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优化从抗性品系(包括非肥胖型糖尿病小鼠)中分离小鼠胚胎干细胞系的方案。

Optimization of protocols for derivation of mouse embryonic stem cell lines from refractory strains, including the non obese diabetic mouse.

机构信息

Sir William Dunn School of Pathology, University of Oxford, Oxford, United Kingdom.

出版信息

Stem Cells Dev. 2012 Jul 1;21(10):1688-700. doi: 10.1089/scd.2011.0427. Epub 2011 Nov 2.

Abstract

The derivation of pluripotent embryonic stem cells (ESCs) from a variety of genetic backgrounds remains a desirable objective in the generation of mice functionally deficient in genes of interest and the modeling of human disease. Nevertheless, disparity in the ease with which different strains of mice yield ESC lines has long been acknowledged. Indeed, the generation of bona fide ESCs from the non obese diabetic (NOD) mouse, a well-characterized model of human type I diabetes, has historically proved especially difficult to achieve. Here, we report the development of protocols for the derivation of novel ESC lines from C57Bl/6 mice based on the combined use of high concentrations of leukemia inhibitory factor and serum-replacement, which is equally applicable to fresh and cryo-preserved embryos. Further, we demonstrate the success of this approach using Balb/K and CBA/Ca mice, widely considered to be refractory strains. CBA/Ca ESCs contributed to the somatic germ layers of chimeras and displayed a very high competence at germline transmission. Importantly, we were able to use the same protocol for the derivation of ESC lines from nonpermissive NOD mice. These ESCs displayed a normal karyotype that was robustly stable during long-term culture, were capable of forming teratomas in vivo and germline competent chimeras after injection into recipient blastocysts. Further, these novel ESC lines efficiently formed embryoid bodies in vitro and could be directed in their differentiation along the dendritic cell lineage, thus illustrating their potential application to the generation of cell types of relevance to the pathogenesis of type I diabetes.

摘要

从各种遗传背景中衍生出多能胚胎干细胞(ESCs)仍然是生成基因功能缺失的感兴趣基因的小鼠模型和模拟人类疾病的理想目标。然而,不同品系的小鼠产生 ESC 系的容易程度存在差异,这一点早已得到公认。事实上,从非肥胖型糖尿病(NOD)小鼠中生成真正的 ESCs,这种小鼠是人类 I 型糖尿病的一种典型模型,历来都难以实现。在这里,我们报告了基于高浓度白血病抑制因子和血清替代物联合使用,从 C57Bl/6 小鼠中衍生新型 ESC 系的方案的开发,该方案同样适用于新鲜和冷冻保存的胚胎。此外,我们使用 Balb/K 和 CBA/Ca 小鼠证明了这种方法的成功,这两种小鼠被广泛认为是难以生成的品系。CBA/Ca ESC 有助于嵌合体的体腔上皮层,并显示出非常高的种系传递能力。重要的是,我们能够使用相同的方案从不允许的 NOD 小鼠中衍生 ESC 系。这些 ESCs 显示出正常的核型,在长期培养中非常稳定,能够在体内形成畸胎瘤,并在注射到受体囊胚后形成具有种系能力的嵌合体。此外,这些新型 ESC 系在体外有效地形成类胚体,并可以沿着树突状细胞谱系指导其分化,从而说明了它们在生成与 I 型糖尿病发病机制相关的细胞类型方面的潜在应用。

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