Institute of Human Genetics, University Hospital, Otto von Guericke University Magdeburg, Magdeburg, Germany.
Gynecology and Obstetrics Clinic, GAK Narodni front, Belgrade, Serbia.
J Histochem Cytochem. 2020 Apr;68(4):239-251. doi: 10.1369/0022155420910113. Epub 2020 Feb 28.
To preserve material for future genetic studies, human B-lymphocytes from whole blood samples are routinely transformed into lymphoblastoid cell lines (LCLs) by in vitro infection with Epstein-Barr virus. To determine the rate and frequency of chromosomal changes during long-term culture, we established 10 LCLs (from eight individuals). Before transformation, these cases showed a normal karyotype (three cases), a small supernumerary marker chromosome (three cases), or an aberrant karyotype (four cases). Chromosome analyses were performed at 8-week intervals over a period of at least 1 year, up to 3 years. Surprisingly, we demonstrate that chromosomal instability is the rule, rather than the exception, during long-term culture of LCLs. The most commonly observed acquired clonal aberration was trisomy 12, which emerged in all cell lines within 21 to 49 weeks after infection. Telomeric fusions indicating telomere shortening were found after ~21 weeks. After 1 year of cultivation, the proportion of cells with the original karyotype decreased to ≤10% in 7 of the 10 cell lines. To preserve cells with aberrant genomes, we conclude the cultivation time of LCLs must be restricted to the absolute minimum time required.
为了保存未来进行遗传研究的材料,通常通过体外感染 Epstein-Barr 病毒将全血样本中的人 B 淋巴细胞转化为淋巴母细胞系 (LCL)。为了确定长期培养过程中染色体变化的速度和频率,我们建立了 10 个 LCL(来自 8 个人)。在转化之前,这些病例显示正常核型(3 例)、小额外标记染色体(3 例)或异常核型(4 例)。在至少 1 年、长达 3 年的时间内,每 8 周进行一次染色体分析。令人惊讶的是,我们证明染色体不稳定性是 LCL 长期培养中的常规现象,而不是例外。最常观察到的获得性克隆异常是 12 三体,它在感染后 21 至 49 周内在所有细胞系中出现。在大约 21 周后,发现了表明端粒缩短的端粒融合。培养 1 年后,在 10 个细胞系中的 7 个中,具有原始核型的细胞比例降至≤10%。为了保存具有异常基因组的细胞,我们得出结论,必须将 LCL 的培养时间限制在绝对最小的所需时间内。
