Dilantin™ Infatabs
Phenytoin
Anticonvulsant
Pfizer
http://www.pfizer.com/pfizer/main.jsp
Dilantin Monograph PDF download here.
Dilantin™-30 Suspension
Phenytoin
Anticonvulsant
Pfizer
Dilantin™-125 Suspension
Phenytoin
Anticonvulsant
Pfizer
CPS:PIS_m166400
Pharmacology
Dilantin Infatabs and Dilantin-30/Dilantin-125
suspensions are anticonvulsant drugs which can be useful in the treatment of
epilepsy. The primary site of action appears to be the motor cortex where
spread of seizure activity is inhibited. Possibly by promoting sodium efflux
from neurons, phenytoin tends to stabilize the threshold against
hyperexcitability caused by excessive stimulation or environmental changes
capable of reducing membrane sodium gradient. This includes the reduction of
post-tetanic potentiation at synapses. Loss of post-tetanic potentiation
prevents cortical seizure foci from detonating adjacent cortical areas. Phenytoin
reduces the maximal activity of brain stem centres responsible for the tonic
phase of tonic-clonic (grand mal) seizures.
Clinical studies using
Dilantin Infatabs have shown an average plasma half-life of 14 hours with
a range of 7 to 29 hours. The plasma half-life of phenytoin in man
after oral administration of phenytoin oral suspension averages 22 hours,
with a range of 7 to 42 hours. Steady-state therapeutic levels are
achieved at least 7 to 10 days after initiation of therapy with recommended
doses of 300 mg/day.
When serum level
determinations are necessary, they should be obtained at least 7 to
10 days after treatment initiation, dosage change, or addition or
subtraction of another drug to the regimen so that equilibrium or steady-state
will have been achieved. Trough levels obtained just prior to the patient's
next scheduled dose, provide information about clinically effective serum level
range and confirm patient compliance. Peak drug levels, obtained at the time of
expected peak concentration, indicate an individual's threshold for emergence
of dose-related side effects. For Dilantin Infatabs, Dilantin-30 and
Dilantin-125 suspensions, peak serum levels occur 1˝ to 3 hours after
administration.
In most patients
maintained at a steady dosage, stable phenytoin serum levels are achieved.
There may be wide interpatient variability in phenytoin serum levels with
equivalent dosages. Patients with unusually low levels may be noncompliant or
hypermetabolizers of phenytoin. Unusually high levels result from liver
disease, congenital enzyme deficiency or drug interactions which result in
metabolic interference. The patient with large variations in phenytoin serum
levels, despite standard doses, presents a difficult clinical problem. Serum level
determinations in such patients may be particularly helpful. As phenytoin is
highly protein bound, free phenytoin levels may be altered in patients whose
protein binding characteristics differ from normal.
Most of the drug is
excreted in the bile as inactive metabolites which are then reabsorbed from the
intestinal tract and excreted in the urine. Urinary excretion of phenytoin and
its metabolites occurs partly with glomerular filtration but more importantly
by tubular secretion. Because phenytoin is hydroxylated in the liver by an
enzyme system which is saturable at high serum levels, small incremental doses
may increase the half-life and produce very substantial increases in serum
levels, when these are in or above the upper therapeutic range. The steady-state
level may be disproportionately increased, with resultant intoxication, from an
increase in dosage of 10% or more.
Clinical studies show
that chewed and unchewed Dilantin Infatabs are bioequivalent, yield
approximately equivalent plasma levels, and are more rapidly absorbed than
Dilantin 100 mg capsules.
Indications
Dilantin Infatabs and Dilantin-30/Dilantin-125
suspensions are indicated for the control of generalized tonic-clonic (grand
mal) and complex partial (psychomotor, temporal lobe) seizures. Phenytoin serum
level determinations may be necessary for optimal dosage adjustments (see
Pharmacology and Dosage).
Contraindications
Patients who are hypersensitive to phenytoin or
other hydantoins.
Warnings
Abrupt withdrawal of Dilantin Infatabs or
Dilantin-30/Dilantin-125 suspensions in epileptic patients may precipitate
status epilepticus. When, in the judgment of the clinician, the need for dosage
reduction, discontinuation, or substitution of alternative anticonvulsant
medication arises, this should be done gradually. However, in the event of an
allergic or hypersensitivity reaction, rapid substitution of alternative
therapy may be necessary. In this case, alternative therapy should be an
anticonvulsant drug which does not belong to the hydantoin chemical class.
