1. Interventional Cardiology Live Case Study Series: A Master Class in Procedural Techniques
Samin K. Sharma, MD
Director Cardiac Cath Lab and Intervention Professor of Medicine Co-Director Cardiovascular Institute Mount Sinai Medical Center New York, NY
Annapoorna S. Kini, MD
Associate Director Cardiac Cath Lab Mount Sinai Medical Center New York, NY
Sameer K. Mehta, MD
Voluntary Associate Professor of Medicine University of Miami - Miller School of Medicine, Miami, Florida

2. September 21, 2010: Case #1: NJ, 72-y-o man
Presentation:
Crescendo exertional angina and SOB for 2 months and stress
MPI revealed moderate-to-severe multivessel ischemia and TID
History:
Hypertension, hyperlipidemia, ex-smoker, colon ca s/p colectomy & chemotherapy 2006 CRi
Medications:
ASA, clopidogrel, simvastatin, metoprolol, amlodipine
SOB = shortness of breath; MPI = myocardial perfusion imaging; TID = transient ischemic dilation; Cri = incomplete blood cell count recovery; ASA = acetylsalicylic acid

3. Case #1 (cont) Cardiac Cath: 8/6/2010: PCI 8/6/10: Plan Today:
Three-vessel CAD with LVEF 65%
Left main: no obstruction
LAD: 80% long calcified lesion of proximal LAD (large) with 70% apical lesion and mild diffuse first diagonal
LCx: 50% prox LCx, 80% OM1 & 50% distal LCx (Medina 1,1,1)
RCA: 70%-99% multiple lesions in RCA, fills via LAD
PCI 8/6/10:
PCI of RCA (XienceV® x 4, mm size)
Plan Today:
PCI of calcified LAD lesion using RotaDES and LCx bifurcation
SYNTAX Score 26
CAD = coronary artery disease; LVEF = left ventricular ejection fraction; LAD = left anterior descending; LCx = left circumflex; OMI = first obtuse marginal; RCA = right coronary artery; PCI = percutaneous coronary intervention; RotaDES = rotablation and drug-eluting stent implantation
® Abbott Laboratories, Abbott Park, Ill.

4. Issues Involving the Case
Choice of Antithrombotic Therapy
Treatment of Calcified Lesions
Bifurcation Lesion Intervention

5. REPLACE-2 vs ACUITY PCI: 30-day Events
REPLACE-2 PCI
ACUITY PCI
Heparin + GP IIb/IIIa (n = 3008)
Bivalirudin alone (n = 2994)
Heparin + GP IIb/IIIa (n = 2619)
Bivalirudin alone (n = 2561)
P = .49 %
P = .30 %
P = .45
11.1
P = .40
10.0
10.5
9.2
8.8
8.2
7.6
7.0
P < .001
P < .001
4.1
4.2
2.4
2.1
Ischemic Major Net Clinical
Composite Bleeding Outcomes
Ischemic Major Net Clinical
Composite Bleeding Outcomes
Lincoff AM, et al. JAMA. 2003;289:
Stone GW, et al. N Engl J Med. 2006;355:2203.

6. HORIZONS AMI Trial: 30-Day Mortality of PCI
Heparin + GPIIb/IIIa inhibitor (n = 1662)
Bivalirudin monotherapy (n = 1678)
HR = 0.63 [0.40, 0.99]
P = .049
2.8%
Death (%)
Cardiac
1.8%
Noncardiac
0.2%
0.1%
Time in days
Number at risk
Bivalirudin
Heparin + GPIIb/IIIa
From Stone GW, et al. N Engl J Med .2008;358:2218. © 2008 Massachusetts Medical Society. All rights reserved.

7. HORIZONS AMI Trial: 30-Day Mortality of PCI
This higher early events
in bivalirudin group were due to
higher acute stent thrombosis and can be eliminated by extended (1-3 hours) infusion after PCI or by prasugrel load instead of clopidogrel load.
Heparin + GPIIb/IIIa inhibitor (n = 1662)
Bivalirudin monotherapy (n = 1678)
HR = 0.63 [0.40, 0.99]
P = .049
2.8%
Death (%)
Cardiac
1.8%
Noncardiac
0.2%
0.1%
Time in days
Number at risk
Bivalirudin
Heparin + GPIIb/IIIa
From Stone GW, et al. N Engl J Med .2008;358:2218. © 2008 Massachusetts Medical Society. All rights reserved.

