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肝素-叶酸-视黄酸生物缀合物用于靶向递送疏水性光增敏剂。

Heparin-folate-retinoic acid bioconjugates for targeted delivery of hydrophobic photosensitizers.

机构信息

Department of Polymer Science & Engineering, Chungnam National University, 220, Gung-dong, Yuseng-gu, Daejeon 305-764, Republic of Korea.

出版信息

Carbohydr Polym. 2013 Feb 15;92(2):1615-24. doi: 10.1016/j.carbpol.2012.10.075. Epub 2012 Nov 8.

DOI:10.1016/j.carbpol.2012.10.075
PMID:23399198
Abstract

Amphiphilic heparin-retinoic acid (HR) and heparin-folate-retinoic acid bioconjugates (HFR) were synthesized by chemical conjugation of a hydrophobic anticancer agent all-trans-retinoic acid (RA) and a targeting ligand, folic acid (FA), to the high molecular weight heparin backbone. The HR and HFR bioconjugates had a high RA content (22%, w/w) and could self-assemble into nanoparticles with efficient encapsulation of a hydrophobic photosensitizer, pheophorbide a (PhA). The HFR bioconjugate demonstrated higher PhA loading content and loading efficiency compared to HR bioconjugate. The PhA-loaded HR and HFR nanoparticles had an average diameter of about 70 nm, a negatively charged surface, a sustained release pattern and self-quenching effect in a buffered solution. Furthermore, the cellular uptake of PhA-loaded HFR nanoparticles in folate receptor-positive HeLa cells was higher than that of PhA-loaded HR nanoparticles. Upon irradiation, HFR nanoparticles selectively enhanced the phototoxicity of PhA in HeLa cells while the dark-toxicity of the nanoparticles was minimal without light treatment. HFR nanoparticles also demonstrated targeted anti-cancer effect, improving the cytotoxicity of RA in HeLa cells compared to HR nanoparticles at RA concentration ≥50 μg/mL. The targeting effect of HFR and PhA-loaded HFR nanoparticles was not observed in folate receptor-negative HT-29 cells. The results indicated that HFR nanoparticles may be useful for targeted delivery of hydrophobic PDT agents and as a potential nanocarrier for dual chemo-and photodynamic therapies.

摘要

两亲性肝素-视黄酸(HR)和肝素-叶酸-视黄酸生物缀合物(HFR)通过将疏水性抗癌剂全反式视黄酸(RA)和靶向配体叶酸(FA)化学偶联到高分子量肝素主链上来合成。HR 和 HFR 生物缀合物具有高 RA 含量(22%,w/w),并且可以自组装成纳米颗粒,有效地包封疏水性光敏剂原卟啉 a(PhA)。与 HR 生物缀合物相比,HFR 生物缀合物具有更高的 PhA 载药量和载药效率。载有 PhA 的 HR 和 HFR 纳米颗粒在缓冲溶液中具有约 70nm 的平均直径、带负电荷的表面、持续释放模式和自猝灭效应。此外,在叶酸受体阳性的 HeLa 细胞中,负载 PhA 的 HFR 纳米颗粒的细胞摄取量高于负载 PhA 的 HR 纳米颗粒。照射后,HFR 纳米颗粒在 HeLa 细胞中选择性增强了 PhA 的光毒性,而在没有光处理的情况下,纳米颗粒的暗毒性最小。与 HR 纳米颗粒相比,HFR 纳米颗粒在 RA 浓度≥50μg/mL 时还表现出针对 RA 的靶向抗癌作用,提高了 HeLa 细胞中 RA 的细胞毒性。在叶酸受体阴性的 HT-29 细胞中,未观察到 HFR 和负载 PhA 的 HFR 纳米颗粒的靶向作用。结果表明,HFR 纳米颗粒可能有助于疏水性 PDT 剂的靶向递送,并作为用于化学和光动力双重治疗的潜在纳米载体。

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