VUITY- pilocarpine hydrochloride solution/ drops
AbbVie Inc.
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HIGHLIGHTS OF PRESCRIBING INFORMATION
These highlights do not include all the information needed to use VUITY safely and effectively. See full prescribing information for VUITY.
VUITY® (pilocarpine hydrochloride ophthalmic solution) 1.25%, for topical ophthalmic use Initial U.S. Approval: 1974 RECENT MAJOR CHANGESINDICATIONS AND USAGEVUITY is a cholinergic muscarinic receptor agonist indicated for the treatment of presbyopia in adults. (1) DOSAGE AND ADMINISTRATIONInstill one drop of VUITY in each eye once daily. A second dose (one additional drop in each eye) may be administered 3-6 hours after the first dose. (2) DOSAGE FORMS AND STRENGTHSOphthalmic solution containing pilocarpine hydrochloride 1.25%. (3) CONTRAINDICATIONSHypersensitivity (4) WARNINGS AND PRECAUTIONS
ADVERSE REACTIONSMost common adverse reactions (>5%) are headache, conjunctival hyperemia, and eye irritation. (6.1)
See 17 for PATIENT COUNSELING INFORMATION. Revised: 3/2023 |
The recommended dosage of VUITY is one drop in each eye once daily. A second dose (one additional drop in each eye) may be administered 3-6 hours after the first dose.
If more than one topical ophthalmic product is being used, the products should be administered at least 5 minutes apart.
VUITY (pilocarpine hydrochloride ophthalmic solution) is a clear, colorless, sterile ophthalmic solution containing 1.25% (12.5 mg/mL) of pilocarpine hydrochloride.
VUITY is contraindicated in patients with known hypersensitivity to the active ingredient or to any of the excipients.
Miotics, including VUITY, may cause accommodative spasm. Patients should be advised not to drive or operate machinery if vision is not clear (e.g., blurred vision).
In addition, patients may experience temporary dim or dark vision with miotics, including VUITY. Patients should be advised to exercise caution in night driving and other hazardous activities in poor illumination.
Rare cases of retinal detachment and retinal tear have been reported with miotics, including VUITY.
Individuals with pre-existing retinal disease are at increased risk. Therefore, examination of the retina is advised in all patients prior to the initiation of therapy.
Patients should be advised to seek immediate medical care with sudden onset of flashing lights, floaters, or vision loss.
VUITY is not recommended to be used when iritis is present because adhesions (synechiae) may form between the iris and the lens.
The following clinically significant adverse reactions are described elsewhere in labeling:
Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared to rates in the clinical trials of another drug and may not reflect the rates observed in practice.
VUITY dosed once daily was evaluated in 375 participants with presbyopia in two randomized, double-masked, vehicle-controlled studies (GEMINI 1 and GEMINI 2) of 30 days duration. The most common adverse reactions reported in >5% of participants were headache and conjunctival hyperemia. Ocular adverse reactions reported in 1-5% of participants were blurred vision, eye pain, visual impairment, eye irritation, and increased lacrimation.
VUITY was also evaluated in 114 participants with presbyopia in a randomized, double-masked, vehicle-controlled 14-day study (VIRGO) in which participants received two doses of VUITY in each eye, 6 hours apart daily. The most common adverse reactions reported in >5 % of participants were headache and eye irritation. Ocular adverse reactions reported in 1-5% of participants were visual impairment, eye pain, blurred vision, and vitreous floaters.
The following adverse reactions have been identified during postapproval use of VUITY. Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to VUITY exposure.
Eye disorders: vitreous detachment, vitreomacular traction, retinal tear, retinal detachment.
Risk Summary
There are no adequate and well-controlled studies of VUITY administration in pregnant women to inform a drug-associated risk. Oral administration of pilocarpine to pregnant rats throughout organogenesis and lactation did not produce adverse effects at clinically relevant doses.
Data
Human Data
No adequate and well-controlled trials of VUITY have been conducted in pregnant women. In a retrospective case series of 15 women with glaucoma, 4 patients used ophthalmic pilocarpine either pre-pregnancy, during pregnancy or postpartum. There were no adverse effects observed in patients or in their infants.
Animal Data
In embryofetal development studies, oral administration of pilocarpine to pregnant rats throughout organogenesis produced maternal toxicity, skeletal anomalies and reduction in fetal body weight at 90 mg/kg/day (approximately 485-fold higher than the maximum human ophthalmic dose [MHOD] of 0.03 mg/kg/day assuming administration of 2 drops/eye/day, on a mg/m2 basis).