8. HORIZONS-AMI: Clinical Follow-Up
1-Year FU
2-Year FU %
P = .98 % 20
18.8
Heparin+GP IIb/IIIa (n = 1802)
Bivalirudin group (n = 1800)
Heparin+GP IIb/IIIa (n = 1802)
Bivalirudin group (n = 1800)
18.7
P = .98 15
P < .001
11.9
11.9
P < .001
9.2
9.6 10
P = .03
P = .04
P = .03
P = .22
6.9
6.4
P = .005
5.8
P = .005
6.1
4.8
5.1
4.4
4.6
3.8 5
4.2
3.6
3.5
2.1
2.5
Major Bleeding
Cardiac Mortality
All-Cause Mortality
MACE
Major Reinfarction Cardiac All-Cause MACE
Bleeding Mortality Mortality
Reinfarction
Data presented by Stone GW, Trans Catheter Cardiovascular Therapeutics, 2009, San Francisco, Calif.
Mehran R, et al. Lancet. 2009:374:1149

9. Major Bleed only -Without MI Without Major Bleed (n = 611)
ACUITY Trial: Impact of MI and Major Bleeding (non-CABG) in the First 30 Days on Risk for Death
Mortality at 390 Days %
Both MI and Major Bleed
(n = 94)
Major Bleed only -Without MI
(n = 551)
MI only-
Without Major Bleed (n = 611)
No MI
Major Bleed (n = 12,557)
Stone G, et al. N Engl J Med. 2006;355:

10. Significant Net Clinical Benefit with Prasugrel
TRITON-TIMI 38 Trial: Net Clinical Benefit
Bleeding Risk Subgroups – Therapeutic Consideration
Avoid Prasugrel
Prior CVA/TIA
Reduced maintenance dose guided by PK
Age ≥ 75 or Wt < 60 kg 4%
16%
Subgroups With Positive Benefit:
STEMI
Multivessel/diabetes
SAT on clopidogrel
Clopidogrel non-/hypo-responders
Clopidogrel allergy
Complex or high-risk lesions
Significant Net Clinical Benefit with Prasugrel
80%
Maintenance Dose 10 mg
CVA = cerebrovascular accident; TIA = transient ischemic attack; SAT = subacute stent thrombosis
Wiviott S, et al. Circulation. 2007;116:2923.

11. Updated Dual Anti-Platelet Therapy (DAPT) Post Stenting Incorporating Prasugrel:
Optimal DAPT post stenting continues to evolve with aspirin ( mg PO daily) lifelong and clopidogrel (600 mg load/75 mg PO daily) for 1-12 months being used routinely.
Two new recommendations have emerged from the results of major randomized trials:
Increasing clopidogrel dose to 150 mg for 1 week as per OASIS-7 trial.
Use of prasugrel (TRITON TIMI-38 trial): Prasugrel (60 mg load/10 mg PO daily for 1-15 months) is more effective than clopidogrel in reducing primary endpoints of death, MI, stroke, and stent thrombosis. The relative benefit of prasugrel was higher in patients with STEMI and in diabetes.
But prasugrel use was associated with higher fatal, major and minor bleeding vs clopidogrel especially in patients with prior CVA (also less effective in this subgroup), age > 75 years and weight < 60 kg.

12. Updated DAPT Post Stenting Incorporating Prasugrel
Therefore in following subgroups of PCI patients, prasugrel will be preferred over clopidogrel:
STEMI
Multivessel patients with diabetes
Clopidogrel allergy
Clopidogrel nonresponders
Stent thrombosis in clopidogrel compliant pts
Even in these PCI patients, prasugrel should be absolutely avoided in those with prior CVA and with history of major vascular or nonvascular bleeding (such as GI or GU bleeding) and prasugrel maintenance dose should be decreased to 5 mg PO daily in those > 75 years old or < 60 kg. Patients should be strictly monitored and instructed for signs and symptoms of bleeding. Routine use of PPI for GI prophylaxis is indicated with prasugrel.
For staged procedures in patients on maintenance dose of prasugrel, an extra loading dose of 10 mg before PCI will suffice. To switch patients who are taking clopidogrel maintenance dose, prasugrel loading dose of 30mg followed by 5-10 mg PO daily (as indicated) maintenance is advised.

