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Prognosis related miRNAs, DNA methylation, and epigenetic interactions in lung adenocarcinoma

机译:预后相关的miRNA,DNA甲基化和肺腺癌中的表观遗传相互作用

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Our study aimed to identify prognosis related epigenetic interactions of DNA methylation-miRNA-gene in lung adenocarcinoma. The RNA-seq, DNA methylation and miRNA-seq data of squamous cell cancer samples were downloaded from TCGA. The DNA methylation-miRNA-gene interactions were collected via Illumina methylation platform and miRTar-Base database. Linear regression model was utilized for the identification of epigenetic interactions. The epigenetic interactions related to prognosis were selected via Kaplan-Meier analysis. Genes in the interactions were used for pathway enrichment. Differentially expressed genes (DEGs) between high methylation level/high miRNA expression level (H/H) and low methylation level/low miRNA expression level (L/L) samples were screened. The correlations of epigenetic interactions with clinical features were also explored. Total of 454 lung adenocarcinoma patient samples were collected. The 1063 interactions were comprised of 1083 DNA methylation probes, 271 miRNAs and 528 genes, including cg14146378-hsa-mir-205-ARID1B, cg15375596-has-miR-1275-IGF1R, cg26691953-hsa-mir-195-CCNT1, etc. A total of 95 epigenetic interactions were significantly associated with prognosis. Among all the identified DEGs, low-expressed RASSF4, ZNF704, TFDP1, PLXNB2, TMC04, ZNF878, ARIDIB and high-expressed ZNF704, ZNF451, THOP1, IGF1R were related with poor prognosis, while low-expressed LDHB, ARID2, PRKCSH, HDAC4, NIPA1, RABAC1, TRIM28 and high-expressed FAM160B1, DNAAF3, CCNT1, ADAP1, ZFPM1, CCL11 were related with good prognosis. Fifteen epigenetic interactions were significantly related with clinical features. Gene expression and N-glycan trimming in the ER and Calnexin/Calreticulin cycle were two significant enriched pathways. Interactions of cg14146378-hsa-mir-205-ARID1B and cg15375596-has-miR-1275-IGF1R may be used as prognosis indicators in lung adenocarcinoma.
机译:我们的研究旨在鉴定肺腺癌DNA甲基化 - miRNA-基因的预后相关的表观遗传相互作用。从TCGA下载鳞状细胞癌样品的RNA-SEQ,DNA甲基化和MiRNA-SEQ数据。通过Illumina甲基化平台和Mirtar-Base数据库收集DNA甲基化 - miRNA-基因相互作用。线性回归模型用于鉴定表观遗传相互作用。通过Kaplan-Meier分析选出与预后相关的表观遗传相互作用。相互作用中的基因用于途径富集。筛选高甲基化水平/高miRNA表达水平(H / H)与低甲基化水平/低miRNA表达水平(L / L)样品之间的差异表达基因(DEGS)。还探讨了表观遗传学相互作用的相关性。收集总共454例肺腺癌患者样品。 1063个相互作用由1083个DNA甲基化探针,271 miRNA和528个基因组成,包括CG14146378-HSA-MIR-205-ARID1B,CG15375596 -SMIR-1275-IGF1R,CG26691953-HSA-MIR-195-CCNT1等。总共95个表观遗传学相互作用与预后显着相关。在所有鉴定的DEG,低表达的RASSF4,ZNF704,TFDP1,PLXNB2,TMC04,ZNF878,ARIDIB和高表达ZNF704,ZNF451,THOP1,IGF1R与预后差有关,而低表达的LDHB,ARID2,PRKCSH,HDAC4 ,NIPA1,Rabac1,Trim28和高表达FAM160B1,DNAAF3,CCNT1,ADAP1,ZFPM1,CCL11与预后良好有关。十五个表观遗传相互作用与临床特征显着相关。在ER和Calnexin / Caltreticulin循环中的基因表达和N-甘油修剪是两种显着的富集途径。 CG14146378-HSA-MIR-205-ARID1B和CG15375596-HAS-MIR-1275-IGF1R的相互作用可用作肺腺癌中的预后指标。

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