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在兔眼模型中使用聚合物纳米胶囊双递送环孢素A和依托度酸:眼部生物分布和药代动力学研究

Dual Delivery of Cyclosporin A and Etodolac Using Polymeric Nanocapsules in a Rabbit Eye Model: Ocular Biodistribution and Pharmacokinetic Study.

作者信息

Rahman Syed Nazrin Ruhina, Goswami Abhinab, Sree Amoolya, Jala Aishwarya, Borkar Roshan M, Shunmugaperumal Tamilvanan

机构信息

Department of Pharmaceutics, National Institute of Pharmaceutical Education and Research (NIPER), Guwahati, India.

Department of Pharmaceutical Analysis, National Institute of Pharmaceutical Education and Research (NIPER), Guwahati, India.

出版信息

J Ocul Pharmacol Ther. 2022 Dec;38(10):734-744. doi: 10.1089/jop.2022.0092. Epub 2022 Nov 10.

Abstract

Commercially available eye drops are loaded only with a single drug. By using the polymeric nanocapsules, dual delivery of 0.05% w/w cyclosporin A (CsA) and 0.2% w/w etodolac (Edc) was achieved. An ultraperformance liquid chromatography/tandem mass spectrometry (UPLC-MS/MS) method was developed for determining simultaneously the biodistribution and pharmacokinetic profile of CsA and Edc in ocular tissues. After one single drop instillation of nanocapsules into healthy right eyes of rabbits, the eyeballs were enucleated at 5, 15, 30, 60, and 90 min time periods to separate the 5 different ocular tissues. A liquid/liquid extraction method was used for ocular sample extraction using darunavir as internal standard. Using 3 diverse conditions such as bench-top, autosampler, and freeze-thaw, the stability of the analytes at 3 quality control samples in ocular tissues was also checked. Intra- and interday precisions for both CsA and Edc in multiple ocular tissues were <10.32%, and the accuracy was <11.98%. The % bias and % RSD values for CsA and Edc were found within the acceptable limit of ±15%. The highest C values were attained in cornea for both the drugs at 60 min postinstillation time point. Despite molecular size and structural differences, both CsA and Edc after liberation from nanocapsule drops can permeate into the tissues of the anterior as well as posterior segments of the eye. The biodistribution and pharmacokinetic data might help and strengthen our understanding of synergetic anti-inflammatory activity of CsA and Edc from nanocapsules after its ocular topical application for managing keratoconjunctivitis sicca.

摘要

市售眼药水仅含有单一药物。通过使用聚合物纳米胶囊,实现了0.05% w/w环孢素A(CsA)和0.2% w/w依托度酸(Edc)的双重递送。开发了一种超高效液相色谱/串联质谱(UPLC-MS/MS)方法,用于同时测定CsA和Edc在眼组织中的生物分布和药代动力学特征。将纳米胶囊单次滴入家兔健康右眼后,在5、15、30、60和90分钟时间段摘除眼球,以分离5种不同的眼组织。采用液-液萃取法,以达芦那韦为内标进行眼组织样品萃取。还在3种不同条件下(如台式、自动进样器和冻融),检查了眼组织中3个质量控制样品中分析物的稳定性。CsA和Edc在多种眼组织中的日内和日间精密度均<10.32%,准确度<11.98%。CsA和Edc的%偏差和%相对标准偏差值在±15%的可接受范围内。两种药物在滴注后60分钟时在角膜中达到最高C值。尽管分子大小和结构存在差异,但从纳米胶囊滴剂中释放出来的CsA和Edc均可渗透到眼前段和后段组织中。这些生物分布和药代动力学数据可能有助于并加深我们对纳米胶囊眼部局部应用治疗干眼症时CsA和Edc协同抗炎活性的理解。

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