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Cardiac Infusions

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Peter Mirehouse RN, PNII Ginny Coleman RN, BSN, PNIII Robert Masterson RN, BSN, CCRN, PNIII Acute coronary syndrome Percutaneous coronary intervention Used for ... – PowerPoint PPT presentation

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Title: Cardiac Infusions


1
Cardiac Infusions
  • Peter Mirehouse RN, PNII
  • Ginny Coleman RN, BSN, PNIII
  • Robert Masterson RN, BSN, CCRN, PNIII

Integrilin
Nitroglycerin
Amiodarone
2
Amiodarone
  • Robert Masterson RN, BSN,CCRN
  • PNIII

3
FDA Labeled Indications
  • MANAGEMENT OF LIFE-THREATENUNG RECURRENT Vf /
    UNSTABLE VT
  • IV.ACUTE Vf /UNSTABLE VT
  • OFF-LABEL CONVERSION OF Af TO NSR STABLE VT

4
Clinical Uses
  • CARDIAC ARRESTANTI-ARRHYTHMIC OF CHOICE IN Vf/VT
    ARREST
  • MANAGEMENT OF SERIOUS ARRHYTHMIAS WHEN OTHER
    TREATMENTS HAVE FAILED

5
Drug class
  • AMIODARONE IS A CLASS III ANTI-ARRHYTHMIC BUT
    SHARES PROPERTIES OF CLASSES I-IV
    ANTI-ARRHYTHMICS
  • HIGHLY EFFECTIVE WITH LOW PRO-ARRHYTHMIC RISK

6
Mechanism of Action
  • VAUGHAN WILLIAMS CLASSIFICATION ENTAILS 4 CLASSES
    REFLECTING 4 ACTIONS, i.e. SODIUM,BETA
    ADRENERGIC,POTASSIUM AND CALCIUM BLOCKADE
  • CLASS III DRUGS PROLONGS REPOLARIZATION AND
    REFRACTORY PERIOD THEREBY PREVENTING RE-ENTRY
    ARRTHYMIAS

7
Pharmacokinetics
  • Distribution, Metabolism, Excretion, Elimination
    and Half Life
  • AMIODARONE REQUIRED A LOADING DOSE
  • ORALLY,LOADING TAKES 1-2 WEEKS TO REACH
    THERAPEUTIC SERUM LEVELS
  • IV LOADING DOSE CONSISTS OF 150MG OVER 10, THEN
    360 MG OVER NEXT 6 HOURS THEN 540 MG OVER NEXT 18
    HOURS (TOTAL 1000MG IN FIRST 24 HOURS

8
Pharmacokinetics
  • BEFORE AMIODARONE BECOMES EFFECTIVE, IT MUST
    SATURATE ALL TISSUES OF THE BODY
  • HALF-LIFE OF AMODARONE IS EXTREMELY LONG 1 YEAR
    AFTER DISCONTINUATION, MEASURABLE SERUM LEVELS
    OBTAINABLE
  • NUMEROUS DRUG-DRUG INTERACTIONS ARE KNOWN

9
Contraindications of use
1.PREGNANCY/LACTATION 2.CARDIOGENIC
SHOCK 3.BRADYCARDIA 4.SINUS NODE
DYSFUNCTION 5.THYROID DX 6.LUNG DX
10
Precautions of use
  • PATIENT MUST BE FULLY INFORMED OF RISKS AND HAVE
    GIVEN THEIR CONSENT BEFORE USE IF POSSIBLE
  • 2. OPTIMIZE ELECTROLYTES (POTASSIUM/MAGNESIUM)
    PRIOR TO INITIATING TX

11
Potential side effects
  • SIDE EFFECTS ARE MANY AND POTENTIALLY SEVERE
  • 25-30 OF PATIENTS DEVELOP 1 OR MORE SIDE-EFFECTS
    SUCH AS
  • ARDS (2),PULMONARY FIBROSIS,THYROID DXS, LIVER
    /KIDNEY FAILURE, SEVERE ATAXIA,HALO
    VISION,PERMANENT BLINDNESS, PERIPH.NEUROPATHY,
    SMURF SYNDROME, SUN SENSITIVITY, POOR SLEEP, POOR
    CONCENTRATION, TORSADES, AND MANY MORE MILDER
    SIDE EFFECTS

