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一种稳定表达tau-绿色荧光蛋白的新型恒河猴胚胎干细胞系的衍生与克隆。

Derivation and cloning of a novel rhesus embryonic stem cell line stably expressing tau-green fluorescent protein.

作者信息

Wianny Florence, Bernat Agnieszka, Huissoud Cyril, Marcy Guillaume, Markossian Suzy, Cortay Véronique, Giroud Pascale, Leviel Vincent, Kennedy Henry, Savatier Pierre, Dehay Colette

机构信息

Institut National de la Santé et de la Recherche Médicale, U846 Stem Cell and Brain Research Institute, Bron, France.

出版信息

Stem Cells. 2008 Jun;26(6):1444-53. doi: 10.1634/stemcells.2007-0953. Epub 2008 Mar 20.

Abstract

Embryonic stem cells (ESC) have the ability of indefinite self-renewal and multilineage differentiation, and they carry great potential in cell-based therapies. The rhesus macaque is the most relevant preclinical model for assessing the benefit, safety, and efficacy of ESC-based transplantations in the treatment of neurodegenerative diseases. In the case of neural cell grafting, tracing both the neurons and their axonal projections in vivo is essential for studying the integration of the grafted cells in the host brain. Tau-Green fluorescent protein (tau-GFP) is a powerful viable lineage tracer, allowing visualization of cell bodies, dendrites, and axons in exquisite detail. Here, we report the first rhesus monkey ESC line that ubiquitously and stably expresses tau-GFP. First, we derived a new line of rhesus monkey ESC (LYON-ES1) that show marker expression and cell cycle characteristics typical of primate ESCs. LYON-ES1 cells are pluripotent, giving rise to derivatives of the three germ layers in vitro and in vivo through teratoma formation. They retain all their undifferentiated characteristics and a normal karyotype after prolonged culture. Using lentiviral infection, we then generated a monkey ESC line stably expressing tau-GFP that retains all the characteristics of the parental wild-type line and is clonogenic. We show that neural precursors derived from the tau-GFP ESC line are multipotent and that their fate can be precisely mapped in vivo after grafting in the adult rat brain. Disclosure of potential conflicts of interest is found at the end of this article.

摘要

胚胎干细胞(ESC)具有无限自我更新和多谱系分化的能力,在基于细胞的治疗中具有巨大潜力。恒河猴是评估基于ESC的移植治疗神经退行性疾病的益处、安全性和疗效的最相关临床前模型。在神经细胞移植的情况下,在体内追踪神经元及其轴突投射对于研究移植细胞在宿主脑中的整合至关重要。Tau-绿色荧光蛋白(tau-GFP)是一种强大的活细胞谱系示踪剂,能够极其详细地可视化细胞体、树突和轴突。在此,我们报告了首个普遍且稳定表达tau-GFP的恒河猴ESC系。首先,我们获得了一个新的恒河猴ESC系(LYON-ES1),其表现出灵长类ESC典型的标志物表达和细胞周期特征。LYON-ES1细胞具有多能性,通过畸胎瘤形成在体外和体内产生三个胚层的衍生物。经过长时间培养后,它们保留了所有未分化特征和正常核型。然后,通过慢病毒感染,我们生成了一个稳定表达tau-GFP的猴ESC系,该系保留了亲本野生型系的所有特征且具有克隆性。我们表明,源自tau-GFP ESC系的神经前体细胞具有多能性,并且在移植到成年大鼠脑内后,其命运能够在体内被精确追踪。潜在利益冲突的披露见本文末尾。

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