with longevity
Apolipoprotein A-IMilano
• Antiatherogenic effects
Inhibits progression of atherosclerosis and promotes regression
of atherosclerosis in atherosclerosis-susceptible transgenic
mice, the apo E null mice (Shah et al, Circulation. 1998; 97: 780–5)
• Vascular response to injury
Reduction in neointimal hyperplasia in balloon-injured
ileofemoral arteries of cholesterol-fed rabbits (Ameli et al, Circulation.
1994;90:1935-41)
• After repeated systemic administration of Apo A-IMilano
50 mg/kg IV in rabbits (5 injections every other day)
20-80 mg/kg IV in apo E null mice (18 injections every other day)
Vasculoprotective Effects of Apo A-IMilano
• Utilizing a local intramural drug delivery approach via
the Infiltrator catheter, we sought to examine the
effects
of recombinant apolipoprotein A-IMilano/1-palmitoyl,2-
oleoyl phosphatidylcholine complex (ETC-216)
on luminal narrowing in a porcine coronary artery stent
Aim of the Study
• Intramural delivery into the coronary vessel wall provides
for enhanced delivery efficiency, minimizes agent loss
into the systemic circulation, thereby resulting in lower
doses, longer duration of activity, and improved overall
effectiveness in modulating coronary arterial response to
Hypothesis
Experimental Protocol
• Coronary Stent Overstretch Injury
3.0-4.0 x 15 mm GFX Stent inflated at 8-12 atm x3 (S:A ~ 1.3:1)
• Animal Groups (Adult farm swine: 25-30 kg)
Group I: apo A-1M (n=6, 12 arteries)
Group II: vehicle control (n=6, 12 arteries)
• Histomorphometry
Perfusion-fixation, H&E and special stain, computerized morphometry
Day 0 28
Intramural local
drug delivery
Angio
Coronary
Injury Angio
Histomorphometry
Treatment Interventions
• Reconstituted HDL (ETC-216)
Recombinant mutant apolipoprotein A-IMilano (14mg/ml) complexed
with 1-palmitoyl, 2-oleoyl phosphatidylcholine (POPC, 13mg/ml)
• Vehicle
Sucrose-mannitol
• Dose and Administration
0.19 mg/kg x1 intramural (infusate volume ~ 0.4ml), prior to injury
Quantitative Coronary Angiographic Data
1.5
2
2.5
3
3.5
4
4.5
MeanLumenDiameter
(mm)
Acute Lumen Gain Lumen Loss
Baseline SacrificePost-Injury
Mean+SD
N=12
ETC-216
Control
*P=0.01
Lumen Loss Index
21+22%
43+13% *
Histologic Sections (RCA)
Proximal Segment Distal Segment
Control
ETC-216
Histomorphometric Data
5.1
1.7
3.3
1.5
0
2
4
6
8
Injury ScoreIntima:Media
Ratio
Mean+SD
N=12
P=0.003
Area(mm2
)
Control
ETC-216
6.7
1.4
2.4
2.1
5.2
1.6
1.9
3.7
0
2
4
6
8
10
LumenIntima Media Adventitia
P=0.02
P=0.02
0 1 2 3 4
0.0
2.5
5.0
7.5
10.0
Injury Score
Lumen Area (mm2
)
0 1 2 3 4
0
5
10
15
Injury Score
mm2
Neointimal Area (mm2
)
0 1 2 3 4
0.0
0.5
1.0
1.5
Injury Score
Stenosis Index
0
0
1
2
Injury Score
1 2 3 4
Neointimal Thickness (mm)
P=0.004 P=0.003
P=0.001 P=0.003
Histomorphometric Data
• A single intramural administration of very low-
dose ETC-216 produced a significant reduction
in injury-induced luminal narrowing in the
porcine coronary stent overstretch injury model
through inhibition of intimal hyperplasia
Conclusion
Implication
•The data show that local intracoronary
delivery of ETC-216 may be useful to
prevent restenosis after coronary stenting

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Intramural delivery of recombinant

