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用于生成功能、分子和解剖学回路映射的交叉遗传小鼠模型的 CRISPR 工具包。

A CRISPR toolbox for generating intersectional genetic mouse models for functional, molecular, and anatomical circuit mapping.

机构信息

Department of Neuroscience, Baylor College of Medicine, Houston, TX, USA.

Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, TX, USA.

出版信息

BMC Biol. 2022 Jan 28;20(1):28. doi: 10.1186/s12915-022-01227-0.

Abstract

BACKGROUND

The functional understanding of genetic interaction networks and cellular mechanisms governing health and disease requires the dissection, and multifaceted study, of discrete cell subtypes in developing and adult animal models. Recombinase-driven expression of transgenic effector alleles represents a significant and powerful approach to delineate cell populations for functional, molecular, and anatomical studies. In addition to single recombinase systems, the expression of two recombinases in distinct, but partially overlapping, populations allows for more defined target expression. Although the application of this method is becoming increasingly popular, its experimental implementation has been broadly restricted to manipulations of a limited set of common alleles that are often commercially produced at great expense, with costs and technical challenges associated with production of intersectional mouse lines hindering customized approaches to many researchers. Here, we present a simplified CRISPR toolkit for rapid, inexpensive, and facile intersectional allele production.

RESULTS

Briefly, we produced 7 intersectional mouse lines using a dual recombinase system, one mouse line with a single recombinase system, and three embryonic stem (ES) cell lines that are designed to study the way functional, molecular, and anatomical features relate to each other in building circuits that underlie physiology and behavior. As a proof-of-principle, we applied three of these lines to different neuronal populations for anatomical mapping and functional in vivo investigation of respiratory control. We also generated a mouse line with a single recombinase-responsive allele that controls the expression of the calcium sensor Twitch-2B. This mouse line was applied globally to study the effects of follicle-stimulating hormone (FSH) and luteinizing hormone (LH) on calcium release in the ovarian follicle.

CONCLUSIONS

The lines presented here are representative examples of outcomes possible with the successful application of our genetic toolkit for the facile development of diverse, modifiable animal models. This toolkit will allow labs to create single or dual recombinase effector lines easily for any cell population or subpopulation of interest when paired with the appropriate Cre and FLP recombinase mouse lines or viral vectors. We have made our tools and derivative intersectional mouse and ES cell lines openly available for non-commercial use through publicly curated repositories for plasmid DNA, ES cells, and transgenic mouse lines.

摘要

背景

为了深入了解遗传相互作用网络和调控健康与疾病的细胞机制,需要对发育和成年动物模型中的离散细胞亚型进行剖析和多方面研究。利用重组酶驱动转基因效应等位基因的表达,是对特定细胞群体进行功能、分子和解剖学研究的一种重要而强大的方法。除了单一重组酶系统外,在不同但部分重叠的细胞群体中表达两种重组酶,可以更明确地进行靶向表达。尽管这种方法的应用越来越广泛,但其实验实施在很大程度上仅限于对一组有限的常见等位基因的操作,这些等位基因通常是通过昂贵的商业生产获得的,而交叉小鼠系的生产成本和技术挑战也阻碍了许多研究人员采用定制方法。在这里,我们提出了一个简化的 CRISPR 工具包,用于快速、廉价和方便地产生交叉等位基因。

结果

我们使用双重组酶系统生成了 7 个交叉小鼠系,使用单重组酶系统生成了 1 个小鼠系,还生成了 3 个胚胎干细胞(ES)系,用于研究功能、分子和解剖学特征在构建生理和行为基础的电路中相互关联的方式。作为原理验证,我们将其中的 3 个系应用于不同的神经元群体,进行解剖学图谱绘制,并对呼吸控制的功能进行体内研究。我们还生成了一个具有单一重组酶反应性等位基因的小鼠系,该基因控制钙传感器 Twitch-2B 的表达。该小鼠系被全局应用于研究促卵泡激素(FSH)和促黄体生成素(LH)对卵巢滤泡钙释放的影响。

结论

本文介绍的这些系是成功应用我们的遗传工具包轻松开发多样化、可修饰动物模型的代表性结果。当与合适的 Cre 和 FLP 重组酶小鼠系或病毒载体结合使用时,该工具包将使实验室能够轻松地为任何感兴趣的细胞群体或亚群创建单一或双重重组酶效应系。我们已经将我们的工具和衍生的交叉小鼠和 ES 细胞系通过公开维护的质粒 DNA、ES 细胞和转基因小鼠系公共存储库免费提供给非商业用途。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/18a2/8796356/63e7279d22b7/12915_2022_1227_Fig1_HTML.jpg

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