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Mitotic phase based detection of chromosome segregation errors in embryonic stem cells

机译:基于胚胎干细胞染色体分离误差的有丝分子分子的分子

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The detection of chromosome segregation errors in mitosis is an important area of biological research. Due to the rarity and subtle nature of such errors in untreated cell lines, there is a need for automated, high-throughput systems for quantifying the rates at which such defects occur. This paper presents a novel approach to detecting subtle chromosome segregation errors in mitosis in embryonic stem cells, targeting two cases: misaligned chromosomes in a metaphase cell, and lagging chromosomes between anaphase cells. Our method builds on existing approaches for analysis of other cell lines (e.g. HeLa) which label mitotic phases through mitosis and detect substantial deviations from normal mitotic progression. We apply these to more challenging, denser, stem cell lines. Leveraging the mitotic phase labelling allows us to detect smaller, more subtle defects within mitosis. This results in a very high recall rate, as necessary for detection of such rare events.
机译:有丝分裂中染色体分离误差的检测是生物学研究的重要领域。由于在未处理的细胞系中这种误差的罕见和微妙性质,需要自动化的高通量系统,用于量化这种缺陷的速率。本文提出了一种在胚胎干细胞中检测微妙染色体隔离误差的新方法,靶向两种情况:中期细胞中未对准的染色体,并在后期细胞之间滞后染色体。我们的方法构建了通过丝分裂标记有丝分裂阶段的其他细胞系(例如HELA)的现有方法,并检测与正常有丝分裂进展的大量偏差。我们将这些更具挑战性,更密集,干细胞系。利用有丝分裂相标记使我们能够在有丝分裂中检测更小的更细微的缺陷。这导致非常高的召回率,因为检测这种罕见事件是必要的。

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