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聚-L-精氨酸在兔眼滴注后增强药物向房水和玻璃体吸收的能力。

Ability of poly-L-arginine to enhance drug absorption into aqueous humor and vitreous body after instillation in rabbits.

作者信息

Nemoto Eiichi, Ueda Hideo, Akimoto Masayuki, Natsume Hideshi, Morimoto Yasunori

机构信息

Faculty of Pharmaceutical Sciences, Josai University, Sakado, Saitama 350-0295, Japan.

出版信息

Biol Pharm Bull. 2007 Sep;30(9):1768-72. doi: 10.1248/bpb.30.1768.

DOI:10.1248/bpb.30.1768
PMID:17827737
Abstract

The effect of poly-L-arginine with a molecular weight of 35.5 kDa (PLA) on the ocular absorption of hydrophilic molecules after instillation was examined in rabbits in vivo. FITC-labeled dextran (3.8 kDa, FD-4) and pyridoxamine were used as model hyprophilic molecules for absorption. The potential toxicity of PLA was evaluated by microscopic observation of the cornea, production of TNF-alpha, and the thickness of the corneal epithelia and stroma. The concentration of pyridoxamine and FD-4 in aqueous humor 30 min after a single instillation of a solution of PLA was 29- and 16-fold higher than that without PLA, respectively, but the drug concentrations were not determined in the vitreous body. Repetitive instillation of PLA every 30 min for 150 min achieved 31.1- and 13.3-fold increases in pyridoxamine and FD-4 in aqueous humor, respectively. Furthermore, significant amounts of pyridoxamine and FD-4 were detected in the vitreous body after the repetitive instillation of PLA, even although very little of these drugs was detected in the vitreous body in the control eye without PLA. On the other hand, repetitive instillation of PLA did not induce any alteration of corneal epithelial and stromal thickness, production of TNF-alpha, and disruption of the epithelial and stromal morphologies and neutrophil infiltration. Our findings suggest that PLA may be useful in promoting drug delivery of hydrophilic drugs to the ocular tissues without producing any significant corneal damage and inflammation.

摘要

研究了分子量为35.5 kDa的聚-L-精氨酸(PLA)对兔体内滴注后亲水性分子眼部吸收的影响。使用异硫氰酸荧光素标记的葡聚糖(3.8 kDa,FD-4)和吡哆胺作为亲水性分子吸收的模型。通过角膜显微镜观察、TNF-α的产生以及角膜上皮和基质的厚度来评估PLA的潜在毒性。单次滴注PLA溶液30分钟后,房水中吡哆胺和FD-4的浓度分别比未使用PLA时高29倍和16倍,但未测定玻璃体中的药物浓度。每30分钟重复滴注PLA 150分钟,房水中吡哆胺和FD-4的浓度分别增加了31.1倍和13.3倍。此外,重复滴注PLA后,玻璃体中检测到大量的吡哆胺和FD-4,而在未使用PLA的对照眼中,玻璃体中几乎检测不到这些药物。另一方面,重复滴注PLA并未引起角膜上皮和基质厚度的任何改变、TNF-α的产生以及上皮和基质形态的破坏和中性粒细胞浸润。我们的研究结果表明,PLA可能有助于将亲水性药物递送至眼部组织,而不会造成任何明显的角膜损伤和炎症。

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