尿CtDNA谱分析在乳腺癌治疗中的潜在应用

N. Ivonne
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引用次数: 1

摘要

无细胞循环肿瘤DNA (ctDNA),通过原发或转移部位的凋亡或坏死肿瘤细胞进入血液,成为肿瘤研究中广泛研究和非常有前途的分析物。如果通过肾脏屏障,ctDNA很可能出现在尿液中。文献研究表明,缺乏针对尿ctDNA诊断应用的研究。大多数关于尿ctDNA的研究都是在泌尿系统癌症领域进行的,然而,尿液活检适合于绘制来自循环的ctDNA改变的决定性实时图像,因此加强了尿ctDNA的遗传谱分析对于获得其他实体肿瘤(如乳腺癌)的肿瘤相关信息也有价值的假设。通常,临床治疗决定是基于从最初的组织活检中获得的突变概况。然而,在治疗过程中,遗传肿瘤谱可能会发生变化,例如,可能与靶向治疗选择或治疗耐药性相关的遗传改变的获得和丢失。特别是晚期乳腺癌患者可能在治疗周期中获得突变,可能受益于序列ctDNA测序,以发现新的靶向突变,并获得量身定制的治疗。在这里,使用尿ctDNA可能为非侵入性纵向基因分型和可操作突变测试提供机会。与血浆来源的ctDNA相比,只有少数研究使用乳腺癌患者的尿ctDNA进行,并显示靶向NGS似乎是检测肿瘤特异性遗传特征的敏感方法。在这篇小型综述中,我们试图阐明尿ctDNA对乳腺癌患者进行频繁、低成本的纵向疾病监测的潜在用途。
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The Potential Use of Urinary CtDNA Profiling in the Treatment of Breast Cancer
Cell-free circulating tumor DNA (ctDNA), shed into the blood stream by apoptotic or necrotic tumor cells of either primary or metastatic sites, became an extensively investigated and very promising analyte in oncology research. If passing through the kidney barrier, ctDNA is likely to occur in urine. Literature research revealed a lack of studies aiming at diagnostic use of urinary ctDNA. Most studies investigating urinary ctDNA were performed in the field of urological cancers emphasizing, however, that urinary liquid biopsies were suitable to draw conclusive real time pictures of ctDNA alterations coming from circulation and hence strengthen the hypothesis that genetic profiling of urinary ctDNA could be valuable to gain tumor-related information also in other solid tumors such as breast cancer. Usually, clinical treatment decisions are based on mutation profiles that were received from initial tissue biopsies. Though, during therapy the genetic tumor profile might change e.g. gain and loss of genetic alterations that might be relevant for targeted therapy options or treatment resistance. Particularly patients with advanced breast cancer may acquire mutations during treatment cycles and might benefit from serial ctDNA sequencing to find new targetable mutations and gain access to tailored therapy. Here, the use of urinary ctDNA might offer an opportunity for non-invasive longitudinal genotyping and testing for actionable mutations. In contrast to plasma-derived ctDNA, only a few studies were performed using urinary ctDNA from patients with breast cancer and revealed that targeted NGS appeared to be a sensitive method to detect tumor-specific genetic features. In this mini review we sought to illuminate the potential use of urinary ctDNA for longitudinal disease monitoring at frequent intervals and low effort for patients with breast cancer.
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