Handbook of Critical Care Drug Therapy

Increases O₂ carrying capacity

Increases intravascular volume

After storage, few if any platelets and no factors V or VIII

No major advantage over component therapy

Increases O₂ carrying capacity

Increases intravascular volume

Leukocyte-poor blood prevents fever by lowering exposure to HLA and other antigens

In emergency (risk of exsanguination) group O negative blood can be given. After 2 4 units of O negative blood, subsequent transfusions during the acute episode should continue with O negative to prevent hemolysis

Post-op bleeding, platelets <100,000/mm³

Bleeding patient, platelets <50,000/mm³

Prophylaxis, platelets <20,000/mm^3f

Usual transfusion 6 8 units

Final volume approximately 300 ml

1 unit raises platelet count approximately 5,000 7,000/cu mm

Potential complications: fever, sepsis, DIC, uremia, allo- or autoantibodies

If alloimmunization present (poor 1 h posttransfusion count), HLA match can improve platelet survival; IVIG may also be useful

May need anti-D IgG if Rh negative and given Rh positive platelets

Fever, progressive infection despite antibiotics, hypoplastic marrow

Qualitative function abnormalities (e.g., chronic granulomatous disease)

Fever, chills, dyspnea, leukoagglutination reactions common

Questionable efficacy in neutropenia/sepsis and most other clinical situations

^aPotential for infectious disease transmission.

^bPotential for alloimmunization.

^cPotential for transfusion reaction.

^fProphylaxis in an afebrile patient, not on antibiotics, with no invasive procedures planned, who is not bleeding or has stable platelet counts >10,000/cu mm; may elect to transfuse at a higher platelet count in patients who are febrile, on antibiotics, or have rapidly falling counts.

After transfusion of 10 units PRBCs in patient with excessive bleeding

Bleeding in any patient with elevated PT or aPTT, prolonged thrombin time, or fibrinogen <100 mg/dl

Antithrombin III deficiency requiring heparin therapy

C₁-esterase deficiency with life-threatening laryngeal edema

1 unit has near normal amounts of all coagulation factors and approximately 400 mg fibrinogen

Adequate hemostasis achieved with factor levels of approximately 30% normal

2 units increase levels of factors by approximately 20%

ABO compatibility desirable but not necessary^b

1 ml FFP contains 1 unit of each coagulation factor

Hemophilia A

Von Willebrand disease

Factor XIII deficiency

Uremic bleeding DIC

Does not contain factors II, VII, IX, or X

Off-label use:

Surgical or traumatic bleeding with acquired FVII deficiency

Warfarin-associated bleeding

Coagulopathy of severe liver dysfunction

Management of acute intracerebral hemorrhage

90 120 g/kg IV bolus, may be repeated q2h alternatively

15 30 g/kg IV q12h (warfarin)

2 120 g/kg IV (hepatic coagulopathy)

Generally does not cause systemic thrombosis

Reports of venous thrombosis, myocardial infarction, cerebral sinus thrombosis in patients treated with rFVlla but cause and effect unclear

Refractory bleeding due to inhibitor (<50 Bethesda units/mL) 100 150 porcine units/kg IV

Factor IX deficiency

Warfarin overdose

Factor X deficiency

Hemophilia A (factor VIII inhibitors)

Factor VIII deficiency (Proplex T only)

Factor II deficiency

For warfarin overdose, give 15 U/kg

Thromboembolic problems are common with administration; 5 10 units heparin added to each ml of reconstituted complex

Patients with liver disease or antithrombin III deficiency should not receive complex

Fresh frozen plasma is usually preferred because of clotting problems with factor IX complex; primarily used to control bleeding from warfarin overdose or factor II, VII, IX, or X deficiencies

Factor IX deficiency

Essentially no factors II or VII; <10 units factor X per 100 units factor IX

For serious hemorrhage, factor IX should be increased to 30% to 50%; for surgery, factor IX should be maintained at 30% to 50% for 1 wk postoperatively

1 IU/kg raises level of AT-III by 1% to 2%

Levels should be measured before and 30 min after dose

After 1st dose, level should be >120% of normal and then maintained at >80% of normal with q24h dosing

If administering heparin, lower dose after administering concentrate to prevent excessive bleeding

^aPotential for infectious disease transmission.

