PRODUCT MONOGRAPH VIGAMOX®
Moxifloxacin Hydrochloride Ophthalmic Solution, 0.5% w/v as moxifloxacin
PRODUCT MONOGRAPH VIGAMOX®
Moxifloxacin Hydrochloride Ophthalmic Solution, 0.5% w/v as moxifloxacin
ACTIONS AND CLINICAL PHARMACOLOGY
Moxifloxacin is a synthetic fluoroquinolone antibacterial agent active in vitro against a broad
spectrum of Gram-positive and Gram-negative ocular pathogens, atypical microorganisms and
The antibacterial action of moxifloxacin results from inhibition of topoisomerase II (DNA gyrase)
and topoisomerase IV. DNA gyrase is an essential enzyme that is involved in the replication,
transcription and repair of bacterial DNA. Topoisomerase IV is an enzyme known to play a key
role in the partitioning of the chromosomal DNA during bacterial cell division (see
Pharmacokinetics/Pharmacodynamics: Following topical ocular administration of VIGAMOX®
(moxifloxacin hydrochloride) ophthalmic solution, moxifloxacin was absorbed into the systemic
circulation. Plasma concentrations of moxifloxacin were measured in 21 male and female adult
subjects who received bilateral topical ocular doses of VIGAMOX® solution every 8 hours for a
total of 13 doses. The mean steady-state Cmax and AUC were 2.7 ng/mL and 41.9 nghr/mL,
respectively. These systemic exposure values were at least 1,600 and 1,000 times lower than the
mean Cmax and AUC reported after therapeutic 400 mg oral doses of moxifloxacin. The plasma
half-life of moxifloxacin was estimated to be 13 hours. Moxifloxacin is widely distributed in the
body and is excreted in feces or urine either unchanged or as glucuronide or sulfate conjugates.
Tear film concentrations were studied in 31 healthy male and female adult volunteers who were
administered 1 drop of VIGAMOX® solution to both eyes every 8 hours for a total of 10 doses.
Mean tear concentrations at 5 minutes following the first and last topical dose were 46.0 and
55.2g/mL, respectively. Thereafter, they decline rapidly in a biphasic manner with the means
ranging approximately 1 to 4 g/mL over the 1 to 8 hour sampling period. Pre-dose morning tear
concentrations on Days 2 to 4 averaged over 4 g/mL. Studies conducted in animals indicate
penetration into the conjunctiva and ocular tissues with prolonged binding to melanin.
INDICATIONS AND USAGE
VIGAMOX® (moxifloxacin hydrochloride) ophthalmic solution is indicated for the treatment of
patients 1 year of age and older with bacterial conjunctivitis caused by susceptible strains of the
Aerobic, Gram-Positive Staphylococcus aureus Staphylococcus epidermidis Staphylococcus haemolyticus Staphylococcus hominis Streptococcus pneumoniae Streptococcus viridans group Aerobic, Gram-Negative Acinetobacter species Haemophilus influenzae CONTRAINDICATIONS
VIGAMOX® (moxifloxacin hydrochloride) ophthalmic solution is contraindicated in patients with a
history of hypersensitivity to moxifloxacin, to other quinolones, or to any of the components in this
medication (see PHARMACEUTICAL INFORMATION).
WARNINGS
VIGAMOX® (moxifloxacin hydrochloride) ophthalmic solution is not for injection into the eye.
VIGAMOX® solution should not be injected subconjunctivally, nor should it be introduced directly
In patients receiving systemically administered quinolones, serious and occasionally fatal
hypersensitivity (anaphylactic) reactions have been reported, some following the first dose. Some
reactions were accompanied by cardiovascular collapse, loss of consciousness, angioedema
(including laryngeal, pharyngeal or facial edema), airway obstruction, dyspnea, urticaria, and
itching. If an allergic reaction to moxifloxacin occurs, discontinue use of the drug. Serious acute
hypersensitivity reactions may require immediate emergency treatment. Oxygen and airway
management should be administered as clinically indicated.