12
Mercys protocol for administration
  • CODE BLUE3 AMPS OF AMIODARONE 150MG IN EACH CODE
    CART-DOSAGE IN Vf/VT 300 mg IV/IO PUSHMAY
    REPEAT 150 MG IV/IO PUSH
  • STABLE VT DOSAGE 150 MG /100 D5W OVER 10
  • MIX IN D5W-ALL INFUSIONS LASTING LONGER THAN 2
    HOURS SHOULD BE IN GLASS W/A FILTER
  • CENTRAL LINE PREFERRED

13
Monitoring
  • PATIENT MUST HAVE CARDIAC MONITORING FOR ALL
    AMIODARONE LOADING
  • GREATEST ACUTE RISK IS HYPOTENSION WHICH MAY BE
    TREATED W/ RATE REDUCTION ,VASOPRESSORS,INOTROPES,
    AND VOLUME. 2 OF HYPOTENSIVE PATIENTS REQUIRE
    DISCONTINUATION OF THERAPY

14
Toxicology
  • AMIODARONES LIVER,LUNG,THYROID,EYE, SKIN AND
    NERVE TOXICITIES REQUIRE INTENSIVE MONITORING
  • ADVERSE EFFECTS TAKE WEEKS TO MONTHS TO DEVELOP
    AND MAY BE INSIDIOUS
  • ANTI-ARRHYTHMICS SHOULB BE USED ON
    TRIAL-AND-ERROR BASIS.ONCE YOU ARE ON AMIODARONE,
    YOURE ON IT FOR LIFE!

15
Patient teaching
  • PATIENTS MUST BE FULLY IMFORMED OF RISKS AND
    BENEFITS OF AMIODARONE AND BE PREPARED TO FOLLOW
    THROUGH WITH NECESSARY MONITORING.
  • ALL NEW MEDICATIONS/SUPPLEMENTS MUST BE CLEARED
    BY THEIR PHYSICIAN AND PHARMACIST
  • PATIENT MUST APPRECIATE THE IMPORTANCE OF PROMPT
    REPORTING OF ALL NEW SIGNS/SYMPTOMS

16
REVIEW
  • AMIODARONE IS HIGHLY EFFECTIVE ANTI-ARRHYTHMIC
    WITH A LOW RISK OF PRO-ARRHYTHMIA(SUDDEN DEATH)
  • BIZARRE TOXIC PROFILE

17
Nitroglycerin
  • Peter Mirehouse RN, PNII

18
FDA labeled indications
19
FDA Labeled Indications
  • Angina
  • Not responsive to sublingual nitroglycerin
  • Congestive Heart failure - MI

20
Clinical Uses
  • Treatment or prevention of Angina Pectoris
  • Acute decompensated heart failure (especially
    associated with myocardial infarction)
  • Short-term management of pulmonary hypertension
    (unlabeled/Investigational)

21
Drug class
  • Nitrate

22
Mechanism of Action
  • Produces a vasodilator effect to peripheral veins
    and arteries.
  • Primarily reduces cardiac oxygen demand by
    decreasing preload, and modestly reduce
    afterload.
  • Dilates coronary arteries and increases
    collateral flow to ischemic regions.

23
Pharmacokinetics
  • Distribution, Metabolism, Excretion, Elimination
    and Half Life

24
Pharmacokinetics
  • Onset of action Immediate
  • Peak effect Immediate
  • Duration 3-5 minutes
  • Metabolism in liver and excreted in urine.

