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题名

Comprehensive Analysis of the Transcriptome-wide m6A Methylome in Lung Adenocarcinoma by MeRIP Sequencing

作者
通讯作者Wang,Yukun
发表日期
2022-07-11
DOI
发表期刊
ISSN
2234-943X
卷号12
摘要

N6-methyladenosine (m6A) is the most abundant internal modification on eukaryotic mRNAs. There is increasing evidence that m6A plays a key role in tumor progression, so it is important to analyze m6A modifications within the transcriptome-wide in lung adenocarcinoma (LUAD). Three pairs of LUAD samples and tumor-adjacent normal tissues were obtained from the South University of Science and Technology Hospital. And then methylated RNA immunoprecipitation sequencing (MeRIP-seq) and RNA sequencing (RNA-seq) were used to identify differential m6A modifications between tumor and tumor-adjacent normal tissues. We identified 4041 aberrant m6A peaks, of which 1192 m6A peaks were upregulated and 2849 m6A peaks downregulated. It was found that genes with the dysregulated m6A peaks were enriched in the pathways in cancer, Rap1 signaling pathway, and insulin resistance. Additionally, 612 genes with abnormal regulation of m6A peaks and RNA expression were identified by combining MeRIP-seq and RNA-seq data. Through KEGG analysis, the 612 genes were enriched in cancer-related signaling pathways, such as the cGMP-PKG signaling pathway, and the Rap1 signaling pathway. What's more, GSEA enrichment analysis showed these genes were enriched in cell cycle phase transition, cell division, cellular response to DNA damage stimulus, and chromosome organization. To further explore the relationship between differential m6A modified genes and clinical parameters of LUAD patients, we searched The Cancer Genome Atlas (TCGA) and identified 2 genes (FCRL5 and GPRIN1) that were associated with the prognosis and diagnosis of LUAD patients. Furthermore, we found a positive correlation between GPRIN1 and m6A reader YTHDF1 in the GEPIA2 database. It was verified that YTHDF1 binds to GPRIN1 mRNA and regulates its expression. Our study results suggest that m6A modification plays important role in the progression and prognosis of LUAD and maybe a potential new therapeutic target for LUAD patients in the future.

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语种
英语
学校署名
第一 ; 通讯
WOS研究方向
Oncology
WOS类目
Oncology
WOS记录号
WOS:000832695500001
出版者
Scopus记录号
2-s2.0-85134657163
来源库
Web of Science
引用统计
被引频次[WOS]:3
成果类型期刊论文
条目标识符http://sustech.caswiz.com/handle/2SGJ60CL/359556
专题南方科技大学医学院_药理学系
南方科技大学医学院
南方科技大学医院
作者单位
1.Department of Pharmacology,School of Medicine,Southern University of Science and Technology,Shenzhen,China
2.Medical Research Center,Southern University of Science and Technology Hospital,Shenzhen,China
3.Nutrition Department,Southern University of Science and Technology Hospital,Shenzhen,China
4.Department of Clinical Laboratory,Southern University of Science and Technology Hospital,Shenzhen,China
5.Department of Pharmacy,Southern University of Science and Technology Hospital,Shenzhen,China
第一作者单位药理学系;  南方科技大学医学院
通讯作者单位药理学系;  南方科技大学医学院;  南方科技大学医院
第一作者的第一单位药理学系;  南方科技大学医学院
推荐引用方式
GB/T 7714
Mao,Wenli,Yu,Qingzhen,Wang,Kefeng,et al. Comprehensive Analysis of the Transcriptome-wide m6A Methylome in Lung Adenocarcinoma by MeRIP Sequencing[J]. Frontiers in Oncology,2022,12.
APA
Mao,Wenli.,Yu,Qingzhen.,Wang,Kefeng.,Ma,Qiang.,Zheng,Yuxin.,...&Wang,Yukun.(2022).Comprehensive Analysis of the Transcriptome-wide m6A Methylome in Lung Adenocarcinoma by MeRIP Sequencing.Frontiers in Oncology,12.
MLA
Mao,Wenli,et al."Comprehensive Analysis of the Transcriptome-wide m6A Methylome in Lung Adenocarcinoma by MeRIP Sequencing".Frontiers in Oncology 12(2022).
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