^dTo raise blood level % (factor IX complex): (a) determine plasma volume = wt (kg) 70 ml/kg (adult) [1-Hct (in decimals)]; (b) determine number of units needed = desired - actual level plasma volume (mL).

Maintenance: 25 units/kg IV or SC 3 /wk

Ensure adequate iron stores

Maintenance dose can range from 12.5 525 units/kg 3 /wk, adjusted by increments of 10 25 units/kg

Most frequent adverse effects in chronic renal failure (e.g., hypertension, seizures) are related to the rate and extent of increase in erythrocyte count and hematocrit

Maintenance 300 units/kg 3 wk

Increase dose after 8 wk

Decrease dose by 25% if hemoglobin approaches 12 g/dL or increases by greater than 1 g/dL in 2-wk period

Clinical equivalent to epoetin alfa

Preferred for outpatient therapy rather than inpatient therapy; long half-life offers no advantage for inpatient therapy

May increase blood pressure in chronic renal failure

Rapid increase in hemoglobin (>1 g/dL in a week) increases risk of vascular access thrombosis, stroke, myocardial infarction

May be given until absolute neutrophil count reaches 10,000/cu mm

Side effects: fever, bone pain, headache, rash

Preferred for outpatient therapy rather than inpatient therapy; long half-life offers no advantage for inpatient therapy

Side effects similar to filgastrim

Increase risk of chemotherapy-related myelosuppression if given 14 d before and 1 d after each chemotherapy cycle

Do not use if weight <45 kg

Check for clerical errors

Return blood to blood bank with fresh blood and urine samples to check for hemoglobin, bilirubin, and haptoglobin

Antipyretics

Leukocyte-poor blood as alternative

Antipyretics

Leukocyte-poor blood as alternative

Supportive care

Maintain urine output with furosemide, mannitol; alkalinize urine

Epinephrine 0.3 ml (1:1,000) SC or, if reaction is severe (e.g., shock), 0.5 1.0 ml (1:10,000) IV push

Support circulation

Oxygen

Bronchodilators

See Table 11.2

Infusion rate: 15 mg/kg/h for 15 min; if no adverse reactions, then 30 mg/kg/h for 15 min; then increase to maximum infusion rate of 60 mg/kg/h (volume not to exceed 75 ml/h)

If patient develops nausea, back pain, or flushing during infusion slow rate or temporarily stop infusion

Can precipitate and worsen renal insufficiency

Aseptic meningitis may occur within 2 48 h of therapy

Postexposure prophylaxis following percutaneous bites, direct mucous membrane contact, ingestion, or intimate contact

Derived from plasma from individuals with high HBsAb titers (10% to 18% protein)

Should be combined with active immunization with hepatitis B vaccine at separate site if not previously vaccinated

May be repeated 1 mo later in known vaccine nonresponders

May cause local pain and tenderness at the injection site for several days

Use IgIM when vaccine contraindicated (<1 y of age, pregnancy, immunocompromised)

Not given concurrently with live measles virus vaccine

Idiopathic thrombocytopenic purpura

Refer to manufacturers' instructions

Contraindicated in patients with selective IgA deficiencies; however, some preparations are low in IgA and can be used

When Rh positive blood components are given to Rh negative recipients of childbearing age

300 mg dose is given to Rh negative mothers after exposure to 15 ml fetal blood caused by delivery, abortion, or ectopic pregnancy, or after amniocentesis

Vial should not be shaken because it can damage protein and cause aggregate formation that increases risk of adverse reaction

In ITP, fever can be treated with acetaminophen, diphenhydramine, or prednisone

If Hgb <10, reduced dose (25 40 g/kg) should be given

Frequency and dose of maintenance therapy determined by clinical response, including platelet counts, red cell counts, Hgb, and reticulocyte levels

