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SIDE EFFECTS Pre-Marketing
Experience
Sildenafil citrate
was administered to over 3700 patients (aged 19-87 years)
during clinical trials
worldwide. Over 550 patients were treated for longer than
one year.
In placebo-controlled clinical
studies, the discontinuation rate
due to adverse events for sildenafil citrate
(2.5%) was not significantly different from placebo
(2.3%). The adverse events were generally transient
and mild to moderate in nature.
In trials of all designs, adverse events reported by patients
receiving sildenafil citrate
were generally similar. In fixed-dose studies, the incidence
of some adverse events increased with dose. The nature of
the adverse events in flexible-dose studies, which more
closely reflect the recommended dosage regimen, was similar
to that for fixed-dose studies.
When sildenafil citrate
was taken as recommended (on an as-needed basis) in flexible-dose,
placebo-controlled clinical
trials, the adverse events found in TABLE 2 were reported.
| TABLE
2 Adverse Events Reported by ³2%
of Patients Treated with Sildenafil Citrate and
More Frequent on Drug Than Placebo in PRN Flexible-Dose
Phase II/III Studies |
| Adverse
Event |
Percentage
of Patients Reporting Event |
| |
Sildenafil
Citrate |
Placebo |
| |
N=734 |
N=725 |
| Headache |
16% |
4% |
| Flushing |
10% |
1% |
| Dyspepsia |
7% |
2% |
| Nasal
Congestion |
4% |
2% |
| Urinary
Tract Infection |
3% |
2% |
| Abnormal
Vision* |
3% |
0% |
| Diarrhea |
3% |
1% |
| Dizziness |
2% |
1% |
| Rash |
2% |
1% |
| *
Abnormal Vision: Mild and transient,
predominantly color
tinge to vision, but also increased sensitivity
to light or
blurred vision. In these studies, only one patient
discontinued due to abnormal
vision. |
Other adverse reactions occurred at a rate
of >2%, but equally common on placebo; respiratory tract
infection, back pain,
flu syndrome, and arthralgia.
In fixed-dose studies, dyspepsia
(17%) and abnormal
vision (11%) were more
common at 100 mg than at lower doses. At doses above the
recommended dose range, adverse events were similar to those
detailed above but generally were reported more frequently.
The following events occurred in <2% of patients in controlled
clinical trials; a causal relationship to sildenafil citrate
is uncertain. Reported events include those with a plausible
relation to drug
use; omitted are minor events and reports too imprecise
to be meaningful.
Body as a Whole: Face edema, photosensitivity
reaction, shock, asthenia, pain, chills, accidental fall,
abdominal pain,
allergic reaction, chest
pain, accidental injury.
Cardiovascular: Angina pectoris, AV block,
migraine, syncope, tachycardia, palpitation, hypotension,
postural hypotension,
myocardial ischemia, cerebral thrombosis, cardiac
arrest, heart failure,
abnormal electrocardiogram, cardiomyopathy.
Digestive: Vomiting, glossitis, colitis, dysphagia,
gastritis, gastroenteritis, esophagitis, stomatitis, dry
mouth, liver function
tests abnormal, rectal
hemorrhage, gingivitis.
Hemic and Lymphatic: Anemia and leukopenia.
Metabolic and Nutritional: Thirst, edema,
gout, unstable diabetes, hyperglycemia, peripheral
edema, hyperuricemia, hypoglycemic reaction, hypernatremia.
Musculoskeletal: Arthritis, arthrosis, myalgia,
tendon rupture, tenosynovitis, bone
pain, myasthenia, synovitis.
Nervous: Ataxia, hypertonia, neuralgia, neuropathy,
paresthesia, tremor, vertigo, depression, insomnia, somnolence,
abnormal dreams,
reflexes decreased, hypesthesia.
Respiratory: Asthma, dyspnea, laryngitis,
pharyngitis, sinusitis, bronchitis, sputum
increased, cough increased.
Skin and Appendages: Urticaria, herpes
simplex, pruritus, sweating, skin
ulcer, contact dermatitis,
exfoliative dermatitis.
Special Senses: Mydriasis, conjunctivitis,
photophobia, tinnitus, eye
pain, deafness, ear pain,
eye hemorrhage, cataract,
dry eyes.
Urogenital: Cystitis, nocturia, urinary frequency,
breast enlargement, urinary incontinence, abnormal
ejaculation, genital
edema and anorgasmia.
Post-Marketing Experience
Cardiovascular: Serious cardiovascular
events, including myocardial infarction, sudden cardiac
death, ventricular
arrhythmia, cerebrovascular hemorrhage, transient
ischemic attack and
hypertension, have been reported post-marketing in temporal
association with
the use of sildenafil citrate. Most, but not all, of these
patients had preexisting cardiovascular
risk factors. Many of these events were reported to occur
during or shortly after sexual
activity, and a few were reported to occur shortly after
the use of sildenafil citrate
without sexual activity.
Others were reported to have occurred hours to days after
the use of sildenafil citrate
and sexual activity. It is not possible to determine whether
these events are related directly to sildenafil citrate,
to sexual activity,
to the patient's underlying cardiovascular
disease, to a combination of these factors, or to other
factors (see WARNINGS for
further important cardiovascular
information).
