期刊论文详细信息
Endocrine Journal
Genomic evidence of reactive oxygen species elevation in papillary thyroid carcinoma with Hashimoto thyroiditis
Jihan Yu1  Eun Kyung Paik1  Ju Han Kim1  Kyu Eun Lee2  Sang Yun Ha1  Ji Hyun Chang1  Woo Seung Lee1  Ji-Youn Sung1  Sang Hyuk Kwak1  Su-Jin Kim2  Ji Yeon Park1  Jin Wook Yi1  Jo-Heon Kim1 
[1] Division of Biomedical Informatics, Seoul National University College of Medicine, Seoul, Korea;Department of Surgery, Seoul National University Hospital and College of Medicine, Seoul, Korea
关键词: Reactive oxygen species;    Thyroid cancer;    Hashimoto thyroiditis;    Gene expression;    Bioinformatics;   
DOI  :  10.1507/endocrj.EJ15-0234
学科分类:内分泌与代谢学
来源: Japan Endocrine Society
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【 摘 要 】

References(39)Cited-By(1)Elevated levels of reactive oxygen species (ROS) have been proposed as a risk factor for the development of papillary thyroid carcinoma (PTC) in patients with Hashimoto thyroiditis (HT).However, it has yet to be proven that the total levels of ROS are sufficiently increased to contribute to carcinogenesis.We hypothesized that if the ROS levels were increased in HT, ROS-related genes would also be differently expressed in PTC with HT.To find differentially expressed genes (DEGs) we analyzed data from the Cancer Genomic Atlas, gene expression data from RNA sequencing: 33 from normal thyroid tissue, 232 from PTC without HT, and 60 from PTC with HT.We prepared 402 ROS-related genes from three gene sets by genomic database searching.We also analyzed a public microarray data to validate our results.Thirty-three ROS related genes were up-regulated in PTC with HT, whereas there were only nine genes in PTC without HT (Chi-square p-value < 0.001).Mean log2 fold changes of up-regulated genes was 0.562 in HT group and 0.252 in PTC without HT group (t-test p-value = 0.001).In microarray data analysis, 12 of 32 ROS-related genes showed the same differential expression pattern with statistical significance.In gene ontology analysis, up-regulated ROS-related genes were related with ROS metabolism and apoptosis.Immune function-related and carcinogenesis-related gene sets were enriched only in HT group in Gene Set Enrichment Analysis.Our results suggested that ROS levels may be increased in PTC with HT.Increased levels of ROS may contribute to PTC development in patients with HT.

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