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脂肪酸偶联 siRNA 的直接转染及其对前列腺癌细胞葡萄糖调节伴侣蛋白的敲低作用。

Direct Transfection of Fatty Acid Conjugated siRNAs and Knockdown of the Glucose-Regulated Chaperones in Prostate Cancer Cells.

机构信息

Department of Chemistry and Biochemistry , Seton Hall University , South Orange , New Jersey 07079 , United States.

Nitto Denko Avecia Inc. , 8560 Reading Road , Cincinnati , Ohio 45215 , United States.

出版信息

Bioconjug Chem. 2018 Nov 21;29(11):3638-3648. doi: 10.1021/acs.bioconjchem.8b00580. Epub 2018 Oct 10.

Abstract

The emerging field of RNAi nanotechnology has led to rapid advances in the applications of siRNAs in chemical biology, medicinal chemistry, and biotechnology. In our RNAi approach, bioconjugation of linear, V-, and Y-shaped RNA templates were designed using a series of saturated and unsaturated fatty acids to improve cell uptake and knockdown efficacy of the oncogenic glucose regulated proteins (GRPs) in prostate (PC-3) cancer cells. An optimized HCTU-coupling procedure was developed for tagging variable saturated and unsaturated fatty acids onto the 5'-ends of linear and V-shaped RNA templates that were constructed by semiautomated solid phase RNA synthesis. Hybridization and self-assembly of complementary strands yielded linear, V-, and Y-shaped fatty acid-conjugated siRNAs which were characterized by native PAGE. CD spectroscopy confirmed their A-type helix conformations. RP IP HPLC provided trends in amphiphilic properties, whereas DLS and TEM confirmed multicomponent self-assembled structures that were prone to aggregation. Subsequently, the fatty acid conjugated siRNA bioconjugates were tested for their RNAi activity by direct transfection within PC-3 cells known to overexpress oncogenic GRP activity. The siRNA bioconjugates with sense strand modifiers provided more potent GRP knockdown relative to the antisense modified siRNAs, but to a lesser extent when compared to the unconjugated siRNA controls that were transfected with the commercial Trans-IT X2 dynamic delivery system. Flow cytometry revealed that the latter may be at least in part attributed to limited cell uptake of the fatty acid conjugated siRNAs. Nonetheless, these new constructs represent an entry point in modifying higher-order siRNA constructs that may lead to the generation of more efficient siRNA bioconjugates for screening important oncogene targets and for cancer gene therapy applications.

摘要

RNAi 纳米技术这一新兴领域推动了 siRNA 在化学生物学、药物化学和生物技术中的应用的快速发展。在我们的 RNAi 方法中,使用一系列饱和和不饱和脂肪酸设计了线性、V 型和 Y 型 RNA 模板的生物缀合,以提高前列腺(PC-3)癌细胞中致癌葡萄糖调节蛋白(GRP)的细胞摄取和敲低效率。开发了一种优化的 HCTU 偶联程序,用于将可变饱和和不饱和脂肪酸标记到线性和 V 型 RNA 模板的 5'-端,这些模板是通过半自动化固相 RNA 合成构建的。互补链的杂交和自组装产生了线性、V 型和 Y 型脂肪酸缀合的 siRNA,其通过天然 PAGE 进行表征。CD 光谱学证实了它们的 A 型螺旋构象。RP IP HPLC 提供了两亲性质的趋势,而 DLS 和 TEM 证实了易于聚集的多组分自组装结构。随后,通过直接转染在已知过表达致癌 GRP 活性的 PC-3 细胞中测试了脂肪酸缀合的 siRNA 生物缀合物的 RNAi 活性。与反义修饰的 siRNA 相比,具有 sense 链修饰的 siRNA 生物缀合物提供了更强的 GRP 敲低,但与用商业 Trans-IT X2 动态传递系统转染的未缀合 siRNA 对照相比,其效果要差一些。流式细胞术显示,这可能至少部分归因于脂肪酸缀合的 siRNA 的细胞摄取有限。尽管如此,这些新结构代表了修饰更高阶 siRNA 结构的切入点,这可能会产生更有效的 siRNA 生物缀合物,用于筛选重要的致癌基因靶标和癌症基因治疗应用。

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