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1. Collectin CL-LK Is a Novel Soluble Pattern Recognition Receptor for Mycobacterium tuberculosis

Author

Troegeler, Anthony, primary, Lugo-Villarino, Geanncarlo, additional, Hansen, Søren, additional, Rasolofo, Voahangy, additional, Henriksen, Maiken Lumby, additional, Mori, Kenichiro, additional, Ohtani, Katsuki, additional, Duval, Carine, additional, Mercier, Ingrid, additional, Bénard, Alan, additional, Nigou, Jérome, additional, Hudrisier, Denis, additional, Wakamiya, Nobutaka, additional, and Neyrolles, Olivier, additional

Published
2015
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7. Probing Host Pathogen Cross-Talk by Transcriptional Profiling of Both Mycobacterium tuberculosis and Infected Human Dendritic Cells and Macrophages

Author

Tailleux, Ludovic, primary, Waddell, Simon J., additional, Pelizzola, Mattia, additional, Mortellaro, Alessandra, additional, Withers, Michael, additional, Tanne, Antoine, additional, Castagnoli, Paola Ricciardi, additional, Gicquel, Brigitte, additional, Stoker, Neil G., additional, Butcher, Philip D., additional, Foti, Maria, additional, and Neyrolles, Olivier, additional

Published
2008
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8. Is Adipose Tissue a Place for Mycobacterium tuberculosis Persistence?

Author

Neyrolles, Olivier, primary, Hernández-Pando, Rogelio, additional, Pietri-Rouxel, France, additional, Fornès, Paul, additional, Tailleux, Ludovic, additional, Payán, Jorge Alberto Barrios, additional, Pivert, Elisabeth, additional, Bordat, Yann, additional, Aguilar, Diane, additional, Prévost, Marie-Christine, additional, Petit, Caroline, additional, and Gicquel, Brigitte, additional

Published
2006
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9. Evolutionary History of Contagious Bovine Pleuropneumonia Using Next Generation Sequencing of Mycoplasma mycoides Subsp. mycoides "Small Colony.".

Author

Dupuy, Virginie, Manso-Silván, Lucía, Barbe, Valérie, Thebault, Patricia, Dordet-Frisoni, Emilie, Citti, Christine, Poumarat, François, Blanchard, Alain, Breton, Marc, Sirand-Pugnet, Pascal, Thiaucourt, François, and Neyrolles, Olivier

Subjects
MYCOPLASMA, CONTAGIOUS bovine pleuropneumonia, EPIDEMIOLOGY, PHYLOGENY, BAYESIAN analysis
Abstract

Mycoplasma mycoides subsp. mycoides "Small Colony" (MmmSC) is responsible for contagious bovine pleuropneumonia (CBPP) in bovidae, a notifiable disease to the World Organization for Animal Health (OIE). Although its origin is not documented, the disease was known in Europe in 1773. It reached nearly world-wide distribution in the 19th century through the cattle trade and was eradicated from most continents by stamping-out policies. During the 20th century it persisted in Africa, and it reappeared sporadically in Southern Europe. Yet, classical epidemiology studies failed to explain the re-occurrence of the disease in Europe in the 1990s. The objectives of this study were to obtain a precise phylogeny of this pathogen, reconstruct its evolutionary history, estimate the date of its emergence, and determine the origin of the most recent European outbreaks. A large-scale genomic approach based on next-generation sequencing technologies was applied to construct a robust phylogeny of this extremely monomorphic pathogen by using 20 representative strains of various geographical origins. Sixty two polymorphic genes of the MmmSC core genome were selected, representing 83601 bp in total and resulting in 139 SNPs within the 20 strains. A robust phylogeny was obtained that identified a lineage specific to European strains; African strains were scattered in various branches. Bayesian analysis allowed dating the most recent common ancestor for MmmSC around 1700. The strains circulating in Sub-Saharan Africa today, however, were shown to descend from a strain that existed around 1810. MmmSC emerged recently, about 300 years ago, and was most probably exported from Europe to other continents, including Africa, during the 19th century. Its diversity is now greater in Africa, where CBPP is enzootic, than in Europe, where outbreaks occurred sporadically until 1999 and where CBPP may now be considered eradicated unless MmmSC remains undetected. [ABSTRACT FROM AUTHOR]

Published
2012
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10. Characterization of Clinical and Environmental Mycobacterium avium Spp. Isolates and Their Interaction with Human Macrophages.

