Table 4.
Advanced DDS for anterior segment diseases.
| Disease | Drug | DDS | Administration Route | Advantages and Considerations | Stage (Currently Used vs. Clinical Trial vs. Preclinical Trial) | Reference |
|---|---|---|---|---|---|---|
| Dry eye and corneal ulcer |
Levofloxacin | HPMC and sodium alginate In situ gel |
Topical | -pH-induced gel formation -Adjustable viscosity -High corneal permeability |
Preclinical | [174] |
| Dry eye | cyclosporine A | mPEG-PLA micelles | -Extended shelf life -Reduced leakage of loaded drug -Larger drug retention in rabbit retina compared to the currently approved emulsion |
Preclinical | [23] | |
| Dry eye | Cyclosporine A | Cholesterol-hyaluronate nanomicelles | Contact lens | -Enhanced mechanical strength and wettability -Improved optical transmittance |
Preclinical | [150] |
| Dry eye | Corticosteroid loteprednol etabonate | F127 nanomilled mucus penetrating nanoparticles | Topical | -Drug delivery surpasses the cellular inhibitory concentration of the carrier drug in vivo | Approved | [148] |
| Dry eye | Cyclosporine A | (HCO-40) and octoxynol 40 (OC-40). Polyvinylpyrrolidone, Sodium Phospate Monobasic Dihydrate, Sodium Phosphate Dibasic Anhydrous, and Sodium Hydroxide nanomicelles |
Topical | -Higher bioavailability in vivo than free cyclosporine A -Minimal systemic leaking of Cyclosporine A |
Clinical phase 3 completed | [189] |
| Dry eye | Rebamipide | 2-hydroxypropyl-β-cyclodextrin and methylcellulose) and a gel base (Carbopol) nanoparticles | Topical applied to eyelids | -Prolonged release of Rebamipide -Sustained release exceeds the commercially available Rebamipide nanoparticles |
Preclinical | [151] |
| Dry eye | Rebamipide | HSPC and Chol were dissolved in an appropriate amount of dichloromethane Multilamellar liposomes |
Topical | -Prolonged retention time of RBM liposomes in the cornea -Clear solution increases patient compliance unlike the commercially available options |
Preclinical | [152] |
| Dry eye | FK506 | mono-functional POSS, PEG, and PPG hydrogel | Topical | -Long-acting ocular delivery system in murine animal model | Preclinical | [190] |
| Dry eye | flurbiprofen | N-acetylcysteine-chitosan oligosaccharide-palmitic acid nanomicelles | Topical | -Strong membrane association and prolonged precorneal retention | Preclinical | [187] |
| Sjogren’s dry eye | dexamethasone | PLGA and HPMC | Sub- conjunctival Implant |
-Slow-release rate -High patient compliance |
-Phase 3 clinical trials | [191] |
| Conjunctivitis | Rapamycin | poly (3- hydroxybutyrate-co-3-hydroxyvalerate) microsphere | Topical eye drops | -Trigger increased tear secretion -Reduced corneal fluorescein in vivo |
Preclinical | [153] |
| Conjunctivitis | Ofloxacin | Chitosan and PVA nanofibers | Inserts | -Sustained release pattern for up to 96 h -Reduced burst release due to optimized crosslinking -9–20-fold higher bioavailability compared to the Ofloxacin solution |
preclinical | [166] |
| Conjunctivitis | neomycin sulfate and betamethasone sodium phosphate | poloxamer 407 and chitosan hydrogel |
Topical | -High encapsulation efficiency of hydrogels -Does not cause any irritation to the blood vessels |
Preclinical | [167] |
| Conjunctivitis | Tacrolimus | Compritol, GMS, and dichloromethane solid lipid nanoparticles | Topical eye drop | -Rigid gel formation at 32 °C -In vivo evidence of superior pharmacodynamics compared to eye drops and solid lipid nanoparticles |
Preclinical | [165] |
| Keratoconus | Riboflavin | Stearylamine or Trancutol P nanostructured lipid carriers | Topical | -Improves corneal crosslinking -High corneal transport |
Preclinical | [168] |
| Keratoconus | riboflavin and dexamethasone | poloxamer 407 and HPMC gel |
Topical | -Increases the cell thickness in relevant in vivo model | Preclinical | [169] |
| Keratoconus | Lactoferrin | Chitosan/TPP and Chitosan/Sulfobutylether-β-cyclodextrin Nanoparticles | Topical | -Host-guest complexation with BCD -Corneal residence time of more than 240 min |
