Konstantinos Katsanos, MSc, MD, PhD, EBIR · Step Wires Ather PTA BMS DCB DES Cross X Prep X Debulk...
Transcript of Konstantinos Katsanos, MSc, MD, PhD, EBIR · Step Wires Ather PTA BMS DCB DES Cross X Prep X Debulk...
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Konstantinos Katsanos, MSc, MD, PhD, EBIR
Consultant Vascular & Interventional Radiologist
Guy's and St.Thomas' Hospitals
King's Health Partners
London, UK
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Anatomy Attributes (lesion location,
morphology, length, etc)
Device Attributes (scaffolding, anti-
restenosis, fractures, etc)
Evidence-Based Medicine (EBM-MDM)
Cost-effectiveness analysis (Societal
gains and monetary savings)
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Claudication Critical leg
ischaemia
CONSIDERATIONS
• Lifestyle impairment
• Walking distance
• Exercise therapy
• Risk factor modification
• Lesion anatomy
CONSIDERATIONS
• Limb salvage
• Comorbidities
• Limited life expectancy
• Quality of life
• Lesion anatomy
Conservative approach
LESS STENTING
Aggressive treatment
MORE STENTING
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Step Wires Ather PTA BMS DCB DES
Cross X
Prep X
Debulk X
Dilate X X X X
Scaffold X X
Paclitax X X
Leaving Nothing behind and Unmet needs:
vessel recoil, plaque resistance, severe dissections
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Paclitaxel
Interferes with cell
division at the M phase,
after DNA synthesis has
occurred. Cells are in an
abnormal state with twice
the normal DNA content, which leads to
cell death
by apoptosis
Sirolimus
Everolimus
Interfere with cell
growth at the G1/S
transition, before
DNA synthesis has occurred.
Cells return to the resting phase (G0)
without dying
and can reenter the cell cycle later again
Rep
lica
tion p
rep
Growth
Factor
mTOR
G0
Cell
prepares
for mitosis
DNA
synthesis
Mitosis Protein
synthesis.
Cell
prepares
for mitosis
DNA
synthesis
Mitosis Protein
synthesis.
Cytotoxic Cytostatic
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Arterial Tissue Concentration
Paclit
axel C
on
c.
(ng
/mg
)
Cmax 56-60 Day0.1
1
10
100Zilver PTX
IN.Pact DEB
Paclitaxel concentrations in arterial tissue are comparable with
regard to Cmax values and concentrations at 2 months post-treatment
Tissue paclitaxel kinetics
FDA Zilver Panel Meeting Summary 2012
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Katsanos K, et al. Bayesian meta-analysis in the femoropopliteal artery. JVS 2014
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Balloons vs Nitinol Stents
Balloons vs Covered Stents
Bare vs Covered Stents
Balloon angioplasty ≈ 73.9%
Uncovered nitinol stents ≈ 95.4%
Covered nitinol stents ≈ 97.5%
Bail-out
Δ≈22%
Katsanos K, et al. Bayesian meta-analysis in the femoropopliteal artery. JVS 2014
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Vascular Restenosis Freedom from TLR
Katsanos K, et al. Bayesian meta-analysis in the femoropopliteal artery. JVS 2014
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Zeller T. et al. JEVT 2014: 21: 39-368
n=228 patients and propensity score analysis
lesion length 19cm and bail-out stenting 18.3%
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ZILVER-PTX LEVANT 2
No difference
Improved patency
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Variable ZILVER-PTX DCB Notes
CLI 10% 4-6% DEBELLUM
36%
CTOs 30% 13-41% ISR
excluded
Length 5.4cm 4.0-8.1cm Mostly TASC
A & B
Stenting 100% Very low IN.PACT SFA:
7.3 vs 11.6%
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Real-life practice: 1 in 4 will need a Stent
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DCB DES
Lesion complexity (length, CTO, calcium, etc)
Rutherford Becker classification (CLI)
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POBA
DES DCB
Primary DES versus DCB and stent?
BASIL 3 funded for CLI
Failure Success
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• Paclitaxel proven anti-restenotic effect in
the femoropopliteal artery
• Paclitaxel-stents ballanced against
paclitaxel-balloons according to clinical
indications
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Thank You
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A treatment algorithm for drug eluting technologies
Konstantinos Katsanos, MSc, MD, PhD, EBIR Consultant Vascular & Interventional Radiologist
Guy's and St.Thomas' Hospitals
King's Health Partners
London, UK