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Trial to Assess Chelation Therapy (TACT)

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Trial to Assess Chelation Therapy (TACT) Principal Investigator: Gervasio A. Lamas, MD Mount Sinai Medical Center Miami Heart Institute Miami Beach FL – PowerPoint PPT presentation

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Title: Trial to Assess Chelation Therapy (TACT)


1
Trial to Assess Chelation Therapy (TACT)
  • Principal Investigator Gervasio A. Lamas, MD
  • Mount Sinai Medical Center Miami Heart
    Institute
  • Miami Beach FL

2
TACT Design
  • 5-year randomized, double-blind,
    placebo-controlled
  • 2X2 factorial trial
  • Testing the standard chelation solution versus
    placebo
  • Testing the effects of a high-dose antioxidant
    vitamin and mineral supplementation, versus a low
    dose regimen.

3
Specific Aims
  • To determine whether chelation or high-dose
    supplements in patients with CHD will reduce the
    incidence of clinical cardiovascular events
  • To determine whether chelation and high-dose
    supplements have acceptable safety profiles.

4
Substudy Specific Aims
  • Two substudies will be conducted whose specific
    aims are as follows
  • To determine whether chelation or high-dose
    supplements improve quality of life
  • To conduct an economic analysis of chelation
    therapy and high dose supplements.

5
Inclusion Criteria
  • Men or women age 50 and older
  • MI gt6 weeks prior to randomization

6
Definition of MI
  • Biomarkers (symptoms or ECG changes)
  • OR
  • Imaging evidence of myocardial scar evidence of
    coronary disease on angiography.
  • This requires PI involvement, especially the
    decision that the CAD corresponds to an imaged
    scar. Remember that the CCC is always happy to
    help.

7
Major Exclusion Criteria
  • Chelation within 5 years
  • Known allergy to any components of solutions or
    vitamins
  • Carotid and coronary revascularization within 6
    months, or planned revascularization
  • Symptomatic HF, or HF hospitalization within 6
    months
  • Uncontrolled hypertension
  • No venous access
  • Creatinine gt2.0mg/dL
  • Baseline platelets lt100,000
  • Cigarette smoking within 3 months

8
Primary Endpoint
  • Composite clinical endpoint including
  • all cause mortality
  • myocardial infarction
  • stroke
  • coronary revascularization
  • hospitalization for angina

9
Secondary Endpoints
  • Composite serious irreversible vascular events
    including cardiovascular death, or non-fatal MI
    or non-fatal stroke.

Dr. Lee
10
Event Rate Assumptions
  • 20 event rate (primary endpoint) in control arm
    after 2.5 years of follow-up
  • Chelation therapy will reduce event rate by 25
    (if patients comply)
  • ?7 of patients per year will discontinue the
    infusions (?20 over 3 years)
  • 3 loss to follow-up

11
Statistical Power of TACT
  • With these assumptions, 2,372 patients will
  • provide
  • 85 power for detecting a 25 ? in the primary
    endpoint, taking into account non-compliance and
    loss to follow-up

12
The Clinical Unit
  • Principal Investigator (PI) with NIH Clinical
    Investigator training module completed
  • Research coordinator with NIH Clinical
  • Investigator training module completed
  • Commitment to follow protocol
  • FWA
  • IRB approval
  • Training in chelation
  • Training in evidence-based cardiology
  • Internet access
  • Infusion area
  • Patient base

13
Study Overview
  • Infusion Visits
  • Initial - Weekly X 30 wks
  • Maintenance - Every 5 8 weeks
  • Enter data into internet data collection system
    during or immediately post visit

14
Study Overview
  • Patient Follow-up
  • 3 phone calls/year (average 2.5 years f/u)
  • 1 annual clinic visit
  • Clinic visit at end of study

15
Pharmacy Delivery of Study Drugs
  • Infusion Kits UPS delivery the morning before
    scheduled visit
  • 500 ml bag IV solution
  • 2 - 20ml syringes
  • Vitamins Initial supply shipped with first kit
  • Subsequent shipments on 1st each month
  • Subsequent shipments contain 2-month supply (360
    tablets in a bottle 60 gel-caps in blister packs)

16
Pharmacy Security and Storage
  • Infusion Kit refrigerated (2-8 degrees C)
  • Vitamins at room temperature
  • Store study drugs in secure location with limited
    access

17
Pharmacy Simple Mixing Instructions
  • Prepare infusion just prior to administration
  • Inject 2 syringes of solution into IV bag using
    21 g needles
  • Allow solution to reach room temp prior to
    infusing (30 minutes)
  • Administer within 24 hrs of mixing

18
Potential Toxicity
  • Nephrotoxicity
  • Hypocalcemia
  • Hypoglycemia
  • Hypotension
  • Trace metal and vitamin deficiencies
  • Venous access problems
  • Clotting parameters
  • Febrile episodes
  • ECG changes
  • Fluid overload