Cases of acute
hepatotoxicity, including infrequent cases of acute hepatic failure, have been
reported with phenytoin. These incidents have been associated with a
hypersensitivity syndrome characterized by fever, skin eruptions, and
lymphadenopathy, and usually occur within the first 2 months of treatment.
Other common manifestations include jaundice, hepatomegaly, elevated serum
transaminase levels, leukocytosis, and eosinophilia. The clinical course of
acute phenytoin hepatotoxicity ranges from prompt recovery to fatal outcomes.
In these patients with acute hepatotoxicity, phenytoin should be immediately
discontinued and not re-administered.
There have been a
number of reports suggesting a relationship between phenytoin and the
development of lymphadenopathy (local or generalized) including benign lymph
node hyperplasia, pseudolymphoma, lymphoma, and Hodgkin's Disease. Although a
cause and effect relationship has not been established, the occurrence of
lymphadenopathy indicates the need to differentiate such a condition from other
types of lymph node pathology. Lymph node involvement may occur with or without
symptoms and signs resembling serum sickness, e.g., fever, rash and liver
involvement. In all cases of lymphadenopathy, follow-up observation for an
extended period is indicated and every effort should be made to achieve seizure
control using alternative anticonvulsant drugs.
Acute alcoholic intake
may increase phenytoin serum levels while chronic alcoholic use may decrease
serum levels.
In view of isolated
reports associating phenytoin with exacerbation of porphyria, caution should be
exercised in using this medication in patients suffering from this disease.
Pregnancy
A number of reports suggests an association
between the use of anticonvulsant drugs by women with epilepsy and a higher
incidence of birth defects in children born to these women. Data are more
extensive with respect to phenytoin and phenobarbital, but these are also the
most commonly prescribed anticonvulsant drugs; fewer systematic or anecdotal
reports suggest a possible similar association with the use of all known
anticonvulsant drugs.
The reports suggesting
a higher incidence of birth defects in children of drug-treated epileptic women
cannot be regarded as adequate to prove a definite cause and effect
relationship. There are intrinsic methodologic problems in obtaining adequate
data on drug teratogenicity in humans. Genetic factors or the epileptic
condition itself may be more important than drug therapy in leading to birth
defects. The great majority of mothers on anticonvulsant medication deliver
normal infants. It is important to note that anticonvulsant drugs should not be
discontinued in patients in whom the drug is administered to prevent major
seizures because of the strong possibility of precipitating status epilepticus
with attendant hypoxia and threat to life. In individual cases where the
severity and frequency of the seizure disorder are such that the removal of
medication does not pose a serious threat to the patient, discontinuation of
the drug may be considered prior to and during pregnancy although it cannot be
said with any confidence that even minor seizures do not pose some hazard to
the developing embryo or fetus. The prescribing physician will wish to weigh
these considerations in treating or counseling epileptic women of childbearing
potential.
In addition to the
reports of the increased incidence of congenital malformations, such as cleft
lip/palate and heart malformations in children of women receiving phenytoin and
other anticonvulsant drugs, there have more recently been reports of a fetal
hydantoin syndrome. This consists of prenatal growth deficiency, microcephaly
and mental deficiency in children born to mothers who have received phenytoin,
barbiturates, alcohol, or trimethadione. However, these features are all
interrelated and are frequently associated with intrauterine growth retardation
from other causes.
There have been
isolated reports of malignancies, including neuroblastoma, in children whose
mothers received phenytoin during pregnancy.
An increase in seizure
frequency during pregnancy occurs in a high proportion of patients, because of
altered phenytoin absorption or metabolism. Periodic measurement of serum
phenytoin levels is particularly valuable in the management of a pregnant
epileptic patient as a guide to an appropriate adjustment of dosage. However,
postpartum restoration of the original dosage will probably be indicated.
Neonatal coagulation
defects have been reported within the first 24 hours in babies born to
epileptic mothers receiving phenobarbital and/or phenytoin. Vitamin K has been
shown to prevent or correct this defect and has been recommended to be given to
the mother before delivery and to the neonate after birth.