25
Contraindications
  • Hypersensitivity to organic nitrates.
  • Increase cranial pressure.
  • Severe anemia
  • Constrictive pericarditis
  • Pericardial tamponade
  • Restrictive cardiomyopathy
  • Concomitant use of phosphodiesterase type -5
    (Viagra)

26
Precautions of use
  • Hypotension (SBP lt90 mm hg or 30 mm hg below
    baseline)
  • Extreme bradycardia (lt 50 bpm)
  • Tachycardia without heart failure (100 bpm)
  • Right Ventricular infarct

27
Potential side effects
  • Cardiovascular flushing, hypotension, peripheral
    edema, postural hypotension, syncope, tachycardia
  • Central Nervous headache (common), dizziness,
    lightheadedness
  • Gastrointestinal Nausea, vomiting, xerostomia
  • Respiratory Dyspnea, pharngitis, rhinitis

28
Administration/Dosing
  • IV Nitroglycerin comes in premixed bottles
  • 50mg Nitroglycerin in 250ml D5W
  • 200mcg/ml
  • Must use Nitroglycerin tubing
  • 5 mcg/min, increase by 5 mcg/min every 3-5
    minutes to 20mcg/min. If no response at 20
    mcg/min, may increase by 10 to 20 mcg/min every
    3-5 minutes.
  • Generally accepted maximum dose is 400mcg/min

29
Monitoring
  • Blood pressure
  • Heart rate

30
Toxicology
  • Clinical effects, treatment and range of
    toxicology

Toxicity has not been established in adults or
children
31
Patient teaching
  • Report any signs and symptoms
  • headache, dizziness, lightheadedness, nausea,
    vomiting.

32
Integrilin
  • Ginny Coleman RN, BSN, PNIII

33
FDA labeled indications
34
FDA Labeled Indications
  • Acute coronary syndrome
  • Percutaneous coronary intervention

35
Clinical uses
36
Clinical Uses
  • Used for anticoagulation in patients with acute
    coronary syndrome or undergoing percutaneous
    coronary intervention
  • May be used concurrently with IV Heparin, low
    molecular weight heparin and po Aspirin

37
Drug class
  • Glycoprotein IIb IIIa receptor antagonists

38
Mechanism of action
39
Mechanism of Action
  • Inhibits platelet aggregation
  • Reversibly binds to the platelet receptor
    glycoprotein IIb/IIIa of human platelets
  • Prevents the binding of fibrinogen, von
    Willebrand factor and other adhesive ligands to
    inhibit blood clot formation

40
Platelet aggregation
41
Pharmacokinetics
  • Distribution, Metabolism, Excretion, Elimination
    and Half Life

42
Pharmacokinetics
  • Distribution Human plasma protein binding
    25 Volume distribution of 0.2L/kg
  • Steady state of medication achieved within 4-6
    hours
  • Excretion Renal 50 to 71.4, hemodialysis
    yes 73 to 83
  • Elimination Half-life 1.13 to 2.5 hours

43
Contraindications of use
44
Contraindications of use
  • Abnormal bleeding, either active or within the
    previous 30 days
  • Administration of other parenteral glycoprotein
    IIb/IIIa inhibitors, current or planned (ReoPro
    or Aggrastat)
  • Hypersensitivity to Integrilin
  • Uncontrolled severe hypertension (SBP gt 200 mmHg
    or DBP gt 110)
  • Major surgery within previous 6 weeks
  • Renal dialysis
  • Stroke within previous 30 days
  • Any history of hemmorhagic stroke

45
Precautions of use
46
Precautions of use
  • Arterial sheath removal ensure PTT is lt 45
    seconds, recommend heparin d/c 3-4 hours prior
  • Major or minor bleeding
  • Non-compressable IV sites (subclavian or jugular
    vein)
  • Platelet count lt 100,000 mm recommend
    monitoring
  • Renal insufficiency adjust dosing
  • Vascular or other trauma minimize arterial and
    venous punctures, IM injections, nasogastric
    tubes, nasotracheal intubation or urinary
    catheters

47
Potential side effects
48
Potential side effects
  • Bleeding, may be major or minor
  • Cerebral hemmorhage
  • Intracranial hemmorhage
  • Pulmonary hemmorhage
  • Hypotension
  • Anaphylaxis
  • Thrombocytopenia

