Drug Interactions of Oral Anticoagulants (Warfarin) PDF

Summary

This document describes drug interactions related to oral anticoagulants, specifically warfarin. It covers potentiating and inhibiting drugs, as well as fibrinolytic agents and related enzymes. It also briefly touches on recombinant tissue plasminogen activators and urokinase.

Full Transcript

Drug in
nteraction
ns of oral anticoagu
a ulants (warfarin)

Dru
ugs that potentiate
p warfarin Drugs
s that inhib
bit warfariin
 Mic
crosomal enzyme
e in
nhibitors  Microsomal enzym ers (e.g.
me induce
(e.g
g. cimetidinne, chloram mphenicol)) ↓ phenoba mpin) ↑
arbital, rifam
mettabolism of o warfarin. metabolism of warffarin.
 Oraal antibiotiics: ↓ vit K synthesiss  Oral con
ntraceptive es and vit K. ↑
by kkilling the gut
g flora synthesis
s of clottin g factors
 Liquuid paraffiin: ↓ vit K absorption
a  Aluminum hydroxxide: ↓ warffarin
 NSA AIDs: disp place warfa arin from p
pp. absorptio
on

█ FIBR
RINOLYTIC (THROM
MBOLYTIC
C) DRUGS
S

 Norrmally, whe en a fibrin clot is form
med, plasm minogen gets
g in conntact with this
t clot
andd becomess activated d into plas smin by th he help off naturally occurring g tissue
plassminogen n activatorrs (t-PAs). Plasmin causes
c lysis of the clo
ot.
 Theese endoge enous activators pre eferentially
y activate plasminog gen that is
s bound
to ffibrin, which (in the eory) confiines fibrinolysis to the formeed thromb bus and
avooids systemmic activatiion.
 Fibrrinolytic drrugs cause rapid ac ctivation of
o plasminogen to fo orm plasmmin, but
unfoortunately,, they may y activate both fibrin n-bound plasminoge
p en and circculating
plassminogen thus, bo oth prote ective hemostatic thrombi and path hogenic
thro
omboembo oli are brok
ken down ((→ risk of bleeding).
b

Strepttokinase
 Streeptokinasee is a prote
ein (not an
n enzyme) that is isoolated from
m streptoc
cocci; it
activates plassminogen into plasmiin non-enzzymaticallyy.
 It m
may be antigenic (cauuses allergyy) in some people.

213
 Urokin
nase
 Uro okinase is a proteas se originallly isolated
d from
urinne; the druug is now prepared in recomb binant
formm from culttured kidney cells.
 It is less antigenic than streptokina
s ase.

Recommbinant tissue
t pla
asminoge en activa
ators (t-
PAs): ((Alteplase
e, reteplas
se, and ten
necteplase
e)
 Theey are recoombinant human protteins produ uced in cultured cellss.
 Theey are mos c to fibrin-b
st specific bound pla asminogen; local actiivation of plasmin
p
at th
he thrombus site red duces the incidence of o systemic bleeding g.
 Retteplase an nd tenectteplase h have long half-life. The long half-life permits
admministrationn as a bolus i.v. injeection rath
her than byy continuoous infusio on. (two
injections i.v. separatedd by 30 minutes for reteplase,
r , one singlle i.v. injec
ction for
teneecteplase e).

Therap
peutic use
es of throm
mbolytic d
drugs
 Theey are giveen by i.v. route
r in ca
ases of ac cute myoc arction, is
cardial infa schemic
stro
oke, pulmo onary embo olism, and arterial thrombosis.
 In c
cases of ac cute MI, th hey should d be givenn within 12
2 h of onseet. The ma aximum
bennefit is obta
ained if treatment is ggiven within 90 minuutes of the onset of pain.
p
 Befoore throm mbolysis, care
c shouldd be take en to ensu
ure there is no liab bility for
blee
eding in a critical
c site
e e.g. retina
a, CNS, ettc.

Advers
se effects of thromb
bolytic dru
ugs
– Sysstemic ble
eeding is the major adverse effect. The
e risk is hhigh with strepto-
s
kina
ase and loww with the recent rec
combinant tissue pla
asminogen activators s.
– Streeptokinasee can cause allergy, fever, and
d hypotenssion during
g i.v. infusion.

█ ANT
TIPLATELE
ET (ANTIT
THROMBO
OTIC) DRU
UGS

Aspirin
 Asp
pirin inhibit platelet ag
ggregation
n by:
– Irreverssible inhibition of COOX enzyme e → ↓ TXA2 → ↓ plateleet aggregattion.
– Irreverssible acetylation of plaatelet cell membrane
m s → ↓ platellet adhesio
ons.
– Decreaase platele et ADP synnthesis → decrease platelet accuumulation.
 At h
higher dosses (> 325 5 mg/day), aspirin maym decrea ase endothhelial synth hesis of
PGII2, which inhibits pla
atelet activvity. Low doses
d (75-150 mg/daay) ↓ synth
hesis of
plattelet TXA2 more thann PGI2 in eendothelial cells and avoid this effect.
 Othher NSAIDss do not haave compa arable antithrombotic activity.

214