Serious and sometimes fatal events, some due to hypersensitivity and some due to uncertain
etiology, have been reported in patients receiving therapy with all oral antibiotics. These events
may be severe and generally occur following the administration of multiple doses. Clinical
manifestations may include one or more of the following: fever, rash or severe dermatologic
reactions (e.g. toxic epidermal necrolysis, Stevens-Johnson Syndrome), vasculitis, arthralgia,
myalgia, serum sickness, allergic pneumonitis, interstitial nephritis, acute renal insufficiency or
failure, hepatitis, jaundice, acute hepatic necrosis or failure, anemia including hemolytic and
aplastic, thrombocytopenia including thrombotic thrombocytopenic purpura, leukopenia,
agranulocytosis, pancytopenia, and/or other hematologic abnormalities.
PRECAUTIONS General: As with other anti-infectives, prolonged use may result in overgrowth of non-susceptible
organisms, including fungi. If superinfection occurs, discontinue use and institute alternative
therapy. Whenever clinical judgment dictates, the patient should be examined with the aid of
magnification, such as slit-lamp biomicroscopy, and, where appropriate, fluorescein staining.
In general, patients with signs and symptoms of bacterial conjunctivitis should be advised not to
Information for Patients: Avoid contaminating the applicator tip with material from the eye,
Systemically administered quinolones have been associated with hypersensitivity reactions, even
following a single dose. Discontinue use immediately and contact your physician at the first sign of
The potential of VIGAMOX® (moxifloxacin hydrochloride) ophthalmic solution to produce
arthropathy in animals has not been studied. Moxifloxacin and other members of the quinolone
class have been shown to cause arthropathy in immature Beagle dogs following oral administration
Drug Interactions: Drug-drug interaction studies have not been conducted with VIGAMOX®
solution. Moxifloxacin can be chelated by polyvalent ions such as Mg++, Al+++, Fe++ and Zn++.
There is limited information available on the concurrent use of VIGAMOX® solution and other
Following oral administration, no clinically significant drug-drug interactions between theophylline,
warfarin, digoxin, oral contraceptives or glyburide have been observed with moxifloxacin.
Theophylline, digoxin, probenecid, and ranitidine have been shown not to alter the
pharmacokinetics of moxifloxacin. In vitro studies indicate that moxifloxacin does not inhibit
CYP3A4, CYP2D6, CYP2C9, CYP2C19 or CYP1A2 indicating that moxifloxacin is unlikely to
alter the pharmacokinetics of drugs metabolized by these cytochrome P450 isozymes.
Pregnancy: Since there are no adequate and well-controlled studies in pregnant women
VIGAMOX® solution should only be used during pregnancy if the potential benefit justifies the
VIGAMOX® solution has not been studied in pregnant animals. Oral and IV studies in pregnant
animals indicated that moxifloxacin is not teratogenic. Decreased fetal birth weights and slightly
delayed fetal skeletal development were observed in rats and rabbits following oral and intravenous
administration of moxifloxacin, respectively. An increased incidence of smaller fetuses was
observed in monkeys following oral dosing (see TOXICOLOGY). When 14C-moxifloxacin was
administered orally to pregnant rats, radioactivity penetrated the placenta and was absorbed to a
moderate extent by the fetus. The ratio for AUC (0-24 h) for fetal plasma to maternal plasma was
As with other members of the quinolone class, moxifloxacin has caused arthropathy in immature
Beagle dogs following oral administration. The significance of these findings to humans is
Nursing Mothers: Moxifloxacin is excreted in the breast milk of rats following oral and
intravenous administration. Because of the potential for unknown effects from moxifloxacin in
infants being nursed by mothers taking VIGAMOX® solution, a decision should be made to either
discontinue nursing or discontinue the administration of VIGAMOX® solution, taking into account
the importance of VIGAMOX® solution therapy to the mother and the possible risk to the infant
Pediatric Use: The safety and efficacy of VIGAMOX® solution in patients less than one year of
The effect of VIGAMOX® solution on weight bearing joints has not been assessed. Oral
administration of some quinolones, including moxifloxacin, has been shown to cause arthropathy in
Geriatric Use: No overall differences in safety and effectiveness have been observed between ADVERSE REACTIONS
In clinical trials involving 1068 subjects/patients, VIGAMOX® (moxifloxacin hydrochloride)
ophthalmic solution was administered twice-daily for three days, three-times-daily for four to
fourteen days and eight-times-daily for fourteen days. During treatment with VIGAMOX®
solution, 6.6% (71 out of 1068) subjects/patients experienced treatment-related adverse drug
reactions and of these only two (0.2%) discontinued study participation. No serious ophthalmic or
systemic adverse reactions related to VIGAMOX® solution were reported.
