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两性霉素B——在角膜中的生物利用度。脂质体包裹两性霉素B局部给药的研究

[Amphotericin B--bioavailability in the cornea. Studies with local administration of liposome incorporated amphotericin B].

作者信息

Pleyer U, Grammer J, Pleyer J H, Kosmidis P, Friess D, Schmidt K H, Thiel H J

机构信息

Augenklinik, Universität Tübingen.

出版信息

Ophthalmologe. 1995 Aug;92(4):469-75.

PMID:7549331
Abstract

Amphotericin B remains an important antifungal agent in the treatment of ocular mycosis. Since topical ocular application is limited because of ocular irritation and poor penetration, we studied the pharmacokinetics of amphotericin B encapsulated in unilamellar liposomes (AmBisome). One drop (20 microliters) of AmBisome or an equivalent concentration of amphotericin B was applied to rabbit eyes. Drug concentrations were measured 15, 60, 120 and 240 min following administration of the agents by HPLC in cornea and aqueous humor. The effect of intact (group A) and debrided corneal epithelium (group B) was also studied. Corneal amphotericin B levels were significantly higher (P < 0.01) after 15 min in animals receiving amphotericin B as compared to AmBisome in group A. At later time points no differences in the corneal drug levels were found, and the drug levels following AmBisome application were remarkably stable. Epithelial removal resulted in increased corneal drug levels following application of both amphotericin B preparations. Significantly higher drug levels were observed after free amphotericin B treatment at 15-60 min (P < 0.01). Drug levels in the aqueous humor did not differ between the two amphotericin B preparations and remained below therapeutically effective concentrations. These results suggest that topically delivered AmBisome provides stable corneal drug levels, but has the potential benefit of lowered ocular toxicity.

摘要

两性霉素B仍然是治疗眼部真菌病的一种重要抗真菌药物。由于局部眼部应用因眼部刺激和穿透性差而受到限制,我们研究了包裹在单层脂质体(两性霉素B脂质体)中的两性霉素B的药代动力学。将一滴(20微升)两性霉素B脂质体或同等浓度的两性霉素B滴入兔眼。给药后15、60、120和240分钟,通过高效液相色谱法测量角膜和房水中的药物浓度。还研究了完整角膜上皮(A组)和清创角膜上皮(B组)的影响。在A组中,给药后15分钟,接受两性霉素B的动物角膜中的两性霉素B水平显著高于接受两性霉素B脂质体的动物(P<0.01)。在随后的时间点,未发现角膜药物水平有差异,并且应用两性霉素B脂质体后的药物水平非常稳定。上皮去除导致两种两性霉素B制剂应用后角膜药物水平升高。在15至60分钟时,游离两性霉素B治疗后观察到显著更高的药物水平(P<0.01)。两种两性霉素B制剂在房水中的药物水平没有差异,并且保持在治疗有效浓度以下。这些结果表明,局部递送的两性霉素B脂质体可提供稳定的角膜药物水平,但具有降低眼部毒性的潜在益处。

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