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Genome-wide profiling reveals cancer-related genes with switched alternative polyadenylation sites in colorectal cancer

机译:全基因组分析揭示大肠癌中与癌症相关的基因,其多聚腺苷酸化位点已切换

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Background: Alternative polyadenylation (APA) is an important post-transcriptional regulation in eukaryotic cells. It plays considerable roles in many biological processes and diseases, such as cell differentiation, proliferation and cancer. Colorectal cancer (CRC) is one of the most common malignancies worldwide, which is among the top five in incidence and mortality of all cancers in China. Although there have been some studies on the APA of CRC, the normal and carcinoma samples used for genome-wide profiling were not matched. The purpose of this study was to obtain genes with switched 3'-untranslated region (UTR) that may be associated with intracellular regulation of CRC by analyzing APA patterns of strict control groups from clinical patients. Materials and methods: CRC and matched normal tissues were acquired from surgical specimens from three CRC patients. Their libraries of 3'-terminal fragments of mRNA with poly(A) tails were constructed by 3T-seq technology and sequenced by Illumina Hiseq X Ten. APA patterns of cancer and matched normal tissues were analyzed by bioinformatics analysis, and a representative gene, GPI , was verified by quantitative reverse transcription PCR. Results: Overall, we identified 35,076 poly(A) sites in total. Compared to the matched normal tissues, we detected 350, 405 and 375 genes with significantly APA-mediated 3'-UTR alteration in cancer tissues of three patients, respectively. Forty-seven genes with switched 3'-UTR were shared in all three patients. In addition, most of these genes have shortened 3'-UTRs, some of which were associated with cancers, such as GPI . Conclusion: Our studies found several genes with switched 3'-UTR in CRC patients, which may provide some important clues for more in-depth study of the cellular regulation in CRC from the perspective of post-transcriptional regulation. It may also help in the search for new biomarkers of CRC.
机译:背景:替代多腺苷酸化(APA)是真核细胞中重要的转录后调控。它在许多生物过程和疾病中扮演重要角色,例如细胞分化,增殖和癌症。大肠癌(CRC)是全球最常见的恶性肿瘤之一,在中国所有癌症的发病率和死亡率中均排名前五。尽管已经对CRC的APA进行了一些研究,但用于全基因组概况分析的正常样品和癌样品却不匹配。这项研究的目的是通过分析来自临床患者的严格对照组的APA模式来获得具有3'非翻译区(UTR)的基因,这些基因可能与CRC的细胞内调控有关。材料和方法:从三名CRC患者的手术标本中获得CRC和匹配的正常组织。通过3T-seq技术构建了它们的具有poly(A)尾巴的3'-端mRNA片段文库,并通过Illumina Hiseq X Ten测序。通过生物信息学分析来分析癌症和匹配的正常组织的APA模式,并通过定量逆转录PCR验证代表性基因GPI。结果:总体而言,我们共鉴定了35,076个poly(A)位点。与匹配的正常组织相比,我们在三名患者的癌组织中分别检测到350、405和375个具有显着APA介导的3'-UTR改变的基因。在三位患者中共有47个带有转换3'-UTR的基因。此外,这些基因中的大多数已缩短了3'-UTR,其中一些与癌症有关,例如GPI。结论:我们的研究在CRC患者中发现了几个具有3'-UTR转换的基因,这可能为从转录后调控的角度更深入地研究CRC中的细胞调控提供一些重要的线索。它也可能有助于寻找CRC的新生物标记。

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