angiomax (bivalirudin) in peripheral vascular disease (pvd)

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Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Page 1: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

Page 2: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Anticoagulation in PVD

► Thrombus occurs in 100% of peripheral percutaneous intervention (PPI) cases

► Bleeding risks are greater in PPI than PCI

► PPI and PCI are different

► PPI requires superior anticoagulation

Page 3: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Clinical Differences in PVD vs. PCI

► Longer length diseased vessel

► Larger sheath size requirement

► Longer PTA/stented segments

► Larger acute and chronic thrombus burden

► Longer procedural times (sheath dwell times)

► Multiple catheter, guidewire, devices, etc exchanges (oftentimes crossover techniques)

Page 4: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Clinical Differences in PVD vs. PCI (con’t)

► “Low flow” state in peripheral versus coronary flow beds

► Increased incidence of CRF (renal insufficiency)

► Postprocedural anticoagulation (infrainguinal, limb salvage, ALI, etc.)

► PVD- > 50-60% Diabetes: PCI- 20-30% Diabetes

► PVD patients are hypercoaguable

Page 5: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Peripheral interventions

► Percutaneous peripheral interventions (PPI) require predictable and reliable anticoagulation that also minimizes risk of bleeding

Large sheaths

Renal dysfunction

Long interventions

► Strategies needed to improve throughput

Reduce time to sheath removal

Reduce time to ambulation

► Heparin is typically used in PPI, but no data exist on the optimal level of anticoagulation

► The limitations of heparin persist in PPI…

Page 6: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Bivalirudin in peripheral interventions

► Bivalirudin: a thrombin-specific anticoagulant, superior efficacy, significantly less bleeding vs heparin in PTCA1

► Bivalirudin used in PPI registries: St Joseph’s, Naples Endovascular, Cardiovascular Institute of the South, Cardiovascular Research Foundation/Lenox Hill

► Based on these limited data, bivalirudin may be an attractive alternative to heparin in peripheral interventions

► May offer decreased vascular complications, earlier sheath removal time, earlier ambulation and decreased length of stay

► Further studies are warranted

1Bittl et al AJC 2001

Page 7: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Overview

Peripheral experienceSt Joseph’s Hospital Registry

Naples Endovascular

Cardiovascular Research Foundation & Lenox Hill

Cardiovascular Inst of the South

Angiomax clinical program APPROVE trial

Page 8: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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St. Joseph’s Hospital Registry

► 72 Patients, elective procedures

► 88 Lesions (4 with concomitant PCI)

► Mean Age 65.8 yrs (Range 43-84)

► 60% Male

► 73% HTN

► 23% Diabetes

► Prior MI 25%

► Prior PCI 62%

► Prior CABG 27%

► Prior CVA 10%

Knopf et al, TCT 2002

Demographics

Page 9: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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St. Joseph’s Hospital Registry

► Bivalirudin bolus 0.75mg/kg in 100%

► Infusion 1.75 mg/kg/hr used in 50% of cases

► Mean ACT 286.6 (224-389)

► Sheath 6F-11F

► Mean creatinine pre 1.17 (0.7-2.7)

► Plavix 99%

► GP IIb/IIIa 0%

► Closure devices 20%

Knopf et al, TCT 2002

Methods

Page 10: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Location of the 88 lesions

► Iliac 33

► Renal 26

► Femoral 12

► Carotid 16

► Distal Aorta 1

► Subclavian 1

Knopf et al, TCT 2002

St. Joseph’s Hospital Registry

Page 11: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Results► Success 100%

► Bleeding 0%

► Mortality 0%

► Subacute closure 0%

► Vascular repair 0%

► CVA 0%

► Post-procedure creatinine increase > 0.5 0%

► Mean sheath removal 108 minutes

► LOS 0.6 days (0-2)