Clinical Trial Adverse Drug Reactions
The most frequently reported treatment-related adverse drug reactions were transient eye irritation
(3.9%) (burning and/or stinging) and eye pruritus (1.1%).
Treatment-related adverse drug reactions that occurred at an incidence of 0.1% to less than 1.0%
Eye disorders: ocular hyperaemia, keratoconjunctivitis sicca, abnormal sensation in eye, ocular
discomfort, corneal epithelium defect, conjunctivitis, conjunctival haemorrhage, visual acuity
General disorders and administration site conditions: sensation of foreign body.
Investigations: corneal staining, alanine aminotransferase increased.
Nervous system disorders: dysgeusia, headache.
Respiratory, thoracic, and mediastinal disorders: pharyngolaryngeal pain.
Post-Market Adverse Drug Reactions
All adverse drug reactions with VIGAMOX® solution based on post-marketing reports (from more
than 1.1 million units sold) have been reported at an incidence of less than 0.01%. The most
frequently reported adverse reactions with VIGAMOX® solution based on post-marketing reports
Eye disorders: endophthalmitis, eye irritation, corneal infiltrates, anterior chamber cells, corneal
Immune system disorders: hypersensitivity NOS.
Skin and subcutaneous disorders: erythema.
SYMPTOMS AND TREATMENT OF OVERDOSE
No information is available on overdose of VIGAMOX® (moxifloxacin hydrochloride) ophthalmic
solution in humans. A topical overdose of VIGAMOX® solution may be flushed from the eye(s)
In an oral (gavage) monkey study, doses of moxifloxacin hydrochloride up to 15 mg/kg/day did not
produce any toxicity. This dose is at least 10 times higher than the accidental ingestion of the
contents of a 3 mL bottle of VIGAMOX® solution by a 10 kg child.
DOSAGE AND ADMINISTRATION
The recommended dosage regimen for patients one year of age and older is one drop in the affected
PHARMACEUTICAL INFORMATION
1-Cyclopropyl-6-fluoro-1,4-dihydro-8-methoxy-7-[(4aS,7aS)-octahydro-6H-
pyrrolol [3,4-b]pyridin-6-yl]-4-oxo-3-quinolinecarboxylic acid,
monohydrochloride. Moxifloxacin differs from other quinolones in that it
has a methoxy function at the 8 position, and an S,S- configured
diazabicyclononyl ring moiety at the 7-position.
Moxifloxacin hydrochloride is a slightly yellow to yellow crystalline powder.
Moxifloxacin differs from other quinolones in that it has a methoxy function
at the 8-position, and an S,S configurated diazabicyclononyl ring moiety at
Composition: Each mL of VIGAMOX® (moxifloxacin hydrochloride) ophthalmic solution
contains 5.45 mg moxifloxacin hydrochloride equivalent to 5 mg moxifloxacin base. Contains: Active: Moxifloxacin 0.5% (5,000 g/mL); Preservative: None. Product is self-preserved. Inactives: sodium chloride, boric acid and purified water. May also contain hydrochloric
VIGAMOX® solution is isotonic and formulated at pH 6.8 with an osmolality of approximately 290
Stability & Storage Recommendations: Store at 4 - 25 C. Discard 28 days after opening. AVAILABILITY
VIGAMOX® (moxifloxacin hydrochloride) ophthalmic solution, 0.5% is supplied as a 3 mL sterile
ophthalmic solution in the Alcon DROP-TAINER® dispensing system consisting of a natural low
density polyethylene bottle and dispensing plug and white polypropylene closure. Tamper evidence
is provided with a shrink band around the closure and neck area of the package.
INFORMATION FOR THE CONSUMER - VIGAMOX® (moxifloxacin hydrochloride) OPHTHALMIC SOLUTION
VIGAMOX® 0.5% solution Moxifloxacin hydrochloride Medicine to treat eye infections.
