A1,
A2,
B,
C1,
C2,
D,
E,
F,
G-H,
I-K,
L,
M,
N,
O,
P1,
P2,
Q-R,
S,
T,
U-V,
W-Z
Norvir Side Effects, and Drug Interactions - Ritonavir
Norvir Side Effects, and Drug Interactions - Ritonavir
SIDE EFFECTS
The safety of NORVIR alone and in combination with nucleoside analogues was
studied in 1270 patients. Table 5 lists treatment-emergent adverse events (at
least possibly related and of at least moderate intensity) that occurred in
2% or greater of patients receiving NORVIR alone or in combination with nucleosides
in Study 245 or Study 247 and in combination with saquinavir in ongoing Study
462. In that study, 141 protease inhibitor-naive, HIV-infected patients with
mean baseline CD 4 of 300 cells/µL were randomized to one of four
regimens of NORVIR + saquinavir, including NORVIR 400 mg b.i.d. + saquinavir
400 mg b.i.d. Overall the most frequently reported clinical adverse events,
other than asthenia, among patients receiving NORVIR were gastrointestinal and
neurological disturbances including nausea, diarrhea, vomiting, anorexia, abdominal
pain, taste perversion, and circumoral and peripheral paresthesias. Similar
adverse event profiles were reported in patients receiving ritonavir in other
trials.
Table 5
Percentage of Patients with Treatment-Emergent Adverse Events 1
of Moderate or
Severe Intensity Occurring in ≥2% of Patients Receiving NORVIR
|
|
Study 245
Naive Patients 2 |
Study 247
Advanced Patients 3 |
Study 462
PI-Naive
Patients 4 |
|
Adverse
Events
|
NORVIR
+ ZDV
n=116 |
NORVIR
n=117 |
ZDV
n=119 |
NORVIR
n=541 |
Placebo
n=545 |
NORVIR +
Saquinavir
n=141 |
|
Body as a Whole
|
|
Abdominal Pain
|
5.2 |
6.0 |
5.9 |
8.3 |
5.1 |
2.1 |
|
Asthenia
|
28.4 |
10.3 |
11.8 |
15.3 |
6.4 |
16.3 |
|
Fever
|
1.7 |
0.9 |
1.7 |
5.0 |
2.4 |
0.7 |
|
Headache
|
7.8 |
6.0 |
6.7 |
6.5 |
5.7 |
4.3 |
|
Malaise
|
5.2 |
1.7 |
3.4 |
0.7 |
0.2 |
2.8 |
|
Pain (unspecified)
|
0.9 |
1.7 |
0.8 |
2.2 |
1.8 |
4.3 |
|
Cardiovascular
|
|
Syncope
|
0.9 |
1.7 |
0.8 |
0.6 |
0.0 |
2.1 |
|
Vasodilation
|
3.4 |
1.7 |
0.8 |
1.7 |
0.0 |
3.5 |
|
Digestive
|
|
Anorexia
|
8.6 |
1.7 |
4.2 |
7.8 |
4.2 |
4.3 |
|
Constipation
|
3.4 |
0.0 |
0.8 |
0.2 |
0.4 |
1.4 |
|
Diarrhea
|
25.0 |
15.4 |
2.5 |
23.3 |
7.9 |
22.7 |
|
Dyspepsia
|
2.6 |
0.0 |
1.7 |
5.9 |
1.5 |
0.7 |
|
Fecal
|
|
Incontinence
|
0.0 |
0.0 |
0.0 |
0.0 |
0.0 |
2.8 |
|
Flatulence
|
2.6 |
0.9 |
1.7 |
1.7 |
0.7 |
3.5 |
|
Local Throat Irritation
|
0.9 |
1.7 |
0.8 |
2.8 |
0.4 |
1.4 |
|
Nausea
|
46.6 |
25.6 |
26.1 |
29.8 |
8.4 |
18.4 |
|
Vomiting
|
23.3 |
13.7 |
12.6 |
17.4 |
4.4 |
7.1 |
|
Metabolic and Nutritional
|
|
Weight Loss
|
0.0 |
0.0 |
0.0 |
2.4 |
1.7 |
0.0 |
|
Musculoskeletal
|
|
Arthralgia
|
0.0 |
0.0 |
0.0 |
1.7 |
0.7 |
2.1 |
|
Myalgia
|
1.7 |
1.7 |
0.8 |
2.4 |
1.1 |
2.1 |
|
Nervous
|
|
Anxiety
|
0.9 |
0.0 |
0.8 |
1.7 |
0.9 |
2.1 |
|
Circumoral Paresthesia
|
5.2 |
3.4 |
0.0 |
6.7 |
0.4 |
6.4 |
|
Confusion
|
0.0 |
0.9 |
0.0 |
0.6 |
0.6 |
2.1 |
|
Depression
|
1.7 |
1.7 |
2.5 |
1.7 |
0.7 |
7.1 |
|
Dizziness
|
5.2 |
2.6 |
3.4 |
3.9 |
1.1 |
8.5 |
|
Insomnia
