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Impact of RAS and BRAF mutations on carcinoembryonic antigen production and pattern of colorectal metastases

机译:RAS和BRAF突变对癌胚抗原产生和结直肠转移模式的影响

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摘要

AIM: To investigate the impact of RAS and BRAF mutations on the pattern of metastatic disease and carcinoembryonic antigen (CEA) production.METHODS: In this retrospective study, we investigated the impact of RAS and BRAF mutational status on pattern of metastatic disease and CEA production. Only patients presenting with a newly diagnosed metastatic colorectal cancer (CRC) were included. Patients’ characteristics, primary tumor location, site of metastatic disease and CEA at presentation were compared between those with and without RAS and BRAF mutations.RESULTS: Among 174 patients, mutations in KRAS, NRAS and BRAF were detected in 47%, 3% and 6% respectively. RAS mutations (KRAS and NRAS) were more likely to be found in African American patients (87% vs 13%; P value = 0.0158). RAS mutations were associated with a higher likelihood of a normal CEA (< 5 ng/mL) at presentation. BRAF mutations were more likely to occur in females. We were not able to confirm any association between mutational status and site of metastatic disease at initial diagnosis.CONCLUSION: No association was found between RAS and BRAF mutations and sites of metastatic disease at the time of initial diagnosis in our cohort. Patients with RAS mutations were more likely to present with CEA levels < 5 ng/mL. These findings may have clinical implications on surveillance strategies for RAS mutant patients with earlier stages of CRC.
机译:目的:研究RAS和BRAF突变对转移性疾病和癌胚抗原(CEA)产生的影响。方法:在这项回顾性研究中,我们调查RAS和BRAF突变状态对转移性疾病及CEA产生的影响。 。仅包括出现新诊断的转移性结直肠癌(CRC)的患者。比较了有无RAS和BRAF突变的患者的特征,原发肿瘤位置,转移性疾病的部位和出现的CEA。结果:在174例患者中,发现KRAS,NRAS和BRAF突变的比例分别为47%,3%和22%。分别为6%。在非裔美国人患者中更可能发现RAS突变(KRAS和NRAS)(87%比13%; P值= 0.0158)。呈现时,RAS突变与正常CEA的可能性更高(<5 ng / mL)有关。女性更有可能发生BRAF突变。结论初诊时RAS和 BRAF 突变与转移病部位之间无关联。我们的队列。具有 RAS 突变的患者更有可能出现CEA水平<5 ng / mL。这些发现可能对具有早期CRC的 RAS 突变患者的监测策略具有临床意义。

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