The diagnostic significance of integrating m6A modification and immune microenvironment features based on bioinformatic investigation in aortic dissection

PURPOSE: The aim of this study was to investigate the role of m6A modification and the immune microenvironment (IME) features in aortic dissection (AD) and establish a clinical diagnostic model for AD based on m6A and IME factors. METHODS: GSE52093, GSE98770, GSE147026, GSE153434, and GSE107844 data...

Descripción completa

Detalles Bibliográficos
Autores principales: Guo, Ruiming, Dai, Jia, Xu, Hao, Zang, Suhua, Zhang, Liang, Ma, Ning, Zhang, Xin, Zhao, Lixuan, Luo, Hong, Liu, Donghai, Zhang, Jian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Cardiovascular Medicine
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9464924/
https://www.ncbi.nlm.nih.gov/pubmed/36105536
http://dx.doi.org/10.3389/fcvm.2022.948002
_version_ 1784787679210110976
author Guo, Ruiming
Dai, Jia
Xu, Hao
Zang, Suhua
Zhang, Liang
Ma, Ning
Zhang, Xin
Zhao, Lixuan
Luo, Hong
Liu, Donghai
Zhang, Jian
author_facet Guo, Ruiming
Dai, Jia
Xu, Hao
Zang, Suhua
Zhang, Liang
Ma, Ning
Zhang, Xin
Zhao, Lixuan
Luo, Hong
Liu, Donghai
Zhang, Jian
author_sort Guo, Ruiming
collection PubMed
description PURPOSE: The aim of this study was to investigate the role of m6A modification and the immune microenvironment (IME) features in aortic dissection (AD) and establish a clinical diagnostic model for AD based on m6A and IME factors. METHODS: GSE52093, GSE98770, GSE147026, GSE153434, and GSE107844 datasets were downloaded from the GEO database. The expression of 21 m6A genes including m6A writers, erasers, readers, and immune cell infiltrates was analyzed in AD and healthy samples by differential analysis and ssGSEA method, respectively. Both correlation analyses between m6A genes and immune cells were conducted by Pearson and Spearman analysis. XGboost was used to dissect the major m6A genes with significant influences on AD. AD samples were classified into two subgroups via consensus cluster and principal component analysis (PCA) analysis, respectively. Among each subgroup, paramount IME features were evaluated. Random forest (RF) was used to figure out key genes from AD and healthy shared differentially expressed genes (DEGs) and two AD subgroups after gene ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) analysis. Finally, we constructed an AD diagnostic model combining important m6A regulatory genes and assessed its efficacy. RESULTS: Among 21 m6A genes, WTAP, HNRNPC, and FTO were upregulated in AD samples, while IGF2BP1 was downregulated compared with healthy samples. Immune cell infiltrating analysis revealed that YTHDF1 was positively correlated with γδT cell level, while FTO was negatively correlated with activated CD4+ T cell abundance. FTO and IGF2BP1 were identified to be crucial genes that facilitate AD development according to the XGboost algorithm. Notably, patients with AD could be classified into two subgroups among which 21 m6A gene expression profiles and IME features differ from each other via consensus cluster analysis. The RF identified SYNC and MAPK1IP1L as the crucial genes from common 657 shared common genes in 1,141 DEGs between high and low m6A scores of AD groups. Interestingly, the AD diagnostic model coordinating SYNC and MAPK1IP1L with FTO and IGF2BP1 performed well in distinguishing AD samples. CONCLUSION: This study indicated that FTO and IGF2BP1 were involved in the IME of AD. Integrating FTO and IGF2BP1 and MAPK1IP1L key genes in AD with a high m6A level context would provide clues for forthcoming AD diagnosis and therapy.
format Online
Article
Text
id pubmed-9464924
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-94649242022-09-13 The diagnostic significance of integrating m6A modification and immune microenvironment features based on bioinformatic investigation in aortic dissection Guo, Ruiming Dai, Jia Xu, Hao Zang, Suhua Zhang, Liang Ma, Ning Zhang, Xin Zhao, Lixuan Luo, Hong Liu, Donghai Zhang, Jian Front Cardiovasc Med Cardiovascular Medicine PURPOSE: The aim of this study was to investigate the role of m6A modification and the immune microenvironment (IME) features in aortic dissection (AD) and establish a clinical diagnostic model for AD based on m6A and IME factors. METHODS: GSE52093, GSE98770, GSE147026, GSE153434, and GSE107844 datasets were downloaded from the GEO database. The expression of 21 m6A genes including m6A writers, erasers, readers, and immune cell infiltrates was analyzed in AD and healthy samples by differential analysis and ssGSEA method, respectively. Both correlation analyses between m6A genes and immune cells were conducted by Pearson and Spearman analysis. XGboost was used to dissect the major m6A genes with significant influences on AD. AD samples were classified into two subgroups via consensus cluster and principal