Read all of this information carefully before you start taking/using this medicine. Read this leaflet carefully because it contains important information for you.
If you have further questions, please ask your doctor or your pharmacist.
This medicine has been prescribed for you personally. Never give it to anyone else. It may harm them, even if their symptoms are the same as yours.
Keep this information. You may need to read it again. VIGAMOX® SOLUTION AND OTHER MEDICINES Please tell your doctor or pharmacist if you are taking (or recently took) any other medicines. Remember to mention medicines that you bought without prescription, over-the-counter. Do not use other eye products with VIGAMOX® solution unless advised by your doctor. WHAT MEDICATION HAS BEEN PRESCRIBED? VIGAMOX® solution contains the fluoroquinolone antibiotic, moxifloxacin. VIGAMOX® solution is an eye drop solution that treats bacterial conjunctivitis (sometimes referred to as "pink eye"), an infection of the white of the eye, and works by killing the bacteria causing the infection. WHAT DOES VIGAMOX® SOLUTION CONTAIN AND HOW IS IT SUPPLIED? VIGAMOX® solution eye drops contains moxifloxacin 0.5% (as base), sodium chloride, boric acid, and purified water. Very small amounts of hydrochloric acid or sodium hydroxide are sometimes added to keep acidity levels (pH levels) normal. VIGAMOX® solution is a liquid (a solution) supplied in an oval plastic bottle which contains 3 ml VIGAMOX® solution. VIGAMOX® solution is a clear greenish-yellow solution. WHEN SHOULD I NOT USE VIGAMOX® SOLUTION? If you have ever had any unusual or allergic reaction to moxifloxacin or other quinolones or any of the ingredients detailed in the section entitled "WHAT DOES VIGAMOX® SOLUTION CONTAIN AND HOW IS IT SUPPLIED?". Do not use VIGAMOX® solution longer than directed by your doctor. If you get a worsening of your infection, contact your doctor as soon as possible.
ARE THERE SPECIAL CONSIDERATIONS FOR PREGNANT WOMEN AND WOMEN WHO ARE BREAST FEEDING? If you are pregnant, suspect you may be pregnant or are breast feeding consult your doctor or pharmacist before using VIGAMOX® solution. ARE THERE SPECIAL CONSIDERATIONS FOR CHILDREN? VIGAMOX® solution can be used in children as young as one year of age. The dosage instructions for children are the same as for adults and are described in the section entitled "How do I use VIGAMOX® solution?" ARE THERE SPECIAL CONSIDERATIONS FOR PATIENTS OVER 65 YEARS OF AGE? VIGAMOX® solution can be used safely in patients over 65 years of age. ARE THERE SPECIAL CONSIDERATIONS FOR PATIENTS WITH KIDNEY OR LIVER PROBLEMS? VIGAMOX® solution can be used safely in patients with kidney or liver problems. CAN I DRIVE WHILE USING VIGAMOX® SOLUTION? If you experience temporary blurred vision or discomfort after using VIGAMOX® solution you should wait until these symptoms go away before driving or using machinery. CAN I WEAR CONTACT LENSES WHILE USING VIGAMOX® SOLUTION? You should not wear contact lenses if you have any signs or symptoms of an eye infection. HOW DO I USE VIGAMOX® SOLUTION? The normal dosage is one drop in the affected eye(s) three times a day (in the morning, in the afternoon, and at night). Use this much unless your doctor told you to do something different. Only use VIGAMOX® solution eye drops in both eyes if your doctor told you to. Use VIGAMOX® solution for seven days or for as long as your doctor told you to. If you miss a dose of this medicine, use the missed dose as soon as possible and then go back to your regular dosing schedule. If the drop misses your eye, try again. To keep the dropper tip and solution clean, be careful not to touch the eyelids or surrounding areas with the dropper tip of the bottle. Keep the bottle tightly closed when not in use. Get the bottle of VIGAMOX® solution eye drops and a mirror. Wash your hands. Open the bottle being careful not to touch the dropper tip. Hold the bottle, pointing down, between your thumb and fingers. Tilt your head back. Pull down your eyelid with a clean finger, until there is a 'pocket' between the eyelid and your eye. The drop will go in there.