Author

Guirado, Evelyn, Arcos, Jesus, Knaup, Rose, Reeder, Rebecca, Betz, Bret, Cotton, Cassie, Patel, Tejal, Pfaller, Stacy, Torrelles, Jordi B., Schlesinger, Larry S., and Neyrolles, Olivier

Subjects
MYCOBACTERIUM avium, MICROBIAL virulence, CONTAMINATION of drinking water, LIPOARABINOMANNANS, GLYCOLIPIDS, MACROPHAGES
Abstract

Members of the Mycobacterium avium complex (MAC) are naturally occurring bacteria in the environment. A link has been suggested between M. avium strains in drinking water and clinical isolates from infected individuals. There is a need to develop new screening methodologies that can identify specific virulence properties of M. avium isolates found in water that predict a level of risk to exposed individuals. In this work we have characterized 15 clinical and environmental M. avium spp. isolates provided by the US Environmental Protection Agency (EPA) to improve our understanding of the key processes involved in the binding, uptake and survival of these isolates in primary human macrophages. M. avium serovar 8 was predominant among the isolates studied. Different amounts and exposure of mannose-capped lipoarabinomannan (ManLAM) and glycopeptidolipids (GPLs), both major mycobacterial virulence factors, were found among the isolates studied. Reference clinical isolate 104 serovar 1 and clinical isolates 11 and 14 serovar 8 showed an increased association with macrophages. Serum opsonization increased the cell association and survival at 2 h post infection for all isolates. However, only the clinical isolates 104 and 3 among those tested showed an increased growth in primary human macrophages. The other isolates varied in their survival in these cells. Thus we conclude that the amounts of cell envelope ManLAM and GPL, as well as GPL serovar specificity are not the only important bacterial factors for dictating the early interactions of M. avium with human macrophages. [ABSTRACT FROM AUTHOR]

Published
2012
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11. Attenuated Mycobacterium tuberculosis SO2 Vaccine Candidate Is Unable to Induce Cell Death.

Author

Aporta, Adriana, Arbues, Ainhoa, Aguilo, Juan I., Monzon, Marta, Badiola, Juan J., De Martino, Alba, Ferrer, Nadia, Marinova, Dessislava, Anel, Alberto, Martin, Carlos, Pardo, Julian, and Neyrolles, Olivier

Subjects
MYCOBACTERIUM tuberculosis, APOPTOSIS, CELL death, MACROPHAGES, NATURAL immunity, TUBERCULOSIS vaccines
Abstract

It has been proposed that Mycobacterium tuberculosis virulent strains inhibit apoptosis and trigger cell death by necrosis of host macrophages to evade innate immunity, while non-virulent strains induce typical apoptosis activating a protective host response. As part of the characterization of a novel tuberculosis vaccine candidate, the M. tuberculosis phoP mutant SO2, we sought to evaluate its potential to induce host cell death. The parental M. tuberculosis MT103 strain and the current vaccine against tuberculosis Bacillus Calmette-Guérin (BCG) were used as comparators in mouse models in vitro and in vivo. Our data reveal that attenuated SO2 was unable to induce apoptotic events neither in mouse macrophages in vitro nor during lung infection in vivo. In contrast, virulent MT103 triggers typical apoptotic events with phosphatidylserine exposure, caspase-3 activation and nuclear condensation and fragmentation. BCG strain behaved like SO2 and did not induce apoptosis. A clonogenic survival assay confirmed that viability of BCG- or SO2-infected macrophages was unaffected. Our results discard apoptosis as the protective mechanism induced by SO2 vaccine and provide evidence for positive correlation between classical apoptosis induction and virulent strains, suggesting apoptosis as a possible virulence determinant during M. tuberculosis infection. [ABSTRACT FROM AUTHOR]

Published
2012
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12. The Role of Lipid Raft Aggregation in the Infection of Type II Pneumocytes by Mycobacterium tuberculosis.

Author

Fine-Coulson, Kari, Reaves, Barbara J., Karls, Russell K., Quinn, Frederick D., and Neyrolles, Olivier

Subjects
LIPID rafts, MYCOBACTERIUM tuberculosis, EPITHELIAL cells, TUBERCULOSIS research, LIPIDS, RESEARCH
Abstract

