safety of cetirizine ophthalmic solution 0.24% for the treatment of allergic conjunctivitis in adult and pediatric subjects

Purpose: The studies reported here aimed to assess the safety and tolerability of cetirizine ophthalmic solution 0.24%, a new topical ophthalmic medication approved by the US Food and Drug Administration for the treatment of ocular itching associated with allergic conjunctivitis. Patients and methods: Three clinical studies evaluated cetirizine ophthalmic solution 0.24% administration: a Phase I prospective, single-center, open-label, pharmacokinetic (PK) study (N = 11) evaluating single-dose administration and twice-daily (BID) administration for 1 week in healthy adults, and two Phase III, multi-center, randomized, double-masked, vehicle-controlled, parallel-group studies evaluating the safety and tolerability in adult and pediatric populations (2–18 years of age) for up to 6 consecutive weeks. The first safety and tolerability study evaluated cetirizine BID (study 1, N = 512), while the second study examined cetirizine three times daily (TID) (study 2, N = 516). Each study assessed best corrected visual acuity, slit-lamp biomicroscopy, IOP, dilated ophthalmoscopy, treatment-emergent adverse events, vital signs, urine pregnancy test, and physical examination (general health, head, eyes, ears, nose, and throat). The PK study also measured hematology, blood chemistry, and urinalysis, while the two Phase III studies additionally assessed corneal endothelial cell counts (ECC) and ECC density in a subset of subjects (via specular microscopy), and drug administration tolerability. Results: Bilateral administration of cetirizine ophthalmic solution 0.24% resulted in low systemic exposure in the PK study and was associated with a low incidence of mild adverse events. There were no drug-related severe or serious adverse events. The tolerability scores between the active and vehicle groups were comparable, demonstrating high comfort in the administration of cetirizine ophthalmic solution 0.24%. Conclusion: Cetirizine ophthalmic solution 0.24% dosed BID or TID demonstrated an acceptable safety profile and was well-tolerated when administered to subjects aged $ 2 years.

[1]  J. Ciolino,et al.  An evaluation of Retaine™ ophthalmic emulsion in the management of tear film stability and ocular surface staining in patients diagnosed with dry eye , 2015, Clinical ophthalmology.

[2]  N. Ebihara,et al.  Efficacy of Olopatadine versus Epinastine for Treating Allergic Conjunctivitis Caused by Japanese Cedar Pollen: A Double-Blind Randomized Controlled Trial , 2014, Advances in Therapy.

[3]  R. Eliashar,et al.  Mast cell stabilizing properties of antihistamines. , 2009, The Journal of investigative dermatology.

[4]  G. Ousler,et al.  An evaluation of the ocular drying effects of 2 systemic antihistamines: loratadine and cetirizine hydrochloride. , 2004, Annals of allergy, asthma & immunology : official publication of the American College of Allergy, Asthma, & Immunology.

[5]  Frederick W. Fraunfelder,et al.  Oculogyric crisis in patients taking cetirizine. , 2004, American journal of ophthalmology.

[6]  M. Abelson,et al.  Conjunctival allergen challenge: Models in the investigation of ocular allergy , 2003, Current allergy and asthma reports.

[7]  L. Bielory Allergic and immunologic disorders of the eye. Part II: ocular allergy. , 2000, The Journal of allergy and clinical immunology.

[8]  S. Holgate,et al.  Tear and conjunctival changes during the allergen-induced early- and late-phase responses. , 2000, The Journal of allergy and clinical immunology.

[9]  G. Canonica,et al.  Ocular challenge and hyperresponsiveness to histamine in patients with allergic conjunctivitis. , 1993, The Journal of allergy and clinical immunology.

[10]  P. Donshik,et al.  Allergic ocular disorders: a spectrum of diseases. , 1992, The CLAO journal : official publication of the Contact Lens Association of Ophthalmologists, Inc.

[11]  A. Kagey‐Sobotka,et al.  Effect of cetirizine on mast cell-mediator release and cellular traffic during the cutaneous late-phase reaction. , 1989, The Journal of allergy and clinical immunology.

[12]  Wellbutrin,et al.  Prescribing Information , 2015, European journal of haematology.