Bring the bottle tip close to the eye. Use the mirror if it helps. Don't touch your eye or eyelid, surrounding areas or other surfaces with the bottle tip. It could contaminate the drops. Gently squeeze the bottle to release one drop of VIGAMOX® solution. If you take drops in both eyes, repeat the steps for your other eye. VIGAMOX® solution is for use as an eye drop only. WHAT DO I DO IF I TAKE TOO MUCH VIGAMOX® SOLUTION? If you put too much of this medicine in your eye(s), rinse it all out with warm tap water. Don't put in any more drops until it's time for your next regular dose. If VIGAMOX® solution is accidentally taken by mouth or injected, contact your doctor or pharmacist for advice. WHAT SIDE EFFECTS MIGHT I HAVE WITH VIGAMOX® SOLUTION? Some people who use VIGAMOX® solution may get side effects. They can be unpleasant, but most of them soon pass. You can usually keep using the drops, unless the effects are serious. If you're worried, talk to your doctor or pharmacist. While using VIGAMOX® eye drops you may experience some or all of the following reactions in your eye: mild temporary burning or stinging, itching, redness, dryness, sensation of pressure, discomfort, corneal irritations or changes, broken blood vessels in the white part of the eye, swelling of the eye or eyelid, temporary reduction of vision, pain or other ocular irritations. You may also experience reactions in other areas of your body, including: altered, bitter or bad taste, headache, throat irritation and inflammation, a change in liver enzymes, allergic reaction or skin redness following administration of the drops. Other side effects not listed above may also occur in some patients. If you notice any undesirable effects not mentioned in this information, you should stop using VIGAMOX® solution and call your doctor or pharmacist immediately and follow his/her advice. HOW LONG CAN I KEEP, AND HOW LONG SHOULD I STORE, VIGAMOX® SOLUTION? Keep these eye drops in a safe place out of the reach and sight of children. Store between 4ºC and 25ºC. Do not use this medicine after the expiry date (shown as "EXP" on the bottle and on the carton). This medicine should be thrown away 28 days after opening. FURTHER INFORMATION Contact your doctor or pharmacist. MANUFACTURER Alcon Canada Inc. 2665 Meadowpine Blvd., Mississauga, Canada L5N 8C7 MICROBIOLOGY
Moxifloxacin has in vitro activity against a wide range of Gram-positive and Gram-negative
The antibacterial action of moxifloxacin results from inhibition of topoisomerase II (DNA gyrase)
and topoisomerase IV. DNA gyrase is an essential enzyme that is involved in the replication,
transcription and repair of bacterial DNA. Topoisomerase IV is an enzyme known to play a key
role in the partitioning of the chromosomal DNA during bacterial cell division. The presence of the
bulky bicycloamine substituent at the C-7 position prevents active efflux, a proposed mechanism of
Moxifloxacin concentrations at twice the MIC are sufficient to be bactericidal for most strains of
Staphylococcus aureus, Streptococcus pneumoniae, and Haemophilus influenzae. Concentrations
of moxifloxacin somewhat greater than twice the MIC were bactericidal for strains of Escherichia coli while those greater than ten times the MIC were bactericidal for Streptococcus pyogenes.
Resistance: The mechanism of resistance of quinolones, including moxifloxacin, is different from
that of macrolides, aminoglycosides, tetracyclines or -lactams. Therefore, moxifloxacin may be
active against pathogens that are resistant to these antibiotics and these antibiotics may be active
against pathogens that are resistant to moxifloxacin. There is no cross-resistance between
moxifloxacin and the aforementioned classes of antibiotics. Cross resistance has been observed
between systemic moxifloxacin and some other quinolones.
In vitro resistance to moxifloxacin develops slowly via multiple-step mutations and occurs in vitro
at a general frequency of between 1.8 x 10-9 to less than 1 x 10-11 in one strain of Staphylococcus aureus and one strain of Streptococcus pneumoniae.
