4.7 Article

Major changes of cell function and toxicant sensitivity in cultured cells undergoing mild, quasi-natural genetic drift

期刊

ARCHIVES OF TOXICOLOGY
卷 92, 期 12, 页码 3487-3503

出版社

SPRINGER HEIDELBERG
DOI: 10.1007/s00204-018-2326-5

关键词

Human genome; Cell stability; Dopamine transporter; genome comparison; genotype-phenotype correlation

资金

  1. Luxembourg government through the plan Technologies de la Sante
  2. National Centre of Excellence in Research on Parkinson's disease (NCER-PD) grant from the FNR
  3. Land Baden Wurttemberg
  4. German Federal Ministry of Education and Research (BMBF)
  5. EU-ToxRisk

向作者/读者索取更多资源

Genomic drift affects the functional properties of cell lines, and the reproducibility of data from in vitro studies. While chromosomal aberrations and mutations in single pivotal genes are well explored, little is known about effects of minor, possibly pleiotropic, genome changes. We addressed this question for the human dopaminergic neuronal precursor cell line LUHMES by comparing two subpopulations (SP) maintained either at the American-Type-Culture-Collection (ATCC) or by the original provider (UKN). Drastic differences in susceptibility towards the specific dopaminergic toxicant 1-methyl-4-phenylpyridinium (MPP+) were observed. Whole-genome sequencing was performed to identify underlying genetic differences. While both SP had normal chromosome structures, they displayed about 70 differences on the level of amino acid changing events. Some of these differences were confirmed biochemically, but none offered a direct explanation for the altered toxicant sensitivity pattern. As second approach, markers known to be relevant for the intended use of the cells were specifically tested. The ATCC cells rapidly down-regulated the dopamine-transporter and tyrosine-hydroxylase after differentiation, while UKN cells maintained functional levels. As the respective genes were not altered themselves, we conclude that polygenic complex upstream changes can have drastic effects on biochemical features and toxicological responses of relatively similar SP of cells.

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