13. Issues Involving the Case
Choice of Antithrombotic Therapy
Treatment of Calcified Lesions
Bifurcation Lesion Intervention

14. Treatment of Calcified Lesions
Interventional Techniques
Noncompliant (NC) balloon (high pressure inflation up to atm)
NC balloon with another side-by-side wire in the vessel and high pressure inflation
Cutting balloon (up to 8-12 atm)
AngioSculpt® balloon (up to atm)
Rotational atherectomy (heavily calcified)
® AngioScore Inc., Fremont, Calif

15. Atherectomy: Rotablator®
Diamond
microchips
Differential cutting
PTCA PRCA
Rotablator®; Boston Scientific, Inc., Natick, Mass.

16. Rotational Atherectomy (RA, PRCA, PTRCA)
Indications:
Calcified lesion
Undilatable/chronic lesion
Diffuse long lesion
Small vessels (< 2.5 mm)
In-stent restenosis
Bifurcation lesion
Ostial lesion
Rotastent (SPORT trial)
Limitations:
Slow flow / No flow
Perforation
CK-MB release
Wire bias and dissection
Technically challenging
PRCA = percutaneous rotational coronary atherectomy; PTCRA = percutaneous transluminal coronary rotational ablation; CK-MB = creatine kinase-MB isoenzyme

17. Rotational Atherectomy: Current Issues
Slow / no-flow
CPK, CK-MB release
Coronary spasm
Intimal dissections and acute closure
Perforation
Wire bias problems
Heat generation
CPK = creatine phosphokinase

18. Rotational Atherectomy: Complications
Mechanism of No/Slow-flow
Atheromatous debris embolism
Platelet and microthrombi
Platelet activation, aggregation, lysis (by rota burr)
Microcirculatory (vasculature) spasm
Heightened microvasculature reactivity / tone
Microcavitation
Impaired local synthesis of EDRF
Neuro-humoral reflex
Lower epicardial vessel pressure and higher LVEDP
Extreme cases: free radical injury, local edema, microvascular plugging, no-reflow
EDRF = endothelium-derived relaxing factor; LVEDP = left ventricular end-diastolic pressure

19. Rotational Atherectomy: Complications
Slow-flow
Settings:
Long calcified lesions
Total occlusion and right coronary artery
Poor LV function and hemodynamic instability
Thrombotic lesions (also post-MI)
? on -blockers
Technical modifications:
Small initial burr size and small upsizing
Short ablation runs and avoid RPM drops ?Slow-speed
Avoid hypotension and bradycardia
Rota flush & GP IIb/IIIa inhibitors
Treatment: verapamil, nitro, adenosine, nitroprusside, IABP
Best treatment to prevent slow flow is to avoid it from happening.
IABP = intra-aortic balloon pump

20. Activation of Platelets by Rotablation Is Speed-Dependent
Rotational Atherectomy and GPIIb/IIIa Inhibitors
Activation of Platelets by Rotablation Is Speed-Dependent
Transmission electron micrography:
Platelet-rich plasma through chamber with rota burr held stationary (0 rpm) and stirred in an aggregometer for 5 minutes:
Intact platelet membrane, intracellular granules, and clear background.
Platelet-rich plasma was subjected to rotablation at 180,000 rpm and stirred in an aggregometer for 5 minutes: Ruptured platelet membranes, depletion of intracellular organelles (“ghost platelets”),
and cloudy background.
From Williams MS. Circulation. 1998;98:

21. Rotational Atherectomy and Platelets
Effect of Rotablation on Platelet Aggregation
Initial Aggregation Slope
(units/min)
Rotablation Speed (rpm x 10-3)
From Williams MS, et al. Circulation. 1998;98:

22. Rotational Atherectomy
Activation of Platelets by Rotablation Is Speed-Dependent
Rotational
Speed (rpm)
Platelet Aggregates
(> 20 m)/mL blood
180,000
7434  2193
140,000
2269  627
Control
633  258
P < for all groups
Slower rotational speed results in a significantly lower number of platelet aggregates.
Porcine blood exposed to a rotating burr resulted in: Platelet aggregation and red blood cell crenation.
From Reisman M, et al. Cathet Cardiovasc Diagn. 1998;45:

23. STRATAS Trial Technique Matters: Incidence of Slow-Flow % P = .008
Predictors of CK-MB release:
deceleration > 5000 rpm > 5 sec
Predictors of restenosis:
deceleration > 5000 rpm
LAD location
P = .008 %
Current optimal Burr-to-Artery
Ratio (BA):
Aggressive strategy (n = 249) BA: > 0.9
Routine strategy (n = 248) BA: < 0.8
Whitlow PL, et al. Am J Cardiol. 2001;87:

24. Rotational Atherectomy: Complications
Perforation
Settings:
Lesion in a bend > 90
Calcified lesion
Large burr-to-artery ratio
Total occlusion
Wire - bias situations
Technical modifications:
Smaller initial burr size (start with 1.25 mm burr)
Bending the wire technique
Rota extra support wire
?Predilatation with a smaller balloon
Avoid abciximab before rotablation

25. ---DES--- Rotational Atherectomy
Mount Sinai Hospital Experience (6%-9% of PCI)
Complications %
---DES---
short burr runs, rota-flush,
abciximab, stent, experience
slow speed ( ,000 rpm)
rotational atherectomy, BA:

26. STEPS for Rotational Atherectomy
Mechanism of action: Plaque ablation and pulverization by the abrasive diamond-coated burr:
Physical principles: 1. Differential cutting is defined as the ability to ablate one material selectively while sparing and maintaining the integrity of another, based on differences in substrate composition, resulting in a polished smooth lumen compared with multiple intimal tears/dissections with balloon angioplasty; ie, able to ablate inelastic tissue selectively (ie, plaque) while maintaining the integrity of elastic tissue (ie, the normal vessel wall) due to the principle of differential cutting.

27. STEPS for Rotational Atherectomy (cont)
Physical principles:
2. Orthogonal displacement of friction at rotational speeds
> 60,000 rpm; the friction, which occurs when sliding surfaces are in contact, is virtually eliminated. As a result, there is reduced surface drag and unimpeded advancement and withdrawal of the burr, allowing the rotating burr to pass through tortuous and diseased segments of the coronary tree.
The abraded plaque is pulverized into microparticles (size of RBCs), which are 5–10 μm in diameter. These particles are small enough to pass through the coronary microcirculation and ultimately undergo phagocytosis in the liver, spleen, and lung.

28. STEPS for Rotational Atherectomy (cont)
Indications:
Severely calcified lesions
Undilatable/inelastic lesions
Diffuse recurrent In-stent restenosis with multiple jailed side branches
Contraindications:
Acute myocardial infarction
Saphenous vein graft/thrombotic lesions
Presence of dissection

29. STEPS for Rotational Atherectomy (cont)
Preparation for procedure:
Proper burr size selection (~0.5:1 burr-to-artery ratio).
Proper guide catheter size selection (6F for up to 1.75 mm burr and 7F for 2.0 mm or bigger burr).
Additional guidewire (Runthrough NS®/Fielder®) with J-tip prepped.
Noncompliant balloon (1:1 balloon size-to-artery ratio) prepped.
Temporary pacemaker for RCA/dominant LCx lesions (optional at attending discretion).
Make connections to tachometer, NO tank, and flush solution (use the 3-way stopcock for flush).
Gently remove the rota-floppy wire from the packing (first remove distal wire tip from the back-stopper), and wipe with generously wet 4x4. It is a very delicate wire, so handle with care and loop the wire making only 3 loops.
Runthrough NS®; Terumo Interventional Systems, Somerset, NJ . Fielder®; Abbott Vascular, Redwood City, Calif.

30. STEPS for Rotational Atherectomy (cont)
Steps for operator:
Place the rota-floppy guidewire beyond lesion (direct wire placement/wire exchange with over-the-wire 1.5 mm balloon / fine cross).
Backload and advance the burr over the guidewire to the co-pilot.
Place the wire-clip at the end of rota-wire, and reconfirm verbally that wire clip is in place.
Turn on the flush solution and do RPM check while holding the co-pilot in the hand (to prevent entanglement of rota burr and blue drape/4x4 gauze).
Press foot pedal to activate dynaglide mode.