|
3.4 |
2.6 |
0.8 |
2.0 |
1.8 |
2.8 |
|
Paresthesia
|
5.2 |
2.6 |
0.0 |
3.0 |
0.4 |
2.1 |
|
Peripheral Paresthesia
|
0.0 |
6.0 |
0.8 |
5.0 |
1.1 |
5.7 |
|
Somnolence
|
2.6 |
2.6 |
0.0 |
2.4 |
0.2 |
0.0 |
|
Thinking Abnormal
|
2.6 |
0.0 |
0.8 |
0.9 |
0.4 |
0.7 |
|
Respiratory
|
|
Pharyngitis
|
0.9 |
2.6 |
0.0 |
0.4 |
0.4 |
1.4 |
|
Skin and Appendages
|
|
Rash
|
0.9 |
0.0 |
0.8 |
3.5 |
1.5 |
0.7 |
|
Sweating
|
3.4 |
2.6 |
1.7 |
1.7 |
1.1 |
2.8 |
|
Special Senses
|
|
Taste Perversion
|
17.2 |
11.1 |
8.4 |
7.0 |
2.2 |
5.0 |
|
Urogenital
|
|
Nocturia
|
0.0 |
0.0 |
0.0 |
0.2 |
0.0 |
2.8 |
|
1 Includes those adverse events at least
possibly related to study drug or of unknown relationship and
excludes concurrent HIV conditions.
|
|
2 The median duration of treatment for
patients randomized to regimens containing NORVIR in Study 245
was 9.1 months.
|
|
3 The median duration of treatment for
patients randomized to regimens containing NORVIR in Study 247
was 9.4 months.
|
|
4 The median duration of treatment for
patients in ongoing Study 462 was 48 weeks.
|
Adverse events occurring in less than 2% of patients receiving NORVIR in all
phase II/phase III studies and considered at least possibly related or of unknown
relationship to treatment and of at least moderate intensity are listed below
by body system.
Body as a Whole: Abdomen enlarged, accidental injury, allergic
reaction, back pain, cachexia, chest pain, chills, facial edema, facial pain,
flu syndrome, hormone level altered, hypothermia, kidney pain, neck pain, neck
rigidity, pelvic pain, photosensitivity reaction, and substernal chest pain.
Cardiovascular System: Cardiovascular disorder, cerebral
ischemia, cerebral venous thrombosis, hypertension, hypotension, migraine, myocardial
infarct, palpitation, peripheral vascular disorder, phlebitis, postural hypotension,
tachycardia and vasospasm.
Digestive System: Abnormal stools, bloody diarrhea, cheilitis,
cholestatic jaundice, colitis, dry mouth, dysphagia, eructation, esophageal
ulcer, esophagitis, gastritis, gastroenteritis, gastrointestinal disorder, gastrointestinal
hemorrhage, gingivitis, hepatic coma, hepatitis, hepatomegaly, hepatosplenomegaly,
ileus, liver damage, melena, mouth ulcer, pancreatitis, pseudomembranous colitis,
rectal disorder, rectal hemorrhage, sialadenitis, stomatitis, tenesmus, thirst,
tongue edema, and ulcerative colitis.
Endocrine System: Adrenal cortex insufficiency and diabetes
mellitus.
Hemic and Lymphatic System: Acute myeloblastic leukemia,
anemia, ecchymosis, leukopenia, lymphadenopathy, lymphocytosis, myeloproliferative
disorder, and thrombocytopenia.
Metabolic and Nutritional Disorders: Albuminuria, alcohol
intolerance, avitaminosis, BUN increased, dehydration, edema, enzymatic abnormality,
glycosuria, gout, hypercholesteremia, peripheral edema, and xanthomatosis.
Musculoskeletal System: Arthritis, arthrosis, bone disorder,
bone pain, extraocular palsy, joint disorder, leg cramps, muscle cramps, muscle
weakness, myositis, and twitching.
