A comparative survey of the influence of small self-cleaving ribozymes on gene expression in human cell culture.

IF 3.6 3区 生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY RNA Biology Pub Date : 2024-01-01 Epub Date: 2023-12-25 DOI:10.1080/15476286.2023.2296203
Dennis Kläge, Elisabeth Müller, Jörg S Hartig
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Abstract

Self-cleaving ribozymes are versatile tools for synthetic biologists when it comes to controlling gene expression. Up to date, 12 different classes are known, and over the past decades more and more details about their structure, cleavage mechanisms and natural environments have been uncovered. However, when these motifs are applied to mammalian gene expression constructs, the outcome can often be unexpected. A variety of factors, such as surrounding sequences and positioning of the ribozyme influences the activity and hence performance of catalytic RNAs. While some information about the efficiency of individual ribozymes (each tested in specific contexts) is known, general trends obtained from standardized, comparable experiments are lacking, complicating decisions such as which ribozyme to choose and where to insert it into the target mRNA. In many cases, application-specific optimization is required, which can be very laborious. Here, we systematically compared different classes of ribozymes within the 3'-UTR of a given reporter gene. We then examined position-dependent effects of the best-performing ribozymes. Moreover, we tested additional variants of already widely used hammerhead ribozymes originating from various organisms. We were able to identify functional structures suited for aptazyme design and generated highly efficient hammerhead ribozyme variants originating from the human genome. The present dataset will aide decisions about how to apply ribozymes for affecting gene expression as well as for developing ribozyme-based switches for controlling gene expression in human cells.

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小型自裂解核酶对人类细胞培养中基因表达影响的比较研究。
自裂解核糖酶是合成生物学家控制基因表达的多功能工具。迄今为止,已知的自裂解核糖酶有 12 个不同的类别,在过去的几十年里,人们发现了越来越多有关其结构、裂解机制和自然环境的细节。然而,当这些基元应用于哺乳动物基因表达构建体时,结果往往出人意料。核糖酶的周围序列和定位等多种因素会影响催化 RNA 的活性,进而影响其性能。虽然人们知道一些有关单个核糖酶效率的信息(每种核糖酶都在特定情况下进行过测试),但缺乏从标准化、可比性实验中获得的总体趋势,这使得选择哪种核糖酶以及将其插入目标 mRNA 的位置等决策变得更加复杂。在许多情况下,需要针对具体应用进行优化,这可能非常费力。在这里,我们系统地比较了特定报告基因 3'-UTR 内不同类别的核糖酶。然后,我们研究了表现最好的核糖酶的位置依赖效应。此外,我们还测试了源于各种生物的、已被广泛使用的锤头核糖酶的其他变体。我们确定了适合设计肽酶的功能结构,并生成了源自人类基因组的高效锤头核糖酶变体。本数据集将有助于决定如何应用核糖酶来影响基因表达,以及开发基于核糖酶的开关来控制人类细胞中的基因表达。
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来源期刊
RNA Biology
RNA Biology 生物-生化与分子生物学
CiteScore
8.60
自引率
0.00%
发文量
82
审稿时长
1 months
期刊介绍: RNA has played a central role in all cellular processes since the beginning of life: decoding the genome, regulating gene expression, mediating molecular interactions, catalyzing chemical reactions. RNA Biology, as a leading journal in the field, provides a platform for presenting and discussing cutting-edge RNA research. RNA Biology brings together a multidisciplinary community of scientists working in the areas of: Transcription and splicing Post-transcriptional regulation of gene expression Non-coding RNAs RNA localization Translation and catalysis by RNA Structural biology Bioinformatics RNA in disease and therapy
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