首页> 美国卫生研究院文献>Cancer Biology Therapy >Clinico-pathological correlation of serial measurement of circulating tumor cells in 24 metastatic colorectal cancer patients receiving chemotherapy reveals interpatient heterogeneity correlated with CEA levels but independent of KRAS and BRAF mutation
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Clinico-pathological correlation of serial measurement of circulating tumor cells in 24 metastatic colorectal cancer patients receiving chemotherapy reveals interpatient heterogeneity correlated with CEA levels but independent of KRAS and BRAF mutation

机译:接受化疗的24例转移性结直肠癌患者循环肿瘤细胞系列检测的临床病理相关性显示患者间异质性与CEA水平相关但与KRAS和BRAF突变无关

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摘要

>Background: The Veridex CellSearch is an FDA-approved technology for enumerating circulating tumor cells in blood samples of metastatic colorectal cancer mCRC) patients and has prognostic value. It is important to understand how counts of circulating tumor cells (CTCs), which are advocated to be tools for “liquid biopsy” of tumors, correlate with clinical and pathologic variables of significance in these patients. In this study, we have attempted to make such correlations along with evaluating how CTC counts change during the course of chemotherapy. >Patients and methods: Following an IRB-approved protocol, blood samples were collected from 24 patients with mCRC along with relevant clinico-pathological data. Blood was collected at defined time-points both prior to as well as during the course of treatment with combination chemotherapy, and CTC counts were enumerated from7.5 ml of blood. >Results: Seventeen out of 24 patients with mCRC showed a CTC count of 2 or less cells in 7.5 ml of blood at base-line assessment before chemotherapy while 7 patients showed 3 or more cells in 7.5 ml of blood at that point. A correlation was found between high carcino-embryonic antigen (CEA) levels and high CTC counts (P = 0.018) although it was also found that some patients had elevated CTCs without an elevated CEA. No correlation with the time interval between detection of primary tumor and appearance of secondary (metastatic) tumor(s) was found. CTC counts did not correlate with the presence of lung or liver metastases, i.e. a number of mCRC patients with lung or liver metastases had a count of zero CTCs at baseline. We also noted no correlation between CTC number and the status of KRAS or BRAF mutation. CTC counts dropped immediately after the start of chemotherapy in 11 out of 21 patients, and also reduced from the baseline at the end of chemotherapy in 5 out of 10 patients. Six of 7 patients who started with 3 or more CTCs in 7.5 ml at baseline also showed a final CTC reduction at the end of the therapy assessment. >Conclusions: Analysis of circulating tumor cells may be of use in monitoring response to therapy in mCRC, either in combination with CEA monitoring or alone when CTCs are elevated but CEA level is not.
机译:>背景:Veridex CellSearch是一项FDA批准的技术,可用于计数转移性结直肠癌(mCRC)患者血液样本中的循环肿瘤细胞,并具有预后价值。重要的是要了解循环肿瘤细胞(CTC)的计数如何与这些患者的临床和病理变量相关联,而循环肿瘤细胞(CTC)的计数被认为是对肿瘤进行“液体活检”的工具。在这项研究中,我们尝试建立这种关联性,并评估化学疗法过程中CTC计数的变化。 >患者和方法:按照IRB批准的方案,从24例mCRC患者中收集血液样本以及相关的临床病理数据。在联合化疗治疗之前和期间的指定时间点采集血液,并从7.5 ml血液中计数出CTC计数。 >结果:24名mCRC患者中有17名在化疗前的基线评估中发现7.5 ml血液中CTC计数在2个或更少的细胞中,而7名患者在7.5 ml血液中显示3个或更多的细胞在那时候。尽管发现一些患者的CTC升高而CEA却没有升高,但高癌胚抗原(CEA)水平与高CTC计数之间存在相关性(P = 0.018)。未发现与检测到原发肿瘤和继发(转移)肿瘤之间的时间间隔相关。 CTC计数与肺或肝转移的存在无关,即,许多患有肺或肝转移的mCRC患者在基线时的CTC计数为零。我们还注意到CTC数量与KRAS或BRAF突变状态之间没有相关性。在开始化疗后的21位患者中,有11位患者的CTC计数立即下降,并且在化疗结束后的10位患者中,有5位的CTC计数也从基线开始下降。在基线时开始使用7.5 ml的3个或更多CTC的7名患者中有6名在治疗评估结束时也显示出最终的CTC降低。 >结论:循环肿瘤细胞分析可用于监测mCRC对治疗的反应,可以与CEA监测结合使用,或者在CTC升高但CEA水平没有升高时单独监测。

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