采用高效液相色谱-电喷雾质谱法测定局部和全身应用环孢素a及其代谢物在前房中的含量。

German journal of ophthalmology Pub Date : 1996-07-01
C Althaus, E Dagres, T Reinhard, U Christians, R Sundmacher
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引用次数: 0

摘要

环孢素A (CSA)由于其疏水结构,局部应用后很难通过完整的角膜进入前房。系统应用后,前房CSA水平升高。CSA代谢物比CSA更亲水。只有高效液相色谱-电喷雾质谱法可以精确定量CSA水平和鉴定所有CSA代谢物。我们研究了外用和全身应用后CSA的前房水平和不同的CSA代谢物。49例患者在常规白内障手术前使用2% CSA滴眼液(两种不同的应用方案)和7例患者在高危穿透性角膜移植术后接受全身CSA后,测量CSA和CSA代谢物前房水平。局部应用后,前房平均CSA水平为81 ng/ml。csa代谢物水平要高得多,平均达到378 ng/ml。全身治疗后,前房CSA水平和代谢物水平分别在256和317 ng/ml时更加平衡。局部滴眼液后CSA可进入前房,但这些水平远低于全身CSA治疗后的水平。外用后CSA代谢物可能起重要作用;它们在前房的浓度比CSA高得多,代谢物模式与全身治疗后所见的不同。然而,这些发现与CSA代谢物的免疫抑制活性的相关性尚不清楚。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cyclosporin-A and its metabolites in the anterior chamber after topical and systemic application as determined with high-performance liquid chromatography-electrospray mass spectrometry.

Penetration of cyclosporin A (CSA) into the anterior chamber through the intact cornea after topical application is difficult due to its hydrophobic structure. Following systemic application the anterior-chamber levels of CSA are reported to be higher. CSA metabolites are more hydrophilic than CSA. Only high-performance liquid chromatography-electrospray mass spectrometry allows exact quantification of the CSA level and the identification of all CSA metabolites. We studied the anterior-chamber levels of CSA and different CSA metabolites after topical and systemic application. CSA and CSA-metabolite anterior-chamber levels were measured in 49 patients after topical application of CSA 2% eye drops preceding routine cataract surgery with 2 different application schemes and in 7 patients receiving systemic CSA after high-risk penetrating keratoplasty. After topical application the average CSA level measured in the anterior chamber was 81 ng/ml. The CSA-metabolite levels were much higher, reaching an average of 378 ng/ml. After systemic therapy the anterior-chamber levels of CSA and of the metabolites were much more balanced at 256 and 317 ng/ml, respectively. CSA penetrates into the anterior chamber after topical eye-drop application, but these levels are much lower than those measured after systemic CSA therapy. After topical application the CSA metabolites might play an important role; they are found in the anterior chamber in much higher concentrations than is CSA, and the metabolite pattern differs from that seen after systemic therapy. The relevance of these findings to the immunosuppressive activity of the CSA metabolites, however, remains unclear.

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