低浓度他克莫司/半氟化烷烃(SFA)滴眼液可抑制葡萄膜炎实验模型中的眼内炎症。
A Low Concentration of Tacrolimus/Semifluorinated Alkane (SFA) Eyedrop Suppresses Intraocular Inflammation in Experimental Models of Uveitis.
作者信息
De Majumdar S, Subinya M, Korward J, Pettigrew A, Scherer D, Xu H
机构信息
The Wellcome-Wolfson Institute of Experimental Medicine, School of Medicine, Dentistry and Biomedical Sciences, Queen's University Belfast, Belfast. United Kingdom.
Formulation Development, Novaliq GmbH, Im Neuenheimer Feld 515, DE-69120 Heidelberg. Germany.
出版信息
Curr Mol Med. 2017;17(3):211-220. doi: 10.2174/1566524017666170807144009.
PURPOSE
Corticosteroids remain the mainstay therapy for uveitis, a major cause of blindness in the working age population. However, a substantial number of patients cannot benefit from the therapy due to steroids resistance or intolerance. Tacrolimus has been used to treat refractory uveitis through systemic administration. The aim of this study was to evaluate the therapeutic potential of 0.03% tacrolimus eyedrop in mouse models of uveitis.
METHODS
0.03% tacrolimus in perfluorobutylpentane (F4H5) (0.03% Tacrolimus/SFA) was formulated using a previously published protocol. Tacrolimus suspended in PBS (0.03% Tacrolimus/PBS) was used as a control. In addition, 0.1% dexamethasone (0.1% DXM) was used as a standard therapy control. Endotoxin-induced uveitis (EIU) and experimental autoimmune uveoretinitis (EAU) were induced in adult C57BL/6 mice using protocols described previously. Mice were treated with eyedrops three times/day immediately after EIU induction for 48 h or from day 14 to day 25 post-immunization (for EAU). Clinical and histological examinations were conducted at the end of the experiment. Pharmacokinetics study was conducted in mice with and without EIU. At different times after eyedrop treatment, ocular tissues were collected for tacrolimus measurement.
RESULTS
The 0.03% Tacrolimus/SFA eyedrop treatment reduced the clinical scores and histological scores of intraocular inflammation in both EIU and EAU to the levels similar to 0.1% DXM eyedrop treatment. The 0.03% Tacrolimus/PBS did not show any suppressive effect in EIU and EAU. Pharmacokinetic studies showed that 15 min after topical administration of 0.03% Tacrolimus/SFA, low levels of tacrolimus were detected in the retina (48 ng/g tissue) and vitreous (2.5 ng/ml) in normal mouse eyes, and the levels were significantly higher in EIU eyes (102 ng/g tissue in the retina and 24 ng/ml in the vitreous). Tacrolimus remained detectable in intraocular tissues of EIU eyes 6 h after topical administration (68 ng/g retinal tissue, 10 ng/ml vitreous). Only background levels of tacrolimus were detected in the retina (2-8 ng/g tissue) after 0.03% Tacrolimus/PBS eyedrop administration.
CONCLUSION
0.03% Tacrolimus/SFA eyedrop can penetrate ocular barrier and reach intraocular tissue at therapeutic levels in mouse eyes, particularly under inflammatory conditions. 0.03% Tacrolimus/SFA eyedrop may have therapeutic potentials for inflammatory eye diseases including uveitis.
目的
皮质类固醇仍然是葡萄膜炎的主要治疗方法,葡萄膜炎是工作年龄人群失明的主要原因。然而,相当数量的患者由于对类固醇耐药或不耐受而无法从该治疗中获益。他克莫司已被用于通过全身给药治疗难治性葡萄膜炎。本研究的目的是评估0.03%他克莫司滴眼液在葡萄膜炎小鼠模型中的治疗潜力。
方法
使用先前发表的方案配制0.03%他克莫司于全氟丁基戊烷(F4H5)中(0.03%他克莫司/全氟丁基戊烷)。悬浮于PBS中的他克莫司(0.03%他克莫司/PBS)用作对照。此外,0.1%地塞米松(0.1% DXM)用作标准治疗对照。使用先前描述的方案在成年C57BL/6小鼠中诱导内毒素诱导的葡萄膜炎(EIU)和实验性自身免疫性葡萄膜视网膜炎(EAU)。EIU诱导后立即用滴眼液每天治疗3次,持续48小时,或在免疫后第14天至第25天(用于EAU)对小鼠进行治疗。实验结束时进行临床和组织学检查。在有和没有EIU的小鼠中进行药代动力学研究。在滴眼液治疗后的不同时间,收集眼组织用于他克莫司测量。
结果
0.03%他克莫司/全氟丁基戊烷滴眼液治疗可将EIU和EAU中眼内炎症的临床评分和组织学评分降低至与0.1% DXM滴眼液治疗相似的水平。0.03%他克莫司/PBS在EIU和EAU中未显示任何抑制作用。药代动力学研究表明,局部应用0.03%他克莫司/全氟丁基戊烷15分钟后,在正常小鼠眼中视网膜(48 ng/g组织)和玻璃体(2.5 ng/ml)中检测到低水平的他克莫司,而在EIU眼中水平显著更高(视网膜中102 ng/g组织,玻璃体中24 ng/ml)。局部给药6小时后,他克莫司仍可在EIU眼的眼内组织中检测到(视网膜组织68 ng/g,玻璃体10 ng/ml)。0.03%他克莫司/PBS滴眼液给药后,仅在视网膜中检测到背景水平的他克莫司(2 - 8 ng/g组织)。
结论
0.03%他克莫司/全氟丁基戊烷滴眼液可穿透眼屏障并在小鼠眼中达到治疗水平的眼内组织,特别是在炎症条件下。0.03%他克莫司/全氟丁基戊烷滴眼液可能对包括葡萄膜炎在内的炎症性眼病具有治疗潜力。
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