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Early detection of poor outcome in patients with metastatic colorectal cancer: tumor kinetics evaluated by circulating tumor cells

机译:早期发现转移性结直肠癌患者预后不良:通过循环肿瘤细胞评估肿瘤动力学

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Background: Colorectal cancer (CRC) is the third most prevalent cancer worldwide. New prognostic markers are needed to identify patients with poorer prognosis, and circulating tumor cells (CTCs) seem to be promising to accomplish this. Patients and methods: A prospective study was conducted by blood collection from patients with metastatic CRC (mCRC), three times, every 2?months in conjunction with image examinations for evaluation of therapeutic response. CTC isolation and counting were performed by Isolation by Size of Epithelial Tumor Cells (ISET). Results: A total of 54 patients with mCRC with a mean age of 57.3?years (31–82 years) were included. Among all patients, 60% (n=32) were carriers of wild-type KRAS (WT KRAS ) tumors and 90% of them (n=29) were exposed to monoclonal antibodies along with systemic treatment. Evaluating CTC kinetics, when we compared the baseline (pretreatment) CTC level (CTC1) with the level at first follow-up (CTC2), we observed that CTC1-positive patients (CTCs above the median), who became negative (CTCs below the median) had a favorable evolution (n=14), with a median progression-free survival (PFS) of 14.7?months. This was higher than that for patients with an unfavorable evolution (CTC1– that became CTC2+; n=13, 6.9?months; P =0.06). Patients with WT KRAS with favorable kinetics had higher PFS (14.7?months) in comparison to those with WT KRAS with unfavorable kinetics (9.4?months; P =0.02). Moreover, patients whose imaging studies showed radiological progression had an increased quantification of CTCs at CTC2 compared to those without progression ( P =0.04). Conclusion: This study made possible the presentation of ISET as a feasible tool for evaluating CTC kinetics in patients with mCRC, which can be promising in their clinical evaluation.
机译:背景:结直肠癌(CRC)是全球第三大流行的癌症。需要新的预后标志物来鉴定预后较差的患者,而循环肿瘤细胞(CTC)似乎有望实现这一目标。患者和方法:前瞻性研究是通过每2个月一次从转移性CRC(mCRC)患者的血液收集中进行的,每2个月进行3次,并结合图像检查来评估治疗效果。通过上皮肿瘤细胞大小(ISET)的分离进行CTC分离和计数。结果:共纳入54例mCRC患者,平均年龄57.3岁(31-82岁)。在所有患者中,有60%(n = 32)是野生型KRAS(WT KRAS)肿瘤的携带者,其中90%(n = 29)曾接受单克隆抗体以及全身治疗。在评估CTC动力学时,当我们将基线(预处理)CTC水平(CTC1)与首次随访(CTC2)的水平进行比较时,我们发现CTC1阳性患者(CTC高于中位数)变为阴性(CTC低于中位数)。中位数)有良好的进化(n = 14),中位数无进展生存期(PFS)为14.7个月。这比那些有不利进展的患者(CTC1–变成CTC2 +; n = 13,6.9?个月; P = 0.06)高。 WT KRAS动力学良好的患者的PFS(14.7?months)比WT KRAS动力学不良的患者(9.4?month; P = 0.02)高。此外,影像学检查显示放射学进展的患者与未进展的患者相比,CTC2处的CTC定量增加(P = 0.04)。结论:这项研究使ISET成为评估mCRC患者CTC动力学的可行工具成为可能,这在他们的临床评估中很有希望。

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