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Mycobacterium tuberculosis associated with severe tuberculosis evades cytosolic surveillance systems and modulates IL-1β production
by
Simões-Costa, Luisa
, Vieira, Cristina P.
, Saraiva, Margarida
, Castro, António Gil
, Machado, Henrique
, Vieira, Jorge
, Sousa, Jeremy
, Gagneux, Sebastien
, Fernandes, Ana Isabel
, Ramos, Angélica
, Cá, Baltazar
, Bhatt, Apoorva
, Chiner-Oms, Álvaro
, Guimarães, João Tiago
, Barros, Leandro
, Singh, Albel
, Rodrigues, Pedro N. S.
, Bastos, Helder Novais
, Carvalho, Teresa
, Magalhães, Carlos
, Amorim, António
, Rodrigues, Fernando
, Maceiras, Ana Raquel
, Fonseca, Kaori L.
, Comas, Iñaki
, Pereira, Rui
, Veiga, Maria Isabel
, Osório, Nuno S.
in
13/106
/ 13/21
/ 38/91
/ 49
/ 631/250/2161
/ 631/250/255/1856
/ 692/420/254
/ Animals
/ Bacterial Proteins - genetics
/ Cells, Cultured
/ Cytokines
/ Cytokines - metabolism
/ Cytosol - immunology
/ Female
/ Genetic diversity
/ Genome, Bacterial - genetics
/ Host-pathogen interactions
/ Humanities and Social Sciences
/ Humans
/ IL-1β
/ Immune Evasion
/ Immune response
/ Immunomodulation
/ Inflammasomes
/ Inflammasomes - immunology
/ Interleukin-1beta - metabolism
/ Macrophages
/ Macrophages - immunology
/ Macrophages - microbiology
/ Male
/ Mice
/ multidisciplinary
/ Mutation
/ Mycobacterium tuberculosis
/ Mycobacterium tuberculosis - classification
/ Mycobacterium tuberculosis - genetics
/ Mycobacterium tuberculosis - isolation & purification
/ Mycobacterium tuberculosis - pathogenicity
/ Phylogeny
/ Polymorphism, Single Nucleotide
/ Science
/ Science (multidisciplinary)
/ Signal Transduction - immunology
/ Strains (organisms)
/ Surveillance
/ Surveillance systems
/ Tuberculosis
/ Tuberculosis, Pulmonary - immunology
/ Tuberculosis, Pulmonary - microbiology
/ Virulence - genetics
2020
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Mycobacterium tuberculosis associated with severe tuberculosis evades cytosolic surveillance systems and modulates IL-1β production
by
Simões-Costa, Luisa
, Vieira, Cristina P.
, Saraiva, Margarida
, Castro, António Gil
, Machado, Henrique
, Vieira, Jorge
, Sousa, Jeremy
, Gagneux, Sebastien
, Fernandes, Ana Isabel
, Ramos, Angélica
, Cá, Baltazar
, Bhatt, Apoorva
, Chiner-Oms, Álvaro
, Guimarães, João Tiago
, Barros, Leandro
, Singh, Albel
, Rodrigues, Pedro N. S.
, Bastos, Helder Novais
, Carvalho, Teresa
, Magalhães, Carlos
, Amorim, António
, Rodrigues, Fernando
, Maceiras, Ana Raquel
, Fonseca, Kaori L.
, Comas, Iñaki
, Pereira, Rui
, Veiga, Maria Isabel
, Osório, Nuno S.
in
13/106
/ 13/21
/ 38/91
/ 49
/ 631/250/2161
/ 631/250/255/1856
/ 692/420/254
/ Animals
/ Bacterial Proteins - genetics
/ Cells, Cultured
/ Cytokines
/ Cytokines - metabolism
/ Cytosol - immunology
/ Female
/ Genetic diversity
/ Genome, Bacterial - genetics
/ Host-pathogen interactions
/ Humanities and Social Sciences
/ Humans
/ IL-1β
/ Immune Evasion
/ Immune response
/ Immunomodulation
/ Inflammasomes
/ Inflammasomes - immunology
/ Interleukin-1beta - metabolism
/ Macrophages
/ Macrophages - immunology
/ Macrophages - microbiology
/ Male
/ Mice
/ multidisciplinary
/ Mutation
/ Mycobacterium tuberculosis
/ Mycobacterium tuberculosis - classification
/ Mycobacterium tuberculosis - genetics
/ Mycobacterium tuberculosis - isolation & purification
/ Mycobacterium tuberculosis - pathogenicity
/ Phylogeny
/ Polymorphism, Single Nucleotide
/ Science
/ Science (multidisciplinary)
/ Signal Transduction - immunology
/ Strains (organisms)
/ Surveillance
/ Surveillance systems
/ Tuberculosis
/ Tuberculosis, Pulmonary - immunology
/ Tuberculosis, Pulmonary - microbiology
/ Virulence - genetics
2020
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Mycobacterium tuberculosis associated with severe tuberculosis evades cytosolic surveillance systems and modulates IL-1β production
by
Simões-Costa, Luisa
, Vieira, Cristina P.
