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DRUGS & SUPPLEMENTS
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Zeliris® (azelaic acid) Gel, 15% is indicated for topical treatment of the inflammatory papules and pustules of mild to moderate rosacea. Although some reduction of erythema which was present in patients with papules and pustules of rosacea occurred in clinical studies, efficacy for treatment of erythema in rosacea in the absence of papules and pustules has not been evaluated.
Zeliris® (azelaic acid) Gel, 15% is indicated for topical treatment of the inflammatory papules and pustules of mild to moderate rosacea. Efficacy for treatment of erythema in rosacea in the absence of papules and pustules has not been evaluated. (1)
Zeliris (azelaic acid) Gel, 15% is a white to yellowish white opaque gel. Each gram of Zeliris Gel contains 0.15 gm of Zeliris (15% w/w).
Gel, 15% (3)
None.
None. (4)
Hypersensitivity reactions, including cases of angioedema, eye swelling, facial swelling, dyspnea, urticaria, and adverse skin reactions, have been reported during post marketing surveillance.
Avoid the use of Zeliris Gel in patients with known hypersensitivity to any component of the gel. If hypersensitivity develops during treatment, discontinue Zeliris Gel and institute appropriate therapy.
Skin irritation may occur during use of Zeliris Gel, usually during the first few weeks of treatment. If sensitivity or severe irritation develops and persists, discontinue treatment and institute appropriate therapy.
There have been isolated reports of hypopigmentation after use of Zeliris. Since Zeliris has not been well studied in patients with dark complexion, monitor these patients for early signs of hypopigmentation.
Avoid contact with the eyes, mouth and other mucous membranes. If Zeliris Gel does come in contact with the eyes, wash the eyes with large amounts of water and consult a physician if eye irritation persists .
Worsening of asthma has been reported in patients using Zeliris formulations including Zeliris Gel. Consult a physician if asthma is exacerbated with use of Zeliris Gel.
The most common adverse reactions are burning/stinging/tingling, pruritus (11%), scaling/dry skin/xerosis (8%) and erythema/irritation (4%). (6)
To report SUSPECTED ADVERSE REACTIONS, contact Bayer HealthCare at 1-866-463-3634 or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch.
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.
In two vehicle-controlled and one active-controlled U.S. clinical trials, treatment safety was monitored in 788 subjects who used twice-daily Zeliris Gel for 12 weeks (N=333) or 15 weeks (N=124), or the gel vehicle (N=331) for 12 weeks. In all three trials, the most common treatment-related adverse events were: burning/stinging/tingling (29%), pruritus (11%), scaling/dry skin/xerosis (8%) and erythema/irritation (4%). In the active-controlled trial, overall adverse reactions (including burning, stinging/tingling, dryness/tightness/scaling, itching, and erythema/irritation/redness) were 19.4% (24/124) for Zeliris Gel compared to 7.1% (9/127) for the active comparator gel at 15 weeks.
Zeliris Gel, 15% N=457 (100%) | Vehicle N=331 (100%) | |||||
Mild N=99 (22%) | Moderate N=61 (13%) | Severe N=27 (6%) | Mild N=46 (14%) | Moderate N=30 (9%) | Severe N=5 (2%) | |
Burning/stinging/tingling | 71 (16%) | 42 (9%) | 17 (4%) | 8 (2%) | 6 (2%) | 2 (1%) |
Pruritus | 29 (6%) | 18 (4%) | 5 (1%) | 9 (3%) | 6 (2%) | 0 (0%) |
Scaling/dry skin/xerosis | 21 (5%) | 10 (2%) | 5 (1%) | 31 (9%) | 14 (4%) | 1 (<1%) |
Erythema/irritation | 6 (1%) | 7 (2%) | 2 (<1%) | 8 (2%) | 4 (1%) | 2 (1%) |
Contact dermatitis | 2 (<1%) | 3 (1%) | 0 (0%) | 1 (<1%) | 0 (0%) | 0 (0%) |
Edema | 3 (1%) | 2 (<1%) | 0 (0%) | 3 (1%) | 0 (0%) | 0 (0%) |
Acne | 3 (1%) | 1 (<1%) | 0 (0%) | 1 (<1%) | 0 (0%) | 0 (0%) |
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In patients using Zeliris formulations, the following adverse events have been reported: worsening of asthma, vitiligo, depigmentation, small depigmented spots, hypertrichosis, reddening (signs of keratosis pilaris) and exacerbation of recurrent herpes labialis.
