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Serum DNA methylation for monitoring response to neoadjuvant chemotherapy in breast cancer patients

机译:血清DNA甲基化用于监测对乳腺癌患者Neoadjuvant化疗的反应

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摘要

Patients with large or nonoperable breast cancers often receive neoadjuvant chemotherapy to facilitate full resection of the tumor and enable conservation of the breast. However, currently available methods for evaluation of response during therapy are limited and the actual effect of the treatment is only recognized at surgery upon completion of chemotherapy. Timely assessment of response could allow individual tailoring of the treatment and save noneffective drugs and unnecessary toxicity. Here, we suggest that tumor derived DNA methylation in the serum may reflect changes in tumor burden and allow early recognition of responders versus nonresponders. In this pilot study, we collected 7 consecutive serum samples from 52 patients with locally advanced breast cancer during neoadjuvant chemotherapy. We selected RASSF1, which was methylated in more than 80% of the tumors, for serum analysis. Using the “methylation sensitive PCR and high resolution melting,” we detected RASSF1 methylation in the serum of 21 patients prior to therapy. In four patients who achieved complete pathological response, RASSF1 methylation in the serum became undetectable early during therapy. In contrast, in 17 patients that had partial or minimal pathological response, serum RASSF1 methylation persisted longer or throughout the treatment (complete versus partial response p = 0.02). These findings support further development of this assay for monitoring response during neoadjuvant therapy.
机译:患有大型或不可操作的乳腺癌的患者通常会接受Neoadjuvant化疗,以促进肿瘤的全部切除并能够保护乳房。然而,目前用于评估治疗期间反应的可用方法是有限的,并且在完成化疗后,待遇在手术中仅识别治疗的实际效果。及时评估反应可以允许个人剪裁治疗,并节省非缺乏药物和不必要的毒性。在这里,我们表明血清中的肿瘤衍生的DNA甲基化可能反映肿瘤负荷的变化,并允许早期识别响应者与无反应者。在该试点研究中,我们在新辅助化疗期间收集了52例局部晚期乳腺癌患者的连续血清样本。我们选择了RASSF1,其在80%以上的肿瘤中甲基化,用于血清分析。使用“甲基化敏感PCR和高分辨率熔化”,我们在治疗前21例患者的血清中检测到RASSF1甲基化。在达到完全病理反应的四名患者中,血清中的RASSF1甲基化在治疗期间早期无法察觉。相比之下,在具有部分或最小病理反应的17名患者中,血清Rassf1甲基化持续或整个处理(完全与部分反应P = 0.02)。这些发现还支持进一步发展该测定以在新辅助治疗期间监测响应。

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