Knopf et al, TCT 2002

St. Joseph’s Hospital Registry

Page 12: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

Naples Endovascular Registry

Grubbs, CRT 2003

Type N cases Bivalirudin Rx Success rate

Arterial lysis 12 bolus+ inf 100%

Endovascular AAA 8 bolus+ inf 100%

Carotid art. stent 3 bolus+ inf 100%

Venous interventions 13 bolus 94%

Arterial interventions 16 bolus 100%

Venous dialysis

Graft declots w/lytic

13 bolus 100%

Venous dialysis

Graft declots w/mech device

4 bolus 100%

69 proceduresBivalirudin bolus 0.75mg/kg Infusion 1.75 mg/kg/hr

Page 13: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

Naples Endovascular Registry

Grubbs, CRT 2003

• Bivalirudin provided adequate anticoagulation for all peripheral interventions

• Achieved ACT targets immediately

• No adverse events (bleeding, procedural failure, acute thrombosis, or death) were seen.

• Historical analysis of usual complication rates for this composite set of procedures w/ heparin= 6% >1200 interventions.

• Bivalirudin procedural success rate of 100% on 12 consecutive arterial lysis cases is of note, historical complete lysis rate of 78% in >100 cases using tPA alone during the past 4 years.

Conclusions

Page 14: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Cardiovascular Research Fdn& LHH

► 59 consecutive pts with bivalirudin (bolus 75mg/kg, 1.75 mg/kg/hr infusion throughout the procedure)

► 83 case-matched controls with UFH (5,000U), same timeframe

► mean age = 72 + 9 yrs

► 60.4% male

► No GP IIb/IIIa inhibitors

► Neurological events, bleeding and vascular complications were recorded and adjudicated by an independent committee

Adamyan et al, ACC 2003

Carotid Stenting

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Cardiovascular Research Fdn& LHH

Adamyan et al, ACC 2003

Clinical Outcomes Bivalirudin n=59

UFH n=83

P value

Death , n% 0 (/59) 0 (0/83) NS

Major stroke, n% 0 (0/59) 1.2 (1/83) 1.00

Minor stroke, n% 0 (0/59) 0 (0/83) NS

Hematoma > 5cm (%) 1.7 (1/59) 3.6(3/83) 0.64

Pseudoaneurysm(%) 0 (0/59) 2.4 (2/83) 0.51

Transfusion (%) 0 (0/59) 8.6 (7/81) 0.02

Vascular complication 1.7 (1/59) 4.9 (4/81) 0.39

Results

Page 16: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Bivalirudin in peripheral interventions

► Based on these limited data, bivalirudin may be an attractive alternative to heparin in peripheral interventions

► May offer decreased vascular complications, earlier sheath removal time, earlier ambulation and decreased length of stay

► Further studies are warranted

Page 17: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Direct Thrombin Inhibition in PVD

Bivalirudin as Sole Anticoagulant in Peripheral Vascular Disease: A Safety and Feasible Alternative in Renal and Iliac Interventions

David E. Allie, Mitchell D. Lirtzman, V. Antoine Keller, Mohamed H. Khan, Muhammad A. Khan, Peter S. Fail, Chris J. Hebert, Adam A. Allie, Craig M. Walker, Cardiovascular Institute of the South, LA, HCA, LA

Allie et al ACC 2003

Page 18: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Bivalirudin as Anticoagulant Foundation in PVD: A Safety and Feasibility Study in Renal and Iliac PTA

Design/ Methods

• Retrospective, consecutive review of 180 renal, 75 iliac

• Bivalirudin: 0.75 mg/kg bolus with 1.75 mg/kg/hr infusion for procedural duration

• Variables: Sheath removal time (SRT), access complication (AC), time to ambulate (TA), and length of stay (LOS).

• Follow up: 6 month renal and iliac duplex ultrasound and ankle-brachial index

• Matched historical control with UFH

Allie, ACC 2003

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Bivalirudin as Anticoagulant Foundation in PVD: A Safety and Feasibility Study in Renal and Iliac PTA

Results:

Allie, ACC 2003

Variables Bivalirudin Renal, n=180

Historical Control Renal, n=180

P-value

PPI Success, n (%) 180 (100) 179 (99) 0.31 73 AC (Major1), n (%) 2(1.1) 6 (3.3) 0.1532 AC (Minor2), n(%) 5(2.7) 8 (4.4) 0.3974 SRT <60 min, n (%) 152 (84) 106 (59) <0.0001 SRT >60 m in, n (%) 28 (16) 74 (41) <0.0001 LOS <24 hrs, n (%) 154(85.5) 130 (72) 0.002 LOS >24 hrs, n (%) 26(14.5) 50 (28) 0.002 TA <6 hrs, n (%) 136(75.5) 105 (58) 0.0005 TA >6 hrs, n (%) 44(24.5) 75 (42) 0.0005

1="Major’ = any surgery, > 5 cm hematoma, or > 2u transfusion2="Minor’ = all other non-intracranial or retroperitoneal bleeding

RT, LOS and TA all significantly shorter with bivalirudin

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Bivalirudin as Anticoagulant Foundation in PVD: A Safety and Feasibility Study in Renal and Iliac PTA

Results

Allie, ACC 20031="Major’ = any surgery, > 5 cm hematoma, or > 2u transfusion2="Minor’ = all other non-intracranial or retroperitoneal bleeding

Variables Bivalirudin Iliac n=75

Historical control Iliac n=75

P-value

PPI Success, n (%) 75 (100) 74 (98.6) 0.3173

AC (Major1), n (%) 2(2.5) 3 (4) 0.6503

AC (Minor2), n(%) 3(4) 5 (6.6) 0.4689

SRT <60 min, n (%) 36 (48) 21 (28) 0.0119

SRT >60 min, n (%) 39 (52) 54 (72) 0.0119

LOS <24 hrs, n (%) 42(56) 32 (43) 0.1036

LOS >24 hrs, n (%) 33(44) 43 (57) 0.1036

TA <6 hrs, n (%) 31(41) 19 (25) 0.0383

TA >6 hrs, n (%) 44(59) 56 (75) 0.0383

Page 21: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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► Procedural success and clinical outcomes similar in both PVD groups with bivalirudin and UFH

► Fewer access site complications in all groups

Renal Iliac

Bivalirudin UFH BivalirudinUFH

Overall 3.9% 7.7% 6.5%10.6%

Major 1.1% 3.3% 2.5% 4.0%

Minor 2.7% 4.4% 4.0%6.6%

Overall Access Site ComplicationsBivalirudin = 3.8% UFH = 6.6%

Bivalirudin as Anticoagulant Foundation in PVD: A Safety and Feasibility Study in Renal and Iliac PTA

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Bivalirudin as Anticoagulant Foundation in PVD: A Safety and Feasibility Study in Renal and Iliac PTA

► No thrombotic events, intracranial bleeding, or major surgical complications occurred in bivalirudin group

► Sheath removal time, time to ambulation and length of stay were reduced compared to historical control

► 6 month repeat PPI:

Renal 7/180 (3.9%) bivalirudin 8/180 (5%) UFH

Iliac and 3/75 (4%) bivalirudin 4/75 (5.3%) UFH

Allie, ACC 2003

Page 23: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

Principal Investigators:

David Allie MD Cardiovascular Institute of the South Patrick Hall MD South Carolina Heart Center

Direct Thrombin Inhibition in PVD

Page 24: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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To demonstrate that Angiomax can safely replace unfractionated heparin as the primary anticoagulant in patients undergoing peripheral interventions, including outpatient interventions (<23hour)

Open label trial of Angiomax anticoagulation in renal, femoral, and Iliac lesions

505 patients

26 sites

Study Objective and Design

Page 25: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Angiomax 0.75 mg/kg IV bolus + 1.75 mg/kg-hr IV

infusion for duration of procedure

GP IIb/IIIa’s at physician discretion

Bivalirudin post-procedural infusion 0.25 mg/kg/hr at physician discretion

Study Drug Administration

Page 26: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Primary: Procedural success defined as ≤ 20% residual stenosis as determined by the treating physician.

Secondary:     

·  Activated clotting times (ACTs)

·  Health economics (sheath size, time to sheath removal, time to ambulation, time to discharge, use of closure devices)

·  Death

·  Bleeding

·  Myocardial infarction (MI)

·  Unplanned revasc or surgical intervention for ischemia

·  Amputation

·  Renal function (relation to ischemic and bleeding outcomes).