Other Events: Other events reported post-marketing
to have been observed in temporal
association with
sildenafil citrate
and not listed in Pre-Marketing Experience include:
Nervous: Seizure and anxiety.
Urogenital: Prolonged erection, priapism
(see WARNINGS) and hematuria.
Ocular: Diplopia, temporary vision
loss/decreased vision, ocular redness or bloodshot
appearance, ocular
burning, ocular swelling/pressure,
increased intraocular
pressure, retinal
vascular disease
or bleeding, vitreous detachment/traction and paramacular
edema.
DRUG INTERACTIONS
Effects of Other Drugs on Sildenafil Citrate
In Vitro Studies: Sildenafil metabolism
is principally mediated by the cytochrome
P450 (CYP) isoforms 3A4 (major route) and 2C9 (minor route).
Therefore, inhibitors of these isoenzymes may reduce
sildenafil clearance.
In Vivo Studies: Cimetidine (800 mg), a nonspecific
CYP inhibitor, caused a 56% increase in plasma
sildenafil concentrations when coadministered with sildenafil
citrate (50 mg) to
healthy volunteers.
When a single 100 mg dose
of sildenafil citrate
was administered with erythromycin, a specific
CYP3A4 inhibitor, at
steady state (500 mg
bid for 5 days), there was a 182% increase in sildenafil
systemic exposure
(AUC). In addition, coadministration
of the HIV protease inhibitor
saquinavir, also a CYP3A4
inhibitor, at steady state
(1200 mg tid) with sildenafil citrate (100 mg single dose)
resulted in a 140% increase in sildenafil Cmax
and a 210% increase in sildenafil AUC. Sildenafil citrate
had no effect on saquinavir
pharmacokinetics. Stronger CYP3A4
inhibitors such as ketoconazole or itraconazole would be
expected to have still greater effects, and population
data from patients in clinical
trials did indicate a reduction
in sildenafil clearance
when it was coadministered with CYP3A4 inhibitors (such
as ketoconazole, erythromycin, or cimetidine) (see DOSAGE
AND ADMINISTRATION).
Coadministration with the HIV
protease inhibitor
ritonavir, which is a highly potent
P450 inhibitor, at steady state
(400 mg bid) with sildenafil citrate (100 mg single dose)
resulted in a 300% (4-fold) increase in sildenafil Cmax
and a 1000% (11-fold) increase in sildenafil plasma
AUC. At 24 hours the plasma
levels of sildenafil were still approximately 200 ng/mL,
compared to approximately 5 ng/mL when sildenafil was dosed
alone. This is consistent with ritonavir's marked effects
on a broad range of
P450 substrates. Sildenafil citrate
had no effect on ritonavir
pharmacokinetics (see DOSAGE AND
ADMINISTRATION).
It can be expected that concomitant
administration
of CYP3A4 inducers,
such as rifampin, will
decrease plasma levels
of sildenafil.
Single doses of antacid
(magnesium hydroxide/aluminum hydroxide) did not affect
the bioavailability of sildenafil citrate.
Pharmacokinetic data from patients in clinical
trials showed no effect on sildenafil pharmacokinetics
of CYP2C9 inhibitors (such as tolbutamide, warfarin), CYP2D6
inhibitors (such as selective serotonin
reuptake inhibitors, tricyclic antidepressants), thiazide
and related diuretics, ACE
inhibitors, and calcium
channel blockers.
The AUC of the active
metabolite, N-desmethyl sildenafil, was increased 62% by
loop and potassium-sparing
diuretics and 102% by nonspecific
beta-blockers. These effects on the metabolite
are not expected to be of clinical
consequence.
Effects of Sildenafil Citrate on Other Drugs
In Vitro Studies: Sildenafil is a weak
inhibitor of the
cytochrome P450 isoforms 1A2, 2C9, 2C19, 2D6, 2E1 and 3A4
(IC50 >150 mM). Given sildenafil peak plasma
concentrations of approximately 1 mcM after recommended
doses, it is unlikely that sildenafil citrate
will alter the clearance
of substrates of these isoenzymes.
In Vivo Studies: When sildenafil citrate
100 mg oral was coadministered
with amlodipine, 5 mg or 10 mg oral, to hypertensive
patients, the mean additional
reduction on supine
blood pressure
was 8 mmHg systolic and 7 mmHg diastolic.
No significant
interactions were shown with tolbutamide
(250 mg) or warfarin (40 mg), both of which are metabolized
by CYP2C9.
Sildenafil citrate
(50 mg) did not potentiate
the increase in bleeding time caused by aspirin
(150 mg).
Sildenafil citrate
(50 mg) did not potentiate
the hypotensive
effect of alcohol
in healthy volunteers with mean
maximum blood
alcohol levels of
0.08%.
Sildenafil (100 mg) did not affect
the steady state pharmacokinetics
of the HIV protease inhibitors,
saquinavir and
ritonavir, both of which are CYP3A4
substrates.
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