49
Mercys protocol for administration
50
Mercys protocol for administration
  • Integrilin is administered based on patient
    weight
  • Initial bolus to be given which is based on
    patient weight (180 mcg/kg)
  • Second bolus (180 mcg/kg) administered 10 minutes
    after first bolus for percutaneous coronary
    intervention ONLY
  • Infusion rate (which must follow first bolus for
    both PCI and ACS) for creatinine lt 2 mg/dL 2
    mcg/kg/minute
  • Infusion rate for creatinine 2-4 mg/dL 1
    mcg/kg/minute

51
Monitoring
52
Monitoring
  • Obtain prothrombin time (PT) and/or activated
    partial thromboplastin time (aPTT) prior to
    initiation of therapy
  • aPTT during therapy to maintain a target aPTT
    between 50 and 70 seconds, unless percutaneous
    coronary intervention is to be performed
  • Activated clotting time (ACT) during PCI to
    target of 200 to 300 seconds
  • aPTT or ACT prior to arterial sheath removal

53
Toxicology
  • Clinical effects, treatment and range of
    toxicology

54
Toxicology
  • Clinical effects of toxicity bleeding,
    thrombocytopenia, hypotension, anaphylaxis,
    neurological or pulmonary changes
  • Treatments discontinue therapy platelet
    transfusion if count is lt 20,000 vasopressive
    medications for hypotension antihistamines and
    epinephrine, IVF for anaphylaxis
  • Monitor CBC, aPTT, INR

55
Patient teaching
56
Patient teaching
  • Educate patient it may take longer to stop
    bleeding during and after drug infusion.
    Pressure needs to be applied to bleeding sites
  • Bed rest may be required during and several hours
    post infusion
  • Educate patient to avoid cuts and bruising for up
    to 3 days post infusion
  • Educate patient to report signs and symptoms of
    bleeding or hypotension

57
Case STudy
58
Case study
  • 54-year-old female with history of HTN,
    hyperlipidemia, obesity and tobacco use
  • Presents to ER with complaints of exertional
    upper sub-sternal chest pain relieved with IV
    morphine, nitrates and heparin in the ER
  • Peak troponin I of 6.17
  • No EKG changes
  • Cardiology consulted and placed patient on IV
    Heparin, po ASA, beta blockers, po statin, IV
    Nitroglycerin gtt titrate to chest pain and IV
    Integrilin at 2 mcg/kg/minute

59
Case Study medication calculation
  • Integrilin gtt ordered at 2 mcg/kg/minute
  • Patient is 122 kg
  • 2mcg x 122 kg x 60 minutes 14640 mcg/hr
  • Infusion contains Integrilin 75 mg/100 mL
  • Concentration 0.75 mg/mL
  • Concentration 750 mcg/mL (0.75mg x 1000 mcg)
  • 14640 mcg/hr / 750 mcg/hr 19.5 mL/hr

60
IV Medication Titration Intervention
61
IV Medication Titration Intervention
62
Complete with each rate change. Minimum of
once a shift.
63
Case study
  • Patient underwent cardiac catheterization
    results normal EF, left coronary artery - no
    obstruction, right coronary artery - greater than
    90 focal obstruction mid-vessel with slow
    distal flow
  • Patient transferred to MMC with sheath left in
    place for intervention on her right coronary
    artery

64
References
  • Curran, M.P. Keating, G.M. (2005).
    Eptifibatide A Review of its Use in Patients
    with Acute Coronary Syndrome and/or Undergoing
    Percutaneous Coronary Intervention. Drugs2005.
    65(14), 2009-2035. Retrieved from CINAHL.
  • Micromedex 2.0. (2012). Eptifibatide. Retrieved
    from http//www.thomsonhc.com/micromedex2/libraria
    n/ND_T/evidencexpert/ND_PR/evidencexpert/CS/4F2B70
    /ND_AppProduct/evidencexpert/DUPLICATIONSHIELDSYNC
    /ED70C0/ND_PG/evidencexpert/ND_B/evidencexpert/ND_
    P/evidencexpert/PFActionId/evidencexpert.DoIntegra
    tedSearch?SearchTermintegrilin
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