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Transcript 
NON-STEROIDAL ANTIINFLAMMATORY DRUGS
ANTI-INFLAMMATORY
DRUGS
A class of drugs that lower
inflammation and that
includes NSAIDs and
DMARDs.
NSAID
NON SELECTIVE
COX INHIBITOR
Others
Salicylates
Fenamates
SELECTIVE COX
2 INHIBITOR
Indole
derivatives
Aryl acetic
Acid derivatives
Oxicams
Propionic acid
Derivatives
PHARMACOKINETIC
Oral administration
Most NSAIDs are
weak acid (absorbed
well in stomach and
intestinal mucosa)
Most metabolized in
liver (oxidation &
conjugation)
95% bound to
plasma-protein
(high
bioavailability)
MECHANISM OF
ACTION OF NSAIDS
ASPIRIN IS IRREVERSIBLE
INHIBITOR TO COX ENZYMES
NON- SLECTIVE -NON -STEROIDAL
ANTI-INFLAMMATORY DRUGS
Are group of drugs that share in common the
capacity to induce:
 Analgesic effect.
 Antipyretic effect.
 Anti-inflammatory effect.
 Antiplatelet effect
MECHANISM OF ACTION
Analgesic
• Inhibition of
COX enzymes
in CNS
• AntiInflammatory
action
Antipyretic
• Centrally
inhibiting
Prostaglandins
• production
• Inhibit
interleukin-1
release
• Peripheral
vasodilation
Anti-Inflam.
• Peripherally
inhibiting
Prostaglandins
secretion
• Stabilization of
lysosomes
• Inhibits
phagocytosis
• Anti-oxidant
MECHANISM OF ACTION ( CONTINUE)
Antiplatelet
•Inhibition of platelet
COX1 enzyme & TXA2
ANALGESIC
Drug that relieve
pain.
ANTIPYRETIC
Drug that lower the
elevated body
temperature to normal.
CONTINUE
 Effect
on GIT
Inhibition of PGI2 & PGE2
& PGF2 resulting in gastric
upset up to gastric
ulceration & bleeding
CONTINUE

Kidney
Inhibit PGE2 & PGI2
resulting in salt & water
retention , edema ,
hyperkalemia & interstitial
nephritis
CONTINUE
 Respiratory system
With aspirin
High dose act directly on respiratory center
causing hyperventilation & respiratory
alkalosis
Toxic doses causing central respiratory
paralysis& respiratory acidosis
THERAPEUTIC
USES SHARED BY
NS-NSAIDs
Fever.
Analgesic
(Type of
pain?)
Headache, Migraine,
Dental pain
Common
cold.
CONTINUE
 Rheumatic
/ Rheumatoid
arthritis
 Dysmenorrhea
Muscular
pain
ADVERSE EFFECTS
GIT upsets ( nausea, vomiting)
 GIT bleeding & ulceration
 Bleeding
 Hypersensitivity reaction
 Inhibition of uterine
contraction
 Salt & water retention

CLINICAL USES
 Acute
rheumatic fever
 Reducing
the risk of myocardial
infarction
 Prevention
of pre-eclampsia
Adverse Effects Related to
(A)Therapeutic Doses Of Aspirin
Gastric
irritation
Hypersensitivity
( aspirin asthma)
Acute Gouty arthritis
Reye's syndrome
(B) TO HIGH DOSES
&PROLONGED USE OF ASPIRIN


Salicylism ( ringing of ears (tinnitus),
vertiog)
Hyperthermia
 Gastric
ulceration & bleeding
 Metabolic
acidosis
SIDE EFFECTS
RELATED TO HIGH DOSES
CONTRAINDICATIONS
 Peptic
ulcer
 Pregnancy
 Hemophilic patients
 Patients taking anticoagulants
 Children with viral infections
 Gout ( small doses )
PARACETAMOL
A commonly used analgesic
antipyretic instead of
aspirin in cases of :
Peptic
or gastric ulcers.
Bleeding tendency.
Allergy to aspirin.
Viral infections in
children .
Pregnancy.
ADVERSE EFFECTS