Precautions
General
The liver is the chief site of biotransformation
of Dilantin Infatabs and Dilantin-30/Dilantin-125 suspensions. Patients with
impaired liver function, elderly patients, or those who are gravely ill may
show early signs of toxicity.
A small percentage of
individuals who have been treated with phenytoin have been shown to metabolize
the drug slowly. Slow metabolism may be due to limited enzyme availability and
lack of induction; it appears to be genetically determined.
Toxic hepatitis, liver
damage, and hypersensitivity syndrome have been reported and may, in rare
cases, be fatal (see Adverse Effects).
Phenytoin should be
discontinued if a skin rash appears (see Warnings section regarding drug
discontinuation). If the rash is exfoliative, purpuric, or bullous or if lupus
erythematosus or Stevens-Johnson syndrome or toxic epidermal necrolysis is
suspected, use of this drug should not be resumed and alternative therapy
should be considered (see Adverse Effects). If the rash is of a milder type
(measles-like or scarlatiniform), therapy may be resumed after the rash has
completely disappeared. If the rash recurs upon reinstitution of therapy,
further phenytoin medication is contraindicated.
Literature reports
suggest that the combination of phenytoin, cranial irradiation and the gradual
reduction of corticosteroids may be associated with the development of erythema
multiforme, and/or Stevens-Johnson syndrome, and/or toxic epidermal necrolysis.
In any of the above
instances, caution should be exercised if using structurally similar compounds
(e.g., barbiturates, succinimides, oxazolidinediones and other related
compounds) in these same patients.
While macrocytosis and
megaloblastic anemia have occurred, these conditions usually respond to folic
acid therapy. If folic acid is added to phenytoin therapy, a decrease in
seizure control may occur.
Hyperglycemia,
resulting from the drug's inhibitory effects on insulin release, has been
reported. Phenytoin may also raise the serum glucose level in diabetic
patients.
Osteomalacia has been
associated with phenytoin therapy and is considered to be due to phenytoin's
interference with Vitamin D metabolism.
Phenytoin is not
indicated for seizures due to hypoglycemic or other metabolic causes.
Appropriate diagnostic procedures should be performed as indicated.
Phenytoin is not
effective for absence (petit mal) seizures. If tonic-clonic (grand mal) and
absence (petit mal) seizures are present, combined drug therapy is needed.
Serum levels of
phenytoin sustained above the optimal range may produce confusional states
referred to as delirium, psychosis, or encephalopathy, or rarely irreversible
cerebellar dysfunction. Accordingly, at the first sign of acute toxicity, serum
drug level determinations are recommended. Dose reduction of phenytoin therapy
is indicated if serum levels are excessive; if symptoms persist, termination of
phenytoin therapy is recommended (see Warnings).
Information to Be Provided to the Patient
Patients taking phenytoin should be advised of
the importance of adhering strictly to the prescribed dosage regimen, and of
informing their physician of any clinical condition in which it is not possible
to take the drug orally as prescribed, e.g., surgery, etc.
Patients should also be
cautioned on the use of other drugs or alcoholic beverages without first
seeking their physician's advice.
Patients should be
instructed to call their physician if skin rash develops.
The importance of good
dental hygiene should be stressed in order to minimize the development of
gingival hyperplasia and its complications.
Laboratory Tests
Phenytoin serum level determinations may be
necessary to achieve optimal dosage adjustments.
Drug Interactions
There are many drugs which may increase or
decrease serum phenytoin levels or which phenytoin may affect. Determinations
of serum phenytoin concentrations are especially helpful when possible drug
interactions are suspected. The most commonly occurring drug
interactions are listed below. See Table 1.
Drugs which may
increase phenytoin serum levels include: acute alcohol intake, cimetidine,
dicumarol, disulfiram, ethosuximide, methylphenidate, omeprazole, phenothiazines,
ticlopidine and topiramate. Coadministration with topiramate reduces serum
topiramate levels by 59%, and has the potential to increase phenytoin levels by
25% in some patients. The addition of topiramate therapy to phenytoin should be
guided by clinical outcome. The following drug classes are also included.