In a peri-/postnatal study in rats, oral administration of pilocarpine during late gestation through lactation increased stillbirths at a dose of 36 mg/kg/day (approximately 195-fold higher than the MHOD). Decreased neonatal survival and reduced mean body weight of pups were observed at ≥18 mg/kg/day (approximately 100 times the maximum human ophthalmic dose of VUITY).
Risk Summary
There is no information regarding the presence of pilocarpine in human milk, the effects on the breastfed infants, or the effects on milk production to inform risk of VUITY to an infant during lactation.
Pilocarpine and/or its metabolites are excreted in the milk of lactating rats. Systemic levels of pilocarpine following topical ocular administration are low [see Clinical Pharmacology (12.3)], and it is not known whether measurable levels of pilocarpine would be present in maternal milk following topical ocular administration.
The developmental and health benefits of breastfeeding should be considered along with the mother’s clinical need for VUITY and any potential adverse effects on the breastfed child from VUITY.
Data
Animal Data
Following a single oral administration of 14C-pilocarpine to lactating rats, the radioactivity concentrations in milk were similar to those in plasma.
Clinical studies of VUITY did not include participants aged 65 and over to determine whether they respond differently from younger participants. Other reported clinical experience with ophthalmic pilocarpine solutions have not identified overall differences in safety between elderly and younger participants.
Systemic toxicity following topical ocular administration of pilocarpine is rare, but occasionally patients who are sensitive may develop sweating and gastrointestinal overactivity. Accidental ingestion can produce sweating, salivation, nausea, tremors and slowing of the pulse and a decrease in blood pressure. In moderate overdosage, spontaneous recovery is to be expected and is aided by intravenous fluids to compensate for dehydration. For patients demonstrating severe poisoning, atropine, the pharmacologic antagonist to pilocarpine, should be used.
VUITY (pilocarpine hydrochloride ophthalmic solution) 1.25% is a cholinergic muscarinic receptor agonist prepared as an isotonic, clear, colorless, sterile ophthalmic solution containing 1.25% of pilocarpine hydrochloride. The chemical name for pilocarpine hydrochloride is (3S,4R)-3-ethyl-4-[(1-methyl-1H-imidazol-5-yl)methyl]oxolan-2-one hydrochloride. Its molecular weight is 244.72 and its molecular formula is C11H16N2O2 · HCl. Its structural formula is:
Each mL of VUITY contains pilocarpine hydrochloride 1.25% (12.5 mg) as the active ingredient, equivalent to 1.06% (10.6 mg) pilocarpine free-base. Preservative is: benzalkonium chloride 0.0075%. Inactive ingredients in the ophthalmic solution are: boric acid, sodium citrate dihydrate, sodium chloride, purified water, and may also include hydrochloric acid and/or sodium hydroxide for pH adjustment to between 3.5 and 5.5, if necessary.
Pilocarpine hydrochloride is a cholinergic muscarinic agonist which activates muscarinic receptors located at smooth muscles such as the iris sphincter muscle and ciliary muscle. VUITY contracts the iris sphincter muscle, constricting the pupil to improve near and intermediate visual acuity while maintaining some pupillary response to light. VUITY also contracts the ciliary muscle and may shift the eye to a more myopic state.
Systemic exposure to pilocarpine was evaluated in 22 participants with presbyopia who were administered 1 drop of VUITY in each eye once daily for 30 days (GEMINI 1). The mean (SD) Cmax and AUC values from time 0 to last measurable concentration over 10-hour period post-last dose on Day 30 were 1.95 (0.98) ng/mL and 4.14 (2.16) ng·hr/mL, respectively. The median Tmax value on Day 30 was 0.3 hours postdose with a range from 0.2 to 0.5 hours postdose.
Systemic exposure to pilocarpine was also evaluated in 8 participants with presbyopia who were administered 1 drop of VUITY in each eye twice daily for 14 days (VIRGO). The Day 14 mean (SD) Cmax following first daily dosing was 1.81 (0.51) ng/mL and following second daily dosing was 2.12 (1.75) ng/mL. The Day 14 mean (SD) AUC over 6-hour post-dose following first daily dose was 4.35 (1.50) ng·hr/mL and following second daily dose was 4.22 (3.14) ng·hr/mL. There was no significant systemic drug accumulation over time, with accumulation index ratios between Day 1 and Day 14 based on AUC as 1.42 and 1.03 for the first and second daily dose, respectively.
Carcinogenesis
Pilocarpine did not induce tumors in mice at any dosage level studied (up to 30 mg/kg/day; approximately 80-times the MHOD). In rats, an oral dose of 18 mg/kg/day (approximately 100 times the MHOD), resulted in a statistically significant increase in the incidence of benign pheochromocytomas in both male and female rats, and a statistically significant increase in the incidence of hepatocellular adenomas in female rats.
