TLR4/CD14 Variants-Related Serologic and Immunologic Dys-Regulations Predict Severe Sepsis in Febrile De-Compensated Cirrhotic Patients

Genetic variants and dysfunctional monocyte had been reported to be associated with infection susceptibility in advanced cirrhotic patients. This study aims to explore genetic predictive markers and relevant immune dysfunction that contributed to severe sepsis in febrile acute de-compensated cirrhot...

Descripción completa

Detalles Bibliográficos
Autores principales: Fan, Wen-Chien, Liu, Chih-Wei, Ou, Shuo-Ming, Huang, Chia-Chang, Li, Tzu-Hao, Lee, Kuei-Chuan, Huang, Shiang-Fen, Yang, Ying-Ying, Hsieh, Yun-Cheng, Hsieh, Shie-Liang, Hou, Ming-Chih, Lin, Han-Chieh
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5115743/
https://www.ncbi.nlm.nih.gov/pubmed/27861595
http://dx.doi.org/10.1371/journal.pone.0166458
_version_ 1782468562702565376
author Fan, Wen-Chien
Liu, Chih-Wei
Ou, Shuo-Ming
Huang, Chia-Chang
Li, Tzu-Hao
Lee, Kuei-Chuan
Huang, Shiang-Fen
Yang, Ying-Ying
Hsieh, Yun-Cheng
Hsieh, Shie-Liang
Hou, Ming-Chih
Lin, Han-Chieh
author_facet Fan, Wen-Chien
Liu, Chih-Wei
Ou, Shuo-Ming
Huang, Chia-Chang
Li, Tzu-Hao
Lee, Kuei-Chuan
Huang, Shiang-Fen
Yang, Ying-Ying
Hsieh, Yun-Cheng
Hsieh, Shie-Liang
Hou, Ming-Chih
Lin, Han-Chieh
author_sort Fan, Wen-Chien
collection PubMed
description Genetic variants and dysfunctional monocyte had been reported to be associated with infection susceptibility in advanced cirrhotic patients. This study aims to explore genetic predictive markers and relevant immune dysfunction that contributed to severe sepsis in febrile acute de-compensated cirrhotic patents. Polymorphism analysis of candidate genes was undergone in 108 febrile acute de-compensated cirrhotic patients and 121 healthy volunteers. Various plasma inflammatory/regulatory cytokines, proportion of classical (CD 16(-), phagocytic) and non-classical (CD16(+), inflammatory) monocytes, lipopolysaccharide (LPS)-stimulated toll-like receptor 4 (TLR4) and intracellular/extracellular cytokines on cultured non-classical monocytes, mCD14/HLA-DR expression and phagocytosis of classical monocytes were measured. For TLR4+896A/G variant allele carriers with severe sepsis, high plasma endotoxin/IL-10 inhibits HLA-DR expression and impaired phagocytosis were noted in their classical monocyte. In the same group, increased non-classical monocyte subset, enhanced LPS-stimulated TLR4 expression and TNFα/nitrite production, and systemic inflammation [high plasma soluble CD14 (sCD14) and total nitric oxide (NOx) levels] were noted. For CD14-159C/T variant allele carriers with severe sepsis, persist endotoxemia inhibited mCD14/HLA-DR expression and impaired phagocytosis of their classical monocyte. In the same group, increased non-classical monocyte subset up-regulated TLR4-NFκB-iNOS and p38MAPK pathway, stimulated TNFα/nitrite production and elicited systemic inflammation. In febrile acute de-compensated cirrhotic patients, TLR4+896A/G and CD14-159C/T polymorphisms-related non-classical and classical monocytes dysfunction resulted in increased severe sepsis risk. Malnutrition, high plasma endotoxin and sCD14 levels, single TLR4+896A/G or CD14-159C/T variant allele carriers and double variant allele carriers are significant predictive factors for the development of severe sepsis among them.
format Online
Article
Text
id pubmed-5115743
institution National Center for Biotechnology Information
language English
publishDate 2016
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-51157432016-12-08 TLR4/CD14 Variants-Related Serologic and Immunologic Dys-Regulations Predict Severe Sepsis in Febrile De-Compensated Cirrhotic Patients Fan, Wen-Chien Liu, Chih-Wei Ou, Shuo-Ming Huang, Chia-Chang Li, Tzu-Hao Lee, Kuei-Chuan Huang, Shiang-Fen Yang, Ying-Ying Hsieh, Yun-Cheng Hsieh, Shie-Liang Hou, Ming-Chih Lin, Han-Chieh PLoS One Research Article Genetic variants and dysfunctional monocyte had been reported to be associated with infection susceptibility in advanced cirrhotic patients. This study aims to explore genetic predictive markers and relevant immune dysfunction that contributed to severe sepsis in febrile acute de-compensated cirrhotic