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Detection of TP53 and PIK3CA Mutations in Circulating Tumor DNA Using Next-Generation Sequencing in the Screening Process for Early Breast Cancer Diagnosis

机译:在早期乳腺癌诊断筛选过程中使用新一代测序技术检测循环肿瘤DNA中TP53和PIK3CA突变。

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摘要

Circulating tumor DNA (ctDNA) has emerged as a non-invasive “liquid biopsy” for early breast cancer diagnosis. We evaluated the suitability of ctDNA analysis in the diagnosis of early breast cancer after mammography findings, comparing PIK3CA and TP53 mutations between tumor biopsies and pre-biopsy circulating DNA. Matched plasma and frozen fresh tissue biopsies from patients with Breast Imaging-Reporting and Data System (BIRADS) 4c/5 mammography findings and subsequent diagnosis of primary breast cancer were analyzed using NGS TruSeq Custom Amplicon Low Input Panel (Illumina) and plasma SafeSEQ (Sysmex Inostics). The same plasma and tumor mutations were observed in eight of 29 patients (27.6%) with four in TP53 and five in PIK3CA mutations. Sequencing analysis also revealed four additional ctDNA mutations (three in TP53 and one in PIK3CA) previously not identified in three patients tissue biopsy. One of these patients had mutations in both genes. Age, tumor grade and size, immunohistochemical (IHC) subtype, BIRADS category, and lymph node positivity were significantly associated with the detectability of these blood tumor-derived mutations. In conclusion, ctDNA analysis could be used in early breast cancer diagnosis, providing critical clinical information to improve patient diagnosis.
机译:循环肿瘤DNA(ctDNA)已成为一种早期乳腺癌诊断的非侵入性“液体活检”方法。我们评估了ctDNA分析在乳房X线检查后发现的早期乳腺癌诊断中的适用性,比较了肿瘤活检和活检前循环DNA之间的PIK3CA和TP53突变。使用NGS TruSeq定制扩增子低输入面板(Illumina)和血浆SafeSEQ(Sysmex)对来自具有乳腺成像报告和数据系统(BIRADS)4c / 5乳腺造影检查结果并随后诊断为原发性乳腺癌的患者的血浆和冷冻新鲜组织活检进行匹配分析骨科)。在29例患者中有8例(27.6%)观察到相同的血浆和肿瘤突变,其中TP53突变4例,PIK3CA突变突变5例。测序分析还揭示了先前在三位患者组织活检中未发现的另外四个ctDNA突变(TP53中的三个,PIK3CA中的一个)。这些患者之一在两个基因中均具有突变。年龄,肿瘤等级和大小,免疫组化(IHC)亚型,BIRADS类别和淋巴结阳性与这些血液肿瘤衍生突变的可检测性显着相关。总之,ctDNA分析可用于早期乳腺癌诊断,为改善患者诊断提供重要的临床信息。

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