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支化和超支化 siRNA 的固相合成、表征和 RNAi 活性。

Solid-phase synthesis, characterization and RNAi activity of branch and hyperbranch siRNAs.

机构信息

Department of Chemistry and Biochemistry, Seton Hall University, South Orange, NJ 07079, USA.

出版信息

Bioorg Med Chem Lett. 2013 Oct 1;23(19):5270-4. doi: 10.1016/j.bmcl.2013.08.033. Epub 2013 Aug 12.

Abstract

Linear, branch and hyperbranch siRNAs were effectively prepared for down-regulating GRP78 expression and inducing cell death in HepG2 liver cancer cells. Branch and hyperbranch GRP78 siRNAs were synthesized by automated solid-phase synthesis in good yields (44-78%) and isolated in excellent purities (>99%) following HPLC purification. Moreover, siRNAs adopted stable intramolecular hybrids as discerned by native PAGE and thermal denaturation studies. These sequences also exhibited the pre-requisite A-type helical trajectory for triggering RNAi activity as determined by CD spectroscopy. Biological studies confirmed potent suppression of GRP78 expression (50-60%) while compromising cancer cell viability by ~20%. Thus, branch and hyperbranch siRNAs may serve as potent siRNA candidates in cancer gene therapy applications.

摘要

线性、分支和超分支 siRNA 被有效地制备用于下调 GRP78 表达并诱导 HepG2 肝癌细胞死亡。分支和超分支 GRP78 siRNA 通过自动固相合成以高产率(44-78%)合成,并在 HPLC 纯化后以优异的纯度(>99%)分离。此外,siRNA 通过天然 PAGE 和热变性研究识别为稳定的分子内杂交体。这些序列还通过 CD 光谱学确定了触发 RNAi 活性所必需的 A 型螺旋轨迹。生物学研究证实,这些序列能有效抑制 GRP78 表达(50-60%),同时使癌细胞活力降低约 20%。因此,分支和超分支 siRNA 可能成为癌症基因治疗应用中的有效 siRNA 候选物。

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