Moxifloxacin has been shown to be active against most strains of the following microorganisms
(see Table 1), both in vitro and in clinical infections from the US and India as described in the
Table 1: Moxifloxacin In Vitro Activity Against Clinical Isolates Pathogen MIC Range Aerobic, Gram-Positive Aerobic, Gram-Negative Acinetobacter species
The following in vitro data (Table 2) are also available, but their clinical significance in ophthalmic
infections is unknown. The safety and effectiveness of VIGAMOX® (moxifloxacin hydrochloride)
ophthalmic solution in treating ophthalmic infections due to these organisms have not been
established in adequate and well-controlled trials. The following organisms are considered
susceptible when evaluated using systemic breakpoints. However, a correlation between the in vitro
systemic breakpoint and ophthalmic efficacy has not been established. This list of organisms (Table
2) is provided as guidance only in assessing the potential treatment of conjunctival infections.
Moxifloxacin exhibits in vitro minimal inhibitory concentrations (MICs) of 2 g/mL or less
(systemic breakpoint susceptibility) against most (greater than or equal to 90%) strains of the
Table 2: Susceptibility of Bacterial Conjunctivitis Isolates to Moxifloxacin Bacterial Species MIC Range Aerobic Gram-positive Microorganisms Bacillus cereus Aerobic, Gram-negative Microorganisms Acinetobacter baumannii Susceptibility Tests: There are currently no NCCLS approved standards for assessing in vitro
susceptibility of conjunctival isolates to topical antibiotics, including moxifloxacin. Standardized
systemic susceptibility tests may not be appropriate to predict clinical effectiveness in treating
PHARMACOLOGY Animal Pharmacokinetics:
Ocular tissue concentrations of moxifloxacin were determined in pigmented rabbits following a
single bilateral 30 L topical administration of 0.3% ophthalmic solution of moxifloxacin (n=3
rabbits sampled at each time point). Mean maximum concentrations (Cmax) in cornea and aqueous
humor were 12.5 3.8 g/g and 1.78 0.39 g/mL, respectively, and were achieved within 30
minutes after dosing. In iris-ciliary body, a moxifloxacin Cmax of 10.4 5.6 g/g was observed at 1
hour and declined slowly relative to other tissues, presumably due to binding to melanin pigment,
which is characteristic of fluoroquinolones. The accumulation in ocular tissues of moxifloxacin
after multiple dosing has not been studied. Maximum plasma concentrations were low
(approximately 0.01 g/mL) and declined rapidly.
The distribution of radiolabeled moxifloxacin was also studied in pigmented rabbits after a single
unilateral 30 L dose of a 0.3% 14C-moxifloxacin solution (n=4 rabbits sampled at each time point).
Mean Cmax values in cornea, conjunctiva, aqueous humor and iris-ciliary body were 10.6 2.8 g/g,
2.54 0.40 g/g, 1.36 0.33 g/mL and 7.54 3.34 g/g, respectively. Maximum concentrations
and half-lives in ocular tissues are summarized in Table 3.
Table 3: Maximum Concentrations and Half-Lives of Radiolabeled Moxifloxacin in Ocular Tissues from Pigmented Rabbits Cmax (g equivalents/g) SD t½ (hours)
Tear film concentrations of moxifloxacin were measured in pigmented rabbits (n=3) after single
unilateral administration of 30 L of a 0.3% moxifloxacin ophthalmic solution. The mean
concentration of moxifloxacin was 366 214 g/mL at the first sampling point of 1 minute after
dosing. The levels then declined rapidly such that by 5 minutes after dosing the concentrations
were approximately 20 g/mL. The concentrations in the tear film were 1.73 1.50 g/mL at 6
hours post-dosing. Tear concentration data are summarised in Table 4.
Table 4: Tear Concentrations of Moxifloxacin Following Administration of a 0.3% Moxifloxacin Solution to Pigmented Rabbits Time After Dose (minutes) Mean Concentration SD Sample Size (g/mL)
* 1of 3 samples below quantitation limit of the assay. These samples were assigned a value of one half the limit of quantitation for calculation of the mean (1 g/mL/2 = 0.5 g/mL).
