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首页> 外文期刊>Archives of pharmacal research >Long chain microRNA conjugates in calcium phosphate nanoparticles for efficient formulation and delivery
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Long chain microRNA conjugates in calcium phosphate nanoparticles for efficient formulation and delivery

机译:磷酸钙纳米颗粒中的长链microRNA缀合物可有效配制和输送

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摘要

A long chain microRNA-34a conjugate (lc-miRNA) was prepared by chemical crosslinking in order to improve entrapment efficiency into calcium phosphate nanoparticles (CaPs) and intracellular delivery. Thiol-modified miRNA at both terminal ends was chemically conjugated using crosslinkers to form lc-miRNA which was encapsulated within CaPs by a conventional coprecipitation method. Encapsulation efficiencies, physicochemical properties, and in vitro intracellular delivery efficiencies of the prepared linear polyethyleneimine (LPEI)-coated CaPs (LPEI-CaP) containing common miRNA and lc-miRNA were comparatively evaluated. The prepared lc-miRNA exhibited noticeably enhanced encapsulation efficiency during the CaP formulation process when compared to common miRNA. LPEI-CaP/lc-miRNAs consisted of nano-sized particles with great homogeneity and were observed to be successfully delivered into PC-3 cells. Fabricated LPEI-CaPs with duplex form of lc-miRNA (lc-miRNA-d) suppressed cancer cell proliferation as well as migration much more efficiently than those with duplex form of miRNA (miRNA-d). In addition, LPEICaP/lc-miRNA-d conferred negligible cytotoxicity on PC-3 cells. Chemical crosslinking of therapeutic miRNAs via a reducible linkage may allow more efficient encapsulation within CaPs as well as homogeneous particle formulation due to a higher spatial charge density than common miRNAs. The well-formulated LPEI-CaPs with lc-miRNA-d have the potential to provide superior miRNA transfection efficiency and inhibition of cancer proliferation.
机译:通过化学交联制备长链microRNA-34a共轭物(lc-miRNA),以提高磷酸钙纳米颗粒(CaPs)的包封效率和细胞内传递。使用交联剂化学偶联两个末端的巯基修饰的miRNA,形成lc-miRNA,然后通过常规共沉淀方法将其包裹在CaP中。比较评估了包含常见miRNA和lc-miRNA的线性聚乙烯亚胺(LPEI)涂层的CaP(LPEI-CaP)的封装效率,理化性质和体外细胞内传递效率。与普通miRNA相比,制备的lc-miRNA在CaP配制过程中表现出明显增强的封装效率。 LPEI-CaP / lc-miRNA由具有极大同质性的纳米级颗粒组成,并被观察到已成功递送到PC-3细胞中。与双链形式的miRNA(miRNA-d)相比,双链形式的lc-miRNA(lc-miRNA-d)制造的LPEI-CaP抑制癌细胞增殖以及迁移效率更高。此外,LPEICaP / lc-miRNA-d对PC-3细胞的细胞毒性可忽略不计。由于与常见miRNA相比具有更高的空间电荷密度,治疗性miRNA经由可还原键的化学交联可使其在CaPs内更有效地包裹,并形成均质颗粒。具有lc-miRNA-d的结构良好的LPEI-CaP具有提供卓越的miRNA转染效率和抑制癌症增殖的潜力。

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