Pharmacology Acetaminophen (Paracetamol) PDF

Summary

This document discusses the pharmacology of acetaminophen, including its pharmacokinetics, mechanism of action, therapeutic uses, and adverse effects. Acetaminophen is a common over-the-counter analgesic and antipyretic.

Full Transcript

█ NON
N-OPIOID ANALGES
SICS

1. Ace
etaminophen (Para
acetamoll)

Pharm
macokinetics
 Abssorption is complete and rapid from GIT with
w peak levels afteer 30 min.
 Mettabolism: liver by conjugation
c n. At highh doses, it is convverted into
o toxic
mettabolite (N
N-acetyl-be ne) that is responsible for hepaatotoxicity..
enzoquinon
 Exc
cretion: maainly renal.

Mecha
anism & Ph
harmacolo
ogical effe
ects
 It iss a selectivve Cox III inhibitor sso it inhibitts PGs syn
nthesis in tthe brain only
o and
hass analgesic & antip pyretic acttions witho
out effects on the eenzymes that t are
respponsible fo or synthesis of perip
pheral PGss and so it has no a nti-inflammatory
action.
 It ha
as little orr No effects on the C
CVS, GIT, re
espiratory or platelett functions
s.

Therap
peutic use
es
As anaalgesic andd antipyretic when aspirin is s contraindicated (ee.g. patien
nts with
peptic ulcer, hemmophilia, etc).
e Aceta
aminophen
n can be administer
a red in preggnancy
with greater safetty than asp
pirin.

Advers
se effects
 At therapeuttic doses: acetami nophen iss
well-tolerated but may cause:
c
– Skin rash h& drug fever (a as allergic c
reactions)..
– Long term m use may lead
l to ren
nal failure.

 In ttoxic dose
es: dose-d
dependen
nt hepato--
toxiicity (centtrilobular necrosis): It occurs
s
with
h large dosses (about 15 gm in a adults and
d
m in childrren)
4 gm

Mec
chanism of
o hepatottoxicity
 A
Acetamino
ophen is converted
d to toxic
c
metabolite
e (N-acety
yl-benzoquuinone) inn
tthe liver that need
ds detoxifiication by
y
reduced glutathione
e.

337
  When glutathione store is depleted, the toxic metabolite binds covalently to
cellular proteins producing hepatocellular damage.
 Clinical symptoms of toxicity (e.g. vomiting) occur within 24 hrs but signs of
hepatic damage (e.g. jaundice) occur after 2-6 days.

Treatment of toxicity
The 20 hour IV protocol of
 Gastric lavage with activated charcoal. acetylcysteine
 Sulfhydryl donors (acetylcysteine) to
– First, administer an initial
restore hepatic glutathione. It must be
loading dose of 150 mg/kg IV
started within 8 hours of toxicity. over 60 minutes.
 Hemodialysis: better within the first 12
– Next, administer 12.5 mg
hrs after ingestion. /kg per hour IV for 4 hours.
– Finally, administer 6.25 mg
Nefopam (Acupan) /kg per hour IV for 16 hours.

Mechanism and effects
 It is a central analgesic without antipyretic or anti-inflammatory activity. It is
more potent than NSAIDs.
 The analgesic mechanism is unclear but may be related to inhibition of many
transmitters reuptake or blocking central voltage-gated Na+ channels.
 Nefopam is also used to combat severe hiccups.

Adverse effects
– Precipitation of epileptic convulsions in patients with epilepsy.
– Weak atropine-like actions: dry mouth, urine retention, etc.

Contraindications: history of epilepsy

Dipyrone (Novalgin)

Mechanism and effects
 Analgesic antipyretic that is more potent than aspirin. It has no anti-
inflammatory action.
 Its use was restricted in many countries because of risk of agranulocytosis
which is not dose-dependent.

Adverse effects
– Agranulocytosis: reversible in 10 days after stoppage of the drug but lethal in
10% of cases.
– Allergic reactions and anaphylaxis.
– It can trigger bronchoconstriction in patients with Asthma.

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