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用于皮质类固醇和抗 VEGF Fab 片段眼部药物递送的温度响应型 Diels-Alder 稳定水凝胶。

Thermo-responsive Diels-Alder stabilized hydrogels for ocular drug delivery of a corticosteroid and an anti-VEGF fab fragment.

机构信息

Department of Pharmaceutics, Utrecht Institute for Pharmaceutical Sciences, Faculty of Science, Utrecht University, PO box 80082, 3508, TB, Utrecht, the Netherlands.

University of Lille, College of Pharmacy, 3 Rue du Prof. Laguesse, 59006 Lille, France; INSERM U 1008, Controlled Drug Delivery Systems and Biomaterials, 3 Rue du Prof. Laguesse, 59006 Lille, France.

出版信息

J Control Release. 2023 Sep;361:334-349. doi: 10.1016/j.jconrel.2023.07.052. Epub 2023 Aug 10.

Abstract

In the present study, a novel in situ forming thermosensitive hydrogel system was investigated as a versatile drug delivery system for ocular therapy. For this purpose, two thermosensitive ABA triblock copolymers bearing either furan or maleimide moieties were synthesized, named respectively poly(NIPAM-co-HEA/Furan)-PEG-P(NIPAM-co-HEA/Furan) (PNF) and poly(NIPAM-co-HEA/Maleimide)-PEG-P(NIPAM-co-HEA/-Maleimide) (PNM). Hydrogels were obtained upon mixing aqueous PNF and PNM solutions followed by incubation at 37 °C. The hydrogel undergoes an immediate (<1 min) sol-gel transition at 37 °C. In situ hydrogel formation at 37 °C was also observed after intravitreal injection of the formulation into an ex vivo rabbit eye. The hydrogel network formation was due to physical self-assembly of the PNIPAM blocks and a catalyst-free furan-maleimide Diels-Alder (DA) chemical crosslinking in the hydrophobic domains of the polymer network. Rheological studies demonstrated sol-gel transition at 23 °C, and DA crosslinks were formed in time within 60 min by increasing the temperature from 4 to 37 °C. When incubated at 37 °C, these hydrogels were stable for at least one year in phosphate buffer of pH 7.4. However, the gels degraded at basic pH 10 and 11 after 13 and 3 days, respectively, due to hydrolysis of ester bonds in the crosslinks of the hydrogel network. The hydrogel was loaded with an anti-VEGF antibody fragment (FAB; 48.4 kDa) or with corticosteroid dexamethasone (dex) by dissolving (FAB) or dispersing (DEX) in the hydrogel precursor solution. The FAB fragment in unmodified form was quantitatively released over 13 days after an initial burst release of 46, 45 and 28 % of the loading for the 5, 10 and 20 wt% hydrogel, respectively, due to gel dehydration during formation. The low molecular weight drug dexamethasone was almost quantitively released in 35 days. The slower release of dexamethasone compared to the FAB fragment can likely be explained by the solubilization of this hydrophobic drug in the hydrophobic domains of the gel. The thermosensitive gels showed good cytocompatibility when brought in contact with macrophage-like mural cells (RAW 264.7) and human retinal pigment epithelium-derived (ARPE-19) cells. This study demonstrates that PNF-PNM thermogel may be a suitable formulation for sustained release of bioactive agents into the eye for treating posterior segment eye diseases.

摘要

在本研究中,我们研究了一种新型的原位形成温敏水凝胶系统,将其作为用于眼部治疗的多功能药物递送系统。为此,我们合成了两种带有呋喃或马来酰亚胺部分的温敏 ABA 三嵌段共聚物,分别命名为聚(NIPAM-co-HEA/呋喃)-PEG-P(NIPAM-co-HEA/呋喃)(PNF)和聚(NIPAM-co-HEA/马来酰亚胺)-PEG-P(NIPAM-co-HEA/-马来酰亚胺)(PNM)。将 PNF 和 PNM 水溶液混合后,在 37°C 孵育,即可得到水凝胶。水凝胶在 37°C 时会立即(<1 分钟)发生溶胶-凝胶转变。在将制剂通过玻璃体内注射到离体兔眼后,也可以在 37°C 下观察到原位水凝胶形成。水凝胶网络的形成是由于 PNIPAM 嵌段的物理自组装以及聚合物网络的疏水区中无催化剂呋喃-马来酰亚胺 Diels-Alder(DA)化学交联。流变学研究表明,在 23°C 时发生溶胶-凝胶转变,并且通过将温度从 4°C 升高到 37°C,在 60 分钟内形成 DA 交联。在 37°C 下孵育时,这些水凝胶在 pH 值为 7.4 的磷酸盐缓冲液中至少稳定一年。然而,在碱性 pH 值为 10 和 11 时,凝胶分别在 13 和 3 天后降解,这是由于水凝胶网络交联中的酯键水解所致。通过将抗 VEGF 抗体片段(FAB;48.4 kDa)或皮质类固醇地塞米松(dex)溶解(FAB)或分散(DEX)在水凝胶前体溶液中,水凝胶被负载 FAB 片段或地塞米松。未修饰的 FAB 片段在初始突释 46%、45%和 28%的加载量后,在 13 天内定量释放,分别为 5wt%、10wt%和 20wt%的水凝胶,这是由于形成过程中水凝胶的脱水所致。低分子量药物地塞米松在 35 天内几乎完全释放。与 FAB 片段相比,地塞米松的释放速度较慢,这可能是由于疏水性药物在凝胶的疏水区中溶解所致。温敏凝胶与巨噬细胞样壁细胞(RAW 264.7)和人视网膜色素上皮衍生(ARPE-19)细胞接触时表现出良好的细胞相容性。本研究表明,PNF-PNM 温敏凝胶可能是一种适合将生物活性剂持续递送到眼睛中以治疗后节眼病的制剂。

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