Coronary Artery Disease Clinical Trial
Official title:
IN-PACT CORO INtimal hyPerplasia evAluated by oCT in de Novo COROnary Lesions Treated by Drug-eluting Balloon and Bare-metal Stent
Restenosis due to neointimal hyperplasia causes repeat target vessel revascularization in a
relevant number of patients undergoing percutaneous coronary interventions (PCI).
Drug-eluting stents (DES) are currently adopted to reduce the rate of restenosis; however,
they may increase risk of stent thrombosis.
Experimental data and first clinical experiences showed that inhibition of neointimal
hyperplasia may be obtained by local administration of anti-proliferative drugs (like
paclitaxel) loaded on the surface of angioplasty balloons. Data on the efficacy of novel
coronary drug-eluting balloons (DEBs) are lacking.
Aims of this open label prospective, randomized trial is to evaluate neointimal hyperplasia
in patients undergoing bare-metal stent (BMS) implantation alone compared to those receiving
additional DEB use and to assess if the technique of DEB use may affect the degree of
neointimal hyperplasia.
Neointimal hyperplasia will be assessed by Optical coherence tomography (OCT).
Background. Restenosis due to neointimal hyperplasia causes repeat target vessel
revascularization in a relevant number of patients undergoing percutaneous coronary
interventions (PCI). Drug-eluting stents (DES) are currently adopted to reduce the rate of
restenosis and repeat revascularizations in the majority of cases. However, a known drawback
that limits the clinical application of DES technology is the possible increased risk of
stent thrombosis, requiring the need of a prolonged dual antiplatelet therapy. Such
phenomenon is strongly related to the profound inhibition of stent strut endothelization,
that leads to the presence of uncovered stent struts, and to the persistence of polymer
molecules which may induce inflammatory reactions in the vessel wall.
Experimental data and first clinical experiences showed that inhibition of neointimal
hyperplasia may be obtained by local administration of anti-proliferative drugs (like
paclitaxel) loaded on the surface of angioplasty balloons. Accordingly, drug-eluting
balloons (DEBs) are a promising tool to prevent restenosis and avoid the undesiderable
persistence of polymer molecules of DES in the vessel wall, thus potentially increasing the
safety of PCI Data on the efficacy of novel coronary DEBs and on the best technique to use
them are lacking.
Optical coherence tomography (OCT), has a resolution of 5-10 μm, 10 times higher than
intravascular ultrasound, thus allowing fine characterization of stent strut coverage and
apposition and detection of minimal degree of in-stent neointima hyperplasia.
Objective of the study:
- To evaluate the degree of neointimal hyperplasia in patients undergoing bare-metal
stent (BMS) implantation alone compared to those receiving additional DEB use.
- To assess if the technique of DEB use (pre-dilation or post-dilation) may affect the
degree of neointimal hyperplasia after BMS implantation.
Study Design. Open label prospective randomized trial comparing the degree of neointimal
hyperplasia assessed by OCT in patients treated by BMS implantation alone, BMS implantation
after DEB predilation or BMS followed by DEB postdilation.
Consecutive patients undergoing BMS implantation and agreeing to enter the study will be
randomized 1:1:1 to
1. BMS implantation.
2. BMS implantation after lesion predilation with DEB
3. BMS implantation followed by post-dilation with DEB. Enrolled patients will undergo a
6-month follow up coronary angiography with OCT evaluation of the stented segment. OCT
analysis will be performed by an expert OCT analyst (GF) blinded to the treatment
assignment.
Study population. 30 subjects.
Procedure Description. In all eligible patients, PCI with BMS implantation will be performed
according to the physician standard practice. All patients will be pre-treated with dual
antiplatelet therapy.
General considerations on DEB usage. DEB is mainly intended to serve as drug delivery to the
vessel wall and should therefore always cover the stenotic area as well as any extended
pre-treated (injured) vessel area including the target lesion and any adjacent (prox and
distal) portions when these were eventually previously covered by a stent or dilated by a
balloon catheter, incidentally or by intention.
DEB length and positioning within the target lesion must be therefore carefully chosen to
avoid geographic miss between the DEB and such extended pre-treated vessel area.
1. BMS group procedure:
- Lesion predilation with an undersized semi-compliant balloon (balloon to artery
ratio: 0.5/1).
- BMS implantation (stent to artery ration: 1.1/1).
- Post-dilation of the stented segment with a non-compliant balloon at high pressure
(16-18 atm)
2. PRE-DEB group procedure:
1. Pre-dilation
- Pre-dilatation of the target lesion with an undersized semi-compliant
standard PTCA balloon (balloon to artery ratio: 0.5/1)
2. DEB dilation:
- DEB diameter and pressure: nominal DEB diameter must be chosen to guarantee
full vessel wall contact at a pressure close or slightly higher of the DEB
nominal pressure (balloon to artery ratio: 1/1)
- DEB length: nominal DEB length must exceed 10 mm (5mm per edge) the length of
the stent which is planned to be deployed
- DEB inflation time: 45 seconds
3. BMS implantation
4. Post-dilation
- Post dilatation of the stented segment must be performed with a non-compliant
PTCA balloon
- Balloon diameter: nominal PTCA balloon diameter must be chosen to reach a
balloon to stent ratio of 1:1 at high pressure (16-18 atm)
- Balloon length and positioning: PTCA balloon length should be shorter than
the length of the deployed stent . In case of post stent edge residual
stenosis post-dilation balloon must fall within are outside the stent (5mm
per edge) which was the previously dilated by the DEB
3. POST-DEB group procedure:
1. Pre-dilation
- Pre-dilatation of the target lesion must be performed with an undersized
semi-compliant standard PTCA balloon (balloon to artery ratio: 0.5/1)
2. BMS implantation
- stent to artery ratio: 1.1/1
- stent length must allow full coverage of the target lesion with a single
stent as well as be 10 mm shorter than the DEB which the operator is planning
to use next
3. Post-dilation
- Post dilatation of the stented segment must be performed with a non-compliant
PTCA balloon
- Balloon diameter: nominal PTCA balloon diameter must be chosen to reach a
balloon to stent ratio of 1:1 at high pressure (16-18 atm)
4. DEB-dilation
- DEB length and positioning: DEB length must be 10 mm longer than the
previously deployed stent (or than the extended pre-treated area in case of
former post-dilation outside the stent edges) and centred within such
pre-treated length (5mm per edge)
- DEB inflation time: 45 seconds
- Balloon to stent ratio: 1.1:1 at a pressure close or slightly higher of the
DEB nominal pressure
The result of the procedure will be assessed by 3-dimensional QCA.
