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CLINICAL PHARMACOLOGY
Pharmacodynamics and pharmacokinetics of diclofenac
sodium
Diclofenac sodium is a nonsteroidal anti-inflammatory
drug (NSAID). In pharmacologic studies, diclofenac sodium
has shown anti-inflammatory, analgesic and antipyretic
properties. The mechanism of action of diclofenac sodium,
like other NSAIDs, is not completely understood but may
be related to prostaglandin synthetase inhibition.
Diclofenac sodium is completely absorbed from the GI
tract after fasting, oral administration. The diclofenac
sodium in ARTHROTEC is in a pharmaceutical formulation
that resists dissolution in the low pH of gastric fluid
but allows a rapid release of drug in the higher pH environment
of the duodenum. Only 50% of the absorbed dose is systemically
available due to first pass metabolism. Peak plasma levels
are achieved in 2 hours (range 1-4 hours), and the area
under the plasma concentration curve (AUC) is dose proportional
within the range of 25 mg to 150 mg. Peak plasma levels
are less than dose proportional and are approximately
1.5 and 2.0 mcg/mL for 50 mg and 75 mg doses, respectively.
Plasma concentrations of diclofenac sodium decline from
peak levels in a biexponential fashion, with the terminal
phase having a half-life of approximately 2 hours. Clearance
and volume of distribution are about 350 mL/min and 550
mL/kg, respectively. More than 99% of diclofenac sodium
is reversibly bound to human plasma albumin.
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Diclofenac sodium is eliminated through metabolism and
subsequent urinary and biliary excretion of the glucuronide
and the sulfate conjugates of the metabolites. Approximately
65% of the dose is excreted in the urine and 35% in the
bile.
Conjugates of unchanged diclofenac account for 5-10%
of the dose excreted in the urine and for less than 5%
excreted in the bile. Little or no unchanged unconjugated
drug is excreted. Conjugates of the principal metabolite
account for 20-30% of the dose excreted in the urine and
for 10-20% of the dose excreted in the bile.
Conjugates of three other metabolites together account
for 10-20% of the dose excreted in the urine and for small
amounts excreted in the bile. The elimination half-life
values for these metabolites are shorter than those for
the parent drug. Urinary excretion of an additional metabolite
(half-life = 80 hours) accounts for only 1.4% of the oral
dose. The degree of accumulation of diclofenac metabolites
is unknown. Some of the metabolites may have activity.
Pharmacodynamics and pharmacokinetics of misoprostol
Misoprostol is a synthetic prostaglandin E 1 analog with
gastric antisecretory and (in animals) muscosal protective
properties. NSAIDs inhibit prostaglandin synthesis. A
deficiency of prostaglandins within the gastric and duodenal
mucosa may lead to diminishing bicarbonate and mucus secretion
and may contribute to the mucosal damage caused by NSAIDs.
Misoprostol can increase bicarbonate and mucus production,
but in humans this has been shown at doses 200 mcg and
above that are also antisecretory. It is therefore not
possible to tell whether the ability of misoprostol to
prevent gastric and duodenal ulcers is the result of its
antisecretory effect, its mucosal protective effect, or
both.
In vitro studies on canine parietal cells using tritiated
misoprostol acid as the ligand have led to the identification
and characterization of specific prostaglandin receptors.
Receptor binding is saturable, reversible, and stereospecific.
The sites have a high affinity for misoprostol, for its
acid metabolite, and for other E type prostaglandins,
but not for F or I prostaglandins and other unrelated
compounds, such as histamine or cimetidine. Receptor-site
affinity for misoprostol correlates well with an indirect
index of antisecretory activity. It is likely that these
specific receptors allow misoprostol taken with food to
be effective topically, despite the lower serum concentrations
attained.
Misoprostol produces a moderate decrease in pepsin concentration
during basal conditions, but not during histamine stimulation.
It has no significant effect on fasting or post-prandial
gastrin nor intrinsic factor output.