Mutagenesis
Pilocarpine did not show any potential to cause genetic toxicity in a series of studies that included: 1) bacterial assays (Salmonella and E. coli) for reverse gene mutations; 2) an in vitro chromosome aberration assay in a Chinese hamster ovary cell line; 3) an in vivo chromosome aberration assay (micronucleus test) in mice; and 4) a primary DNA damage assay (unscheduled DNA synthesis) in rat hepatocyte primary cultures.
Impairment of Fertility
Pilocarpine oral administration to male and female rats at a dosage of 18 mg/kg/day (100 times the MHOD) resulted in impaired reproductive function, including reduced fertility, decreased sperm motility, and morphologic evidence of abnormal sperm. It is unclear whether the reduction in fertility was due to effects on males, females, or both. In dogs, exposure to pilocarpine at a dosage of 3 mg/kg/day for 6 months resulted in evidence of impaired spermatogenesis (approximately 55 times the MHOD).
The efficacy of VUITY dosed once daily for the treatment of presbyopia was demonstrated in two 30‐Day Phase 3, randomized, double‐masked, vehicle‐controlled studies, namely GEMINI 1 (NCT03804268) and GEMINI 2 (NCT03857542). A total of 750 participants aged 40 to 55 years old with presbyopia were randomized (375 to VUITY group) in two studies and participants were instructed to administer one drop of VUITY or vehicle once daily in each eye.
In both studies, the proportion of participants gaining 3 lines or more in mesopic, high contrast, binocular distance corrected near visual acuity (DCNVA), without losing more than 1 line (5 letters) of corrected distance visual acuity (CDVA) with the same refractive correction was statistically significantly greater in the VUITY group compared to the vehicle group at Day 30, Hour 3 (see Table 1).
GEMINI 1 | GEMINI 2 | |||||
VUITY
N=163 | Vehicle
N=160 | p-value | VUITY
N=212 | Vehicle
N=215 | p-value | |
Proportion of participants gaining 3-lines or more in mesopic DCNVA, without losing more than 1 line (5 letters) of CDVA at Day 30, Hour 3 | 31% | 8% | p<0.01 | 26% | 11% | p<0.01 |
Figures 1 and 2 present the proportion of participants who gained 3-lines or more in mesopic DCNVA at Day 30.
Figure 1: Proportion of Participants Achieving 3-Lines or More Improvement in Mesopic, High Contrast, Binocular DCNVA at Day 30 in GEMINI 1 (Intent-to-Treat Population)
Timepoint | Hour 0 | Hour 0.25 | Hour 0.5 | Hour 1 | Hour 3 | Hour 6 | Hour 8 | Hour 10 |
VUITY (%) | 4.3 | 17.7 | 34.8 | 41.6 | 30.7 | 18.4 | 10.6 | 7.5 |
Vehicle (%) | 5.9 | 9.8 | 9.8 | 15.7 | 8.1 | 8.8 | 8.5 | 8.6 |
Difference (95% CI) | -1.5 (-6.4, 3.3) | 7.9 (0.3, 15.5) | 25.0 (16.2, 33.8) | 25.9 (16.4, 35.5) | 22.5 (14.3, 30.8) | 9.7 (2.3, 17.0) | 2.1 (-4.4, 8.5) | -1.1 (-7.1, 5.0) |
Figure 2: Proportion of Participants Achieving 3-lines or More Improvement in Mesopic, High Contrast, Binocular DCNVA at Day 30 in GEMINI 2 (Intent-to-Treat Population)
Timepoint | Hour 0 | Hour 0.25 | Hour 0.5 | Hour 1 | Hour 3 | Hour 6 | Hour 8 | Hour 10 |
VUITY (%) | 7.8 | 16.1 | 32.1 | 37.3 | 27.6 | 16.3 | 14.5 | 12.6 |
Vehicle (%) | 4.0 | 6.6 | 9.6 | 12.1 | 10.8 | 9.9 | 8.6 | 8.7 |
Difference (95% CI) | 3.8 (-0.9, 8.4) | 9.4 (3.2, 15.7) | 22.5 (14.7, 30.3) | 25.2 (17.0, 33.4) | 16.7 (9.1, 24.3) | 6.5 (-0.1, 13.1) | 5.9 (-0.5, 12.2) | 3.8 (-2.3, 10.0) |
The efficacy of VUITY dosed twice daily for the treatment of presbyopia was also demonstrated in a 14-Day, randomized, double-masked, vehicle-controlled study, namely VIRGO (NCT04983589). A total of 230 participants aged 40 to 55 years old with presbyopia were randomized (114 to VUITY group) and participants were instructed to administer one drop of VUITY or vehicle twice daily in each eye, with each dose administered 6 hours apart.