19
Subject Safety
  • EDTA dose is adjusted based on estimated
    creatinine clearance (Jan 15, 2003 section 6.2)
  • Kidney. Doubling of the creatinine from baseline
    or increase to a level of 2.5 mg/dLwill lead to
    cessation of infusions and continuation of the
    vitamin regimen. We will also look for signs of
    hematuria and/or proteinuria, which will prompt
    further evaluation.
  • Liver. Doubling of the ALT, AST, alkaline
    phosphatase or bilirubin will be lead to
    interruption of infusions and a potential
    re-challenge.
  • Hematology. Platelet count lt 100,000, or a 50
    decrease from baseline will lead to elimination
    of heparin.

20
Study Interventions
  • ACAM protocol EDTA chelation vs placebo
  • High dose antioxidant vitamins and minerals vs
    placebo

21
Low-Dose Regimen
Low-Dose Regimen (Taken once daily) Amount Daily Value
Vitamin B6 (as pyridoxine hydrochloride) 25 mg 1250
Zinc (as zinc gluconate) 25 mcg 167
Copper (as copper gluconate) 2 mg 100
Manganese (as manganese gluconate) 15 mg 750
Chromium (as chromium picolinate) 50 mg 42
These supplements, produced by OleoMed S.A.,
Madrid, Spain, are administered in an olive oil
based gel capsule.
22
High Dose Regimen
High Dose Regimen (Taken twice daily) Amount per Serving Daily Value
Vitamin A (as fish liver oil and beta-carotene) 25,000 IU 500
Vitamin C (as calcium ascorbate, magnesium ascorbate and potassium ascorbate 1,200 mg 2000
Vitamin D3 (as cholecalciferol) 100 IU 25
Vitamin E (as d-alpha tocopheryl succinate and d-alpha tocopheryl acetate) 400 IU 1333
Vitamin K1 (as phytonadione) 60 mcg 75
Thiamin (vitamin B1) (as thiamin mononitrate) 100 mg 6667
Niacin (as niacinamide and niacin) 200 mg 1000
Vitamin B6 (as pyridoxine hydrochloride) 50 mg 2500
Folate (as folic acid) 800 mcg 200
Vitamin B12 (as cyanocobalamin) 100 mcg 1667
Biotin 300 mcg 100
Pantothenic acid (as d-calcium pantothenate) 400 mcg 4000
Calcium (as calcium citrate and calcium ascorbate) 500 mcg 50
Iodine (from kelp) 150 mcg 100
23
High Dose Regimen (cont.)
High Dose Regimen (Taken twice daily) Amount per Serving Daily Value
Magnesium (as magnesium aspartate, magnesium ascorbate and magnesium amino acid chelate) 500 mg 125
Zinc (as zinc amino acid chelate) 20 mg 133
Selenium (as selenium amino acid chelate) 200 mcg 286
Copper (as copper amino acid chelate) 2 mg 100
Manganese (as manganese amino acid chelate) 20 mg 1000
Chromium (as chromium polynicotinate) 200 mcg 167
Molybdenum (as molybdenum amino acid chelate) 150 mcg 200
Potassium (as potassium aspartate and potassium ascorbate) 99 mg 3
Choline (as choline bitartrate) 150 mg
Inositol 50 mg
PABA (as para-amino benzoic acid) 50 mg
Boron (as boron aspartate and boron citrate) 2 mg
Vanadium (as vanadyl sulfate) 39 mcg
Citrus Bioflavonoids 100 mg
24
Safety Monitoring
Screen Inf. 1 Inf. 2 Inf. 5 Inf. 10 Inf. 15 Inf. 20 Inf. 25 Inf. 30 Inf. 36 Inf. 40
Creatinine X X X X X X X X X X
Calcium X X X X X X X X X X
Magnesium X X X X X X X X X X
Glucose X X X X X X X X X X
CBC/platelets X X X X X X X X X X
LFT X X X X X X X X X X
Urine Dipstick X X X X
25
Quality of Life Endpoints
Data collected by structured interview in 1000
randomly selected patients
  • Cardiac physical functioning Duke Activity
    Status Index
  • Psychological well-being SF-36 MHI5
  • Patient utilities EuroQoL
  • Analysis by intention to treat

26
Economic Analysis
  • Medical resource consumption on CRF
  • Compared by intention to treat
  • Cost weights assigned from 2º sources
  • CEA if 1º study endpoint positive for
    experimental arms

Dr. Lee
27
Statistical Analysis - Overview
  • Treatment comparisons performed according to
    intention to treat
  • Treatments compared using two-sided statistical
    tests
  • Analysis will incorporate not only how many
    events occur, but also when they occur
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