  • 1. Intramural Delivery of Recombinant Apolipoprotein A-I Milano /Phospholipid Complex (ETC-216) Inhibits In-stent Stenosis in Porcine Coronary Arteries Sanjay Kaul, Vladimir Rukshin, Raul Santos, Babak Azarbal, *Charles L. Bisgaier, *Jan Johansson, Vivian T. Tsang, Kuang-Yuh Chyu, James Mirocha, Bojan Cercek, Prediman K. Shah Atherosclerosis Research Center, Cedars-Sinai Burns & Allen Research Institute, Division of Cardiology, Cedars-Sinai Medical Center and *Esperion Therapeutics
  • 2. • Mutant Apo A-I • Arginine to cysteine substitution at 173 position • Transmitted as an autosomal dominant trait by a single mating couple in Italy in the 18th century • Confers protection from vascular disease despite elevated triglycerides and low HDL levels • Associated with longevity Apolipoprotein A-IMilano
  • 3. • Antiatherogenic effects Inhibits progression of atherosclerosis and promotes regression of atherosclerosis in atherosclerosis-susceptible transgenic mice, the apo E null mice (Shah et al, Circulation. 1998; 97: 780–5) • Vascular response to injury Reduction in neointimal hyperplasia in balloon-injured ileofemoral arteries of cholesterol-fed rabbits (Ameli et al, Circulation. 1994;90:1935-41) • After repeated systemic administration of Apo A-IMilano 50 mg/kg IV in rabbits (5 injections every other day) 20-80 mg/kg IV in apo E null mice (18 injections every other day) Vasculoprotective Effects of Apo A-IMilano
  • 4. • Utilizing a local intramural drug delivery approach via the Infiltrator catheter, we sought to examine the effects of recombinant apolipoprotein A-IMilano/1-palmitoyl,2- oleoyl phosphatidylcholine complex (ETC-216) on luminal narrowing in a porcine coronary artery stent Aim of the Study
  • 5. • Intramural delivery into the coronary vessel wall provides for enhanced delivery efficiency, minimizes agent loss into the systemic circulation, thereby resulting in lower doses, longer duration of activity, and improved overall effectiveness in modulating coronary arterial response to Hypothesis
  • 6. Experimental Protocol • Coronary Stent Overstretch Injury 3.0-4.0 x 15 mm GFX Stent inflated at 8-12 atm x3 (S:A ~ 1.3:1) • Animal Groups (Adult farm swine: 25-30 kg) Group I: apo A-1M (n=6, 12 arteries) Group II: vehicle control (n=6, 12 arteries) • Histomorphometry Perfusion-fixation, H&E and special stain, computerized morphometry Day 0 28 Intramural local drug delivery Angio Coronary Injury Angio Histomorphometry
  • 7. Treatment Interventions • Reconstituted HDL (ETC-216) Recombinant mutant apolipoprotein A-IMilano (14mg/ml) complexed with 1-palmitoyl, 2-oleoyl phosphatidylcholine (POPC, 13mg/ml) • Vehicle Sucrose-mannitol • Dose and Administration 0.19 mg/kg x1 intramural (infusate volume ~ 0.4ml), prior to injury
  • 8. Quantitative Coronary Angiographic Data 1.5 2 2.5 3 3.5 4 4.5 MeanLumenDiameter (mm) Acute Lumen Gain Lumen Loss Baseline SacrificePost-Injury Mean+SD N=12 ETC-216 Control *P=0.01 Lumen Loss Index 21+22% 43+13% *
  • 9. Histologic Sections (RCA) Proximal Segment Distal Segment Control ETC-216
  • 11. 0 1 2 3 4 0.0 2.5 5.0 7.5 10.0 Injury Score Lumen Area (mm2 ) 0 1 2 3 4 0 5 10 15 Injury Score mm2 Neointimal Area (mm2 ) 0 1 2 3 4 0.0 0.5 1.0 1.5 Injury Score Stenosis Index 0 0 1 2 Injury Score 1 2 3 4 Neointimal Thickness (mm) P=0.004 P=0.003 P=0.001 P=0.003 Histomorphometric Data
  • 12. • A single intramural administration of very low- dose ETC-216 produced a significant reduction in injury-induced luminal narrowing in the porcine coronary stent overstretch injury model through inhibition of intimal hyperplasia Conclusion
  • 13. Implication •The data show that local intracoronary delivery of ETC-216 may be useful to prevent restenosis after coronary stenting

Editor's Notes

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