一系列摩洛哥患者的结直肠癌 KRAS、NRAS 和 BRAF 基因突变谱。

IF 2.5 4区 医学 Q3 ONCOLOGY Cancer Control Pub Date : 2024-01-01 DOI:10.1177/10732748241262179
Sara El Zaitouni, Abdelilah Laraqui, Meriem Ghaouti, Asmae Benzekri, Fouad Kettani, Tahar Bajjou, Yassine Sekhsokh, Soukaina Benmokhtar, Meryem Jafari, Walid Baba, Mohamed Oukabli, Hicham El Annaz, Rachid Abi, Mohamed Rida Tagajdid, Safae El Kochri, Idriss Amine Lahlou, Rabii Ameziane El Hassani, Khalid Ennibi
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Among the patients with <i>KRAS</i> exon 2 wild-type (wt), 27.6% (32/116) harbored additional <i>KRAS</i> mutations. Concurrent <i>KRAS</i> mutations were identified in 9.5% (11/116); including six in codon 146 (A146P/T/V), three in codon 61 (Q61H/L/R), one in codon 12 (G12 A and Q61H), and one in codon 13 (G13D and Q61 L). Among the <i>NRAS</i> exon 2 wt patients, 64.3% (9/14) harbored additional <i>NRAS</i> mutations. Concurrent <i>NRAS</i> mutations were identified in 28.6% (4/14) of <i>NRAS</i>-mutant patients. 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引用次数: 0

摘要

研究目的本研究旨在评估 249 名摩洛哥结直肠癌(CRC)患者中 KRAS、NRAS 和 BRAF 突变的频率及其与临床病理特征的可能关联:采用 Idylla™ 技术和热测序技术对 249 例 CRC 患者的福尔马林固定石蜡包埋组织进行了 KRAS/NRAS/BRAF 突变的回顾性调查:结果:46.6%(116/249)、5.6%(14/249)和 2.4%(6/249)的患者发现了 KRAS、NRAS 和 BRAF 突变。87.9%的患者(102/116)发现了 KRAS 第 2 外显子突变。KRAS G12D和G12 C是最常见的突变,分别占32.8%和12.93%。在KRAS外显子2野生型(wt)患者中,27.6%(32/116)的患者携带额外的KRAS突变。9.5%的患者(11/116)发现了并发的KRAS突变,其中6例发生在146密码子(A146P/T/V),3例发生在61密码子(Q61H/L/R),1例发生在12密码子(G12 A和Q61H),1例发生在13密码子(G13D和Q61 L)。在 NRAS 外显子 2 wt 患者中,64.3%(9/14)的患者携带额外的 NRAS 突变。28.6%(4/14)的 NRAS 突变患者同时发现了 NRAS 突变。由于 3.2% 的 KRAS 基因突变患者同时发现了 NRAS 基因突变,2.4% 的患者(6/249)同时发现了 KRAS 和 NRAS 基因突变。KRAS突变在50岁以上年龄组中发生率较高(P = .031),肿瘤位置与KRAS突变显著相关(P = .028),主要发生在左结肠(27.5%)和结肠(42.2%)。NRAS突变在左侧结肠(42.8%)和分化良好的肿瘤(64.2%)中最为常见:结论:KRAS突变的检测,尤其是G12 C亚型的检测,可能对CRC患者有重要意义,并有可能产生治疗效果。然而,CRC 患者中罕见的 KRAS 并发突变表明,每个人可能会有不同的治疗反应。在对同一患者进行 KRAS 检测的同时,对其他受影响基因的鉴定也将有助于临床决策过程,从而使治疗更加个性化。总之,利用新型分子技术进行早期诊断可为摩洛哥患者提供最有效的疗法,从而改善对 CRC 的管理。
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KRAS, NRAS and BRAF Mutational Profile of Colorectal Cancer in a Series of Moroccan Patients.

Objectives: The present study aimed to evaluate the frequencies of KRAS, NRAS, and BRAF mutations and their possible associations with clinicopathological features in 249 Moroccan patients with colorectal cancer (CRC).

Methods: A retrospective investigation of a cohort of formalin-fixed paraffin-embedded tissues of 249 patients with CRC was screened for KRAS/NRAS/BRAF mutations using Idylla™ technology and pyrosequencing.

Results: KRAS, NRAS, and BRAF mutations were revealed in 46.6% (116/249), 5.6% (14/249), and 2.4% (6/249) of patients. KRAS exon 2 mutations were identified in 87.9% of patients (102/116). KRAS G12D and G12 C were the most frequent, at 32.8% and 12.93%, respectively. Among the patients with KRAS exon 2 wild-type (wt), 27.6% (32/116) harbored additional KRAS mutations. Concurrent KRAS mutations were identified in 9.5% (11/116); including six in codon 146 (A146P/T/V), three in codon 61 (Q61H/L/R), one in codon 12 (G12 A and Q61H), and one in codon 13 (G13D and Q61 L). Among the NRAS exon 2 wt patients, 64.3% (9/14) harbored additional NRAS mutations. Concurrent NRAS mutations were identified in 28.6% (4/14) of NRAS-mutant patients. Since 3.2% wt KRAS were identified with NRAS mutations, concomitant KRAS and NRAS mutations were identified in 2.4% (6/249) of patients. KRAS mutations were higher in the >50-year-old age-group (P = .031), and the tumor location was revealed to be significantly associated with KRAS mutations (P = .028) predominantly in left colon (27.5%) and colon (42.2%) locations. NRAS mutations were most prevalent in the left colon (42.8%) and in well-differentiated tumors (64.2%).

Conclusion: Detection of KRAS mutations, particularly the G12 C subtype, may be significant for patients with CRC and has possible therapeutic implications. However, rare KRAS concomitant mutations in CRC patients suggest that each individual may present distinct therapeutic responses. KRAS testing alongside the identification of other affected genes in the same patient will make the treatments even more personalized by contributing more accurately to the clinical decision process. Overall, early diagnosis using novel molecular techniques may improve the management of CRC by providing the most efficient therapies for Moroccan patients.

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来源期刊
Cancer Control
Cancer Control ONCOLOGY-
CiteScore
3.80
自引率
0.00%
发文量
148
审稿时长
>12 weeks
期刊介绍: Cancer Control is a JCR-ranked, peer-reviewed open access journal whose mission is to advance the prevention, detection, diagnosis, treatment, and palliative care of cancer by enabling researchers, doctors, policymakers, and other healthcare professionals to freely share research along the cancer control continuum. Our vision is a world where gold-standard cancer care is the norm, not the exception.
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