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Pharmacokinetic comparison of ketorolac after intracameral, intravitreal, and suprachoroidal administration in rabbits.

Retina (Philadelphia, Pa.) (2012-10-27)
Meizi Wang, Wu Liu, Qingjun Lu, Huiyang Zeng, Sumeng Liu, Yankun Yue, Haiting Cheng, Ying Liu, Ming Xue
RƉSUMƉ

To investigate the concentrations and pharmacokinetics of ketorolac in the rabbits by three different routes of administrations: a single intracameral, intravitreal, and suprachoroidal injection. Fifty-four New Zealand white rabbits received ketorolac (250 Ī¼g/0.05 mL) in one eye by a single intracameral injection (group A, n = 18), single intravitreal injection (group B, n = 18), and single suprachoroidal injection (group C, n = 18). Drug concentrations in the vitreous, retina-choroid (RC), and plasma were determined by the methods of high-performance liquid chromatography at 0.5, 1, 2, 4, 8, and 24 hours after injection. The concentrations in the opposite eyes were also investigated. The mean maximum concentrations (Cmax) of ketorolac in the vitreous and RC were 0.378 Ā± 0.19 Ī¼g/mL and 3.15 Ā± 0.49 Ī¼g/g (at 0.5 hours), respectively, in group A; 156.2 Ā± 20.74 Ī¼g/mL (at 0.5 hours) and 208.0 Ā± 21.67 Ī¼g/g (at 1 hours), respectively, in group B; and 0.873 Ā± 0.34 Ī¼g/mL and 56.71 Ā± 22.64 Ī¼g/g (at 0.5 hours), respectively, in group C. In the RC, the area under the curve (AUC0-t) in group B (866.1 Ā± 52.67 Ī¼g/gĀ·h) was higher (P < 0.01) than that in group C (77.10 Ā± 25.90 Ī¼g/gĀ·h). The elimination half-life (t1/2) in group B (3.09 hours) was longer (P < 0.01) than that in group C (1.19 hours). In the control eyes, a drug level below 2 Ī¼g/g was detected in the RC in group C. Plasma concentrations were below 0.4 Ī¼g/mL in all 3 groups. Ketorolac was detectable in the RC till 24 hours after the intravitreal injection and 8 hours after the suprachoroidal injection. Intravitreal injection of ketorolac produced higher intraocular drug concentrations for a longer period compared with the other two routes. Suprachoroidal injection of ketorolac could reach an effective drug level in the RC with short half-lives and low drug levels in the vitreous. The plasma drug concentrations were low by all three routes.

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Sigma-Aldrich
Ketorolac tris salt, ≥99%, crystalline
Supelco
Ketorolac Tromethamine, Pharmaceutical Secondary Standard; Certified Reference Material
Ketorolac trometamol, European Pharmacopoeia (EP) Reference Standard
Ketorolac trometamol for peak identification, European Pharmacopoeia (EP) Reference Standard