Endpoints

Page 27: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Primary lesion/vessel

• Renal n/N (%) 173/505 (34.3)

• Iliac n/N (%) 140/505 (27.7)

• Femoral n/N (%) 184/505 (36.4)

• Other n/N (%) 8/505 (1.6)

Page 28: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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► Clopidogrel pretreatment 95%

► Aspirin 96.8%

► GP IIb/IIIa inhibitors 4.4%

► Procedural success 95%

Procedural characteristics

Page 29: Angiomax (bivalirudin) in Peripheral Vascular Disease (PVD)

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Patient demographics

Characteristic

Age (mean) 69

Age > 65 yrs n/N (%) 320/505 (63.4)

Age > 75 yrs n/N (%) 164/505 (32.5)

Female n (%) 231 (45.7)

Male n (%) 274 (54.3)

Angina History n/N (%) 178/504 (35.3)

Prior MI n/N (%) 124/505 (24.6)

Prior Vascular Surgery n/N (%) 175/505 (34.7)

Current Smoker (<6 mos) n/N (%) 152/505 (30.1)

Hyperlipidemia n/N (%) 400/505 (72.9)

Hypertension n/N (%) 450/504 (89.3)

Congestive Heart Failure n/N (%) 79/505 (15.6)

Diabetes (insulin-dependent) n/N (%) 63/505 (12.5)

Diabetes (non insulin-dependent n/N (%) 120/505 (23.8)

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Ischemic outcomes: 30 days

Renal Iliac Femoral Total

n/N (%) n/N (%) n/N (%) n/N (%)

Death 0/173 (0.0) 0/139 (0.0) 0/184 (0.0) 0/505 (0.0)

Unplanned revasc 0/173 (0.0) 0/139 (0.0) 4/184 (2.2) 4/504 (0.8)

Amputation 0/173 (0.0) 0/139 (0.0) 2/184 (1.1) 2/504 (0.4)

Myocardial infarction

0/173 (0.0) 0/139 (0.0) 1/184 (0.5) 1/505 (0.2)

New Q- wave* 0/173 (0.0) 0/139 (0.0) 0/184 (0.0) 0/505 (0.0)

CK-MB>3XULN 0/173 (0.0) 0/139 (0.0) 1/184 (0.5) 1/505 (0.2)

* New Q-wave >0.04 sec duration in 2 or more contiguous leads

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Hemorrhagic outcomes: 30 days

Renal Iliac Femoral Total

n/N (%) n/N (%) n/N (%) n/N (%)

Major (protocol) 7/173 (4.0) 5/140 (3.6) 7/184 (3.8) 19/505 (3.8)

Tfx ≥2 U 3/173 (1.7) 5/140 (3.6) 3/184 (1.6) 11/505 (2.2)

Intracranial 0/173 (0.0) 0/139 (0.0) 1/184 (0.5) 1/504 (0.2)

Retroperitoneal 0/173 (0.0) 1/139 (0.7) 1/184 (0.5) 2/504 (0.4)

Fall in Hgb >4g/dL w/no site

2/173 (1.2) 3/140 (2.1) 4/183 (2.2) 9/505 (1.8)

Fall in Hgb >3g/dL overt

2/173 (1.2) 0/139 (0.0) 1/184 (0.5) 3/504 (0.6)

Minor (protocol) 13/173 (7.5) 14/139(10.1) 21/184 (11.4) 48/504 (9.5)

Major (TIMI) 1/168 (0.6) 1/137 (0.7) 4/177 (2.3) 6/490 (1.2)

Minor (TIMI) 4/172 (2.3) 4/139 (2.9) 7/181 (3.9) 15/500 (3.0)

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► Bivalirudin, as the sole procedural anticoagulant, provided similar outcomes in all vessel types treated

► Consistent anticoagulation at the dose tested

► Major & minor hemorrhagic complications were low

► Times to sheath removal, ambulation, and discharge were favorable and appear to increase the potential for same-day discharge without compromising efficacy or safety

Summary:

APPROVE 30-day outcomes