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用于高通量组合式小干扰RNA筛选的单细胞编码基因沉默

Single-cell encoded gene silencing for high-throughput combinatorial siRNA screening.

作者信息

Guo Feng, Ji Xianglin, Xiong Chuxiao, Sun Hailiang, Liang Zhenghua, Yan-Do Richard, Gai Baowen, Gao Feng, Huang Linfeng, Li Zhongping, Kuang Becki Yi, Shi Peng

机构信息

Department of Biomedical Engineering, City University of Hong Kong, Kowloon, Hong Kong SAR, 999077, China.

Hong Kong Centre for Cerebro-Cardiovascular Health Engineering, Hong Kong Science Park, Hong Kong SAR, 999077, China.

出版信息

Nat Commun. 2024 Nov 19;15(1):9985. doi: 10.1038/s41467-024-53419-7.

Abstract

The use of combinatorial siRNAs shows great promise for drug discovery, but the identification of safe and effective siRNA combinations remains challenging. Here, we develop a massively multiplexed technology for systematic screening of siRNA-based cocktail therapeutics. We employ composite micro-carriers that are responsive to near infrared light and magnetic field to achieve photoporation-facilitated siRNA transfection to individual cells. Thus, randomized gene silencing by different siRNA formulations can be performed with high-throughput single-cell-based analyses. For screening anti-cancer siRNA cocktails, we test more than 1300 siRNA combinations for knocking down multiple genes related to tumor growth, discovering effective 3-siRNA formulations with an emphasis on the critical role of inhibiting Cyclin D1 and survivin, along with their complementary targets for synergic efficacy. This approach enables orders of magnitude reduction in time and cost associated with largescale siRNA screening, and resolves key insights to siRNA pharmacology that are not permissive to existing methods.

摘要

组合式小干扰RNA(siRNA)的应用在药物研发方面显示出巨大潜力,但识别安全有效的siRNA组合仍然具有挑战性。在此,我们开发了一种大规模多重技术,用于基于siRNA的鸡尾酒疗法的系统筛选。我们采用对近红外光和磁场有响应的复合微载体,以实现光穿孔促进的siRNA对单个细胞的转染。因此,通过基于高通量单细胞分析,可以进行不同siRNA配方的随机基因沉默。为了筛选抗癌siRNA鸡尾酒,我们测试了1300多种siRNA组合,以敲除多个与肿瘤生长相关的基因,发现了有效的三siRNA配方,重点关注抑制细胞周期蛋白D1和生存素的关键作用,以及它们的互补靶点以实现协同疗效。这种方法能够将大规模siRNA筛选相关的时间和成本降低几个数量级,并解决了现有方法无法获得的siRNA药理学关键见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bcfb/11576956/bb707fe9c5fa/41467_2024_53419_Fig1_HTML.jpg

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