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A direct comparison of interphase FISH versus low-coverage single cell sequencing to detect aneuploidy reveals respective strengths and weaknesses

机译:直接比较相间FISH和低覆盖率单细胞测序以检测非整倍性揭示了各自的优缺点

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摘要

Aneuploidy has been reported to occur at remarkably high levels in normal somatic tissues using Fluorescence In Situ Hybridization (FISH). Recently, these reports were contradicted by single-cell low-coverage whole genome sequencing (scL-WGS) analyses, which showed aneuploidy frequencies at least an order of magnitude lower. To explain these seemingly contradictory findings, we used both techniques to analyze artificially generated mock aneuploid cells and cells with natural random aneuploidy. Our data indicate that while FISH tended to over-report aneuploidies, a modified 2-probe approach can accurately detect low levels of aneuploidy. Further, scL-WGS tends to underestimate aneuploidy levels, especially in a polyploid background.
机译:据报道,使用荧光原位杂交(FISH)在正常的体细胞组织中非整倍体发生率很高。最近,这些报告与单细胞低覆盖全基因组测序(scL-WGS)分析相矛盾,该分析显示非整倍性频率至少降低了一个数量级。为了解释这些看似矛盾的发现,我们使用了两种技术来分析人工生成的模拟非整倍体细胞和具有自然随机非整倍体的细胞。我们的数据表明,尽管FISH倾向于过度报告非整倍性,但改良的2-探针方法可以准确检测低水平的非整倍性。此外,scL-WGS倾向于低估非整倍性水平,尤其是在多倍体背景下。

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