从配对的正常和肿瘤组织中鉴定与透明细胞卵巢癌相关的选择性剪接特征

Yu-Ting Huang, M. Shiao, Chen-An Tasi, Kuer-Yuan Lan, Chieh-Hsi Lin, Natini Jianawath, Jia-Ming Chang
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引用次数: 0

摘要

信使rna (mrna)的选择性剪接是真核生物中常见且保守的生物学过程。不同选择剪接形式的异常或破坏可能引起细胞功能的改变并导致疾病。有人提出,选择性剪接可能在癌变机制中起关键作用。通过研究癌症基因组图谱数据库中的大型数据集,最近的一项研究表明,选择性剪接,特别是外显子排除,是卵巢癌严重亚型的一个强有力的预后因素。然而,在其他亚型中,选择性剪接的特征尚未被研究。在这项研究中,我们关注的是透明细胞卵巢癌亚型的选择性剪接事件,即单外显子包含或排除。与欧洲人和美国人相比,这种亚型在亚洲的发病率似乎特别高,而且往往具有耐药性。从5例患者的肿瘤及其配对正常组织中获得转录组。在肿瘤和配对正常组织中计算了psi值,该值表示外显子的可选剪接事件的比例。肿瘤患者与配对正常患者的psi值差异采用条件β回归模型进行显著性检验。我们总共鉴定了约200个外显子,覆盖了52个基因,这些基因在癌症和配对正常组织之间存在显著差异(p < 0.001),包括基因ERP29和PAM,这些基因之前在浆液亚型中被鉴定出来。
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Identification of Alternative Splicing Characteristic Associated with Clear-Cell Ovarian Cancer from Paired Normal and Tumor Tissues
Alternative splicing of messenger RNAs (mRNAs) is a common and conserved biological process in eukaryotes. The aberrancy or disruption of different alternative splicing forms may cause alterations of cell functions and result in diseases. It is proposed that alternative splicing may play a critical role in the mechanisms of carcinogenesis. By studying a large dataset in The Cancer Genome Atlas database, a recent study showed that alternative splicing, particularly exon-exclusion, is a powerful prognosis factor in serious subtype of ovarian cancer. However, the characteristics of alternative splicing has not been studied in other subtypes. In this study, we focus on the alternative splicing events, i.e. single exon-inclusion or -exclusion, in clear-cell ovarian cancer subtype. The subtype appears to have particularly high incidence in Asians comparing to Europeans and Americans and tend to be drug resistant. Transcriptomes were obtained from tumors and their paired-normal tissues from five patients. PSI-values, which represent the proportions of alternative splicing events of an exon, were calculated in both tumor and paired-normal tissues. Differences of PSI-values between tumors and paired-normal were examined by a significant test based on Conditional Beta Regression model. In total, we identified ~200 exons covering 52 genes with significant differences between cancer and paired-normal tissue (p < 0.001) including gene ERP29 and PAM which were previously identified in serous subtypes.
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