Effects on gastric acid secretion: Misoprostol, over
the range of 50-200 mcg, inhibits basal and nocturnal
gastric acid secretion, and acid secretion in response
to a variety of stimuli, including meals, histamine, pentagastrin,
and coffee. Activity is apparent 30 minutes after oral
administration and persists for at least 3 hours. In general,
the effects of 50 mcg were modest and shorter lived, and
only the 200-mcg dose had substantial effects on nocturnal
secretion or on histamine- and meal-stimulated secretion.
Orally administered misoprostol is rapidly and extensively
absorbed, and it undergoes rapid metabolism to its biologically
active metabolite, misoprostol acid. Misoprostol acid
in ARTHROTEC reaches a maximum plasma concentration in
about 20 minutes and is, thereafter, quickly eliminated
with an elimination t 1/2 of about 30 minutes. There is
high variability in plasma levels of misoprostol acid
between and within studies, but mean values after single
doses show a linear relationship with dose of misoprostol
over the range of 200 to 400 mcg. No accumulation of misoprostol
acid was found in multiple dose studies, and plasma steady
state was achieved within 2 days. The serum protein binding
of misoprostol acid is less than 90% and is concentration-independent
in the therapeutic range.
After oral administration of radiolabeled misoprostol,
about 70% of detected radioactivity appears in the urine.
Maximum plasma concentrations of misoprostol acid are
diminished when the dose is taken with food, and total
availability of misoprostol acid is reduced by use of
concomitant antacid. Clinical trials were conducted with
concomitant antacid; this effect does not appear to be
clinically important.
Pharmacokinetic studies also showed a lack of drug interaction
with antipyrine or propranolol given with misoprostol.
Misoprostol given for 1 week had no effect on the steady
state pharmacokinetics of diazepam when the two drugs
were administered 2 hours apart.
Pharmacokinetics of ARTHROTEC
The pharmacokinetics following oral administration of
a single dose (see Table 1) or multiple doses of ARTHROTEC
(diclofenac sodium/misoprostol) to healthy subjects under
fasted conditions are similar to the pharmacokinetics
of the two individual components.
Table 1.
| MISOPROSTOL
ACID Mean ( SD ) |
| Treatment
(n=36) |
C max (pg/mL)
|
t max (hr)
|
AUC (0-4h)
(pg·hr/mL) |
| ARTHROTEC
50 |
441 (137) |
0.30 (0.13) |
266 (95)
|
| Cytotec®
|
478 (201) |
0.30 (0.10) |
295 (143) |
| ARTHROTEC
75 |
304 (110) |
0.26 (0.09) |
177 (49)
|
| Cytotec
|
290 (130) |
0.35 (0.12) |
176 (58)
|
|
DICLOFENAC Mean ( SD ) |
| Treatment
(n=36) |
C max (ng/mL)
|
t max (hr)
|
AUC (0-12h)
(ng·hr/mL) |
| ARTHROTEC
50 |
1207 (364) |
2.4 (1.0) |
1380 (272) |
| Voltaren®
|
1298 (441) |
2.4 (1.0) |
1357 (290) |
| ARTHROTEC
75 |
2025 (2005) |
2.0 (1.4) |
2773 (1347) |
| Voltaren
|
2367 (1318) |
1.9 (0.7) |
2609 (1185) |
| |
AUC:
Area under the curve
|
| |
| |
The rate and extent of absorption of both diclofenac sodium
and misoprostol acid from ARTHROTEC 50 and ARTHROTEC 75
are similar to those from diclofenac sodium and misoprostol
formulations each administered alone.
Neither diclofenac sodium nor misoprostol acid accumulated
in plasma following repeated doses of ARTHROTEC given
every 12 hours under fasted conditions. Food decreases
the multiple-dose bioavailability profile of ARTHROTEC
50 and ARTHROTEC 75.
Special populations
A 4-week study, comparing plasma level profiles of diclofenac
(50 mg bid) in younger (26-46 years) versus older (66-81
years) adults, did not show differences between age groups
(10 patients per age group). In a multiple-dose (bid)
crossover study of 24 people aged 65 years or older, the
misoprostol contained in ARTHROTEC did not affect the
pharmacokinetics of diclofenac sodium.