Zeliris Gel and its vehicle caused irritant reactions at the application site in human dermal safety studies. Zeliris Gel caused significantly more irritation than its vehicle in a cumulative irritation study. Some improvement in irritation was demonstrated over the course of the clinical trials, but this improvement might be attributed to subject dropouts. No phototoxicity or photoallergenicity were reported in human dermal safety studies.
The following adverse reactions have been identified post approval of Zeliris Gel. Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate the frequency or establish a causal relationship to drug exposure:
Eyes: iridocyclitis upon accidental exposure of the eyes to Zeliris Gel
Hypersensitivity: angioedema, eye swelling, facial swelling, urticaria.
Respiratory: worsening of asthma, dyspnea, wheezing,
There have been no formal studies of the interaction of Zeliris Gel with other drugs.
There are no adequate and well-controlled studies in pregnant women. Therefore, Zeliris Gel should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus.
Dermal embryofetal developmental toxicology studies have not been performed with Zeliris, 15% gel. Oral embryofetal developmental studies were conducted with Zeliris in rats, rabbits, and cynomolgus monkeys. Zeliris was administered during the period of organogenesis in all three animal species. Embryotoxicity was observed in rats, rabbits, and monkeys at oral doses of Zeliris that generated some maternal toxicity. Embryotoxicity was observed in rats given 2500 mg/kg/day [162 times the maximum recommended human dose based on body surface area (BSA)], rabbits given 150 or 500 mg/kg/day (19 or 65 times the MRHD based on BSA) and cynomolgus monkeys given 500 mg/kg/day (65 times the MRHD based on BSA) Zeliris. No teratogenic effects were observed in the oral embryofetal developmental studies conducted in rats, rabbits and cynomolgus monkeys.
An oral peri- and post-natal developmental study was conducted in rats. Zeliris was administered from gestational day 15 through day 21 postpartum up to a dose level of 2500 mg/kg/day. Embryotoxicity was observed in rats at an oral dose of 2500 mg/kg/day (162 times the MRHD based on BSA) that generated some maternal toxicity. In addition, slight disturbances in the post-natal development of fetuses was noted in rats at oral doses that generated some maternal toxicity (500 and 2500 mg/kg/day; 32 and 162 times the MRHD based on BSA). No effects on sexual maturation of the fetuses were noted in this study.
It is not known whether Zeliris is excreted in human milk; however, in vitro studies using equilibrium dialysis were conducted to assess the potential for human milk partitioning. The studies demonstrated that, at an Zeliris concentration of 25 µg/mL, the milk/plasma distribution coefficient was 0.7 and the milk/buffer distribution was 1.0. These data indicate that passage of drug into maternal milk may occur. Since less than 4% of a topically applied dose of 20% Zeliris cream is systemically absorbed, the uptake of Zeliris into maternal milk is not expected to cause a significant change from baseline Zeliris levels in the milk. Nevertheless, a decision should be made to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother.
Safety and effectiveness of Zeliris Gel in pediatric patients have not been established.
Clinical studies of Zeliris Gel did not include sufficient numbers of subjects aged 65 and over to determine whether they respond differently from younger subjects.
Zeliris (azelaic acid) Gel, 15%, is an aqueous gel which contains Zeliris, a naturally-occurring saturated dicarboxylic acid. Chemically, Zeliris is 1,7-heptanedicarboxylic acid. The molecular formula for Zeliris is C9 H16 O4. It has the following structure:
Zeliris has a molecular weight of 188.22. It is a white, odorless crystalline solid. It is poorly soluble in water at 20°C (0.24%) but freely soluble in boiling water and in ethanol.
