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首页> 外文期刊>Pathology oncology research: POR >Correlations of IGF-1R and COX-2 Expressions with Ras and BRAF Genetic Mutations, Clinicopathological Features and Prognosis of Colorectal Cancer Patients
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Correlations of IGF-1R and COX-2 Expressions with Ras and BRAF Genetic Mutations, Clinicopathological Features and Prognosis of Colorectal Cancer Patients

机译:IGF-1R和COX-2表达与RAS和BRAF基因突变的相关性,结直肠癌患者的临床病理特征和预后

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Abstract This case-control study aims to investigate the correlations of insulin-like growth factor receptor 1 (IGF-1R) and cyclooxygenase 2 (COX-2) expressions with Ras and BRAF genetic mutations, clinicopathological features and prognosis of colorectal cancer (CRC) patients. A total of 213 CRC patients (case group) and 200 healthy individuals (control group) were selected from our hospital. Ras (K-Ras/N-Ras) and BRAF genetic mutations were detected by direct sequencing. The positive expression rates of IGF-IR and COX-2 in CRC and normal tissues were detected using immunohistochemistry. RT-qPCR and Western blotting were applied to detect the mRNA and protein expressions of IGF-IR and COX-2 in CRC tissues and normal tissues. Total mutation rate of N-Ras , BRAF and K-Ras in case group were 5.2%, 12.2% and 47.4%, respectively. The expressions of IGF-IR and COX-2 were higher in CRC tissues with Ras and BRAF mutations than in those without. CRC tissues with Ras mutation showed higher COX-2 expression than those with BRAF mutation. IGF-IR and COX-2 expressions were correlated to infiltration degree, lymphatic metastasis (in CRC tissues with and without Ras and BRAF mutations), and Dukes stages (only in CRC tissues with Ras and BRAF mutations). CRC patients with negative expressions of IGF-IR and COX-2 had significantly higher accumulative survival rate and longer mean survival duration than those with positive expressions of IGF-IR and COX-2. These findings indicate that IGF-1R and COX-2 expressions may be associated with Ras and BRAF genetic mutations, clinicopathological feature and prognosis of CRC patients.
机译:本病例对照研究旨在探讨胰岛素样生长因子受体1(IGF-1R)和环氧合酶2(COX-2)的表达与大肠癌(CRC)患者Ras和BRAF基因突变、临床病理特征和预后的关系。从我院选取213例结直肠癌患者(病例组)和200例健康人(对照组)。通过直接测序检测Ras(K-Ras/N-Ras)和BRAF基因突变。免疫组化检测大肠癌和正常组织中IGF-IR和COX-2的阳性表达率。应用RT-qPCR和Western blotting检测大肠癌组织和正常组织中IGF-IR和COX-2的mRNA和蛋白表达。病例组N-Ras、BRAF和K-Ras总突变率分别为5.2%、12.2%和47.4%。有Ras和BRAF突变的大肠癌组织中IGF-IR和COX-2的表达高于无Ras和BRAF突变的大肠癌组织。Ras突变的大肠癌组织中COX-2的表达高于BRAF突变的大肠癌组织。IGF-IR和COX-2的表达与浸润程度、淋巴转移(在有和无Ras和BRAF突变的大肠癌组织中)和Dukes分期(仅在有Ras和BRAF突变的大肠癌组织中)相关。IGF-IR和COX-2表达阴性的大肠癌患者的累积生存率和平均生存期明显高于IGF-IR和COX-2表达阳性的大肠癌患者。这些结果表明,IGF-1R和COX-2的表达可能与大肠癌患者的Ras和BRAF基因突变、临床病理特征和预后有关。

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