Nervous System: Abnormal dreams, abnormal gait, agitation,
amnesia, aphasia, ataxia, coma, convulsion, dementia, depersonalization, diplopia,
emotional lability, euphoria, grand mal convulsion, hallucinations, hyperesthesia,
hyperkinesia, hypesthesia, incoordination, libido decreased, manic reaction,
nervousness, neuralgia, neuropathy, paralysis, peripheral neuropathic pain,
peripheral neuropathy, peripheral sensory neuropathy, personality disorder,
sleep disorder, speech disorder, stupor, subdural hematoma, tremor, urinary
retention, vertigo, and vestibular disorder.
Respiratory System: Asthma, bronchitis, dyspnea, epistaxis,
hiccup, hypoventilation, increased cough, interstitial pneumonia, larynx edema,
lung disorder, rhinitis, and sinusitis.
Skin and Appendages: Acne, contact dermatitis, dry skin,
eczema, erythema multiforme, exfoliative dermatitis, folliculitis, fungal dermatitis,
furunculosis, maculopapular rash, molluscum contagiosum, onychomycosis, pruritus,
psoriasis, pustular rash, seborrhea, skin discoloration, skin disorder, skin
hypertrophy, skin melanoma, urticaria, and vesiculobullous rash.
Special Senses: Abnormal electro-oculogram, abnormal electroretinogram,
abnormal vision, amblyopia/blurred vision, blepharitis, conjunctivitis, ear
pain, eye disorder, eye pain, hearing impairment, increased cerumen, iritis,
parosmia, photophobia, taste loss, tinnitus, uveitis, visual field defect, and
vitreous disorder.
Urogenital System: Acute kidney failure, breast pain, cystitis,
dysuria, hematuria, impotence, kidney calculus, kidney failure, kidney function
abnormal, kidney pain, menorrhagia, penis disorder, polyuria, urethritis, urinary
frequency, urinary tract infection, and vaginitis.
Post-Marketing Experience:
There have been postmarketing reports of seizure. Cause and effect relationship
has not been established.
Dehydration, usually associated with gastrointestinal symptoms, and sometimes
resulting in hypotension, syncope, or renal insufficiency has been reported.
Syncope, orthostatic hypotension, and renal insufficiency have also been reported
without known dehydration.
Redistribution/accumulation of body fat has been reported (see PRECAUTIONS
, Fat Redistribution ). There have been reports of increased bleeding
in patients with hemophilia A or B (see PRECAUTIONS , Hemophilia ).
Laboratory Abnormalities
Table 6 shows the percentage of patients who developed marked laboratory abnormalities.
Table 6
Percentage of Patients, by Study and Treatment Group, with Chemistry
and
Hematology Abnormalities Occurring in > 3% of Patients Receiving
NORVIR
| |
|
Study 245
Naive Patients |
Study 247
Advanced Patients |
Study 462
PI-Naive
Patients |
|
Variable
|
Limit
|
NORVIR
+ ZDV |
NORVIR |
ZDV |
NORVIR |
Placebo |
NORVIR +
Saquinavir |
|
Chemistry
|
High
|
|
|
|
Cholesterol
|
>240 mg/dL
|
30.7 |
44.8 |
9.3 |
36.5 |
8.0 |
65.2 |
|
CPK
|
>1000 IU/L
|
9.6 |
12.1 |
11.0 |
9.1 |
6.3 |
9.9 |
|
GGT
|
>300 IU/L
|
1.8 |
5.2 |
1.7 |
19.6 |
11.3 |
9.2 |
|
SGOT (AST)
|
>180 IU/L
|
5.3 |
9.5 |
2.5 |
6.4 |
7.0 |
7.8 |
|
SGPT (ALT)
|
>215 IU/L
|
5.3 |
7.8 |
3.4 |
8.5 |
4.4 |
9.2 |
|
Triglycerides
|
>800 mg/dL
|
9.6 |
17.2 |
3.4 |
33.6 |
9.4 |
23.4 |
|
Triglycerides
|
>1500 mg/dL
|
1.8 |
2.6 |
- |
12.6 |
0.4 |
11.3 |
|
Triglycerides
Fasting
|
>1500 mg/dL
|
1.5 |
1.3 |
- |
9.9 |
0.3 |
- |
|
Uric Acid
|
>12 mg/dL
|
- |
- |
- |
3.8 |
0.2 |
1.4 |
|
Hematology
|
Low
|
|
|
|
Hematocrit
|
<30%
|
2.6 |
- |
0.8 |
17.3 |
22.0 |
0.7 |
|
Hemoglobin
|
<8.0 g/dL
|
0.9 |
- |
- |
3.8 |
3.9 |
- |
|
Neutrophils
|
≤0.5 × 10 9 /L
|
- |
- |
- |
6.0 |
8.3 |
- |
|
RBC
|
<3.0 × 10 12 /L
|
1.8 |
- |
5.9 |
18.6 |
24.4 |
- |
|
WBC
|
<2.5 × 10 9 /L
|
- |
0.9 |
6.8 |
36.9 |
59.4 |
3.5 |
|
1 ULN = upper limit of the normal range.
|
|
- Indicates no events reported.