500 units IM (severe exposure or delayed administration)

TIG does not interfere with immune response to tetanus toxoid

(See comments)

High risk patients: immunocompromised state, pregnant women, neonates, premature infants

Antiviral treatment (acyclovir) can be considered for adolescents and adults if illness occurs

Investigational new drug available under expanded access protocol (FFF Enterprises, Temecula, CA, 24h telephone 800-843-7477). Requires informed consent and possibly local IRB approval

Patients with adequate rabies antibody titer should receive only the vaccine

RIG may be given up to the 8th day after the 1st dose of vaccine is given

^aPotential for infectious disease transmission.

Inhibits platelet function and fibrin polymerization

Contraindicated in established venous thromboembolism and in patients with heart failure or dextran hypersensitivity

No more effective than warfarin or heparin in general surgery patients

Venous thrombosis (perioperatively for most abdominal, thoracic, or urologic procedures)

Fixed low dose 5,000 U SC 2 h prior to surgery, then 5,000 U SC q8 12h 5 7 d, or

Continuous infusion

   1 U/kg/h at surgery, then for 3 5 d after surgery

High-very high risk^b,^c: initial dose 5,000 units SC prior to surgery or 2,500 units 1 2 h prior to surgery, followed 12 h later by 2,500 units SC

After initial dose, 5,000 units SC qd 5 10 d

Dosage adjustment and routine monitoring of coagulation parameters are not necessary

At recommended doses does not affect platelet aggregation fibrinolysis, prothrombin time, thrombin time, activated partial thromboplastin time

Pharmacology differs from heparin or other low molecular weight heparins and is not interchangeable on a unit-for-unit basis

Dosage adjustments in renal and hepatic disease have not been established; use with caution

Use with care in patients receiving oral anticoagulants and/or platelet-aggregation inhibitors

Given for 7 10 d

Daily monitoring of the therapeutic effect is not necessary during therapy if laboratory indices of coagulation are normal prior to hip surgery

At recommended doses, does not affect platelet aggregation or global-clotting tests (PT, aPTT)

Pharmacology differs from heparin or other low molecular weight heparins and is not interchangeable on a unit-by-unit basis

Adjust dose in renal disease

Dosage adjustment in hepatic disease has not been established

Use with care in patients receiving oral anticoagulants and/or platelet-aggregation inhibitors

Does not bind platelet factor IV, does not cause immune-mediated thrombocytopenia

No effect on PT, aPTT time, bleeding time, or platelet function

Renal clearance

Not recommended if creatinine clearance <30 mL/min, platelets below 100,000/ L, or weight <50 mg

Bleeding most common adverse effect especially if given less than 6 h after surgery

Coagulation end point for therapy: 1.3 1.5 control PT (INR 2 3)^d

Requires 2 7 d of therapy to deplete coagulation factors and to initiate anticoagulant effect; should overlap with heparin therapy by 4 5 d

Multiple drug interactions (see Table 13.2)

Cautions: (a) hemorrhage: if minor, hold and reduce dose; if moderate or severe, reverse with phytonadione, fresh frozen plasma, factor IX complex and/or rFVIIa (Table 8.2); (b) necrosis of skin or other tissues (especially in females and in protein C deficiency): treat with phytonadione and heparin

• if history of systemic embolism, or paroxysmal or chronic atrial fibrillation, or sinus rhythm with left atrium diameter >5.5 cm
• if recurrent systemic embolism despite adequate warfarin

INR target 2.5 (range 2.0 3.0) and aspirin PO 80 100 mg/d or INR 2.5 3.5 and dipyridamole PO 400 mg/d or clopidogrel

• with documented but unexplained TIA
• with systemic embolism, chronic or paroxysmal atrial fibrillation, or recurrent TIAs despite aspirin therapy

INR target 2.5 (range 2.0 3.0)

Unfractionated heparin or LMWH should be used until the INR is stable and therapeutic for 2 consecutive days

• if age < 60 y with no risk factors^d

• if age < 60 y with heart disease and no risk factors

• if age > 60 y with no risk factors

• if age > 60 y with diabetes or coronary disease

• if heart failure ejection fraction <.35, thyrotoxicosis, hypertension

• if age > 75 y, especially women, with or without risk factors

• with cardioversion if atrial fibrillation more than 2 d in duration

• in patients with mechanical prosthetic valves

• with systemic or pulmonary emboli

Recommendations based in part on 7th ACCP Conference on Antithrombotic and Thrombolytic Therapy. Chest 2004;126:3(Suppl):457S 482S.

