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Folate receptor-targeted nanoparticle delivery of HuR-RNAi suppresses lung cancer cell proliferation and migration

机译:叶酸受体靶向的HuR-RNAi纳米颗粒传递抑制肺癌细胞的增殖和迁移

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摘要

BackgroundHuman antigen R (HuR) is an RNA binding protein that is overexpressed in many human cancers, including lung cancer, and has been shown to regulate the expression of several oncoproteins. Further, HuR overexpression in cancer cells has been associated with poor-prognosis and therapy resistance. Therefore, we hypothesized that targeted inhibition of HuR in cancer cells should suppress several HuR-regulated oncoproteins resulting in an effective anticancer efficacy. To test our hypothesis, in the present study we investigated the efficacy of folate receptor-α (FRA)-targeted DOTAP:Cholesterol lipid nanoparticles carrying HuR siRNA (HuR-FNP) against human lung cancer cells.
机译:背景人类抗原R(HuR)是一种在许多人类癌症(包括肺癌)中过表达的RNA结合蛋白,并已被证明可调节多种癌蛋白的表达。此外,癌细胞中HuR的过表达与不良预后和治疗抗性有关。因此,我们假设在癌细胞中靶向抑制HuR应该抑制几种HuR调节的癌蛋白,从而产生有效的抗癌功效。为了检验我们的假设,在本研究中,我们研究了以叶酸受体-α(FRA)为靶点的携带HuR siRNA(HuR-FNP)的DOTAP:胆固醇脂质纳米颗粒对人类肺癌细胞的功效。

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