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在分子诊断时代,挤压核流区域应作为肿瘤成分纳入考量。

Areas of Crush Nuclear Streaming Should Be Included as Tumor Content in the Era of Molecular Diagnostics.

作者信息

Noda Yuri, Yamaka Ryosuke, Atsumi Naho, Higasa Koichiro, Tsuta Koji

机构信息

Department of Pathology, Kansai Medical University, 2-5-1 Shin-machi, Hirakata 573-1010, Osaka, Japan.

Department of Pathology and Laboratory Medicine, Kansai Medical University Hospital, 2-3-1 Shin-machi, Hirakata 573-1191, Osaka, Japan.

出版信息

Cancers (Basel). 2023 Mar 22;15(6):1910. doi: 10.3390/cancers15061910.

Abstract

Degenerated tissues are frequently observed in malignant tumors, but are not analyzed. We investigated whether nuclear streaming and necrosis samples could be used for genetic analysis to expand the sample pool. A total of 81 samples were extracted from small cell carcinoma and lymphoma FFPE tissue blocks and classified into three histological cohorts: 33 materials with well-preserved tumor morphology, 31 nuclear streaming samples, and 17 necrosis samples. DNA and RNA integrity numbers, percentage of RNA fragments with >200 nucleotides, and next-generation sequencing quality metrics were compared among the cohorts. DNA quality did not significantly differ between nuclear streaming materials and materials with well-preserved morphology, whereas that of the necrosis samples was inferior. RNA quality decreased in the following order: materials with well-preserved morphology > nuclear streaming > necrosis. The sequencing metrics did not differ significantly between the nuclear streaming samples and materials with well-preserved morphology, and reliable variants were detected. The necrosis samples extracted from resections exhibited sequencing failure and showed significantly fewer on-target aligned reads and variants. However, variant allele frequency did not differ among the cohorts. We revelated that DNA in nuclear streaming samples, especially within biopsies, could be used for genetic analysis. Moreover, degenerated non-tumor cells should be counted when evaluating tumor content to avoid misinterpreting the variant allele frequency.

摘要

在恶性肿瘤中经常观察到退化组织,但未对其进行分析。我们研究了核流和坏死样本是否可用于基因分析以扩大样本库。从小细胞癌和淋巴瘤的福尔马林固定石蜡包埋(FFPE)组织块中总共提取了81个样本,并将其分为三个组织学队列:33个肿瘤形态保存良好的样本、31个核流样本和17个坏死样本。比较了各队列之间的DNA和RNA完整性数值、大于200个核苷酸的RNA片段百分比以及二代测序质量指标。核流样本与形态保存良好的样本之间的DNA质量无显著差异,而坏死样本的DNA质量较差。RNA质量按以下顺序降低:形态保存良好的样本>核流样本>坏死样本。核流样本与形态保存良好的样本之间的测序指标无显著差异,且检测到了可靠的变异。从切除组织中提取的坏死样本出现测序失败,且靶向比对读数和变异显著减少。然而,各队列之间的变异等位基因频率并无差异。我们发现核流样本中的DNA,尤其是活检样本中的DNA,可用于基因分析。此外,在评估肿瘤含量时应将退化的非肿瘤细胞计算在内,以避免误判变异等位基因频率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8d65/10099727/50866bd8b13d/cancers-15-01910-g001.jpg

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