CPS:DilantinInfatabs125_t1Click here for Table 1
Table 1: Dilantin
Infatabs/Dilantin-30/Dilantin-125
Drugs Which May Increase Phenytoin Serum Levels
|
Drug Classes
|
Drugs in Each Class
|
|
Analgesic/Anti-inflammatory Agents
|
azapropazone
phenylbutazone
salicylates
|
|
Anesthetics
|
halothane
|
|
Antibacterial Agents
|
chloramphenicol
erythromycin
isoniazid
sulfonamides
|
|
Anticonvulsants
|
felbamate
succinimides
|
|
Antifungal Agents
|
amphotericin B
fluconazole
ketoconazole
miconazole
itraconazole
|
|
Benzodiazepines/Psychotropic Agents
|
chlordiazepoxide
diazepam
trazodone
|
|
Calcium Channel Blockers/Cardiovascular Agents
|
amiodarone
diltiazem
nifedipine
|
|
H2-antagonists
|
cimetidine
|
|
Hormones
|
estrogens
|
|
Oral Hypoglycemic Agents
|
tolbutamide
|
|
Serotonin Reuptake Inhibitors
|
fluoxetine
paroxetine
|
Drugs that may decrease
phenytoin serum levels include: antibacterial agents/fluoroquinolones (such as
ciprofloxacin and rifampin), carbamazepine, chronic alcohol abuse, diazoxide,
reserpine, sucralfate, theophylline and vigabatrin.
Coadministration with
vigabatrin reduces serum phenytoin levels by 20 to 30%. This may be
clinically significant in some patients and may require dosage adjustment.
Molindone HCl contains calcium ions which interfere with the absorption of
phenytoin. Ingestion times of phenytoin and calcium preparations, including
antacid preparations containing calcium should be staggered to prevent
absorption problems.
Drugs which may either
increase or decrease phenytoin serum levels are included in Table 2.
CPS:DilantinInfatabs125_t2Click here for Table 2
Table 2: Dilantin
Infatabs/Dilantin-30/Dilantin-125
Drugs Which May Either Increase or Decrease
Phenytoin Serum Levels
|
Drug Classes
|
Drugs in Each Class
|
|
Anticonvulsants
|
carbamazepine
phenobarbital
sodium valproate
valproic acid
|
|
Antineoplastic Agents
|
|
|
Benzodiazepines
|
chlordiazepoxide
|
|
Phenothiazines
|
|
|
Psychotropic Agents
|
diazepam
|
Similarly, the effect
of phenytoin on carbamazepine, phenobarbital, valproic acid and sodium
valproate serum levels is unpredictable.
Although not a true
drug interaction, tricyclic antidepressants may precipitate seizures in
susceptible patients and phenytoin dosage may need to be adjusted.
Drugs whose blood
levels and/or effects may be altered by phenytoin include: clozapine,
corticosteroids, coumarin anti-coagulants, cyclosporine, diazoxide, furosemide,
lamotrigine, paroxetine, theophylline, topiramate and vitamin D.
Coadministration with topiramate reduces serum topiramate levels by 59%, and
has the potential to increase phenytoin levels by 25% in some patients. The
addition of topiramate therapy to phenytoin should be guided by clinical
outcome. Coadministration with lamotrigine doubles the plasma clearance and
reduces the elimination half-life of lamotrigine by 50%. This clinically
important interaction requires dosage adjustment. The following drug classes
are also included. See Table 3.
CPS:DilantinInfatabs125_t3Click here for Table 3
Table 3: Dilantin
Infatabs/Dilantin-30/Dilantin-125
Drugs Whose Blood Levels and/or Effects May Be
Altered by Phenytoin
|
Drug Classes
|
Drugs in Each Class
|
|
Antibacterial Agents
|
doxycycline
praziquantel
rifampin
tetracycline
|
|
Antifungal Agents
|
|
|
Antineoplastic Agents
|
|
|
Calcium Channel Blockers/Cardiovascular Agents
|
digitoxin
nicardipine
nimodipine
quinidine
verapamil
|
|
Hormones
|
estrogens
oral contraceptives
|
|
Neuromuscular Blocking Agents
|
alcuronium
pancuronium
vecuronium
|
|
Opioid Analgesics
|
methadone
|
|
Oral Hypoglycemic Agents
|
chlorpropamide
glyburide
tolbutamide
|
Drug-Enteral Feeding/Nutritional Preparations
Interaction: Literature reports suggest that patients who have received enteral
feeding preparations and/or related nutritional supplements have lower than
expected phenytoin plasma levels. It is therefore suggested that phenytoin not
be administered concomitantly with an enteral feeding preparation.
