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A multi-omics investigation of the molecular characteristics and classification of six metabolic syndrome relevant diseases

Metabolic syndrome (MTS) is a cluster of concurrent metabolic abnormal conditions. MTS and its component metabolic diseases are heterogeneous and closely related, making their relationships complicated, thus hindering precision treatment. Methods: We collected seven groups of samples (group a: healt...

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Autores principales: Chen, Di, Zhao, Xinjie, Sui, Zhigang, Niu, Huan, Chen, Luonan, Hu, Cheng, Xuan, Qiuhui, Hou, Xuhong, Zhang, Rong, Zhou, Lina, Li, Yanli, Yuan, Huiming, Zhang, Yukui, Wu, Jiarui, Zhang, Lihua, Wu, Ren'an, Piao, Hai-Long, Xu, Guowang, Jia, Weiping
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7019171/
https://www.ncbi.nlm.nih.gov/pubmed/32089734
http://dx.doi.org/10.7150/thno.41106
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author Chen, Di
Zhao, Xinjie
Sui, Zhigang
Niu, Huan
Chen, Luonan
Hu, Cheng
Xuan, Qiuhui
Hou, Xuhong
Zhang, Rong
Zhou, Lina
Li, Yanli
Yuan, Huiming
Zhang, Yukui
Wu, Jiarui
Zhang, Lihua
Wu, Ren'an
Piao, Hai-Long
Xu, Guowang
Jia, Weiping
author_facet Chen, Di
Zhao, Xinjie
Sui, Zhigang
Niu, Huan
Chen, Luonan
Hu, Cheng
Xuan, Qiuhui
Hou, Xuhong
Zhang, Rong
Zhou, Lina
Li, Yanli
Yuan, Huiming
Zhang, Yukui
Wu, Jiarui
Zhang, Lihua
Wu, Ren'an
Piao, Hai-Long
Xu, Guowang
Jia, Weiping
author_sort Chen, Di
collection PubMed
description Metabolic syndrome (MTS) is a cluster of concurrent metabolic abnormal conditions. MTS and its component metabolic diseases are heterogeneous and closely related, making their relationships complicated, thus hindering precision treatment. Methods: We collected seven groups of samples (group a: healthy individuals; group b: obesity; group c: MTS; group d: hyperglycemia, group e: hypertension, group f: hyperlipidemia; group g: type II diabetes, n=7 for each group). We examined the molecular characteristics of each sample by metabolomic, proteomic and peptidomic profiling analysis. The differential molecules (including metabolites, proteins and peptides) between each disease group and the healthy group were recognized by statistical analyses. Furthermore, a two-step clustering workflow which combines multi-omics and clinical information was used to redefine molecularly and clinically differential groups. Meanwhile, molecular, clinical, network and pathway based analyses were used to identify the group-specific biological features. Results: Both shared and disease-specific molecular profiles among the six types of diseases were identified. Meanwhile, the patients were stratified into three distinct groups which were different from original disease definitions but presented significant differences in glucose and lipid metabolism (Group 1: relatively favorable metabolic conditions; Group 2: severe dyslipidemia; Group 3: dysregulated insulin and glucose). Group specific biological signatures were also systematically described. The dyslipidemia group showed higher levels in multiple lipid metabolites like phosphatidylserine and phosphatidylcholine, and showed significant up-regulations in lipid and amino acid metabolism pathways. The glucose dysregulated group showed higher levels in many polypeptides from proteins contributing to immune response. The another group, with better glucose/lipid metabolism ability, showed higher levels in lipid regulating enzymes like the lecithin cholesterol acyltransferase and proteins involved in complement and coagulation cascades. Conclusions: This multi-omics based study provides a general view of the complex relationships and an alternative classification for various metabolic diseases where the cross-talk or compensatory mechanism between the immune and metabolism systems plays a critical role.
