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Decreased miR-340 Expression in Bone Marrow Is Associated with Liver Metastasis of Colorectal Cancer

机译:miR-340表达减少与大肠癌的肝转移相关。

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Studies have shown the prognostic significance of disseminated tumor cells (DTC) in bone marrow of patients with colorectal cancer. However, the molecular characteristics of DTCs, including their miRNA expression profiles, remain mostly unknown. In this study, we analyzed the miRNA expression of DTCs in bone marrow. EpCAM(dagger) bone marrow cells were collected using immunomagnetic beads after exclusion of CD14(dagger) and CD45(dagger) cells, then subjected to miRNA microarray analysis. Cluster analysis (7 colorectal cancer patients with liver metastasis and 12 colorectal cancer patients without liver metastasis) indicated that miR-340 and miR-542-3p expressions were significantly decreased in EpCAM(dagger) bone marrow cells of patients with liver metastasis (P = 0.019 and 0.037, respectively). We demonstrated that pre-miR-340 administration inhibited growth of colon cancer cells and suppressed c-Met expression in vitro. In clinical samples of colorectal cancer, miR-340 was expressed at significantly lower levels in tumor tissues compared with normal mucosa. Survival analysis in 136 patients with colorectal cancer indicated that low miR-340 expression was correlated with shorter 5-year disease-free survival (P 0.023) and poor 5-year overall survival ( P = 0.046). It was of note that the colorectal cancer group with low miR-340 and high c-Met expression had the worst prognosis. We further demonstrated that systemic pre-miR-340 administration suppressed growth of pre-established HCT116 tumors in animal therapeutic models. These findings indicate that miR-340 may be useful as a novel prognostic factor and as a therapeutic tool against colorectal cancer. Our data suggest that miR-340 in bone marrow may play an important role in regulating the metastasis cascade of colorectal cancer. Mol Cancer Ther; 13(4); 976-85. (C)2014 AACR.
机译:研究表明大肠癌患者骨髓中弥散性肿瘤细胞(DTC)的预后意义。但是,DTC的分子特征(包括其miRNA表达谱)仍然未知。在这项研究中,我们分析了DTC在骨髓中的miRNA表达。排除CD14(匕首)和CD45(匕首)细胞后,使用免疫磁珠收集EpCAM(匕首)骨髓细胞,然后进行miRNA微阵列分析。聚类分析(7例有肝转移的大肠癌患者和12例无肝转移的大肠癌患者)表明,有肝转移的患者的EpCAM(dagger)骨髓细胞中miR-340和miR-542-3p表达显着降低(P = 0.019和0.037)。我们证明pre-miR-340给药可抑制结肠癌细胞的生长并在体外抑制c-Met表达。在大肠癌的临床样本中,与正常粘膜相比,miR-340在肿瘤组织中的表达水平明显较低。 136位大肠癌患者的生存分析表明,低miR-340表达与较短的5年无病生存期(P = 0.023)和较差的5年总生存期(P = 0.046)相关。值得注意的是,低miR-340和高c-Met表达的结直肠癌组的预后最差。我们进一步证明了在动物治疗模型中全身性pre-miR-340给药抑制了预先建立的HCT116肿瘤的生长。这些发现表明,miR-340可用作新型的预后因子和抗结直肠癌的治疗工具。我们的数据表明,miR-340在骨髓中可能在调节结直肠癌转移级联中起重要作用。分子癌疗法; 13(4); 976-85。 (C)2014 AACR。

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