^aPatients at risk for thromboembolic complications who are undergoing abdominal surgery are 40 years of age, obese, or in whom surgical procedure requires general anesthesia greater than 30 minutes in duration.

^bAdditional risk factors include malignancy, history of deep-venous thrombosis, or pulmonary embolism.

^cOther risk factors: prolonged immobility or paralysis, varicose veins, heart failure, myocardial infarction, fractures of the pelvis, hip, or leg, possibly high-dose estrogen therapy, and hypercoagulable states.

^dThe International Normalized Ratio (INR) is used to monitor warfarin therapy. The INR is intended to standardize prothrombin time (PT) reporting by minimizing the variability that can result from differences in the sensitivity of the thromboplastin reagent used to perform the PT test. The sensitivity of the thromboplastin reagent is measured by the ISI, which is referenced to a World Health Organization (WHO) reference standard. The INR is calculated as follows: (patient PT/mean normal control)^ISI. The INR adjusts for differences in sensitivity of the thromboplastin reagent and reflects the result that would be obtained with the WHO reference thromboplastin.

Proximal deep venous thrombosis

Acute myocardial infarction

Acute arterial occlusion

Cerebral embolism or transient ischemic attack

Embolism associated with mitral valve disease and/or atrial fibrillation

Follow hematocrit, platelet count, and fecal occult blood

See also Table 4.11, re: anticoagulation and thrombolytic therapy

Start warfarin therapy on day 1 if long-term anticoagulation anticipated, then stop heparin after 4 7 d of joint therapy and INR 2 3 without heparin (see below)

With acute MI, begin with or after rtPA therapy and administer with aspirin (325 mg PO qd)

Nondose-related thrombocytopenia occurs with bovine lung heparin (15%) and porcine intestinal heparin (5%); when thrombocytopenia develops with one preparation, it may be useful to switch to the other; discontinue heparin if platelet count <100,000/cu mm; heparin is rarely associated with thrombosis (usually arterial) and irreversible in vivo platelet aggregation (white clot syndrome)

Treatment-inpatient with and without pulmonary embolism -outpatient treatment in patients without pulmonary embolism

Renal impairment Clcr <30 ml/min 1mg/kg SC qd

Not approved for dialysis patients

Percutaneous coronary interventions

Acute coronary syndrome

If hepatic dysfunction present, start 0.5 g/kg bolus and increase infusion to 30 g/kg/min

Steady state anticoagulated effect after 1 3 h, monitored by aPTT

Decrease dose with hepatic dysfunction

aPTT returns to normal within 2 h of discontinuation

10% to 15% incidence of hematuria, allergic reactions dyspnea/cough, or rash

No adjustment for renal failure

Conversion to warfarin, no load, start at expected daily dose

If ACT <300 s, give 150 g/kg bolus and increase infusion to 30 g/kg/min

If ACT >450 sec, decrease infusion to 15 g/kg/min

Monitor aPTT 4 h after infusion starts (range 1.5 2.5 ratio)

If aPTT is below target, increase infusion by 20%, if aPTT is too high, decrease infusion by 50%

Repeat aPTT after any dosing change

Dosing with renal failure:-Clcr 45 60 mL/min, Scr 1.6 2.0 mg/dL; 50% std infusion rate or 0.075 mg/kg/h-Clcr 30 44, Scr 2.1 3.0; 30% std infusion rate or 0.045 mg/kg/h-Clcr 15 29, Scr 3.1 6.3; 15% std infusion rate or 0.0225 mg/kg/h-Clcr <15, Scr >6.0 avoid or stop infusion

Over dosage with life threatening bleeding, blood transfusion and hemofiltration or dialysis with high flux dialysis membrane, e.g., AN 69, may be useful

Decreased clearance with severe renal failure, use with caution

Alternative

0.75 mg bolus IV, then 1.75 mg/kg/h for duration of procedure, then D/C

Use in conjunction with aspirin

Not associated with immune thrombocytopenia

^bIf patients are hospitalized, subcutaneous heparin may be administered, but hospitalization is not recommended solely for this purpose.