patents. Polymorphism analysis of candidate genes was undergone in 108 febrile acute de-compensated cirrhotic patients and 121 healthy volunteers. Various plasma inflammatory/regulatory cytokines, proportion of classical (CD 16(-), phagocytic) and non-classical (CD16(+), inflammatory) monocytes, lipopolysaccharide (LPS)-stimulated toll-like receptor 4 (TLR4) and intracellular/extracellular cytokines on cultured non-classical monocytes, mCD14/HLA-DR expression and phagocytosis of classical monocytes were measured. For TLR4+896A/G variant allele carriers with severe sepsis, high plasma endotoxin/IL-10 inhibits HLA-DR expression and impaired phagocytosis were noted in their classical monocyte. In the same group, increased non-classical monocyte subset, enhanced LPS-stimulated TLR4 expression and TNFα/nitrite production, and systemic inflammation [high plasma soluble CD14 (sCD14) and total nitric oxide (NOx) levels] were noted. For CD14-159C/T variant allele carriers with severe sepsis, persist endotoxemia inhibited mCD14/HLA-DR expression and impaired phagocytosis of their classical monocyte. In the same group, increased non-classical monocyte subset up-regulated TLR4-NFκB-iNOS and p38MAPK pathway, stimulated TNFα/nitrite production and elicited systemic inflammation. In febrile acute de-compensated cirrhotic patients, TLR4+896A/G and CD14-159C/T polymorphisms-related non-classical and classical monocytes dysfunction resulted in increased severe sepsis risk. Malnutrition, high plasma endotoxin and sCD14 levels, single TLR4+896A/G or CD14-159C/T variant allele carriers and double variant allele carriers are significant predictive factors for the development of severe sepsis among them. Public Library of Science 2016-11-18 /pmc/articles/PMC5115743/ /pubmed/27861595 http://dx.doi.org/10.1371/journal.pone.0166458 Text en © 2016 Fan et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Fan, Wen-Chien
Liu, Chih-Wei
Ou, Shuo-Ming
Huang, Chia-Chang
Li, Tzu-Hao
Lee, Kuei-Chuan
Huang, Shiang-Fen
Yang, Ying-Ying
Hsieh, Yun-Cheng
Hsieh, Shie-Liang
Hou, Ming-Chih
Lin, Han-Chieh
TLR4/CD14 Variants-Related Serologic and Immunologic Dys-Regulations Predict Severe Sepsis in Febrile De-Compensated Cirrhotic Patients
title TLR4/CD14 Variants-Related Serologic and Immunologic Dys-Regulations Predict Severe Sepsis in Febrile De-Compensated Cirrhotic Patients
title_full TLR4/CD14 Variants-Related Serologic and Immunologic Dys-Regulations Predict Severe Sepsis in Febrile De-Compensated Cirrhotic Patients
title_fullStr TLR4/CD14 Variants-Related Serologic and Immunologic Dys-Regulations Predict Severe Sepsis in Febrile De-Compensated Cirrhotic Patients
title_full_unstemmed TLR4/CD14 Variants-Related Serologic and Immunologic Dys-Regulations Predict Severe Sepsis in Febrile De-Compensated Cirrhotic Patients
title_short TLR4/CD14 Variants-Related Serologic and Immunologic Dys-Regulations Predict Severe Sepsis in Febrile De-Compensated Cirrhotic Patients
title_sort tlr4/cd14 variants-related serologic and immunologic dys-regulations predict severe sepsis in febrile de-compensated cirrhotic patients
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5115743/
https://www.ncbi.nlm.nih.gov/pubmed/27861595
http://dx.doi.org/10.1371/journal.pone.0166458
work_keys_str_mv AT fanwenchien tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT liuchihwei tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT oushuoming tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT huangchiachang tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT litzuhao tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT leekueichuan tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT huangshiangfen tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT yangyingying tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT hsiehyuncheng tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT hsiehshieliang tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT houmingchih tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients
AT linhanchieh tlr4cd14variantsrelatedserologicandimmunologicdysregulationspredictseveresepsisinfebriledecompensatedcirrhoticpatients

Ejemplares similares