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利用 CRISPR/Cas9 系统来理解神经肽生物学和调控。

Using the CRISPR/Cas9 system to understand neuropeptide biology and regulation.

机构信息

University of Aberdeen, Scotland.

University of Aberdeen, Scotland.

出版信息

Neuropeptides. 2017 Aug;64:19-25. doi: 10.1016/j.npep.2016.11.010. Epub 2016 Dec 3.

Abstract

Neuropeptides and their receptors play a role in physiological responses such as appetite, stress and inflammatory pain. With neuropeptides having such diverse and important physiological roles, knocking-out the genes encoding them, their receptors, parts of their regulatory sequences, or reproducing disease associated polymorphic variants are important steps in studying neuropeptides and how they may contribute to disease. Previously, knock-outs were generated using methods such as targeted homologous recombination in embryonic stem cells but this method is costly and time-consuming. The CRISPR/Cas9 system has rapidly taken over the genome editing field and will advance our understanding of neuropeptide genes and their regulation. With CRISPR/Cas9 technology, the time and costs involved in producing transgenic animal models, is greatly reduced. In this review, we describe how the system can be used to manipulate genomic sequences by "knock-out" or "knock-in" mutations in cell lines or in animal models. We also discuss the specificity of the system and methods to limit off-target effects. When combined with the availability of genome sequences, CRISPR/Cas9 directed genome editing in vitro and in vivo, promises to provide a deeper understanding of the biology of the neuropeptides in health and disease than has ever been available before.

摘要

神经肽及其受体在生理反应中发挥作用,如食欲、应激和炎性疼痛。由于神经肽具有如此多样和重要的生理作用,敲除编码它们的基因、其受体、其调节序列的一部分或复制与疾病相关的多态性变体,是研究神经肽及其如何可能导致疾病的重要步骤。以前,通过胚胎干细胞中的靶向同源重组等方法生成敲除,但这种方法成本高且耗时。CRISPR/Cas9 系统已迅速接管基因组编辑领域,并将推进我们对神经肽基因及其调控的理解。使用 CRISPR/Cas9 技术,可大大减少产生转基因动物模型所涉及的时间和成本。在这篇综述中,我们描述了如何通过细胞系或动物模型中的“敲除”或“敲入”突变来操纵基因组序列。我们还讨论了该系统的特异性和限制脱靶效应的方法。当与基因组序列的可用性相结合时,CRISPR/Cas9 指导的体外和体内基因组编辑有望提供比以往任何时候都更深入的了解神经肽在健康和疾病中的生物学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8aca/5645574/dd1f8be1693f/gr1.jpg

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