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Five Circular RNAs in Metabolism Pathways Related to Prostate Cancer

机译:与前列腺癌相关的新陈代谢途径中的五个圆形RNA

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Prostate cancer (PCa) is the most common malignant tumor in men, and its incidence increases with age. Serum prostate-specific antigen and tissue biopsy remain the standard for diagnosis of suspected PCa. However, these clinical indicators may lead to aggressive overtreatment in patients who have been treated sufficiently with active surveillance. Circular RNAs (circRNAs) have been recently recognized as a new type of regulatory RNA that is not easily degraded by RNases and other exonucleases because of their covalent closed cyclic structure. Thus, we utilized high-throughput sequencing data and bioinformatics analysis to identify specifically expressed circRNAs in PCa and filtered out five specific circRNAs for further analysis—hsa_circ_0006410, hsa_circ_0003970, hsa_circ_0006754, hsa_circ_0005848, and a novel circRNA, hsa_circ_AKAP7. We constructed a circRNA-miRNA regulatory network and used miRNA and differentially expressed mRNA interactions to predict the function of the selected circRNAs. Furthermore, survival analysis of their cognate genes and PCR verification of these five circRNAs revealed that they are closely related to well-known PCa pathways such as the MAPK signaling pathway, P53 pathway, androgen receptor signaling pathway, cell cycle, hormone-mediated signaling pathway, and cellular lipid metabolic process. By understanding the related metabolism of circRNAs, these circRNAs could act as metabolic biomarkers, and monitoring their levels could help diagnose PCa. Meanwhile, the exact regulatory mechanism for AR-related regulation in PCa is still unclear. The circRNAs we found can provide new solutions for research in this field.
机译:前列腺癌(PCA)是男性中最常见的恶性肿瘤,其发病率随着年龄的增长而增加。血清前列腺特异性抗原和组织活组织检查仍然是诊断疑似PCA的标准。然而,这些临床指标可能导致患者侵略性过度处理,该患者受到积极监测的充分处理。圆形RNA(CircRNA)最近被认为是由于它们的共价闭合环状结构,因此不容易被RNases和其他外切核酸酶降解的新型调节RNA。因此,我们利用了高吞吐量测序数据和生物信息学分析,以识别PCA中的特异性表达的CircRNA,并为进一步的分析 - HSA_CIRC_0006410,HSA_CIRC_0003970,HSA_CIRC_0005848以及新颖的CircRNA,HSA_CIRC_AKAP7中过滤输出五个特定的CIRCRNA。我们构建了Circrna-miRNA调节网络,并使用MiRNA和差异表达的mRNA相互作用以预测所选Circrnas的功能。此外,对其同源基因的生存分析和这些五个CircrNA的PCR验证揭示它们与众所周知的PCA途径密切相关,例如MAPK信号通路,P53途径,雄激素受体信号传导途径,细胞周期,激素介导的信号通路。和细胞脂代谢过程。通过了解Circrnas相关的新陈代谢,这些Circrnas可以充当代谢生物标志物,并监测其水平可以帮助诊断PCA。同时,PCA中AR相关调节的确切调节机制仍然不清楚。我们发现的Circrnas可以为该领域的研究提供新的解决方案。

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