针对眼睛表面和脂质体给药的适配体的 Cornea-SELEX

Exploration Pub Date : 2024-02-09 DOI:10.1002/exp.20230008
Ka-Ying Wong, Yibo Liu, Man-Sau Wong, Juewen Liu
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引用次数: 0

摘要

角膜是药物输送到眼部的主要障碍,导致眼部局部治疗的生物利用度低、疗效差。在这项工作中,我们首先在猪角膜上利用组织-SELEX筛选出与角膜结合的适配体。含量最高的两种适配体 Cornea-S1 和 Cornea-S2 能与猪角膜结合,它们与人角膜上皮细胞(HCECs)的 Kd 值分别为 361 和 174 nм。该研究开发了负载环孢素 A(CsA)的色素功能化脂质体,用于治疗干眼症。由于多价结合,Cornea-S1 或 Cornea-S2 功能化脂质体的 Kd 分别降至 1.2 和 15.1 nм。在HCECs中,Cornea-S1或Cornea-S2可在15分钟内增强脂质体的吸收,并将保留时间延长至24小时。在兔子干眼症模型中,Cornea-S1 CsA 脂质体与商用 CsA 滴眼液相比,在维持角膜完整性和泪液破裂时间方面表现相当,但使用的 CsA 剂量更低。从角膜-SELEX中获得的适配体可以作为眼部给药的通用配体,为治疗各种眼部疾病甚至其他疾病提供了一种前景广阔的途径。
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Cornea‐SELEX for aptamers targeting the surface of eyes and liposomal drug delivery
Cornea is the major barrier to drug delivery to the eye, which results in low bioavailability and poor efficacy of topical eye treatment. In this work, we first select cornea‐binding aptamers using tissue‐SELEX on pig cornea. The top two abundant aptamers, Cornea‐S1 and Cornea‐S2, could bind to pig cornea, and their Kd values to human corneal epithelial cells (HCECs) were 361 and 174 nм, respectively. Aptamer‐functionalized liposomes loaded with cyclosporine A (CsA) were developed as a treatment for dry eye diseases. The Kd of Cornea‐S1‐ or Cornea‐S2‐functionalized liposomes reduces to 1.2 and 15.1 nм, respectively, due to polyvalent binding. In HCECs, Cornea‐S1 or Cornea‐S2 enhanced liposome uptake within 15 min and extended retention to 24 h. Aptamer CsA liposomes achieved similar anti‐inflammatory and tight junction modulation effects with ten times less CsA than a free drug. In a rabbit dry eye disease model, Cornea‐S1 CsA liposomes demonstrated equivalence in sustaining corneal integrity and tear break‐up time when compared to commercial CsA eye drops while utilizing a lower dosage of CsA. The aptamers obtained from cornea‐SELEX can serve as a general ligand for ocular drug delivery, suggesting a promising avenue for the treatment of various eye diseases and even other diseases.
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