越南非息肉性结肠癌患者的KRAS突变及其与临床病理特征和生存的关系

IF 1.4 Q4 ONCOLOGY
Hoang Minh Cuong, Vu Hong Thang, Bui-Thi Thu Huong, Nguyen Thuan Loi, Nguyen Minh Duc
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引用次数: 0

摘要

本研究的目的是确定越南非息肉性结肠癌(NPCC)患者的Kirsten Ras肉瘤病毒(KRAS)突变及其与临床病理特征和治疗结果的关系。根据美国癌症分期系统联合委员会第8版,本研究的数据涵盖了2016年1月至2020年8月在越南北部的194名II期或III期非息肉性结肠癌患者。所有患者均接受根治性手术和FOLFOX4或XELOX辅助治疗。随后,招募的患者接受了定期的医院检查以诊断复发。从解剖肿瘤中制备基因组DNA样本,并利用聚合酶链反应(PCR)扩增KRAS基因的特异性序列。测定了该基因密码子12、13、59、60、61、117和146的突变位点。分析了KRAS突变与临床病理特性和患者生存的可能关联。越南NPCC患者KRAS突变率为47.9%,其中外显子2突变占全部检测突变的91.4%。突变的kras患者表现出明显更高的贫血率。此外,KRAS在女性中的突变率(57.1%)高于男性(39.8%)。KRAS突变率在右结肠癌患者中也较高。此外,KRAS突变是II期患者无病生存期(DFS)和总生存期(OS)差的独立预后因素。在左侧结肠患者中,KRAS突变是不良DFS的重要预测因素,但不是OS的重要预测因素。本研究显示KRAS在越南NPCC患者中具有很高的突变率。本研究的数据表明,突变状态与女性患者和右侧肿瘤有关。KRAS突变是II期NPCC患者和左侧结肠癌患者生存的负面因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

<i>KRAS</i> mutations and their associations with clinicopathological features and survival in Vietnamese non‑polyp colon cancer patients.

<i>KRAS</i> mutations and their associations with clinicopathological features and survival in Vietnamese non‑polyp colon cancer patients.

<i>KRAS</i> mutations and their associations with clinicopathological features and survival in Vietnamese non‑polyp colon cancer patients.

KRAS mutations and their associations with clinicopathological features and survival in Vietnamese non‑polyp colon cancer patients.

The aim of the present study was to determine Kirsten Ras sarcoma virus (KRAS) mutations and the associations of KRAS mutations with clinicopathological features and treatment outcomes in Vietnamese non-polyp colon cancer (NPCC) patients. The data in the present study covered 194 patients with non-polyp colon cancers at stages II or III, according to the 8th edition of the American Joint Committee on Cancer staging system, in northern Vietnam from January 2016 to August 2020. All patients underwent radical surgery and adjuvant therapy with FOLFOX4 or XELOX. Subsequently, the recruited patients were followed-up with scheduled hospital exams for diagnosing recurrence. Genomic DNA samples were prepared from dissected tumors and specific sequences of the KRAS gene were amplified by polymerase chain reactions (PCR). The mutations at codons 12, 13, 59, 60, 61, 117 and 146 of the gene were determined. Possible associations of the KRAS mutations with clinicopathological properties and the survival of patients were analysed. The KRAS mutation rate was 47.9% in Vietnamese patients with NPCC, of those, mutations in exon 2 accounted for 91.4% of all detected mutations. The mutated-KRAS patients exhibited a significantly higher rate of anemia. Moreover, the KRAS mutation rate was higher in females (57.1%) than in males (39.8%). The KRAS mutation rate was also higher in patients with right colon cancers. Furthermore, KRAS mutations were an independent prognosis for poor disease-free survival (DFS) and overall survival (OS) in stage II patients. Among left-sided colon patients, mutated KRAS was a significant predictive factor for poor DFS but not for OS. The present study revealed a very high mutation rate of KRAS in Vietnamese patients with NPCC. The data of the present study indicated that the mutation status was associated with female patients and right-sided tumors. The KRAS mutations were a negative factor for the survival of patients with stage II NPCC and patients with left-sided colon cancer.

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