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Multi-Omics Analysis of SOX4, SOX11, and SOX12 Expression and the Associated Pathways in Human Cancers
by
Gil, Minchan
, Cho, Ssang-Goo
, Seok, Jaekwon
, Dayem, Ahmed Abdal
, Saha, Subbroto Kumar
in
Cell cycle
/ Datasets
/ Immune system
/ Liver cancer
/ Mitosis
/ Mutation
/ Ovarian cancer
/ Phylogeny
/ Precision medicine
/ Sarcoma
/ Sox protein
/ Transcription factors
/ Tumorigenesis
2021
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Multi-Omics Analysis of SOX4, SOX11, and SOX12 Expression and the Associated Pathways in Human Cancers
by
Gil, Minchan
, Cho, Ssang-Goo
, Seok, Jaekwon
, Dayem, Ahmed Abdal
, Saha, Subbroto Kumar
in
Cell cycle
/ Datasets
/ Immune system
/ Liver cancer
/ Mitosis
/ Mutation
/ Ovarian cancer
/ Phylogeny
/ Precision medicine
/ Sarcoma
/ Sox protein
/ Transcription factors
/ Tumorigenesis
2021
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Multi-Omics Analysis of SOX4, SOX11, and SOX12 Expression and the Associated Pathways in Human Cancers
by
Gil, Minchan
, Cho, Ssang-Goo
, Seok, Jaekwon
, Dayem, Ahmed Abdal
, Saha, Subbroto Kumar
in
Cell cycle
/ Datasets
/ Immune system
/ Liver cancer
/ Mitosis
/ Mutation
/ Ovarian cancer
/ Phylogeny
/ Precision medicine
/ Sarcoma
/ Sox protein
/ Transcription factors
/ Tumorigenesis
2021
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Multi-Omics Analysis of SOX4, SOX11, and SOX12 Expression and the Associated Pathways in Human Cancers
Journal Article
Multi-Omics Analysis of SOX4, SOX11, and SOX12 Expression and the Associated Pathways in Human Cancers
2021
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Overview
The Sry-related HMG BOX (SOX) gene family encodes transcription factors containing highly conserved high-mobility group domains that bind to the minor groove in DNA. Although some SOX genes are known to be associated with tumorigenesis and cancer progression, their expression and prognostic value have not been systematically studied. We performed multi-omic analysis to investigate the expression of SOX genes in human cancers. Expression and phylogenetic tree analyses of the SOX gene family revealed that the expression of three closely related SOX members, SOX4, SOX11, and SOX12, was increased in multiple cancers. Expression, mutation, and alteration of the three SOX members were evaluated using the Oncomine and cBioPortal databases, and the correlation between these genes and clinical outcomes in various cancers was examined using the Kaplan–Meier, PrognoScan, and R2 database analyses. The genes commonly correlated with the three SOX members were categorized in key pathways related to the cell cycle, mitosis, immune system, and cancer progression in liver cancer and sarcoma. Additionally, functional protein partners with three SOX proteins and their probable signaling pathways were explored using the STRING database. This study suggests the prognostic value of the expression of three SOX genes and their associated pathways in various human cancers.
Publisher
MDPI AG,MDPI
Subject
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