, Saraiva, Margarida
, Castro, António Gil
, Machado, Henrique
, Vieira, Jorge
, Sousa, Jeremy
, Gagneux, Sebastien
, Fernandes, Ana Isabel
, Ramos, Angélica
, Cá, Baltazar
, Bhatt, Apoorva
, Chiner-Oms, Álvaro
, Guimarães, João Tiago
, Barros, Leandro
, Singh, Albel
, Rodrigues, Pedro N. S.
, Bastos, Helder Novais
, Carvalho, Teresa
, Magalhães, Carlos
, Amorim, António
, Rodrigues, Fernando
, Maceiras, Ana Raquel
, Fonseca, Kaori L.
, Comas, Iñaki
, Pereira, Rui
, Veiga, Maria Isabel
, Osório, Nuno S.
in
13/106
/ 13/21
/ 38/91
/ 49
/ 631/250/2161
/ 631/250/255/1856
/ 692/420/254
/ Animals
/ Bacterial Proteins - genetics
/ Cells, Cultured
/ Cytokines
/ Cytokines - metabolism
/ Cytosol - immunology
/ Female
/ Genetic diversity
/ Genome, Bacterial - genetics
/ Host-pathogen interactions
/ Humanities and Social Sciences
/ Humans
/ IL-1β
/ Immune Evasion
/ Immune response
/ Immunomodulation
/ Inflammasomes
/ Inflammasomes - immunology
/ Interleukin-1beta - metabolism
/ Macrophages
/ Macrophages - immunology
/ Macrophages - microbiology
/ Male
/ Mice
/ multidisciplinary
/ Mutation
/ Mycobacterium tuberculosis
/ Mycobacterium tuberculosis - classification
/ Mycobacterium tuberculosis - genetics
/ Mycobacterium tuberculosis - isolation & purification
/ Mycobacterium tuberculosis - pathogenicity
/ Phylogeny
/ Polymorphism, Single Nucleotide
/ Science
/ Science (multidisciplinary)
/ Signal Transduction - immunology
/ Strains (organisms)
/ Surveillance
/ Surveillance systems
/ Tuberculosis
/ Tuberculosis, Pulmonary - immunology
/ Tuberculosis, Pulmonary - microbiology
/ Virulence - genetics
2020
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Mycobacterium tuberculosis associated with severe tuberculosis evades cytosolic surveillance systems and modulates IL-1β production
Journal Article
Mycobacterium tuberculosis associated with severe tuberculosis evades cytosolic surveillance systems and modulates IL-1β production
2020
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Overview
Genetic diversity of
Mycobacterium tuberculosis
affects immune responses and clinical outcomes of tuberculosis (TB). However, how bacterial diversity orchestrates immune responses to direct distinct TB severities is unknown. Here we study 681 patients with pulmonary TB and show that
M
.
tuberculosis
isolates from cases with mild disease consistently induce robust cytokine responses in macrophages across multiple donors. By contrast, bacteria from patients with severe TB do not do so. Secretion of IL-1β is a good surrogate of the differences observed, and thus to classify strains as probable drivers of different TB severities. Furthermore, we demonstrate that
M
.
tuberculosis
isolates that induce low levels of IL-1β production can evade macrophage cytosolic surveillance systems, including cGAS and the inflammasome. Isolates exhibiting this evasion strategy carry candidate mutations, generating sigA recognition boxes or affecting components of the ESX-1 secretion system. Therefore, we provide evidence that
M
.
tuberculosis
strains manipulate host-pathogen interactions to drive variable TB severities.
Some strains of
Mycobacterium tuberculosis
seem to be able to avoid host defense systems. Here the authors stratify patients by severity of tuberculosis and find correlations with the level of IL-1β production by macrophages exposed to these isolates.
Publisher
Nature Publishing Group UK,Nature Publishing Group,Nature Portfolio
Subject
/ 13/21
/ 38/91
/ 49
/ Animals
/ Bacterial Proteins - genetics
/ Female
/ Genome, Bacterial - genetics
/ Humanities and Social Sciences
/ Humans
/ IL-1β
/ Interleukin-1beta - metabolism
/ Male
/ Mice
/ Mutation
/ Mycobacterium tuberculosis - classification
/ Mycobacterium tuberculosis - genetics
/ Mycobacterium tuberculosis - isolation & purification
/ Mycobacterium tuberculosis - pathogenicity
/ Polymorphism, Single Nucleotide
/ Science
/ Signal Transduction - immunology
/ Tuberculosis, Pulmonary - immunology
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