Preclinical | [170] |
| Corneal ulcer | phenytoin sodium | crown ether-based nanovesicles | Topical | -Spherical nanovesicles with very high entrapment efficiency -1.78-fold increase in corneal bioavailability compared to the drug suspension |
Preclinical | [192] |
| Infectious Keratitis | hLF 1-11 | HPMC and Hyaluronic Acid mucoadhesive matrices |
unspecified | -6 months of antimicrobial activity -High stability of encapsulated peptides -Entrapment efficiency can be enhanced with Trehalose |
Preclinical | [193] |
| Infectious Keratitis | moxifloxacin | HPMC with PVP and PEG | Ocular insert | -Adjustable concentration of HPMC and PVP reduces crystallization and increases the lamination consistency -Water encapsulation leads to increased bioadhesion -In situ gel formation prolongs the adhesion to the cornea |
Preclinical | [176] |
| Bacterial Keratitis | Ofloxacin | chitosan and PEG-coated solid nanoparticles | Topical | -Slower drug release with 63.6% of the drug released in 3 h compared to 99.55% of the drug being released from the currently used DDS -Reduced average nanoparticle size -Accelerates ocular barrier permeation and increased adherence to the epithelium. |
Preclinical | [194] |
| Fungal Keratitis | Amphotericin B | PVP and PVA patches | Microneedle ocular patch | -Does not contain deoxycholate that renders the currently available Amphotericin B ocular treatment painful -The microneedles completely dissolve within 1 minute in the cornea -More effective in targeting Candida compared to the liposomal amphotericin B-loaded microneedle ocular patch. |
Preclinical | [195] |
| Fungal Keratitis | Amphotericin B | PVP and HA microneedles | Ocular patches | -Overcome the reduced loading capacity, reduced mechanical strength, and potentially high cost that could be associated with liposomal Amphotericin B formulations | Preclinical | [175] |
| Fungal Keratitis | Econazole | Carboxymethyl-alpha-cyclodextrin conjugated with chitosan |
Topical eye drop | -Increased ocular bioavailability in the cornea by 29-times compared to controls in vivo and ex vivo after a single administration | Preclinical | [177] |
| Fungal Keratitis | Natamycin | Precirol ATO 5 and Pluronic f68 solid nanoparticles | Topical | -Extended drug release profile of 10 h -Increased corneal permeation compared to currently used formulation |
preclinical | [196] |
| Keratitis and posterior uveitis | tacrolimus | PLGA, Tween, Cremophor, E80 solution, and PVA Nanocapsules |
Topical eye drops | -Highly stable lyophilized DDS. -High retention and permeation of drug -Reduction in several inflammatory markers in the anterior chamber |
Preclinical | [196] |
| Meibomian gland dysfunction | Cerium oxide nanoparticles | polyhydroxyethyl methacrylate contact lenses | Contact lenses | -In vitro and in vivo reduction of oxidative stress -Prolonged release |
Preclinical | [162] |
| Meibomian gland dysfunction | Cyclosporin A | (Nano-cyclosporine; Cyporin N, Taejoon, Korea) | Topical | -Better corneal staining and increased lipid layer thickness compared to the group receiving the conventional cyclosporine formulation | Phase 3 | [163] |
| Cataract disease | Cerium nanoparticles | PLGA-based nanoformulation | Topical | -Good biocompatibility -Avoids the need for subconjunctival injection |
Preclincal | [185] |
| Cataract disease | Baicalin | mPEG-PLGA nanoparticles | Topical | -Improve precorneal residence time -Enhance the reduction of reactive oxygen species in vivo |
Preclincal | [186] |
| Cataract disease | Lutein | Zein and PLGA | Topical | -Reduce cataracts in rat model -Fully biodegradable system emerging in the treatment of cataracts |
Preclincal | [188] |
| Cataract disease | quercetin | Chitosan-N-acetylcysteine with hydroxypropyl β-CD | Topical | -Enhanced corneal permeability -Strong membrane association |
Preclincal | [178] |