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spelling pubmed-70191712020-02-23 A multi-omics investigation of the molecular characteristics and classification of six metabolic syndrome relevant diseases Chen, Di Zhao, Xinjie Sui, Zhigang Niu, Huan Chen, Luonan Hu, Cheng Xuan, Qiuhui Hou, Xuhong Zhang, Rong Zhou, Lina Li, Yanli Yuan, Huiming Zhang, Yukui Wu, Jiarui Zhang, Lihua Wu, Ren'an Piao, Hai-Long Xu, Guowang Jia, Weiping Theranostics Research Paper Metabolic syndrome (MTS) is a cluster of concurrent metabolic abnormal conditions. MTS and its component metabolic diseases are heterogeneous and closely related, making their relationships complicated, thus hindering precision treatment. Methods: We collected seven groups of samples (group a: healthy individuals; group b: obesity; group c: MTS; group d: hyperglycemia, group e: hypertension, group f: hyperlipidemia; group g: type II diabetes, n=7 for each group). We examined the molecular characteristics of each sample by metabolomic, proteomic and peptidomic profiling analysis. The differential molecules (including metabolites, proteins and peptides) between each disease group and the healthy group were recognized by statistical analyses. Furthermore, a two-step clustering workflow which combines multi-omics and clinical information was used to redefine molecularly and clinically differential groups. Meanwhile, molecular, clinical, network and pathway based analyses were used to identify the group-specific biological features. Results: Both shared and disease-specific molecular profiles among the six types of diseases were identified. Meanwhile, the patients were stratified into three distinct groups which were different from original disease definitions but presented significant differences in glucose and lipid metabolism (Group 1: relatively favorable metabolic conditions; Group 2: severe dyslipidemia; Group 3: dysregulated insulin and glucose). Group specific biological signatures were also systematically described. The dyslipidemia group showed higher levels in multiple lipid metabolites like phosphatidylserine and phosphatidylcholine, and showed significant up-regulations in lipid and amino acid metabolism pathways. The glucose dysregulated group showed higher levels in many polypeptides from proteins contributing to immune response. The another group, with better glucose/lipid metabolism ability, showed higher levels in lipid regulating enzymes like the lecithin cholesterol acyltransferase and proteins involved in complement and coagulation cascades. Conclusions: This multi-omics based study provides a general view of the complex relationships and an alternative classification for various metabolic diseases where the cross-talk or compensatory mechanism between the immune and metabolism systems plays a critical role. Ivyspring International Publisher 2020-01-12 /pmc/articles/PMC7019171/ /pubmed/32089734 http://dx.doi.org/10.7150/thno.41106 Text en © The author(s) This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Chen, Di
Zhao, Xinjie
Sui, Zhigang
Niu, Huan
Chen, Luonan
Hu, Cheng
Xuan, Qiuhui
Hou, Xuhong
Zhang, Rong
Zhou, Lina
Li, Yanli
Yuan, Huiming
Zhang, Yukui
Wu, Jiarui
Zhang, Lihua
Wu, Ren'an
Piao, Hai-Long
Xu, Guowang
Jia, Weiping
A multi-omics investigation of the molecular characteristics and classification of six metabolic syndrome relevant diseases
title A multi-omics investigation of the molecular characteristics and classification of six metabolic syndrome relevant diseases
title_full A multi-omics investigation of the molecular characteristics and classification of six metabolic syndrome relevant diseases
title_fullStr A multi-omics investigation of the molecular characteristics and classification of six metabolic syndrome relevant diseases
title_full_unstemmed A multi-omics investigation of the molecular characteristics and classification of six metabolic syndrome relevant diseases
title_short A multi-omics investigation of the molecular characteristics and classification of six metabolic syndrome relevant diseases
title_sort multi-omics investigation of the molecular characteristics and classification of six metabolic syndrome relevant diseases
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7019171/
https://www.ncbi.nlm.nih.gov/pubmed/32089734
http://dx.doi.org/10.7150/thno.41106
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