Coating methotrexate-PLGA nanoparticles with folic acid-chitosan conjugate for cancer targeting

Nusaiba Al-Nemrawi, Rowaida Altawabeyeh, Ruba S. Darweesh, Soraya Alnabulsi
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Abstract

Background: Loading Methotrexate, a chemotherapeutic agent, in a nanocarrier can improve its efficacy and lower its side effects. Both PLGA and chitosan were used to formulate Methotrexate nanoparticles. Folate acts as a targeting ligand for anticancer medications. Therefore, folate, chitosan, and PLGA were used to deliver methotrexate. Methods: Folic acid and Chitosan (FA-CS) were conjugated and used to coat Methotrexate-PLGA nanoparticles. The conjugate and the nanoparticles were characterized using Zetasizer to test particle size, polydispersity and charge, SEM was used to test particles’ morphology. Both %EE and %LC of MTX in the NPs were measured. Finally, MTX release and the system cytotoxicity were tested in vitro. Results: FTIR, NMR, and XRD proved the successful formation of FA-CS, and the formation of the coated nanoparticles. The particles were spherical with a size ~385 nm, a disparity ~0.27, and a charge ~+15 mV. The %EE and the % LC were 79% and 21.2%, respectively. In vitro release studies revealed nearly complete MTX release after 48 h. In vitro cytotoxicity testing demonstrated that the formulation components are safe and that the incorporation of MTX within the nanoparticles enhanced the drug’s cytotoxic effect in comparison to the free drug. Conclusion: loading of MTX in the NPs enhances its chemotherapeutic effect, hence, this system can be used to target carcinogenic cells.
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用叶酸-壳聚糖共轭物包覆甲氨蝶呤-PLGA 纳米粒子,实现癌症靶向治疗
背景:在纳米载体中添加甲氨蝶呤这种化疗药物可以提高其疗效并降低其副作用。PLGA和壳聚糖都被用来配制甲氨蝶呤纳米颗粒。叶酸是抗癌药物的靶向配体。因此,我们使用叶酸、壳聚糖和聚乳酸来递送甲氨蝶呤。方法:叶酸和壳聚糖叶酸与壳聚糖(FA-CS)共轭,用于包裹甲氨蝶呤-PLGA 纳米粒子。使用 Zetasizer 对共轭物和纳米颗粒进行表征,以测试粒度、多分散性和电荷;使用 SEM 测试颗粒的形态。还测量了 NPs 中 MTX 的 %EE 和 %LC。最后,在体外测试了 MTX 的释放和系统的细胞毒性。结果傅立叶变换红外光谱(FTIR)、核磁共振成像(NMR)和 X 射线衍射(XRD)证明了 FA-CS 的成功形成以及包覆纳米粒子的形成。颗粒呈球形,大小 ~385 nm,不等度 ~0.27,电荷 ~+15 mV。EE%和 LC%分别为 79% 和 21.2%。体外细胞毒性测试表明,制剂成分是安全的,与游离药物相比,在纳米颗粒中加入 MTX 增强了药物的细胞毒性作用。结论:在纳米粒子中加入 MTX 可增强其化疗效果,因此该系统可用于靶向致癌细胞。
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