More frequent serum
phenytoin level monitoring may be necessary in these patients.
Drug/Laboratory Test Interactions: Phenytoin may
cause decreased serum levels of protein-bound iodine (PBI). It may also produce
lower than normal values for dexamethasone or metyrapone tests. Phenytoin may
cause increased serum levels of glucose, alkaline phosphatase, and gamma glutamyl
transpeptidase (GGT). Phenytoin may affect blood calcium and blood sugar
metabolism tests.
Carcinogenesis: See Warnings.
Pregnancy
See Warnings.
Lactation
Infant breast-feeding is not recommended for
women taking this drug because phenytoin appears to be secreted in low
concentrations in human milk.
Children
See Dosage.
Adverse Effects
CNS
The most common manifestations encountered with
Dilantin Infatabs and Dilantin-30/Dilantin 125 suspensions therapy are
referable to this system and are usually dose-related. These include nystagmus,
ataxia, slurred speech, decreased coordination and mental confusion. Dizziness,
insomnia, transient nervousness, motor twitchings, and headaches have also been
observed. There have also been rare reports of phenytoin induced dyskinesias,
including chorea, dystonia, tremor and asterixis, similar to those induced by
phenothiazine and other neuroleptic drugs.
A predominantly sensory
peripheral polyneuropathy has been observed in patients receiving long-term
phenytoin therapy.
Gastrointestinal
nausea, vomiting, constipation, toxic hepatitis,
and liver damage (see Precautions).
Integumentary System
Dermatological manifestations sometimes
accompanied by fever have included scarlatiniform or morbilliform rashes. A
morbilliform rash (measles-like) is the most common; other types of dermatitis
are seen more rarely. Other more serious forms which may be fatal have included
bullous, exfoliative or purpuric dermatitis, lupus erythematosus,
Stevens-Johnson syndrome and toxic epidermal necrolysis (see Precautions).
Hemopoietic
Hemopoietic complications, some fatal, have
occasionally been reported in association with administration of phenytoin.
These have included thrombocytopenia, leukopenia, granulocytopenia,
agranulocytosis, and pancytopenia with or without bone marrow suppression.
While macrocytosis and megaloblastic anemia have occurred, these conditions
usually respond to folic acid therapy. Lymphadenopathy including benign lymph
node hyperplasia, pseudolymphoma, lymphoma, and Hodgkin's Disease have been
reported (see Warnings).
Connective Tissue
Coarsening of the facial features, enlargement
of the lips, gingival hyperplasia, hypertrichosis and Peyronie's Disease.
Immunologic
Hypersensitivity syndrome (which may include, but
is not limited to symptoms such as arthralgias, eosinophilia, fever, liver
dysfunction, lymphadenopathy or rash), systemic lupus erythematosus,
periarteritis nodosa, and immunoglobulin abnormalities. Several individual case
reports have suggested that there may be an increased, although still rare,
incidence of hypersensitivity reactions, including skin rash and
hepatotoxicity, in black patients.
Overdose
For management of a
suspected drug overdose, CPhA recommends that you contact your regional
Poison Control Centre. See the CPS Directory section for a list of
Poison Control Centres.
Symptoms
The lethal dose of Dilantin Infatabs and
Dilantin-30/Dilantin-125 suspensions in pediatric patients is not known. The
lethal dose of phenytoin in adults is estimated to be 2 to 5 g. The
initial symptoms are nystagmus, ataxia, and dysarthria. Other signs are tremor,
hyperreflexia, somnolence, drowsiness, lethargy, slurred speech, blurred
vision, nausea, vomiting. The patient may become comatose and hypotensive. Death
is due to respiratory and circulatory depression.
There are marked
variations among individuals with respect to phenytoin plasma levels where
toxicity may occur. Nystagmus on lateral gaze, usually appears at
80 µmol/L (20 µg/mL), ataxia at 119 µmol/L (30 µg/mL).