Differences in the pharmacokinetics of diclofenac have
not been detected in studies of patients with renal (50
mg intravenously) or hepatic impairment (100 mg oral solution).
In patients with renal impairment (N = 5, creatinine clearance
3 to 42 mL/min), AUC values and elimination rates were
comparable to those in healthy people. In patients with
biopsy-confirmed cirrhosis or chronic active hepatitis
(variably elevated transaminases and mildly elevated bilirubins,
N = 10), diclofenac concentrations and urinary elimination
values were comparable to those in healthy people.
Pharmacokinetic studies with misoprostol in patients
with varying degrees of renal impairment showed an approximate
doubling of t 1/2 , C max and AUC compared to healthy
people. In people over 64 years of age, the AUC for misoprostol
acid is increased.
Misoprostol does not affect the hepatic mixed function
oxidase (cytochrome P-450) enzyme system in animals. In
a study of people with mild to moderate hepatic impairment,
mean misoprostol acid AUC and C max showed approximately
double the mean values obtained in healthy people. Three
people who had the lowest antipyrine and lowest indocyanine
green clearance values had the highest misoprostol acid
AUC and C max values.
CLINICAL STUDIES
Osteoarthritis
Diclofenac sodium, as a single ingredient or in combination
with misoprostol, has been shown to be effective in the
management of the signs and symptoms of osteoarthritis.
Rheumatoid arthritis
Diclofenac sodium, as a single ingredient or in combination
with misoprostol, has been shown to be effective in the
management of the signs and symptoms of rheumatoid arthritis.
Upper gastrointestinal safety
Diclofenac, and other NSAIDs, have caused serious gastrointestinal
toxicity, such as bleeding, ulceration and perforation
of the stomach, small intestine or large intestine. Misoprostol
has been shown to reduce the incidence of endoscopically
diagnosed NSAID-induced gastric and duodenal ulcers. In
a 12-week, randomized, double-blind, dose response study,
misoprostol 200 mcg administered qid, tid or bid, was
significantly more effective than placebo in reducing
the incidence of gastric ulcer in OA and RA patients using
a variety of NSAIDs. The tid regimen was therapeutically
equivalent to misoprostol 200 mcg qid with respect to
the prevention of gastric ulcers. Misoprostol 200 mcg
given bid was less effective than 200 mcg given tid or
qid. The incidence of NSAID-induced duodenal ulcer was
also significantly reduced with all three regimens of
misoprostol compared to placebo (see Table 2).
Table 2.
Misoprostol 200 mcg Dosage
Regimen
|
|
Placebo |
bid |
tid |
qid |
|
|
11% |
6% * |
3% * |
3% * |
|
|
6% |
2% * |
3% * |
1% * |
| N = 1623; 12 weeks. |
| * Misoprostol significantly
different from placebo
(p<0.05) |
Results of a study in 572 patients with osteoarthritis
demonstrate that patients receiving ARTHROTEC have a lower
incidence of endoscopically defined gastric ulcers compared
to patients receiving diclofenac sodium (see Table 3 ).
|
|
Incidence
of ulcers |
| Gastric |
Duodenal |
Table 3.
|
ARTHROTEC 50 tid
|
3% * |
6% |
|
ARTHROTEC 75 bid
|
4% * |
3% |
|
|
11% |
7% |
|
placebo
|
3% |
1% |
| * Statistically significantly
different from diclofenac (p<0.05) |
Animal toxicology
A reversible increase in the number of normal surface gastric
epithelial cells occurred in the dog, rat, and mouse during
long-term toxicology studies with misoprostol. No such increase
has been observed in humans administered misoprostol for
up to 1 year. An apparent response of the female mouse to
misoprostol in long-term studies at 100 to 1000 times the
human dose was hyperostosis, mainly of the medulla of sternebrae.
Hyperostosis did not occur in long-term studies in the dog
and rat and has not been seen in humans treated with misoprostol. |