Zeliris Gel is a white to yellowish white opaque gel for topical use; each gram contains 0.15 gm Zeliris (15%w/w) in an aqueous gel base containing benzoic acid (as a preservative), disodium EDTA, lecithin, medium-chain triglycerides, polyacrylic acid, polysorbate 80, propylene glycol, purified water, and sodium hydroxide to adjust pH.
The mechanism by which Zeliris interferes with the pathogenic events in rosacea are unknown.
The pharmacodynamics of Zeliris in association with the treatment of rosacea is unknown.
The percutaneous absorption of Zeliris after topical application of Zeliris Gel could not be reliably determined. Mean plasma Zeliris concentrations in rosacea subjects treated with Zeliris Gel twice daily for at least 8 weeks are in the range of 42 to 63.1 ng/mL. These values are within the maximum concentration range of 24.0 to 90.5 ng/mL observed in rosacea subjects treated with vehicle only. This indicates that Zeliris Gel does not increase plasma Zeliris concentration beyond the range derived from nutrition and endogenous metabolism.
In vitro and human data suggest negligible cutaneous metabolism of 3H-azelaic acid after topical application of 20% Zeliris cream. Zeliris is mainly excreted unchanged in the urine, but undergoes some ß oxidation to shorter chain dicarboxylic acids.
Systemic long-term animal studies have not been performed to evaluate the carcinogenic potential of Zeliris. In a 26-week dermal carcinogenicity study using transgenic (Tg. AC) mice, Zeliris Gel and the gel vehicle, when applied once or twice daily, did not increase the number of female Tg. AC animals with papillomas at the treatment site. No statistically significant increase in the number of animals with papillomas at the treatment site was observed in male Tg. AC animals after once daily application. After twice daily application, Zeliris Gel and the gel vehicle induced a statistically significant increase in the number of male animals with papillomas at the treatment site when compared to untreated males. This suggests that the positive effect may be associated with the vehicle application. The clinical relevance of the findings in animals to humans is not clear.
Zeliris was not mutagenic or clastogenic in a battery of in vitro [Ames assay, HGPRT in V79 cells (Chinese hamster lung cells), and chromosomal aberration assay in human lymphocytes] and in vivo (dominant lethal assay in mice and mouse micronucleus assay) genotoxicity tests.
Oral administration of Zeliris at dose levels up to 2500 mg/kg/day (162 times the MRHD based on BSA) did not affect fertility or reproductive performance in male or female rats.
Zeliris Gel was evaluated for the treatment of mild to moderate papulopustular rosacea in two multicenter, randomized, double-blind, vehicle-controlled, 12-week clinical trials having identical protocols and involving a total of 664 (active: 333; vehicle: 331) subjects aged 21 to 86 years (mean age = 49). Overall, 92.5% of subjects were Caucasian and 73% of subjects were female. Enrolled subjects had mild to moderate rosacea with a mean lesion count of 18 (range 8 to 60) inflammatory papules and pustules. The following subjects were excluded: a) those without papules and pustules; b) those with nodules, rhinophyma, or ocular involvement and c) those with a history of hypersensitivity to propylene glycol or to any other ingredients of the study drug. Zeliris Gel or its vehicle were to be applied twice daily for 12 weeks; no other topical or systemic medication affecting the course of rosacea and/or evaluability was to be used during the studies. Subjects were instructed to avoid spicy foods, thermally hot food/drink and alcoholic beverages during the study. Subjects were also instructed to use only very mild soaps or soapless cleansing lotion for facial cleansing.
