Host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.

Host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.

Melioidosis (Burkholderia pseudomallei infection) is a common cause of community-acquired sepsis in Northeast Thailand and northern Australia. B. pseudomallei is a soil saprophyte endemic to Southeast Asia and northern Australia. The clinical presentation of melioidosis may mimic tuberculosis (both...

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Main Authors: Gavin C K W Koh, M Fernanda Schreiber, Ruben Bautista, Rapeephan R Maude, Susanna Dunachie, Direk Limmathurotsakul, Nicholas P J Day, Gordon Dougan, Sharon J Peacock
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23383015/pdf/?tool=EBI
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spelling doaj-ffe53b43f87e44d0b91dc40b9f535cd72021-03-03T20:25:06ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0181e5496110.1371/journal.pone.0054961Host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.Gavin C K W KohM Fernanda SchreiberRuben BautistaRapeephan R MaudeSusanna DunachieDirek LimmathurotsakulNicholas P J DayGordon DouganSharon J PeacockMelioidosis (Burkholderia pseudomallei infection) is a common cause of community-acquired sepsis in Northeast Thailand and northern Australia. B. pseudomallei is a soil saprophyte endemic to Southeast Asia and northern Australia. The clinical presentation of melioidosis may mimic tuberculosis (both cause chronic suppurative lesions unresponsive to conventional antibiotics and both commonly affect the lungs). The two diseases have overlapping risk profiles (e.g., diabetes, corticosteroid use), and both B. pseudomallei and Mycobacterium tuberculosis are intracellular pathogens. There are however important differences: the majority of melioidosis cases are acute, not chronic, and present with severe sepsis and a mortality rate that approaches 50% despite appropriate antimicrobial therapy. By contrast, tuberculosis is characteristically a chronic illness with mortality <2% with appropriate antimicrobial chemotherapy. We examined the gene expression profiles of total peripheral leukocytes in two cohorts of patients, one with acute melioidosis (30 patients and 30 controls) and another with tuberculosis (20 patients and 24 controls). Interferon-mediated responses dominate the host response to both infections, and both type 1 and type 2 interferon responses are important. An 86-gene signature previously thought to be specific for tuberculosis is also found in melioidosis. We conclude that the host responses to melioidosis and to tuberculosis are similar: both are dominated by interferon-signalling pathways and this similarity means gene expression signatures from whole blood do not distinguish between these two diseases.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23383015/pdf/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Gavin C K W Koh
M Fernanda Schreiber
Ruben Bautista
Rapeephan R Maude
Susanna Dunachie
Direk Limmathurotsakul
Nicholas P J Day
Gordon Dougan
Sharon J Peacock
spellingShingle Gavin C K W Koh
M Fernanda Schreiber
Ruben Bautista
Rapeephan R Maude
Susanna Dunachie
Direk Limmathurotsakul
Nicholas P J Day
Gordon Dougan
Sharon J Peacock
Host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.
PLoS ONE
author_facet Gavin C K W Koh
M Fernanda Schreiber
Ruben Bautista
Rapeephan R Maude
Susanna Dunachie
Direk Limmathurotsakul
Nicholas P J Day
Gordon Dougan
Sharon J Peacock
author_sort Gavin C K W Koh
title Host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.
title_short Host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.
title_full Host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.
title_fullStr Host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.
title_full_unstemmed Host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.
title_sort host responses to melioidosis and tuberculosis are both dominated by interferon-mediated signaling.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Melioidosis (Burkholderia pseudomallei infection) is a common cause of community-acquired sepsis in Northeast Thailand and northern Australia. B. pseudomallei is a soil saprophyte endemic to Southeast Asia and northern Australia. The clinical presentation of melioidosis may mimic tuberculosis (both cause chronic suppurative lesions unresponsive to conventional antibiotics and both commonly affect the lungs). The two diseases have overlapping risk profiles (e.g., diabetes, corticosteroid use), and both B. pseudomallei and Mycobacterium tuberculosis are intracellular pathogens. There are however important differences: the majority of melioidosis cases are acute, not chronic, and present with severe sepsis and a mortality rate that approaches 50% despite appropriate antimicrobial therapy. By contrast, tuberculosis is characteristically a chronic illness with mortality <2% with appropriate antimicrobial chemotherapy. We examined the gene expression profiles of total peripheral leukocytes in two cohorts of patients, one with acute melioidosis (30 patients and 30 controls) and another with tuberculosis (20 patients and 24 controls). Interferon-mediated responses dominate the host response to both infections, and both type 1 and type 2 interferon responses are important. An 86-gene signature previously thought to be specific for tuberculosis is also found in melioidosis. We conclude that the host responses to melioidosis and to tuberculosis are similar: both are dominated by interferon-signalling pathways and this similarity means gene expression signatures from whole blood do not distinguish between these two diseases.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23383015/pdf/?tool=EBI
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