31. STEPS for Rotational Atherectomy (cont)
Steps for operator: (cont)
Advance the burr inside the guiding catheter to the ostium of the coronary artery.
Three steps to remove tension/inertia from the system:
Move advancer knob back and forth to remove tension between drive shaft and Teflon® sleeve.
Open copilot and move burr back and forth under fluoroscopic guidance to remove tension between guidewire and rota burr.
Brief Dyna-tap under fluoroscopic guidance. If there is residual tension/inertia and there is sudden burr advancement/jump – it occurs at low speed and therefore is safer; ie, prevents dissection.
For distal lesions: advance the burr manually/at dynaglide mode to just proximal to lesion.

32. STEPS for Rotational Atherectomy (cont)
Technique of rotablation:
Slow burr advancement
To-and-fro pecking motion of the burr
Shorter burr run times (15–20 sec)
Low burr speeds (140,000–150,000 RPM)
Strict avoidance of significant drops in rpm (> 5000 RPM for > 5 sec)
Flush the system with diluted contrast (1:10 dye-to-saline ratio) during the ablation runs.
Keep systolic blood pressure > 100 mm Hg during the procedure, use 1-2 cc of diluted IV neosynephrine ug as needed (neosynephrine may cause reflex bradycardia).

33. STEPS for Rotational Atherectomy (cont)
After completion of rotablation:
1. Activate the dynaglide mode and remove the burr from the guiding catheter on dynaglide mode, while pressing brake release (the black button on the Rotablator® console), and advancing the wire as the burr is withdrawn.
2. Three steps after completion of procedure:
Remove wire clip
Turn off the flush solution
Remove the burr from the wire
3. Take a cine image to rule out complications
4. Advance another guidewire (Runthrough NS®/Fielder®) across the lesion, parallel to rota-floppy wire
5. Use NC balloon for post-rota PTCA (modified CB-PTCA with rota-floppy wire in-situ) to prepare lesion for stent delivery.
6. Remove rota-floppy after stent placement, and before deploying the stent.

34. Rota+BMS vs Rota+DES Procedural and Clinical Results
Rota + BMS (n = 284)
Rota + DES (n = 130)
P = NS
P = NS
P < .01
P = .62
P = .09 % %
P = NS
Procedural Clinical
Success Success
CK-MB day Stent TVR
>3x MACE Thrombosis
MACE = major adverse cardiac events; TVR = target vessel revascularization
Data presented by Sharma S, et al. American College of Cardiology Scientific Sessions, Chicago, Ill, 2008

35. RotaDES Issues
Procedural and clinical results — as restenosis will be determined by stent expansion
What should be DES length post-rotablation? All ablated areas or lesion coverage only
No randomized trial yet — ongoing ROTAXUS Trial

36. Issues Involving the Case
Choice of Antithrombotic Therapy
Treatment of Calcified Lesions
Bifurcation Lesion Intervention

37. Medina Classification
Bifurcation Lesion Classification
Duke’s Classification
Medina: 1,0,0
Medina: 1,1,1
Medina: 0,0,1
Medina: 1,0,1
Medina: 1,1,0
Medina: 0,1,0
Medina Classification
Prebranch
Postbranch
Pre- and postbranch
Ostial
and Ostial
True
Bifurcation A B C
< 5%
5%-10%
10%-15%
15%-20% D E F
Causes:
Plaque shift
Spasm
Dissection
Most common = 45%

38. MADS (Main, Across, Distal, Side) Classification of Techniques Based on the Manner in which First Stent Is Implanted With Multiple Final Stent Strategy M
Main prox. first A
Main Across side first D
Distal first S
Side branch first
Reprinted from EuroIntervention Vol 5(1), 39-49, Stankovic G, et al. © 2009, with permission from Europa Edition.

39. Complex Bifurcation Lesion Interventions
Technical Issues
How big is the sidebranch(es). Ready to lose the sidebranch (SB)?
Wire both branches. Difficult wiring?
Jailing the sidebranch wire(s). Hydrophilic?
Good back-up support guide catheter: 6, 7, or 8Fr?
Optimal views. Orthogonal projections?
Provisional or systematic SB stenting (1 vs 2 stents?)
Dedicated 2/3 stent technique (T, Culotte, Crush, SKS, V or W?)