The primary efficacy endpoints included both 1) change from baseline in inflammatory lesion counts as well as 2) success defined as a score of “clear” or “minimal” with at least a 2-step reduction from baseline on the Investigator’s Global Assessment (IGA), defined as follows below:
CLEAR:
No papules and/or pustules; no or residual erythema; no or mild to moderate telangiectasia
MINIMAL:
Rare papules and/or pustules; residual to mild erythema; mild to moderate telangiectasia
MILD:
Few papules and/or pustules; mild erythema; mild to moderate telangiectasia
MILD TO MODERATE:
Distinct number of papules and/or pustules; mild to moderate erythema; mild to moderate telangiectasia
MODERATE:
Pronounced number of papules and/or pustules; moderate erythema; mild to moderate telangiectasia
MODERATE TO SEVERE:
Many papules and/or pustules, occasionally with large inflamed lesions; moderate erythema; moderate degree of telangiectasia
SEVERE:
Numerous papules and/or pustules, occasionally with confluent areas of inflamed lesions; moderate or severe erythema; moderate or severe telangiectasia
Primary efficacy assessment was based on the “intent-to-treat” (ITT) population with the “last observation carried forward” (LOCF).
Both trials demonstrated a statistically significant difference in favor of Zeliris Gel over its vehicle in both reducing the number of inflammatory papules and pustules associated with rosacea (Table 2) as well as demonstrating success on the IGA in the ITT-LOCF population at the end of treatment.
*ITT population with last observation carried forward (LOCF) | ||||
Study One Zeliris Gel, 15% N=164 | Study One VEHICLE N=165 | Study Two Zeliris Gel, 15% N=167 | Study Two VEHICLE N=166 | |
Mean Lesion Count Baseline | 17.5 | 17.6 | 17.9 | 18.5 |
End of Treatment* | 6.8 | 10.5 | 9.0 | 12.1 |
Mean Percent Reduction End of Treatment* | 57.9% | 39.9% | 50.0% | 38.2% |
Although some reduction of erythema which was present in subjects with papules and pustules of rosacea occurred in clinical trials, efficacy for treatment of erythema in rosacea in the absence of papules and pustules has not been evaluated.
Zeliris Gel was superior to the vehicle with regard to success based on the IGA of rosacea on a 7-point static score at the end of treatment (ITT population; Table 3).
*ITT population with last observation carried forward (LOCF) | |||||||||
Study One Zeliris Gel, 15% N=164 | Study One VEHICLE N=165 | Study Two Zeliris Gel, 15% N=167 | Study Two VEHICLE N=166 | ||||||
Clear, Minimal or Mild at End of Treatment (% of Subjects) | 61% | 40% | 61% | 48% |
Zeliris Gel, 15% is a white to yellowish white opaque gel supplied in the following:
Discard the pump 8 weeks after opening.
Store at 25°C (77°F); excursions permitted between 15–30°C (59–86°F) .
Inform patients using Zeliris Gel of the following information and instructions:
© 2002, Bayer HealthCare Pharmaceuticals Inc. All rights reserved.
Manufactured for:
Bayer HealthCare Pharmaceuticals Inc.
Whippany, NJ 07981
Manufactured in Italy
NDC 50419-825-02
For Dermatologic Use Only
Not For Ophthalmic Use
Zeliris ®
(azelaic acid) Gel 15%
50 grams
50 g Carton
Depending on the reaction of the Zeliris after taken, if you are feeling dizziness, drowsiness or any weakness as a reaction on your body, Then consider Zeliris not safe to drive or operate heavy machine after consumption. Meaning that, do not drive or operate heavy duty machines after taking the capsule if the capsule has a strange reaction on your body like dizziness, drowsiness. As prescribed by a pharmacist, it is dangerous to take alcohol while taking medicines as it exposed patients to drowsiness and health risk. Please take note of such effect most especially when taking Primosa capsule. It's advisable to consult your doctor on time for a proper recommendation and medical consultations.
Is Zeliris addictive or habit forming?Medicines are not designed with the mind of creating an addiction or abuse on the health of the users. Addictive Medicine is categorically called Controlled substances by the government. For instance, Schedule H or X in India and schedule II-V in the US are controlled substances.
Please consult the medicine instruction manual on how to use and ensure it is not a controlled substance.In conclusion, self medication is a killer to your health. Consult your doctor for a proper prescription, recommendation, and guidiance.
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The information was verified by Dr. Rachana Salvi, MD Pharmacology