|
DRUG INTERACTIONS
Ritonavir has been found to be an inhibitor of cytochrome P450 3A (CYP3A) both
in vitro and in vivo (Table 2). Agents that are extensively metabolized
by CYP3A and have high first pass metabolism appear to be the most susceptible
to large increases in AUC (>3-fold) when co-administered with ritonavir.
Ritonavir also inhibits CYP2D6 to a lesser extent. Co-administration of substrates
of CYP2D6 with ritonavir could result in increases (up to 2-fold) in the AUC
of the other agent, possibly requiring a proportional dosage reduction. Ritonavir
also appears to induce CYP3A as well as other enzymes, including glucuronosyl
transferase, CYP1A2, and possibly CYP2C9.
Drugs that are contraindicated specifically due to the expected magnitude of
interaction and potential for serious adverse events are listed both in CONTRAINDICATIONS
Table 3 and under Contraindicated Drugs in Table 4.
Those drug interactions that have been established based on drug interaction
studies are listed with the pharmacokinetic results in CLINICAL PHARMACOLOGY
, Table 2. The clinical recommendations based on the results of these studies
are listed in Table 4 Established Drug Interactions: Alteration in Dose or
Regimen Recommended Based on Drug Interaction Studies.
A systematic review of over 200 medications prescribed to HIV-infected patients
was performed to identify potential drug interactions with ritonavir. 2
There are a number of agents in which CYP3A or CYP2D6 partially contribute
to the metabolism of the agent. In these cases, the magnitude of the interaction
and therapeutic consequences cannot be predicted with any certainty.
When co-administering ritonavir with calcium channel blockers, immunosuppressants,
some HMG-CoA reductase inhibitors (see WARNINGS, Drug Interactions
), some steroids, or other substrates of CYP3A, or most antidepressants,
certain antiarrhythmics, and some narcotic analgesics which are partially mediated
by CYP2D6 metabolism, it is possible that substantial increases in concentrations
of these other agents may occur, possibly requiring a dosage reduction (>50%);
examples are listed in Table 4 Predicted Drug Interactions: Use With Caution,
Dose Decrease May be Needed.
When co-administering ritonavir with any agent having a narrow therapeutic
margin, such as anticoagulants, anticonvulsants, and antiarrhythmics, special
attention is warranted. With some agents, the metabolism may be induced, resulting
in decreased concentrations (see Table 4 Predicted Drug Interactions: Use
With Caution, Dose Increase May be Needed).
Table 4
Drug Interactions With NORVIR
CONTRAINDICATED DRUGS
(Same as Table 3)
|
DRUGS THAT ARE CONTRAINDICATED WITH
NORVIR USE
|
|
Drug Class
|
Drugs Within Class That Are
CONTRAINDICATED With NORVIR
|
|
Antiarrhythmics
|
amiodarone, bepridil, flecainide, propafenone, quinidine
|
|
Antihistamines
|
astemizole, terfenadine
|
|
Antimigraine
|
dihydroergotamine, ergotamine
|
|
Sedative/hypnotics
|
midazolam, triazolam
|
|
GI motility agent
|
cisapride
|
|
Neuroleptic
|
pimozide
|
Established
Drug Interactions: Alteration in Dose or
Regimen Recommended Based
on Drug Interaction Studies
(see CLINICAL PHARMACOLOGY
, Table 2 for Magnitude or Interaction)
|
Drug Name
|
Effect
|
Clinical Comment
|
|
Clarithromycin
|
up clarithromycin
concentration
|
For patients with renal impairment the following
dosage adjustments should be considered:
· For patients with CL CR 30 to 60 mL/min the dose
of clarithromycin should be reduced by 50%.
· For patients with CL CR < 30 mL/min the dose of
clarithromycin should be decreased by 75%.
