| Literature DB >> 26984315 |
John D Sheppard1, Timothy L Comstock2, Megan E Cavet3.
Abstract
Corticosteroids are a mainstay therapeutic option for the treatment ofEntities:
Keywords: Corticosteroid; Glaucoma; Intraocular pressure; Loteprednol etabonate; Ophthalmology; Safety; Topical ophthalmic
Mesh:
Substances:
Year: 2016 PMID: 26984315 PMCID: PMC4846687 DOI: 10.1007/s12325-016-0315-8
Source DB: PubMed Journal: Adv Ther ISSN: 0741-238X Impact factor: 3.845
Fig. 1Molecular structure of LE and its inactive metabolites. LE is a 17β-chloromethylester derivative of Δ1-cortienic acid, an inactive metabolite of prednisolone; LE also has a 17α-etabonate moiety. LE undergoes rapid deesterification to the inactive Δ1-cortienic acid after exerting its effect. LE loteprednol etabonate
Summary of studies evaluating the short-term effect of LE on IOP (<28 days dosing)
| Indications | Comparators | Treatment regimens (frequency, duration) | Incidence of clinically significant IOP elevation (≥10 mm Hg, unless otherwise specified) | References | |
|---|---|---|---|---|---|
| LE | Comparator | ||||
| Suspension 0.5% | |||||
| Post-cataract surgery inflammation | Vehicle | QID, 14 days | 0/102 | 1/100 | LE Postoperative Inflammation Study Group 2 [ |
| Post-cataract surgery inflammation | Vehicle | QID, 14 days | 3/109 | 0/113 | Stewart et al. [ |
| Post-cataract surgery inflammation | PA | QID, 21 days | 0/46 | 1/42 | Lane et al. [ |
| Suspension 0.2% | |||||
| SAC | Olopatadine | QID, 15 days | 0/151 | 0/149 | Gong et al. [ |
| CAC | AT | QID, 14 days | Increase of 1.6 ± 2.1 mm Hg (mean ± SD; at day 21) | No CFB | Berdy et al. [ |
| Suspension LE 0.5%/tobramycin 0.3% | |||||
| BKC | DM/T | BID, 3–5 days | 0/20 | 0/20 | Rhee & Mah [ |
| BKC | DM/T | QID, 14 days | 0/138 | 1/138 | White et al. [ |
| BKC | DM/T | QID, 14 days | 6/177 | 13/177 | Chen et al. [ |
| Eyelid inflammation in children (0–6 years) | Vehicle | QID, 7 days, then BID, 7 days | 0/72 | 0/36 | Comstock et al. [ |
| Ointment 0.5% | |||||
| Post-cataract surgery inflammation | Vehicle | QID, 14 days | 3/405 | 1/400 | Comstock et al. [ |
| Gel 0.5% | |||||
| Post-cataract surgery inflammation | Vehicle | QID, 14 days | 1/206 | 0/201 | Fong et al. [ |
| Post-cataract surgery inflammation | Vehicle | QID, 14 days | 1/203 | 1/203 | Rajpal et al. [ |
| Post-LASIK pain and inflammation | None | QID, 7–14 days postoperative | 0/96 | NA | Salinger et al. [ |
| Post-cataract surgery inflammation | Difluprednate | QID, 7 days postoperatively, then BID, 7 days | Equivalent effect on IOP at each visit ( | Abessi et al. [ | |
AC allergic conjunctivitis, AT artificial tear, BID twice daily, CAC conjunctival allergen challenge, CFB change from baseline, CSA cyclosporine A, DED dry eye disease, DM/T dexamethasone/tobramycin ophthalmic suspension, FML fluorometholone, IOP intraocular pressure, LASIK laser-assisted in situ keratomileusis, LE loteprednol etabonate, MGD meibomian gland dysfunction, NA not applicable, PA prednisolone acetate, PRK photorefractive keratectomy, QID four times daily, SAC seasonal allergic conjunctivitis, SD standard deviation
Summary of studies evaluating the long-term effect of LE on IOP (≥28 days dosing)
| Indications | Comparators | Treatment regimens | Incidence of clinically significant IOP elevation (≥10 mm Hg, unless otherwise specified) | References | |
|---|---|---|---|---|---|
| LE | Comparator | ||||
| Suspension 0.5% | |||||
| Post-cataract surgery inflammation | Flurbiprofen | QID, 28 days | 0/20 | 0/20 | Bannale et al. [ |
| Post-cataract surgery inflammation | Ketorolac | QID, for first week, then BID, 30 days | 0/30 | 0/30 | Holzer et al. [ |
| PRK | FML | LE group: PA QID for 1 week, then BID for 3 weeks, LE BID for 1 month, LE QD 1 month FML Group: PA QID for 1 month, FML TID for 1 month, BID for 1 month, QD for 1 month | 3/167 ≥ 25 mm Hg or ≥10 mm Hg CFB | 3/149 ≥ 25 mm Hg or ≥10 mm Hg CFB | Mifflin et al. [ |
| Anterior uveitis | PA | Starting dose 16 times daily, 28 days | 1/81 | 6/89 | LE US Uveitis Study Group [ |
