Brugnera Marco, Vicario-de-la-Torre Marta, González-Cela-Casamayor Miriam Ana, González-Fernández Felipe M, Ferraboschi Ilaria, Andrés-Guerrero Vanessa, Nicoli Sara, Sissa Cristina, Pescina Silvia, Herrero-Vanrell Rocío, Bravo-Osuna Irene
Innovation, Therapy and Pharmaceutical Development in Ophthalmology (InnOftal) Research Group, Universidad Complutense de Madrid (UCM), Madrid, Spain; Department of Pharmaceutics and Food Technology, Faculty of Pharmacy, UCM; Health Research Institute (Instituto de Investigación Sanitaria) of the Hospital Clínico San Carlos (IdISSC), Madrid, Spain; University Institute of Industrial Pharmacy (IUFI), Faculty of Pharmacy, UCM, Madrid, Spain.
Innovation, Therapy and Pharmaceutical Development in Ophthalmology (InnOftal) Research Group, Universidad Complutense de Madrid (UCM), Madrid, Spain; Department of Pharmaceutics and Food Technology, Faculty of Pharmacy, UCM; Health Research Institute (Instituto de Investigación Sanitaria) of the Hospital Clínico San Carlos (IdISSC), Madrid, Spain.
J Control Release. 2025 Mar 10;379:730-742. doi: 10.1016/j.jconrel.2025.01.041. Epub 2025 Jan 25.
Frequent topical administration of hypotensive eye drops in glaucoma patients may lead to the development of dry eye disease (DED) symptoms, because of tear film destabilization and the adverse effects associated with antiglaucoma formulations. To address all this, in the current study preservative-free latanoprost-loaded (0.005 % w/v) synthetic phosphatidylcholine (1,2-dioleoyl-sn-glycero-3-phosphocholine 0.75 % w/v, 1,2-dimyristoyl-sn-glycero-3-phosphocholine 0.25 % w/v) liposomes dispersed in the mucoadhesive polymer hyaluronic acid (0.2 % w/v), containing the osmoprotective ingredients betaine (0.40 % w/v) and leucine (0.90 % w/v) (LAT-HA-LIP), have been prepared and further characterised. Permeation and retention evaluations on a validated ex vivo porcine eye model revealed that the active metabolite latanoprost acid was quantified only starting from LAT-HA-LIP once passing conjunctiva, sclera and choroid compared to the marketed latanoprost (0.005 % w/v) benchmark (MF). The liposomal formulation outperformed MF when applied to the corneal tissue. Additionally, distribution and interactions within corneal and scleral tissues were investigated by means of two-photon microscopy with liposomal formulations containing coumarin-6. Furthermore, acute and chronic tolerance studies on rabbits revealed no signs of discomfort or ocular damage. Schirmer's test, tear osmolarity, tear breakup time (TBUT) and fluorescence staining evaluated through the Oxford grading scale, were assessed as DED diagnostic parameters over a 25-day monitoring period; LAT-HA-LIP consistently maintained levels comparable to physiological solution (0.9 % w/v NaCl) used as control, with a slight increase of TBUT values from day 15 (6.00 ± 0.63 s for control, 7.00 ± 0.78 s for LAT-HA-LIP at day 15, p = 0.0066). A daily topical application of LAT-HA-LIP for 15 consecutive days, effectively lowered IOP in a sustained way (2.51-3.88 mmHg mean IOP reduction over the 5-15-day period). These results highlight the clinical relevance of the proposed technological platform, able to provide IOP reduction during the simulated long-term administration and simultaneous ocular surface protection with potential for the treatment of glaucoma.
青光眼患者频繁局部使用降眼压眼药水可能会导致干眼症(DED)症状的出现,这是由于泪膜不稳定以及抗青光眼制剂的不良反应所致。为了解决这些问题,在当前研究中,制备了分散于粘膜粘附聚合物透明质酸(0.2% w/v)中的无防腐剂载拉坦前列素(0.005% w/v)合成磷脂酰胆碱(1,2 - 二油酰 - sn - 甘油 - 3 - 磷酸胆碱0.75% w/v,1,2 - 二肉豆蔻酰 - sn - 甘油 - 3 - 磷酸胆碱0.25% w/v)脂质体,其中含有渗透保护成分甜菜碱(0.40% w/v)和亮氨酸(0.90% w/v)(LAT - HA - LIP),并对其进行了进一步表征。在经过验证的离体猪眼模型上进行的渗透和滞留评估表明,与市售拉坦前列素(0.005% w/v)基准品(MF)相比,活性代谢物拉坦前列素酸仅在通过结膜、巩膜和脉络膜后才从LAT - HA - LIP中被定量。当应用于角膜组织时,脂质体制剂的表现优于MF。此外,通过双光子显微镜对含有香豆素 - 6的脂质体制剂在角膜和巩膜组织内的分布及相互作用进行了研究。此外,对兔子进行的急性和慢性耐受性研究未发现不适或眼部损伤的迹象。在25天的监测期内,通过牛津分级量表评估的泪液分泌试验、泪液渗透压、泪膜破裂时间(TBUT)和荧光染色被用作DED诊断参数;LAT - HA - LIP始终保持与用作对照的生理溶液(0.9% w/v NaCl)相当的水平,从第15天起TBUT值略有增加(第15天时,对照为6.00±0.63秒,LAT - HA - LIP为7.00±0.78秒,p = 0.0066)。连续15天每日局部应用LAT - HA - LIP可有效持续降低眼压(在5 - 15天期间平均眼压降低2.51 - 3.88 mmHg)。这些结果突出了所提出的技术平台的临床相关性,该平台能够在模拟长期给药期间降低眼压,并同时保护眼表,具有治疗青光眼的潜力。