Mainly on liver due to its active metabolites

Therapeutic doses elevate liver enzymes

High doses cause liver & kidney necrosis

Treatment toxicity of paracetamol:
N- acetylcysteine to neutralize the toxic
metabolites
PROPIONIC ACID DERIVATIVES
IBUPROFEN
CLINICAL USES
 Therapeutic
uses shared by NS-
NSAIDs
 Acute


gouty arthritis
Patent ductus arteriosus
More potent as an anti-inflammatory than
aspirin
PREPARATIONS OF IBUPROFEN
Oral preparations.
 Topical cream for osteoarthritis.
 A liquid gel for rapid relief of postsurgical dental
pain.
 Intravenous route as In patent ductus arteriosus

ADVERSE EFFECTS

Adverse effects shared by NS-NSAIDs
(Gastric upset less frequent
than aspirin)


Rare hematologic effects (agranulocytosis &
aplastic anemia ).
Ocular disturbance
CONTRAINDICATIONS
Peptic ulcer
 Allergic patients to aspirin
 Kidney impairment
 Liver diseases
 Pregnancy
 Haemophilic patients
 The concomitant administration of
ibuprofen antagonizes the irrevesible
platelet inhibition of aspirin( limit
cardioprotective effect of aspirin ).

OXICAM DERIVATIVES
Piroxicam
Tenoxicam
PIROXICAM

Half- Life 45 hours

Given once daily
ADVERSE EFFECTS
Less frequent gastric upset (20%) .
 Dizziness
 Tinnitus
 Headache
 Allergy

ACETIC ACID DERIVATIVES
Diclofenac
PREPARATIONS OF DICLOFENAC
 Diclofenac
with misoprostol decreases
upper gastrointestinal ulceration ,but
result in diarrhea.
 Diclofenac with omeprazole to prevent
recurrent bleeding.
 .1% opthalmic preparation for
postoperative opthalmic inflammation.
 A topical gel 3% for solar keratosis.
 Rectal suppository
CONTINUE
Oral mouth wash.
 Intramuscular preparations.

CLINICAL USES
Clinical uses shared by Ns-NSAIDs
 Acute gouty arthritis
 Locally to prevent or treat post
opthalmic inflammation
 A topical gel for solar keratosis

ADVERSE EFFECTS
Adverse effects shared by
NS-NSAIDs
SELECTIVE COX-2 INHIBITORS
General advantages :
o Potent anti-inflammatory
o Antipyretic & analgesic
o Lower incidence of gastric
upset
o No effect on platelet
aggregation ( COX-1)
GENERAL ADVERSE EFFECTS
Renal toxicity
 Dyspepsia & heartburn
 Allergy
 Cardiovascular ( do not offer the
cardioprotective effects of non-selective
group).

CLINICAL USES
Postoperative patients undergoing bone
repair
 Acute gouty arthritis
 Acute musculoskeletal pain
 Ankylosing spondylitis

CELECOXIB

Half-life 11 hours ( Given twicw daily)

Food decrease its absorption

Highly bound to plasma proteins

Metabolized in liver to inactive metabolites
MELOXICAM
 Relatively
selective Cox2
inhibitors.
Safer
than piroxicam.
PHARMACOKINETICS
 Given
orally ,rectally, I.M.,I.V.
 Metabolized in liver to inactive
metabolites.
 Excreted in urine 50% and in feces
50%.
 Half-life 20 hours.
 Given once daily.
CLINICAL USES
Shared
by selective COX-2
inhibitors
ADVERSE EFFECTS
Shared
by selective COX-2
inhibitors
DRUG INTERACTIONS
Cholestyramine increases the
clearance of the drug .
NABUMETONE
Relatively selective COX-2
inhibitor
Well absorbed orally.
Metabolized in liver to active
metabolites.
Half-life 26 hours.
Taken once daily.
CLINICAL USES
Shared by selective COX-2
inhibitors
ADVERSE EFFECTS
Shared by selective COX-2
inhibitors
Headache
Tinnitus
Photosensitivity
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