首页> 外文期刊>Frontiers in Medicine >Mutant Allele Frequency-Based Intra-Tumoral Genetic Heterogeneity Related to the Tumor Shrinkage Mode After Neoadjuvant Chemotherapy in Breast Cancer Patients
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Mutant Allele Frequency-Based Intra-Tumoral Genetic Heterogeneity Related to the Tumor Shrinkage Mode After Neoadjuvant Chemotherapy in Breast Cancer Patients

机译:突变等位基因频率的肿瘤内遗传异质性与乳腺癌患者新辅助化疗后的肿瘤收缩模式相关

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The shrinkage mode of tumor extent after neoadjuvant chemotherapy (NAC) is an important index to evaluate the odds of breast-conserving surgery. However, there is no sufficient measurement to predict the shrinkage mode after NAC. In this study, we analyzed 24 patients' formalin-fixed, paraffin-embedded samples before and after treatment and analyzed 456 cancer-related genes panel by using target next-generation sequencing. Meanwhile, the pathological shrinkage mode was reconstructed in three dimensions after surgery, and the genetic heterogeneity level was estimated by mutant-allele tumor heterogeneity (MATH). We measured the genetic intra-tumor heterogeneity and explored its correlation with the shrinkage mode after NAC. A total of 17 matched pair samples of primary tumor tissue and residual tumor tissue were successfully accessed. It was found that the most common mutated genes were TP53 and PIK3CA in both samples before and after NAC, and no recurrent mutations were significantly associated with the shrinkage mode. Besides, the MATH value of formalin-fixed, paraffin-embedded samples before and after NAC was analyzed by the area under the curve of the receiver operating characteristic, and it is feasible to classify patients into concentric shrinkage mode and non-concentric shrinkage mode in NAC based on the MATH threshold of 58. Our findings indicate that the MATH value was associated with the shrinkage mode of breast cancer in a non-linear model. Patients with the MATH value below the threshold of 58 before and after NAC displayed a concentric shrinkage mode. The area under the curve was 0.89, with a sensitivity of 0.69 and specificity of 1. Our study might provide a promising application of intra-tumor heterogeneity that is measured by MATH to make a choice of surgery.
机译:Neoadjuvant化疗(NAC)后肿瘤程度的收缩方式是评估哺乳术手术几率的重要指标。然而,没有足够的测量来预测NAC之后的收缩模式。在这项研究中,我们通过使用目标下一代测序分析了治疗前后的24名患者的福尔马林固定的石蜡包埋的样品,并通过使用目标下一代测序分析了456例癌症相关基因面板。同时,手术后三维重建病理收缩模式,突变 - 等位基因肿瘤异质性(数学)估计了遗传异质性水平。我们测量了肿瘤内肿瘤内异质性,并在NAC后与收缩​​模式进行了相关性。总共可获得总共17种匹配对原发性肿瘤组织和残留肿瘤组织的样品。发现,在NAC之前和之后的两个样品中,最常见的突变基因是TP53和PIK3CA,并且没有与收缩模式显着相关的复发突变。此外,通过接收器操作特性的曲线下的区域分析NAC之前和之后NAC之前和之后的福尔马林固定的石蜡包埋的样品的数学值,并且将患者分类为同心收缩模式和非同心收缩模式是可行的NAC基于58的数学阈值。我们的研究结果表明,数学值与非线性模型中乳腺癌的收缩模式相关。患者在NAC之前和之后的58阈值低于阈值显示同心收缩模式。曲线下的面积为0.89,灵敏度为0.69,1.我们的研究可能提供通过数学测量的肿瘤内血管内异质性的有希望的应用。

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