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Jurkat T细胞系表现出明显的基因组不稳定,影响核型、突变谱、基因表达、免疫表型和功能。

Jurkat T-cell lines exhibit marked genomic instability affecting karyotype, mutational profile, gene expression, immunophenotype and function.

作者信息

Wilson Andrew, Dasyam Nathaniel, O'Hagan Felix, Farrell Dianna, Turner Claire, Jay Anne, Schmidt Alfonso, Beddow Rachel, Lillis Tina, Chin Tom, Perret Rachel, McCulley Michelle, Weinkove Robert

机构信息

Department of Pathology and Molecular Medicine, University of Otago Wellington, Wellington, New Zealand.

Cancer Immunotherapy Programme, Malaghan Institute of Medical Research, Wellington, New Zealand.

出版信息

Sci Rep. 2025 Jul 1;15(1):22426. doi: 10.1038/s41598-025-95903-0.

Abstract

The Jurkat cell line, derived from a case of T-cell lymphoblastic leukaemia, is widely employed as a model T-cell for biomedical research, including for the preclinical characterisation of cellular therapies such as chimeric antigen receptor T-cells. Here, we characterised genomic, transcriptomic, and functional features of Jurkat clone E6-1 cells from three different laboratories and compared these with Jurkat E6-1 cells from the American Type Culture Collection (ATCC). We identified marked karyotypic heterogeneity both between and within Jurkat E6-1 populations, confirmed through chromosomal microarray. Whole exome sequencing of each cell population revealed both shared and unique mutational profiles, and transcriptomic profiles varied markedly between Jurkat E6-1 cell populations. Finally, the Jurkat E6-1 cell populations exhibited substantial variations in immunophenotype and cytokine production, which were consistent with the genotypic and transcriptomic changes observed. In summary, we identify substantial genomic heterogeneity both between and within Jurkat E6-1 cell populations, highlighting the genomic instability of this line. These genomic changes were associated with differences in protein expression and cytokine production that may affect functional assays. Our findings highlight the importance of monitoring cell passage number, characterising cell lines, and replacing cell line stocks to assure the accuracy, reproducibility, and translatability of assays employing Jurkat E6-1 cells.

摘要

Jurkat细胞系源自一例T细胞淋巴母细胞白血病,被广泛用作生物医学研究的T细胞模型,包括用于嵌合抗原受体T细胞等细胞疗法的临床前特征分析。在此,我们对来自三个不同实验室的Jurkat克隆E6-1细胞的基因组、转录组和功能特征进行了表征,并将这些特征与美国典型培养物保藏中心(ATCC)的Jurkat E6-1细胞进行了比较。我们通过染色体微阵列证实,在Jurkat E6-1群体之间以及群体内部均存在明显的核型异质性。对每个细胞群体进行全外显子组测序揭示了共同的和独特的突变谱,并且Jurkat E6-1细胞群体之间的转录组谱差异显著。最后,Jurkat E6-1细胞群体在免疫表型和细胞因子产生方面表现出显著差异,这与观察到的基因型和转录组变化一致。总之,我们发现Jurkat E6-1细胞群体之间以及群体内部均存在显著的基因组异质性,突出了该细胞系的基因组不稳定性。这些基因组变化与蛋白质表达和细胞因子产生的差异相关,可能会影响功能分析。我们的研究结果强调了监测细胞传代次数、表征细胞系以及更换细胞系储备以确保使用Jurkat E6-1细胞的分析的准确性、可重复性和可转化性的重要性。

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