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Identifying the key genes and microRNAs in prostate cancer bone metastasis by bioinformatics analysis

机译:通过生物信息学分析鉴定前列腺癌骨转移中的关键基因和微大血清

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摘要

Prostate adenocarcinoma (PCa) is the most common cause of death due to malignancy among men, and bone metastasis is the leading cause of mortality in patients with PCa. Therefore, identifying the causes and molecular mechanism of bone metastasis is important for early detection, diagnosis and personalized therapy. In this study, we systematically analyzed molecular correlates of bone metastasis by bioinformatics analysis. A total of 12 differentially expressed microRNAs (miRNAs) and 102 differentially expressed genes were identified. Five miRNAs had prognostic significance in biochemical recurrence‐free survival (miR‐636, miR‐491‐5p, miR‐199b‐5p, miR‐199b‐3p, miR‐28‐3p). The differentially expressed genes were significantly enriched in extracellular matrix, cell‐substrate adhesion, collagen and integrin. Seven hub genes ( VCAN , COL3A1 , COL1A1 , APOE , COL1A2 , SDC1 , THY1 ) with worse biochemical recurrence‐free survival and one hub gene ( MMP9 ) with worse overall survival were detected. miR‐636, a novel oncogene, was found to be up‐regulated in bone metastatic PCa tissues and also predominately up‐regulated in human PCa cell lines. miR‐636 promoted cellular invasion and migration, and may promote bone metastasis via targeting MBNL2 , TNS1 and STAB1 . In conclusion, we have successfully defined molecular signatures of bone metastasis in PCa.
机译:前列腺腺癌(PCA)是男性恶性肿瘤导致的最常见死因,骨转移是PCA患者死亡率的主要原因。因此,鉴定骨转移的原因和分子机制对于早期检测,诊断和个性化治疗是重要的。在本研究中,我们通过生物信息学分析系统地分析了骨转移的分子相关性。鉴定了总共12种差异表达的微小RNA(miRNA)和102个差异表达基因。五个miRNA在生化复发存活中具有预后意义(MIR-636,MIR-491-5P,MIR-199B-5P,MIR-199B-3P,MIR-28-3P)。细胞外基质,细胞 - 基质粘附,胶原和整联蛋白显着富集差异表达基因。检测到七个集线基因(VCAN,COL3A1,COL1A1,APOE,COL1A2,SDC1,THY1),其具有更差的生物化学复发存活和一个具有更严重的整体存活的集线基因(MMP9)。发现MiR-636,一种新型癌基因,在骨转移PCA组织中被上调,并且在人PCA细胞系中也主要上调。 miR-636促进细胞侵袭和迁移,并可通过靶向MBN12,TNS1和刺激促进骨转移。总之,我们成功地定义了PCA中骨转移的分子鉴定。

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