component analysis (PCA) analysis, respectively. Among each subgroup, paramount IME features were evaluated. Random forest (RF) was used to figure out key genes from AD and healthy shared differentially expressed genes (DEGs) and two AD subgroups after gene ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) analysis. Finally, we constructed an AD diagnostic model combining important m6A regulatory genes and assessed its efficacy. RESULTS: Among 21 m6A genes, WTAP, HNRNPC, and FTO were upregulated in AD samples, while IGF2BP1 was downregulated compared with healthy samples. Immune cell infiltrating analysis revealed that YTHDF1 was positively correlated with γδT cell level, while FTO was negatively correlated with activated CD4+ T cell abundance. FTO and IGF2BP1 were identified to be crucial genes that facilitate AD development according to the XGboost algorithm. Notably, patients with AD could be classified into two subgroups among which 21 m6A gene expression profiles and IME features differ from each other via consensus cluster analysis. The RF identified SYNC and MAPK1IP1L as the crucial genes from common 657 shared common genes in 1,141 DEGs between high and low m6A scores of AD groups. Interestingly, the AD diagnostic model coordinating SYNC and MAPK1IP1L with FTO and IGF2BP1 performed well in distinguishing AD samples. CONCLUSION: This study indicated that FTO and IGF2BP1 were involved in the IME of AD. Integrating FTO and IGF2BP1 and MAPK1IP1L key genes in AD with a high m6A level context would provide clues for forthcoming AD diagnosis and therapy. Frontiers Media S.A. 2022-08-29 /pmc/articles/PMC9464924/ /pubmed/36105536 http://dx.doi.org/10.3389/fcvm.2022.948002 Text en Copyright © 2022 Guo, Dai, Xu, Zang, Zhang, Ma, Zhang, Zhao, Luo, Liu and Zhang. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cardiovascular Medicine
Guo, Ruiming
Dai, Jia
Xu, Hao
Zang, Suhua
Zhang, Liang
Ma, Ning
Zhang, Xin
Zhao, Lixuan
Luo, Hong
Liu, Donghai
Zhang, Jian
The diagnostic significance of integrating m6A modification and immune microenvironment features based on bioinformatic investigation in aortic dissection
title The diagnostic significance of integrating m6A modification and immune microenvironment features based on bioinformatic investigation in aortic dissection
title_full The diagnostic significance of integrating m6A modification and immune microenvironment features based on bioinformatic investigation in aortic dissection
title_fullStr The diagnostic significance of integrating m6A modification and immune microenvironment features based on bioinformatic investigation in aortic dissection
title_full_unstemmed The diagnostic significance of integrating m6A modification and immune microenvironment features based on bioinformatic investigation in aortic dissection
title_short The diagnostic significance of integrating m6A modification and immune microenvironment features based on bioinformatic investigation in aortic dissection
title_sort diagnostic significance of integrating m6a modification and immune microenvironment features based on bioinformatic investigation in aortic dissection
topic Cardiovascular Medicine
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9464924/
https://www.ncbi.nlm.nih.gov/pubmed/36105536
http://dx.doi.org/10.3389/fcvm.2022.948002
work_keys_str_mv AT guoruiming thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT daijia thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT xuhao thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zangsuhua thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zhangliang thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT maning thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zhangxin thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zhaolixuan thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT luohong thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT liudonghai thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zhangjian thediagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT guoruiming diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT daijia diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT xuhao diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zangsuhua diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zhangliang diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT maning diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zhangxin diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zhaolixuan diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT luohong diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT liudonghai diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection
AT zhangjian diagnosticsignificanceofintegratingm6amodificationandimmunemicroenvironmentfeaturesbasedonbioinformaticinvestigationinaorticdissection

Ejemplares similares