| Anterior uveitis | PA | Starting dose 8 times daily, 42 days | 0/34 | 1/32 | LE US Uveitis Study Group [ |
| VKC | PA, FML | QID, 28 days | No CFB in mean IOP ( | PA: mean IOP increase, after exclusion of 3 patients with high IOP ( FML: no CFB in mean IOP ( | Oner et al. [ |
| SAC | Vehicle | QID, 6 weeks | 0/145 | 2/143 | Dell et al. [ |
| GPC | Vehicle | QID, 6 weeks | 3/111 | 0/109 | Asbell & Howes [ |
| GPC | Vehicle | QID, 6 weeks | 8/109 | 0/110 | Friedlaender et al. [ |
| DED | None | QID, 28 days | 0/50 | NA | Villani et al. [ |
| DED | Vehicle | QID, 28 days | 0/32 | 0/34 | Pflugfelder et al. [ |
| DED after hematopoietic stem cell transplantation | CsA | BID 1 month before and up to 12 months after transplantation | 0/38 | 0/37 | Boynton et al. [ |
| DED (induction therapy) | None | BID, 2–16 months LE monotherapy followed by 3–6 months concomitant with CsA | 0/36 > 6 mm Hg IOP increase at 2 consecutive visits | NA | Sheppard et al. [ |
| DED (induction therapy) | AT + CsA | QID 2 weeks then BID 6 weeks + CsA | No significant mean IOP CFB or between groups | Sheppard et al. [ | |
| DED (Sjögren’s syndrome) | FML 0.1% | BID, 2 years | 4/66 (6.1%) > 2 mm Hg CFB; mean IOP 15.00 ± 0.82 mm Hg | 9/67 (13.4%) > 2 mm Hg CFB; mean IOP 16.50 ± 1.12 mm Hg ( | Jung et al. [ |
| MGD | None | QID, 2 months | 0/34 | NA | Lee et al. [ |
| Corneal transplant in steroid responders treated with PA | None | Average dose: 2.3 times daily at week 3 and 1.5 times daily at week 39; average duration: 21.6 weeks | Mean IOP decrease: 12.9 mm Hg ( | Holland et al. [ | |
| Steroid responders | PA 1.0% | QID, 42 days | 6–15 mm Hg IOP rise: 3/14, > 15 mm Hg rise: 1/14 | 6–15 mm Hg IOP rise: 4/13, > 15 mm Hg rise: 4/13 | Bartlett et al. [ |
| Suspension 0.2% | |||||
| SAC | Vehicle | QID, 6 weeks | 0/66 | 0/67 | Dell et al. [ |
| SAC | Vehicle | QID, 6 weeks | 1/67 | 1/68 | Shulman et al. [ |
| SAC and PAC | None | 1–4 times daily, over 12 months | 0/159 | NA | Ilyas et al. [ |
| Suspension LE 0.5%/tobramycin 0.3% | |||||
| PRK | DM/T | QID, 1 month | 1/16 ≥ 5 mm Hg CFB | 3/16 ≥ 5 mm Hg CFB ( | Thanathanee et al. [ |
| Healthy volunteers | DM/T | QID, 28 days | 3/156 | 11/150 ( | Holland et al. [ |
| Gel 0.5% | |||||
| Corneal transplant | PA | QID 2 months, TID 1 month, BID 1 month, QD 7 months | 8/116 | 21/116 ( | Price et al. [ |
| PRK | None | 30 days or longer | 2/108 | NA | Salinger et al. [ |
| DED | CsA | BID, LE monotherapy 12 weeks or LE weeks 1–4 with CsA weeks 2–12 | LE: 1/36 LE + CsA: 1/33 > 21 mm Hg | CsA: 0/33 > 21 mm Hg | Williams et al. [ |
AC allergic conjunctivitis, AT artificial tear, BID twice daily, CFB change from baseline, CsA cyclosporine A, DED dry eye disease, DM/T dexamethasone/tobramycin ophthalmic suspension, FML fluorometholone, IOP intraocular pressure, LE loteprednol etabonate, LE/T loteprednol etabonate/tobramycin ophthalmic suspension, MGD meibomian gland dysfunction, NA not applicable, PA prednisolone acetate, PAC perennial allergic conjunctivitis, PRK photorefractive keratectomy, QD once daily, QID four times daily, SAC seasonal allergic conjunctivitis, TID three times daily, VKC vernal keratoconjunctivitis
Fig. 2Cumulative rates of clinically significant IOP elevation with loteprednol etabonate. Short-term (<28 days) and long-term (≥28 days) IOP elevation for all loteprednol etabonate formulations (pooled from 12 studies for short term and 18 studies for long term). For long-term studies, giant papillary conjunctivitis studies are excluded. Clinically significant IOP elevation is defined as ≥10 mm Hg (refer to Tables 1, 2). IOP intraocular pressure
Fig. 3Cumulative rates of clinically significant IOP elevation in head-to-head studies. The proportion of subjects with ≥10 mm Hg IOP elevation in vehicle or active control studies of LE suspension and gel formulations compared to vehicle (ten studies) or PA 1% (five studies) and of LE/T vs. DM/T (four studies). *P < 0.01 vs. comparator. DM/T dexamethasone 0.1%/tobramycin 0.3% suspension, LE loteprednol etabonate, LE/T loteprednol etabonate 0.5%/tobramycin 0.3% suspension, IOP intraocular pressure, PA prednisolone acetate