Diverse Cre recombinase expression pattern in Albumin-Cre driver rats.

IF 1.2 4区 农林科学 Q1 VETERINARY SCIENCES Experimental Animals Pub Date : 2025-07-11 Epub Date: 2025-01-22 DOI:10.1538/expanim.24-0174
Saeko Ishida, Keiko Taguchi, Ryuya Iida, Kosuke Hattori, Hiroaki Taketsuru, Kazuto Yoshimi, Masayuki Yamamoto, Tomoji Mashimo
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Abstract

Rats (Rattus norvegicus) have been widely utilized as model animals due to their physiological characteristics, making them suitable for surgical and long-term studies. They have played a crucial role in biomedical research, complementing studies conducted in mice. The advent of genome editing technologies has facilitated the generation of genetically modified rat strains, advancing studies in experimental animals. Among these innovations, Cre-driver rat models have emerged as powerful tools for spatiotemporal control of gene expression. However, their development and characterization remain less advanced compared to mouse models. In this study, we developed liver-targeting Cre knock-in rats and reporter knock-in rats to evaluate Cre recombinase expression profiles in different genetic contexts. Our results revealed that insertion orientation and promoter origin significantly influence Cre expression patterns. Notably, forward insertion of the Albumin (Alb) promoter-driven Cre sequence at the ROSA26 locus resulted in ubiquitous Cre expression, while reverse insertion confined Cre expression predominantly to the liver. Interestingly, Cre expression under an endogenous Alb promoter unexpectedly induced expression in non-liver tissues, which may suggest a potential link to the in vivo dynamics of albumin. These findings underscore the importance of rigorous characterization in Cre-based transgenic systems. By elucidating the roles of promoter origin, insertion site, and orientation, our study provides valuable insights for optimizing Cre-driver rat models. These findings pave the way for refining genetic strategies to enhance tissue specificity and reliability in functional genomics and disease modeling.

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白蛋白驱动大鼠不同Cre重组酶表达模式。
大鼠(Rattus norvegicus)由于其生理特性被广泛用作模型动物,适合外科和长期研究。它们在生物医学研究中发挥了至关重要的作用,补充了在老鼠身上进行的研究。基因组编辑技术的出现促进了转基因大鼠品系的产生,推进了实验动物的研究。在这些创新中,cre驱动大鼠模型已经成为基因表达时空控制的有力工具。然而,与小鼠模型相比,它们的发展和表征仍然不够先进。在这项研究中,我们开发了肝脏靶向Cre敲入大鼠和报告基因敲入大鼠,以评估不同遗传背景下Cre重组酶的表达谱。我们的研究结果表明,插入方向和启动子起源显著影响Cre的表达模式。值得注意的是,白蛋白(Alb)启动子驱动的Cre序列在ROSA26位点的正向插入导致Cre普遍表达,而反向插入将Cre表达主要限制在肝脏。有趣的是,内源性白蛋白启动子下的Cre表达意外地诱导了非肝组织中的表达,这可能表明与白蛋白的体内动态有关。这些发现强调了在基于cre的转基因系统中严格表征的重要性。通过阐明启动子起源、插入位点和方向的作用,我们的研究为优化cre驱动大鼠模型提供了有价值的见解。这些发现为改进遗传策略以增强功能基因组学和疾病建模中的组织特异性和可靠性铺平了道路。
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来源期刊
Experimental Animals
Experimental Animals 生物-动物学
CiteScore
2.80
自引率
4.20%
发文量
2
审稿时长
3 months
期刊介绍: The aim of this international journal is to accelerate progress in laboratory animal experimentation and disseminate relevant information in related areas through publication of peer reviewed Original papers and Review articles. The journal covers basic to applied biomedical research centering around use of experimental animals and also covers topics related to experimental animals such as technology, management, and animal welfare.
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