40. Various Techniques for Stenting Trifurcation/Bifurcation Lesions
Stent the MV +
balloon or debulk SB
Bifurcation Lesion
..and stent the SB only if suboptimal results:
CP, EKG , < TIMI III flow, > 90% stenosis SB MV
Provisional/
Conventional Stent Technique
Stent + stent
(“T stenting”)
(“reverse-T”)
MV = main vessel; CP = chest pain

41. Various Techniques for Stenting Bifurcation Lesions
Stent + stent
(“T stenting”)
Stent + stent
(“reverse-T”)
Bifurcation Lesion
Stent + PTCA SB MV
Stent + stent
(“Culotte”) 1 2
Stent + stent
(“Kissing”)
Stent + stent
(“Y” or “V”)
“V” 2 1
Stent + stent
(“Crush”) 2 1

42. Bifurcation Lesion Intervention Using DES
“Simultaneous Kissing Stent” (SKS) Technique
Pre
Post

43. Clinical Outcomes in Trials Comparing 1 DES (1S) vs 2 DES (2S) Strategy in Treating Coronary Bifurcations
MACE
TLR % 1S 2S 1S 2S 1S 2S 1S 2S 1S 2S 1S 2S 1S 2S
Colombo A, et al.
SES stents
(n = 85)
Pan M, et al.
SES stents
(n = 91)
Ferenc M, et al.
T-stenting
(n = 202)
Steigen TK, et al.
NORDIC Trial
(n = 413)
Colombo A, et al.
CACTUS trial
(n = 85)
Hildick-Smith D,
et al. BBC ONE
(n = 500)
Sharma SK, et al.
PRECISE-SKS
(n = 100)

44. Clinical Outcomes in Trials Comparing 1 DES (1S) vs 2 DES (2S) Strategy in Treating Coronary Bifurcations (cont)
Incidence of Reported Stent Thrombosis
1S group
2S group % 1S 2S 1S 2S 1S 2S 1S 2S 1S 2S 1S 2S 1S 2S
Colombo A, et al.
SES stents
(n = 85)
Pan M, et al.
SES stents
(n = 91)
Ferenc M, et al.
T-stenting
(n = 202)
Steigen TK, et al.
NORDIC Trial
(n = 413)
Colombo A, et al.
CACTUS trial
(n = 85)
Hildick-Smith D,
et al. BBC ONE
(n = 500)
Sharma SK, et al.
PRECISE-SKS
(n = 100)

45. a complex strategy (done correctly)
Clinical Outcomes in Trials Comparing 1 DES (1S) vs 2 DES (2S) Strategy in Treating Coronary Bifurcations (cont)
Incidence of Reported Stent Thrombosis
1S group
2S group %
Therefore while simple approach of one stent in the main vessel may suffice in most bifurcation lesions,
a complex strategy (done correctly)
of 2 stents by one’s preferred technique may be required
especially if SBr is large size (>3mm) or lesion is long/angulated 1S 2S 1S 2S 1S 2S 1S 2S 1S 2S 1S 2S 1S 2S
Colombo A, et al.
SES stents
(n = 85)
Pan M, et al.
SES stents
(n = 91)
Ferenc M, et al.
T-stenting
(n = 202)
Steigen TK, et al.
NORDIC Trial
(n = 413)
Colombo A, et al.
CACTUS trial
(n = 85)
Hildick-Smith D,
et al. BBC ONE
(n = 500)
Sharma SK, et al.
PRECISE-SKS
(n = 100)

46. Newer Interventions and Stents in 2010
Bifurcation Stents A B C D E F G I J H

47. Interventional Cardiology Live Case Study Series: A Master Class in Procedural Techniques
Samin K. Sharma, MD
Director Cardiac Cath Lab and Intervention Professor of Medicine Co-Director Cardiovascular Institute Mount Sinai Medical Center New York, NY
Annapoorna S. Kini, MD
Associate Director Cardiac Cath Lab Mount Sinai Medical Center New York, NY
Sameer K. Mehta, MD
Voluntary Associate Professor of Medicine University of Miami - Miller School of Medicine, Miami, Florida

48. Take-Home Message: Techniques of Rotational Atherectomy in DES Era
Rotational atherectomy is a useful adjunctive device in interventional treatment of heavily calcified lesions
Optimal technique and strategy are crucial to avoid any potential complications
Properly performed rotational atherectomy followed by DES implantation (RotaDES) may translate into excellent long-term results and will broaden our scope of lesions we can take care of safely

49. Tuesday October 19th Interventional Cardiology Live Case Study Series:
A Master Class in Procedural Techniques
Please join us for our next live case:
Tuesday October 19th
at 8:00 AM EST