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首页> 外文期刊>Tumour biology : >KiSS-1 methylation and protein expression patterns contribute to diagnostic and prognostic assessments in tissue specimens for colorectal cancer
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KiSS-1 methylation and protein expression patterns contribute to diagnostic and prognostic assessments in tissue specimens for colorectal cancer

机译:KiSS-1甲基化和蛋白质表达模式有助于大肠癌组织标本的诊断和预后评估

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KISS1 is a metastasis suppressor lost in several solid malignancies. We evaluated the clinical relevance of KiSS-1 methylation and its protein expression in colorectal cancer. The epigenetic silencing of KiSS-1 by hypermethylation was tested in colon cancer cells (n = 5) before and after azacytidine treatment. KiSS-1 methylation was evaluated by methylation-specific PCR in colorectal cancer cells, and normal, benign, and tumor tissues (n = 352) were grouped in a training set (n = 62) and two independent validation cohorts (n = 100 and n = 190). KiSS-1 protein expression was analyzed by immunohistochemistry on tissue arrays. KiSS-1 hypermethylation correlated with transcript and protein expression loss, being increased in vitro by azacytidine. Methylation rates were 53.1, 70.0, and 80.0 % in the training and validation sets, respectively. In the training set, KiSS-1 methylation rendered a diagnostic accuracy of 72.7 % (p = 0.002). Combination of KiSS-1 methylation and serum CEA (p = 0.001) increased the prognostic utility of CEA alone (p = 0.022). In the first validation set, KiSS-1 methylation correlated with tumor grade (p = 0.011), predicted recurrence (p = 0.009), metastasis (p = 0.004), disease-free (p = 0.034), and overall survival (p = 0.015). In the second validation cohort, KiSS-1 methylation predicted disease-specific survival (p = 0.030). In the training set, cytoplasmic KiSS-1 expression was significantly higher in nonneoplastic biopsies as compared to colorectal tumors (p < 0.0005). In the validation set, loss of cytoplasmic expression correlated with tumor stage (p = 0.007), grade (p = 0.035), recurrence (p = 0.017), and disease-specific survival (p = 0.022). KiSS-1 was revealed epigenetically modified in colorectal cancer. The diagnostic and prognostic utility of KiSS-1 methylation and expression patterns suggests their assessment for the clinical management of colorectal cancer patients.
机译:KISS1是在几种实体恶性肿瘤中丢失的转移抑制因子。我们评估了KiSS-1甲基化及其在结直肠癌中的蛋白表达的临床意义。在氮杂胞苷处理之前和之后,在结肠癌细胞(n = 5)中测试了通过高甲基化对KiSS-1进行表观遗传沉默。通过甲基化特异性PCR在大肠癌细胞中评估KiSS-1甲基化,并将正常,良性和肿瘤组织(n = 352)分组在训练组(n = 62)和两个独立的验证队列(n = 100和n = 190)。通过在组织阵列上的免疫组织化学分析了KiSS-1蛋白的表达。 KiSS-1高甲基化与转录和蛋白质表达损失相关,在体外被氮胞苷增加。在训练和验证组中,甲基化率分别为53.1%,70.0和80.0%。在训练集中,KiSS-1甲基化的诊断准确性为72.7%(p = 0.002)。 KiSS-1甲基化与血清CEA的联合使用(p = 0.001)可提高单独使用CEA的预后效用(p = 0.022)。在第一个验证集中,KiSS-1甲基化与肿瘤等级(p = 0.011),预测的复发率(p = 0.009),转移灶(p = 0.004),无病(p = 0.034)和总生存期(p = 0.015)。在第二个验证队列中,KiSS-1甲基化预测疾病特异性生存率(p = 0.030)。在训练组中,与结直肠肿瘤相比,在非肿瘤活检中细胞质KiSS-1表达明显更高(p <0.0005)。在验证组中,细胞质表达的丧失与肿瘤分期(p = 0.007),等级(p = 0.035),复发(p = 0.017)和疾病特异性存活率(p = 0.022)相关。 KiSS-1在大肠癌中被表观遗传修饰。 KiSS-1甲基化和表达模式的诊断和预后效用表明了他们对大肠癌患者临床治疗的评估。

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