In this study, the proportion of participants gaining 3 lines or more in mesopic, high contrast, binocular distance corrected near visual acuity (DCNVA), without losing more than 1 line (5 letters) of corrected distance visual acuity (CDVA) with the same refractive correction was statistically significantly greater in the VUITY group compared to the vehicle group at Day 14, Hour 9 (3 hours after the second dose) (see Table 2).
VIRGO | |||
VUITY BID
N=114 | Vehicle BID
N=116 | p-value | |
Proportion of participants gaining 3-lines or more in mesopic DCNVA, without losing more than 1 line (5 letters) of CDVA at Day 14, Hour 9 (3 hours after the second dose) | 35% | 8% | p< 0.01 |
Figure 3 presents the proportion of participants who gained 3-lines or more in mesopic DCNVA at Day 14.
Figure 3: Proportion of Participants Achieving 3-lines or More Improvement in Mesopic, High Contrast, Binocular DCNVA at Day 14 in VIRGO (Intent-to-Treat Population)
Timepoint | Hour 0 | Hour 1 | Hour 3 | Hour 6 | Hour 7 | Hour 9 |
VUITY BID (%) | 12.3 | 53.5 | 37.7 | 27.2 | 54.4 | 36.8 |
Vehicle BID (%) | 3.4 | 8.6 | 7.8 | 4.3 | 6.0 | 8.6 |
Difference (95% CI) | 8.8 (2.0, 15.7) | 44.9 (34.4, 55.4) | 30.0 (19.8, 40.1) | 22.9 (13.9, 31.8) | 48.4 (38.2, 58.5) | 28.2 (18.0, 38.4) |
VUITY is supplied as an isotonic, clear, colorless sterile ophthalmic solution in colorless low density polyethylene (LDPE) ophthalmic dispenser bottles and tips, with dark green high impact polystyrene caps as follows:
2.5 mL fill in 5 mL bottle (Box containing 1 bottle) | NDC 0074-7098-01 |
2.5 mL fill in 5 mL bottle (Box containing 3 bottles) | NDC 0074-7098-03 |
2.5 mL fill in 5 mL bottle (Carton containing 1 bottle) | NDC 0074-7098-04 |
5 mL fill in 5 mL bottle (Carton) | NDC 0074-7098-06 |
Storage
Store at 15°C to 25°C (59°F to 77°F). After opening, VUITY can be used until the expiration date on the bottle.
Night Driving
VUITY may cause temporary dim or dark vision. Advise patients to exercise caution with night driving and when hazardous activities are undertaken in poor illumination [see Warnings and Precautions (5.1)].
Accommodative Spasm
Temporary problems when changing focus between near and distant objects may occur. Advise patients not to drive or use machinery if vision is not clear (e.g., blurred vision) [see Warnings and Precautions (5.1)].
When to Seek Physician Advice
Advise patients to seek immediate medical care with sudden onset of flashing lights, floaters, or vision loss [see Warnings and Precautions (5.2)].
Contact Lens Wear
Contact lens should be removed prior to the instillation of VUITY. Wait 10 minutes after dosing before reinserting contact lenses [see Warnings and Precautions (5.4)].
Avoiding Contamination of the Product
Do not touch dropper tip to any surface, as this may contaminate the contents [see Warnings and Precautions (5.5)].
Concomitant Topical Ocular Therapy
If more than one topical ophthalmic medication is being used, the medicines must be administered at least 5 minutes apart.
Distributed by: Allergan, an AbbVie company
Manufactured for:
AbbVie Inc.
North Chicago, IL 60064 USA
© 2023 AbbVie. All rights reserved.
VUITY and its design are trademarks of Allergan Sales, LLC, an AbbVie company.
v5.0USPI7098
NDC 0074-7098-01
Vuity™
(pilocarpine HCI ophthalmic solution) 1.25%
Contains one
2.5 mL bottle
Rx Only
Sterile
For topical
application
in the eye
1 x 2.5 mL
Allergan™
An AbbVie company
NDC 0074-7098-03
Vuity™
(pilocarpine HCI ophthalmic solution) 1.25%
Contains three
2.5 mL bottles
Rx Only
Sterile
For topical
application
in the eye
3 x 2.5 mL
Allergan™
An AbbVie company
NDC 0074-7098-04
Vuity™
(pilocarpine HCI ophthalmic
solution) 1.25%
Rx Only
Sterile
2.5 mL
For Topical Application in the Eye
Allergan™
An AbbVie company
VUITY
pilocarpine hydrochloride solution/ drops |
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Labeler - AbbVie Inc. (078458370) |