Human Pharmacokinetics: Plasma concentrations were studied in 21 healthy male and female
subjects who were administered VIGAMOX® (moxifloxacin hydrochloride) ophthalmic solution to
both eyes every 8 hours for a total of 13 doses. The results showed measurable plasma
concentrations of moxifloxacin (0.75 ng/mL) in 16 of 21 subjects at 4-hours following the first
dose, and in all subjects following the last dose. Figure 1 shows the mean moxifloxacin plasma
The mean steady-state estimates for Cmax and AUC were 2.7 ng/mL and 41.9 nghr/mL,
respectively. The steady-state parameter estimates for Cmax and AUC were at least 1,600 and 1,000
fold lower than mean Cmax and AUC values reported after therapeutic 400 mg oral doses of
moxifloxacin. The steady-state plasma half-life of moxifloxacin was estimated to be 13 hours.
Subgroup analysis by race (Caucasian, Asian) showed no meaningful differences in the mean
steady-state pharmacokinetic parameters of moxifloxacin. Gender differences in the steady-state
Cmax and AUC were seen; however, when adjusted for body weight, the differences were minimized
Tear film concentrations of moxifloxacin were studied in 31 healthy male and female adult
volunteers who were administered 1 drop of VIGAMOX® solution to both eyes every 8 hours for a
Mean tear concentrations at 5 minutes following the first and last topical dose were 46.0 and
55.2g/mL, respectively. Thereafter, mean tear concentrations rapidly declined in a biphasic
manner with means ranging from approximately 1 to 4 g/mL over the 1 to 8 hour sampling period.
Pre-dose morning tear concentrations on Days 2 to 4 averaged over 4 g/mL, demonstrating that
concentrations are above the MICs for most of the common organisms in conjunctivitis over the 24-
Elimination and Metabolism: Moxifloxacin is widely distributed in the body tissues and
approximately 50% is bound to serum proteins. Animal studies indicate some penetration into
conjunctiva and ocular tissues with prolonged binding to melanin. Approximately 45% of an oral
dose is excreted as unchanged drug, and most of the rest as glucuronide and sulfate conjugates in
feces and urine. The cytochrome P450 enzyme system is not involved in metabolizing the drug.
Drug-Drug Interactions: Specific drug-drug pharmacokinetic interaction studies were not
conducted with VIGAMOX® solution. Given the low systemic exposure observed for moxifloxacin
after topical ocular administration of VIGAMOX® solution, clinically relevant drug-drug
interactions through protein binding, renal elimination or hepatic metabolism are unlikely following
topical ocular administration. Moxifloxacin can be chelated by polyvalent ions such as Mg++, Al+++,
In vitro studies with cytochrome P450 isozymes have shown that moxifloxacin does not inhibit
CYP3A4, CYP2D6, CYP2C9, CYP2C19 or CYP1A2 indicating that moxifloxacin is unlikely to
alter the pharmacokinetics of drugs metabolized by these enzymes.
The pharmacokinetics of VIGAMOX® solution has not been studied in patients with hepatic or
renal impairment. However, the pharmacokinetics of orally administered moxifloxacin has been
The pharmacokinetic parameters of oral moxifloxacin are not significantly altered by mild,
moderate or severe renal impairment. No dosage adjustment of VIGAMOX® solution is necessary
Pharmacokinetic parameters of oral moxifloxacin were not significantly altered in patients with
mild to moderate hepatic insufficiency (Child Pugh Classes A and B). Studies were not performed
in patients with severe hepatic impairment (Child Pugh Class C). Because of the low systemic
exposure by the topical route of administration, no dosage adjustment of VIGAMOX® solution is
needed in patients with hepatic impairment.
Clinical Studies: In two, randomized, double-masked, multicenter, controlled trials in which 547
patients dosed with VIGAMOX® solution 3 times a day for 4 days, VIGAMOX® solution produced
clinical cures on day 5 to 6 in 66% to 69% of patients treated for bacterial conjunctivitis.
Microbiological success rates for the eradication of the baseline pathogens ranged from 84% to 94%
at the test-of-cure visit (day 9). Please note that microbiologic eradication does not always correlate
with clinical outcome in anti-infective trials.
TOXICOLOGY Topical Ocular Studies: Ophthalmic solutions of moxifloxacin were evaluated in repeat-dose
topical ocular studies in rabbits (pigmented) and Cynomolgus monkeys (see Table 5).