Dysarthria and lethargy appear when the serum concentration is
>159 µmol/L (40 µg/mL), but a concentration as high as
198 µmol/L (50 µg/mL) has been reported without evidence of toxicity.
As much as 25 times the therapeutic dose has been taken to result in a
serum concentration over >396 µmol/L (100 µg/mL) with complete
recovery.
Treatment
Treatment is nonspecific since there is no known
antidote.
The adequacy of the
respiratory and circulatory systems should be carefully observed and appropriate
supportive measures employed. Hemodialysis can be considered since phenytoin is
not completely bound to plasma proteins. Total exchange transfusion has been
used in the treatment of severe intoxication in pediatric patients.
In acute overdosage the
possibility of the presence of other CNS depressants, including alcohol, should
be borne in mind.
Dosage
Dilantin suspensions are not for parenteral use. Serum phenytoin
concentrations should be monitored and care should be taken when switching a
patient from the sodium salt to the free acid form.
Dilantin extended
release capsules are formulated with the sodium salt of phenytoin. The free
acid form of phenytoin is used in Dilantin-30 and Dilantin-125 suspensions and
Dilantin Infatabs. Because there is approximately an 8% increase in drug
content with the free acid form over that of the sodium salt, dosage
adjustments and serum level monitoring may be necessary when switching from a
product formulated with the free acid to a product formulated with the sodium
salt and vice versa.
General
Dilantin Infatabs and Dilantin-30/Dilantin-125
suspensions are not for once-a-day dosing.
Dosage should be
individualized to provide maximum benefit. In some cases, serum blood level
determinations may be necessary for optimal dosage adjustments. The clinically
effective serum level is usually 40 to 80 µmol/L (10 to
20 µg/mL). Serum blood level determinations are especially helpful when
possible drug interactions are suspected. With recommended dosage, a period of
7 to 10 days may be required to achieve therapeutic blood levels with
phenytoin and changes in dosage (increase or decrease) should not be carried
out at intervals shorter than 7 to 10 days.
Adults
Patients who have received no previous treatment
may be started on 2 Dilantin Infatabs 3 times daily or on 5 mL
of Dilantin-125 Suspension 3 times daily, and the dose then adjusted to
suit individual requirements. For some adults, the satisfactory maintenance
dosage will be 8 Dilantin Infatabs daily; an increase to 12 Dilantin
Infatabs be made, if necessary. With Dilantin-125, an increase to 25 mL
daily may be made if necessary.
Children
Initially, 5 mg/kg/day of Dilantin
Infatabs, Dilantin-30 or Dilantin-125 suspension may be given in 2 or
3 equally divided doses, with subsequent dosage individualized to a
maximum of 300 mg daily. A recommended daily maintenance dosage is usually
4 to 8 mg/kg. Children over 6 years may require the minimum adult
dose (300 mg/day). If the daily dosage cannot be divided equally, the
larger dose should be given at bedtime.
Supplied
Dilantin Infatabs
Each flavored, triangular shaped, grooved tablet
contains: phenytoin (free acid form) 50 mg. Nonmedicinal ingredients:
alcohol, magnesium stearate, spearmint oil, sugar and talc. Bottles of 100.
Store at controlled room temperature 15 to 30°C. Protect from light and
moisture.
Dilantin-30 Suspension
Each 5 mL of flavored, colored suspension
contains: phenytoin (free acid form) 30 mg. Nonmedicinal ingredients:
alcohol, banana oil, citric acid, glycerin, magnesium aluminum silicate, orange
oil, polysorbate 40, Red #2 FD&C, sodium benzoate, sodium
carboxymethylcellulose, sugar, vanillin and yellow #6 FD&C. Bottles of
250 mL.
Dilantin-125 Suspension
Each 5 mL of flavored, colored suspension
contains: phenytoin (free acid form) 125 mg. Nonmedicinal ingredients:
alcohol, banana oil, citric acid, glycerin, magnesium aluminum silicate, orange
oil, polysorbate 40, sodium benzoate, sodium carboxymethyl- cellulose,
sugar, vanillin and yellow #6 FD&C. Bottles of 250 mL.
Suspension should be
stored at controlled room temperature 15 to 30°C and protected from freezing
and light.