Post-procedural management. All patients will undergo cardiac damage markers
(Creatin-kinase-MB and Troponin I) assessment before the procedure, 6 hours after PCI and 24
hours after PCI. Thereafter, further blood samples will be performed only if clinically
indicated.
After PCI, patients will be given aspirin (75-100 mg/die) life-long and clopidogrel (75
mg/die) for 3 months (according to the on-label prescription for DEB-treated patients).
Follow-up. Clinical follow-up will take place at 1 month (±1 week), 6 months (±2 weeks) and
1 year (±30 days). At 6-month follow-up all patients will undergo a quantitative coronary
angiography (3-dimensional QCA) and Optical Coherence Tomography (OCT) study.
OCT analysis. OCT will be performed with the Imaging system M2 (LightLab Imaging Inc.,
Westford, Massachusetts), capable of a pullback speed of 2 mm/sec and acquisition frame rate
of 15.6/sec, using a non-occlusive technique, with continuous intracoronary iso-osmolar
contrast injection.
The entire stent length will be assessed and cross sectional images will be analysed every
0.5 mm.
STRUT COVERAGE The struts will be classified as uncovered if a tissue layer on the
endoluminal surface is not visible or covered in the presence of visibile tissue between the
endoluminal surface and the lumen.
The tissue coverage thickness will be measured in each strut as the distance from the strut
endoluminal surface to the lumen. In each cross section analysed, the following parameters
will be calculated: the percentage of covered struts (the number of covered struts/ total
number of struts), the percentage of uncovered struts (number of uncovered struts/ total
number of struts), the tissue coverage thickness (μm), the tissue coverage area (stent area
- lumen area) and its percentage (tissue coverage area/stent area X 100); the tissue volume
coverage (tissue coverage area x stent length) and its percentage (tissue coverage
volume/stent volume X 100). To assess the pattern of coverage, the ratio between the
difference of maximum and the minimum tissue thickness/maximum tissue coverage will be
calculated in each frame. A ratio close to 1 indicates an asymmetric tissue coverage, on the
opposite a ratio close to 0 indicates a symmetric tissue coverage.
INCOMPLETE STENT APPOSITION A single stent strut will be defined with incomplete stent
apposition (ISA) when the distance between its endoluminal surface and the vessel wall will
be higher than the entire strut thickness. ISA will be considered present if at least one
single strut will be incompletely apposed to the vessel wall. In each OCT frame analysed,
the number of struts with ISA and the maximum distance from the endoluminal stent strut to
the vessel wall will be measured. The percentage of struts with ISA (number of struts with
ISA/total number of struts), according to the presence/absence of tissue coverage, will also
be reported. A strut will be defined as protruding when the strut will protrude into the
lumen relative to the intima between the adjacent strut sections and the distance between
its endoluminal surface and the vessel wall will be less than the entire strut thickness and
higher than half of strut thickness. The percentage of protruding struts (number of
protruding struts/total number of strut X 100) will be reported, according to the
presence/absence of tissue coverage.
Sample size calculation and statistical analysis. The primary endpoint is the neointimal
area. Secondary endpoints will be the percentage of uncovered struts, the percentage of
struts with ISA and the percentage of protruding struts.
This OCT study is a superiority study and it is expected that additional DEB use to BMS
implantation will lead to a reduction of the primary endpoint compared to BMS implantation
alone.
Few information is available on neointimal proliferation after BMS implantation: two small
non randomized studies reported maximal and minimal neointimal thickness (mm) at 7.3 month
follow up (first study) and mean neointimal thickness at 8 month follow up (latter study)
being > 4 folds higher in the BMS group compared to the rapamycin eluting stent group,
although data on neointimal area are not available. A recent randomized study comparing 12
polymer coated rapamycin-eluting stents to 12 non polymer rapamycin eluting stents reported
a neointimal area of 0.3 ± 0.2 mm2 in the polymer stent vs 1.2 ± 0.8 mm2in the non polymer
stent, thus with a difference of 0.9 (95% CI 0.3-1.4). Based on these findings, we may
hypothesize that additional DEB use will yield to a value of neointimal area close to that
reported in the non polymer rapamycin eluting stent and that this would correspond to
approximately 50% reduction of neointimal area in the BMS group. To detect such difference,
10 patients will be required in each group with a power of 0.9 at a two- sided type I error
of 0.05. As we cannot anticipate whether the timing of additional DEB use: pre or post
stenting, might have a different effect on the reduction of neointimal hyperplasia, 10
patients will be allocated in a randomized fashion to the predilatation DEB use group, 10
patients to the postdilatation DEB use group and 10 to the BMS group.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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