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小鼠胚胎干细胞的支原体污染会影响细胞参数、种系传递和嵌合后代。

Mycoplasma contamination of murine embryonic stem cells affects cell parameters, germline transmission and chimeric progeny.

作者信息

Markoullis Kyriaki, Bulian Diana, Hölzlwimmer Gabriele, Quintanilla-Martinez Leticia, Heiliger Katrin-Janine, Zitzelsberger Horst, Scherb Hagen, Mysliwietz Josef, Uphoff Cord C, Drexler Hans G, Adler Thure, Busch Dirk H, Schmidt Jörg, Mahabir Esther

机构信息

Department of Comparative Medicine, Helmholtz Center Munich, German Research Center for Environmental Health, Ingolstädter Landstrasse 1, 85764, Neuherberg, Germany.

出版信息

Transgenic Res. 2009 Feb;18(1):71-87. doi: 10.1007/s11248-008-9218-z. Epub 2008 Sep 26.

Abstract

Murine embryonic stem cells (mESCs) inoculated at passage P13 with the mycoplasma species M. hominis, M. fermentans and M. orale and cultured over 20 passages showed reduced growth rate and viability (P < 0.0001) compared to control mESCs. Spectral karyotypic analysis of mycoplasma-infected mESCs showed a number of non-clonal chromosomal aberrations which increased with the duration of infection. The differentiation status of the infected mESCs was most affected at passage P13+6 where the infection was strongest and 46.3% of the mESCs expressed both POU5F1 and SSEA-1 markers whereas 84.8% of control mESCs expressed both markers. The percentage of germline chimeras from mycoplasma-infected mESCs was examined after blastocyst injection and embryo transfer to suitable recipients at different passages and, compared to the respective control group, was most affected at passage P13+5 (50% vs. 90%; P < 0.07). Further reductions were obtained at the same passage in the percentage of litters born (50% vs. 100%; P < 0.07) and in the percentage of pups born (22% vs. 45%; P < 0.001). Thirty three chimeras (39.8%) obtained from blastocyst injection with mycoplasma-infected mESCs showed reduced body weight (P < 0.0001), nasal discharge, osteoarthropathia, and cachexia. Flow cytometric analysis of plasma from chimeras produced with mycoplasma-infected mESCs revealed statistically significant differences in the proportions of T-cells and increased levels of IgG1 (P < 0.001), IgG2a (P < 0.05) and IgM (P < 0.05), anti-DNA antibodies (P < 0.05) and rheumatoid factor (P < 0.01). The present data indicate that mycoplasma contamination of mESCs affects various cell parameters, germline transmission, and postnatal development of the resulting chimeras.

摘要

将第13代(P13)的小鼠胚胎干细胞(mESCs)接种人型支原体、发酵支原体和解脲脲原体,并培养超过20代,结果显示与对照mESCs相比,其生长速率和活力降低(P < 0.0001)。对支原体感染的mESCs进行光谱核型分析,结果显示存在一些非克隆性染色体畸变,且随着感染时间的延长而增加。在感染最强的第13 + 6代时,感染的mESCs的分化状态受影响最大,此时46.3%的mESCs同时表达POU5F1和SSEA - 1标记物,而对照mESCs中有84.8%表达这两种标记物。在不同代次将支原体感染的mESCs注射到囊胚并移植到合适的受体后,检测其种系嵌合体的百分比,与各自的对照组相比,在第13 + 5代时受影响最大(50%对90%;P < 0.07)。在同一代次,出生窝数的百分比(50%对100%;P < 0.07)和出生幼崽的百分比(22%对45%;P < 0.001)进一步降低。从注射支原体感染的mESCs的囊胚中获得的33只嵌合体(39.8%)体重减轻(P < 0.0001),出现鼻分泌物、骨关节病和恶病质。对由支原体感染的mESCs产生的嵌合体的血浆进行流式细胞术分析,结果显示T细胞比例存在统计学显著差异,且IgG1(P < 0.001)、IgG2a(P < 0.05)和IgM(P < 0.05)水平升高,抗DNA抗体(P < 0.05)和类风湿因子(P < 0.01)水平升高。目前的数据表明,mESCs的支原体污染会影响各种细胞参数、种系传递以及所产生嵌合体的产后发育。

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