No dose adjustment for patients with normal renal function is
necessary.
|
|
Desipramine
|
up desipramine concentration
|
Dosage reduction and concentration monitoring of
desipramine is recommended
|
|
Didanosine
|
|
Dosing of didanosine and ritonavir should be separated
by 2.5 hours to avoid formulation incompatibility
|
|
Disulfiram/Metronidazole
|
|
Ritonavir formulations contain alcohol, which can
produce disulfiram-like reactions when co-administered with disulfiram
or other drugs that produce this reaction (e.g., metronidazole)
|
|
Indinavir
|
up indinavir concentration
|
Appropriate doses for this combination, with respect
to efficacy and safety, have not been established
|
|
Ketoconazole
|
up ketoconazole concentration
|
High doses of ketoconazole (>200 mg/day) are
not recommended
|
|
Meperidine
|
down meperidine concentration/
up normeperidine
concentration (metabolite)
|
Dosage increase and long-term use of meperidine
with ritonavir are not recommended due to the increased concentrations
of the metabolite normeperidine which has both analgesic activity
and CNS stimulant activity (e.g., seizures)
|
|
Methadone
|
down methadone concentration
|
Dosage increase of methadone may be considered
|
|
Oral Contraceptives
|
down ethinyl estradiol
concentration
|
Dosage increase or alternate contraceptive measures
should be considered
|
|
Rifabutin
|
up rifabutin and rifabutin
metabolite concentration
|
Dosage reduction of rifabutin by at least three-quarters
of the usual dose of 300 mg/day is recommended (e.g., 150 mg every
other day or three times a week). Further dosage reduction may
be necessary
|
|
Rifampin
|
down ritonavir concentration
|
Alternate antimycobacterial agents such as rifabutin
should be considered (see Rifabutin, for dose reduction recommendations)
|
|
Saquinavir
|
up saquinavir concentration
|
When used in combination therapy for up to 24 weeks,
doses of 400 mg b.i.d. of ritonavir and saquinavir were better
tolerated than the higher doses of the combination. Saquinavir
plasma concentrations achieved with Invirase® (saquinavir mesylate)
(400 mg b.i.d.) and ritonavir (400 mg b.i.d.) are similar to those
achieved with Fortovase™ (saquinavir) (400 mg b.i.d.) and ritonavir
(400 mg b.i.d.)
|
|
Sildenafil
|
up sildenafil concentration
|
Sildenafil should not exceed a maximum single dose
of
25 mg in a 48-hour period in patients receiving concomitant ritonavir
therapy (see WARNINGS)
|
|
Theophylline
|
down theophylline concentration
|
Increased dosage of theophylline may be required;
therapeutic monitoring should be considered
|
|
Predicted Drug Interactions: Use With Caution,
Dose
Decrease of Coadministered Drug May Be Needed
(see WARNINGS)
|
Examples of Drugs in Which Plasma Concentrations
May Be Increased
By Co-Administration With NORVIR |
|
Drug Class
|
Examples of Drugs
|
|
Analgesics, narcotic
|
tramadol, propoxyphene
|
|
Antiarrhythmics
|
disopyramide, lidocaine, mexilitine
|
|
Anticonvulsants
|
carbamazepine, clonazepam, ethosuximide
|
|
Antidepressants
|
bupropion, nefazodone, selective serotonin reuptake
inhibitors (SSRIs), tricyclics
|
|
Antiemetics
|
dronabinol
|
|
Antiparasitics
|
quinine
|
|
(beta)-blockers
|
metoprolol, timolol
|
|
Calcium channel blockers
|
diltiazem, nifedipine, verapamil
|
|
Hypolipidemics, HMG CoA reductase inhibitors 1
|
atorvastatin, cerivastatin, lovastatin, simvastatin
|
|
Immunosuppressants
|
cyclosporine, tacrolimus
|
|
Neuroleptics
|
perphenazine, risperidone, thioridazine
|
|
Sedative/hypnotics
|
clorazepate, diazepam, estazolam, flurazepam, zolpidem
|
|
Steroids
|
dexamethasone, prednisone
|
|
Stimulants
|
methamphetamine
|
|
1 Coadministration with lovastatin and
simvastatin is not recommended (see WARNINGS
, Drug Interactions ).
|
|
Predicted Drug Interactions: Use With Caution,
Dose Increase of Coadministered Drug May Be Needed (see WARNINGS
)
|
|
Examples of Drugs in Which Plasma Concentrations
May Be Decreased By Co-Administration
With NORVIR
|
|
Anticoagulants
|
warfarin
|
|
Anticonvulsants
|
phenytoin, divalproex, lamotrigine
|
|
Antiparasitics
|
atovaquone
|
Post-Marketing Experience with Drugs Listed in Table 4
Cardiac and neurologic events have been reported when ritonavir has been co-administered
with disopyramide, mexiletine, nefazodone, fluoxetine, and beta blockers. The
possibility of drug interaction cannot be excluded.
top
