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首页> 外文期刊>Methods: A Companion to Methods in Enzymology >Identifying HIV-1 host cell factors by genome-scale RNAi screening.
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Identifying HIV-1 host cell factors by genome-scale RNAi screening.

机译:通过基因组规模的RNAi筛选鉴定HIV-1宿主细胞因子。

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摘要

Advances in the application of RNA interference (RNAi) have facilitated the establishment of systematic cell-based loss-of-function screening platforms. Widespread implementation of this technology has enabled genome-wide genetic analysis of a diverse array of cellular phenotypes, including the identification of host cell factors involved in viral replication. Four recent studies employed whole-genome RNAi technologies to elucidate cellular genes important for the replication of HIV-1. While these four genome-scale screens shared a common objective, they differ in their scope and experimental design. In this review we explore alternative strategies for developing RNAi screens, and discuss potential pitfalls of the technology. Important technical considerations include the choice of silencing reagents, experimental systems, assay readout and analysis methods. We focus on experimental and computational parameters that can impact the outcome of high-throughput genetic screens, and provide guidelines for the development of reliable cell-based RNAi screens.
机译:RNA干扰(RNAi)应用的进展促进了系统的基于细胞功能丧失的筛选平台的建立。这项技术的广泛实施使得能够对多种细胞表型进行全基因组遗传分析,包括鉴定参与病毒复制的宿主细胞因子。最近的四项研究采用了全基因组RNAi技术来阐明对于HIV-1复制非常重要的细胞基因。尽管这四个基因组规模的筛选具有相同的目标,但它们的范围和实验设计不同。在这篇综述中,我们探索了开发RNAi筛查的替代策略,并讨论了该技术的潜在陷阱。重要的技术考虑因素包括选择沉默试剂,实验系统,测定读数和分析方法。我们专注于可能影响高通量遗传筛选结果的实验​​和计算参数,并为开发可靠的基于细胞的RNAi筛选提供指导。

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