Table 5: Results of Topical Ocular Studies Species/No. per Dose/Route Duration of Findings Treatment Ocular Toxicity Study: A special ocular toxicity study was conducted in dogs following systemic
(oral) administration of moxifloxacin (see Table 6). The daily dosages of moxifloxacin evaluated in
this study are significantly higher than the recommended daily dose of VIGAMOX® (moxifloxacin
Table 6: Results of Ocular Toxicity Study Species/No. per Dose/Route Duration of Findings Treatment
NOEL = 30 mg/kg orally (over 1300 times > the human dose of VIGAMOX® ophthalmic solution) Single and Repeat-Dose Oral and IV Studies: Oral and intravenous single-dose studies
conducted with moxifloxacin are summarized in Table 7, and repeat-dose systemic studies that
included ocular evaluations are summarized in Table 8. The daily dose levels of moxifloxacin
evaluated in these studies are significantly higher than the recommended daily dose of VIGAMOX®
Table 7: Single-Dose Systemic Studies Strain/Sex No./Group LD50 mg/kg B.W.(Conf. AdministrationInt. for 95%) Table 8: Repeat-Dose Systemic Studies Species/No. Dose/Route Duration of Findings per Group Treatment
body wt. gain at 100, 500, 750 mg/kg
mg/kg; histopath unremarkable; NOAEL for females 100 mg/kg, 20 mg/kg for males
body wt. gain at 500 mg/kg both sexes;
mg/kg males; ocular evaluations (indirect ophthalmoscope and slit-lamp) unremarkable; histopath 500 mg/kg both sexes, thyroid 500 mg/kg males NOAEL females 100 mg/kg, males 20 mg/kg
Vacuolization of subcapsular lens cortex
cataractogenesis; prolongation of QT interval at 90 mg/kg; histopath chondropathy at 30 and 90 mg/kg
Vomiting, salivation, body wt. gain at 90
blistering of articular cartilage at 30 and 90 mg/kg
vomiting, body wt. gain at 135 mg/kg;
ophthalmoscope) unremarkable; NOAEL 15 mg/kg
Mutagenicity: Moxifloxacin was not mutagenic in four bacterial strains used in the Ames Salmonella reversion assay. As with other quinolones, the positive response observed with
moxifloxacin in strain TA 102 using the same assay may be due to the inhibition of DNA gyrase.
Moxifloxacin was not mutagenic in the CHO/HGPRT mammalian cell gene mutation assay. An
equivocal result was obtained in the same assay when v79 cells were used. Moxifloxacin was
clastogenic in the v79 chromosome aberration assay, but it did not induce unscheduled DNA
synthesis in cultured rat hepatocytes. There was no evidence of genotoxicity in vivo in a
micronucleus test or dominant lethal test in mice.
Carcinogenicity: Long term studies in animals to determine the carcinogenic potential of
moxifloxacin have not been performed. However, in an accelerated study with initiators and
promoters, moxifloxacin was not carcinogenic following up to 38 weeks of oral dosing at 500
Reproduction and Teratology: Moxifloxacin had no effect on fertility in male and female rats
at oral doses as high as 500 mg/kg/day, approximately 21,700 times the highest recommended
Moxifloxacin was not teratogenic when administered to pregnant rats during organogenesis at
oral doses as high as 500 mg/kg/day (approximately 21,700 times the highest recommended total
human ophthalmic dose); however, decreased fetal body weights and slightly delayed fetal
skeletal development were observed. There was no evidence of teratogenicity when pregnant
Cynomolgus monkeys were given oral doses as high as 100 mg/kg/day (approximately 4,300
times the highest recommended total daily human ophthalmic dose). An increased incidence of
smaller fetuses was observed at 100 mg/kg/day. In an oral peri/postnatal development study
conducted in rats, marginal effects observed at 500 mg/kg/day included extended duration of
pregnancy, increased prenatal loss, reduced birth weight and decreased survival index. Maternal
In an intravenous rabbit study, moxifloxacin at 20 mg/kg (approximately 860 times the highest
recommended total daily human ophthalmic dose) was found to decrease the gestation rate,
decrease fetal weights and delay ossification.
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