^cThe term refers to patients whose last episode of venous thromboembolism occurred more than 3 months before evaluation but who require long-term anticoagulation because of a high risk of recurrence.

^dIntravenous heparin should be used after surgery only if the risk of bleeding is low.

0 29 min: 1 1.5 mg protamine/100 U heparin

30 60 min: 0.5 0.75 mg/100 U heparin >120 min: 0.25 0.375 mg/100 U heparin

Infuse protamine slowly IV, rate not to exceed 50 mg in 10 min (50 mg protamine in 5 ml sterile water = 10 mg/ml)

Monitor effect with ACT or aPTT

Can cause hypotension, bradycardia, dyspnea, allergic reactions

Relatively contraindicated in diabetics who have received NPH insulin because of risk of hypersensitivity

PO dose same as IV dose

Do not exceed 30 g/d

Adverse effects: muscle necrosis with prolonged administration, cardiac myocyte injury, intrarenal or ureteral thrombosis

Reduce dose in renal, cardiac, or hepatic disease

Effects last 7 14 d

Hemophilia A von Willebrand disease

Cardiac surgery

Effects last 8 12 h

Side effects: facial flushing, conjunctival erythema, headache, blood pressure reduction, tachycardia

Generally does not cause systemic thrombosis

Reports of venous thrombosis, myocardial infarction, cerebral sinus thrombosis in patients treated with rFVlla but cause and effect unclear

Profuse bleeding: 1,000 2,000 U/ml applied topically

Contraindicated in patients with acquired defective color vision and subarachnoid hemorrhage; if patients are going to be treated for more than several days, a full ophthalmologic examination is required

Dose adjusted for moderate to severe renal failure

Adjunct with thienopyridine in PCI

Enteric-coated preparations may be better tolerated by some patients

5% to 45% of patients with coronary artery disease may be relatively resistant to antiplatelet effects

PCI including the prevention of myocardial infarct poststent placement

Initiated 2 6 h prior to PCI

Often used in combination with aspirin

Thrombotic thrombocytopenia purpura rare

Unstable angina pending PCI

Binds both activated and nonactivated platelets

Reverse effects with platelet transfusions

Adjunctive therapy for PCI

Reduce dose in renal failure

Single bolus used in patients with ACS

Partially metabolized by liver

Reduce dose in renal failure

Indications include complete catheter occlusion and the inability to withdraw blood

Should be administered locally in clotted port or ports of catheter; after indicated dwell time duration, the drug should be aspirated from the catheter with a syringe; assessment of catheter patency should then occur catheter should not be flushed to avoid systemic administration of the drug

   May occur 5 14 days after initiating heparin therapy

   Rapid-onset HIT where counts fall within 24 hours of starting heparin after recent heparin exposure (within past 100 days)

Skin lesions at heparin injection sites

or

Acute systemic reaction such as chills, cardiorespiratory distress after IV heparin bolus (obtain platelet count immediately)

or

Venous or arterial thrombosis.

Monitor aPTT 1.5 2.0 times baseline

Renal excretion

HIT undergoing PCI IV bolus of 350 g/kg then 25 g/kg/min IV

Anticoagulation during angioplasty

Increases INR

Hepatobiliary excretion

Anticoagulation during PCI

Monitor aPTT 1.5 2.5 times baseline

(*Adapted from the 7th ACCP Conference on Antimicrobial and Thrombolytic Therapy. Chest 2004;126:Supplement.)