Ch. 11 - Pharmacologic agents Flashcards

1
Q

What pharmacologic agents may require reversal for hemostasis?

A
Warfarin
Heparin
Antiplatelet drugs
Direct thrombin inhibitors
Anti-Xa inhibitors
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2
Q

Describe the mechanism of action of warfarin.

A

Racemic warfarin (of which the S-racemer is more potent) acts as a vitamin K antagonist to inhibit VKORC in the synthesis of factors II, VII, IX, and X (and protein S, C)

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3
Q

How can a supratherapeutic INR with bleeding be reversed?

A
Stop warfarin!
Vitamin K (IV), FFP (multiple units), or PCC
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4
Q

How is a very supratherapeutic INR (>9) without bleeding managed?

A

High dosage of vitamin K (5mg or more), possibly IV

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5
Q

How is a somewhat supratherapeutic INR without bleeding managed?

A

Give vitamin K if INR >4 (oral, 1-5mg), or simply discontinue oral therapy.

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6
Q

What are the advantages of prothrombin complex concentrates over FFP in reversing warfarin?

A

Smaller doses are needed, ABO blood typing is not required, and there is less risk of reaction.

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7
Q

What are the different types of PCCs?

A

Three-factor PCCs (Profilnine, Bebulin)
Four-factor PCCs (K-centra) *better
Activated PCC (FEIBA?)

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8
Q

What is the indication for activated prothrombin complex concentrates?

A

Hemophilia–not reversal of warfarin.

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9
Q

How are PCC products prepared?

A

Solvent detergent treatment of human plasma with fractionation.

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10
Q

What are the indications for K-centra?

A

Reversal of warfarin coagulopathy (FDA-approved)

Coagulopathy due to other oral anticoagulants

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11
Q

How is K-centra dosed?

A

If INR 2-4: 25u/kg
If INR 4-6: 35u/kg
If INR >6: 50u/kg
(assign a max weight of 100kg)

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12
Q

What should follow after K-centra administration?

A

Re-check PT/PTT 2hrs later. Add vitamin K 10-12hrs later when K-centra effect is weaning off.

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13
Q

What are some contraindications for K-centra?

A

Thrombotic conditions (DIC, APS, Protein C/S/AT deficiency)
Pregnancy
Recent history of DVT/PE/MI/TIA

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14
Q

How is heparin produced, and how does it exert anticoagulant effect?

A

Heparin is isolated from bovine or porcine sources. Heparin binds to antithrombin III, greatly potentiating its effect.

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15
Q

How is LMWH produced, and how does it compare to UFH?

A

Heparin is depolymerized or digested to yield smallermolecules which have more predictable dose reponse.

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16
Q

How is heparin eliminated? How should it be monitored?

A

80% via renal route.

Measure PTT for UFH, Anti-Xa activity for LMWH.

17
Q

How is protamine produced? What is its indication?

A

Derived from salmon sperm/gonad, it is a highly basic/cationic polypeptide which is used as a heparin antidote.

18
Q

In general, how is protamine dosed?

A

1mg protamine neutralizes 100U of heparin. IT can also neutralize 1mg of enoxaparin,or 100u of dalteparin.

19
Q

What is the heparin rebound phenomenon, and why is it significant?

A

Hypocoagulability which resurfaces following heparin neutralization with protamine. It is a concern in the early post-op period after cardiac surgery and it cannot be detected by ACT.

20
Q

How can residual heparin effect be monitored following neutralization with protamine?

A

TEG (thromboelastography) with or without heparinase (compare R-times)

Review DIC panel (look for prolonged PTT and TT, but rule out hypofibrinogenemia first)

21
Q

What is NovoSeven, and what is its use?

A

Recombinant factor VIIa (expressed from cultured hamster kidney cells), which is approved for prevention or treatment of bleeding in patients with hemophilia and antibodies. However, it is almost always used off-label for other bleeders.

22
Q

What is the mechanism of action of desmopressin and what is it used for?

A

It increases plasma levels of fVIII and vWF probably by release from vascular endothelium. Used for von Willebrand disease, uremic thrombocytopathy, and other bleeding conditions.

23
Q

When should RhoGAM be given?

A

At 28wks of pregnancy, within 72hrs of childbirth, and anytime fetomaternal hemorrhage is suspected.

24
Q

What are three indications for RhIG treatment?

A

Prevention of HDFN
Prevention of D-sensitization in mismatch
ITP

25
Q

What is aprotinin?

A

A serine protease inhibitor which acts as a fibrinolytic agent but is too toxic for most clinical use.

26
Q

When are antifibrinolytic agents used?

A

In situations of primary fibrinolysis (not in secondary cases such as in DIC).

27
Q

What are the indications for aminocaproic acid? How is it dosed?

A

For fibrinolytic bleeding (eg following tPA). Dose 5gm first, then 1gm per hour until bleeding stops (up to 8hrs).

28
Q

How is aminocaproic acid eliminated? What is its half life? Should it be used in neonates?

A

65% renally excreted, with a half-life of 2hrs. It should not be given to neonates as it contains benzyl alcohol (associated with fatal “gasping syndrome”).

29
Q

What is the approved indication for tranexamic acid?

A

To reduce or prevent bleeding during tooth extraction in patients with hemophilia. It is also helpful for reducing instrumented bleeding, post-delivery hemorrhage.

30
Q

How is tranexamic acid dosed? Describe its kinetics.

A

10mg/kg IV given 2-3 times per day. It is renally excreted with a half-life of 2hrs.