Dynamic, cholesterol-dense regions of the plasma membrane, known as lipid rafts (LR), have been observed to develop during and may be directly involved in infection of host cells by various pathogens. This study focuses on LR aggregation induced in alveolar epithelial cells during infection with Mycobacterium tuberculosis (Mtb) bacilli. We report dose- and time-dependent increases in LR aggregation after infection with three different strains at multiplicities of infection of 1, 10 and 100 from 2-24 hr post infection (hpi). Specific strain-dependent variations were noted among H37Rv, HN878 and CDC1551 with H37Rv producing the most significant increase from 15 aggregates per cell (APC) to 27 APC at MOI 100 during the 24 hour infection period. Treatment of epithelial cells with Culture Filtrate Protein, Total Lipids and gamma-irradiated whole cells from each strain failed to induce the level of LR aggregation observed during infection with any of the live strains. However, filtered supernatants from infected epithelial cells did produce comparable LR aggregation, suggesting a secreted mycobacterial product produced during infection of host cells is responsible for LR aggregation. Disruption of lipid raft formation prior to infection indicates that Mtb bacilli utilize LR aggregates for internalization and survival in epithelial cells. Treatment of host cells with the LR-disruption agent Filipin III produced a nearly 22% reduction in viable bacteria for strains H37Rv and HN878, and a 7% reduction for strain CDC1551 after 6 hpi. This study provides evidence for significant mycobacterial-induced changes in the plasma membrane of alveolar epithelial cells and that Mtb strains vary in their ability to facilitate aggregation and utilization of LR. [ABSTRACT FROM AUTHOR]

Published
2012
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13. Differential Regulation of Smad3 and of the Type II Transforming Growth Factor-β Receptor in Mitosis: Implications for Signaling.

Author

Neyrolles, Olivier, Pontiroli, Francesca, Dussurget, Olivier, Zanoni, Ivan, Urbano, Matteo, Beretta, Ottavio, Granucci, Francesca, Ricciardi-Castagnoli, Paola, Cossart, Pascale, and Foti, Maria

Subjects
*DENDRITIC cells, *INFECTION, *TUMORS, *LISTERIA monocytogenes, *GENE expression, *GENOMICS
Abstract

Dendritic cells (DCs) and natural killer (NK) cells are essential components of the innate immunity and play a crucial role in the first phase of host defense against infections and tumors. Listeria monocytogenes (Lm) is an intracellular pathogen that colonizes the cytosol of eukaryotic cells. Recent findings have shown Lm specifically in splenic CD8a+ DCs shortly after intravenous infection. We examined gene expression profiles of mouse DCs exposed to Lm to elucidate the molecular mechanisms underlying DCs interaction with Lm. Using a functional genomics approach, we found that Lm infection induced a cluster of late response genes including type I IFNs and interferon responsive genes (IRGs) in DCs. Type I INFs were produced at the maximal level only at 24 h post infection indicating that the regulation of IFNs in the context of Lm infection is delayed compared to the rapid response observed with viral pathogens. We showed that during Lm infection, IFNγ production and cytotoxic activity were severely impaired in NK cells compared to E. coli infection. These defects were restored by providing an exogenous source of IFNβ during the initial phase of bacterial challenge. Moreover, when treated with IFNβ during early infection, NK cells were able to reduce bacterial titer in the spleen and significantly improve survival of infected mice. These findings show that the timing of IFNβ production is fundamental to the efficient control of the bacterium during the early innate phase of Lm infection. [ABSTRACT FROM AUTHOR]

Published
2012
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14. Class IA Phosphatidylinositol 3-Kinase p110a Regulates Phagosome Maturation.

Author

Thi, Emily P., Lambertz, Ulrike, Reiner, Neil E., and Neyrolles, Olivier

Subjects
PHOSPHATIDYLINOSITOL 3-kinases, ENZYMES, CELL membranes, PHAGOSOMES, ORGANELLES, GALACTOSIDASES
Abstract

Of the various phosphatidylinositol 3- kinases (PI3Ks), only the class III enzyme Vps34 has been shown to regulate phagosome maturation. During studies of phagosome maturation in THP-1 cells deficient in class IA PI3K p110α, we discovered that this PI3K isoform is required for vacuole maturation to progress beyond acquisition of Rab7 leading to delivery of lysosomal markers. Bead phagosomes from THP-1 cells acquired p110α and contained PI3P and PI(3,4,5)P3; however, p110α and PI(3,4,5)P3 levels in phagosomes from p110α knockdown cells were decreased. Phagosomes from p110a knock down cells showed normal acquisition of both Rab5 and EEA-1, but were markedly deficient in the lysosomal markers LAMP-1 and LAMP-2, and the lysosomal hydrolase, β-galactosidase. Phagosomes from p110a deficient cells also displayed impaired fusion with Texas Red dextran-loaded lysosomes. Despite lacking lysosomal components, phagosomes from p110α deficient cells recruited normal levels of Rab7, Rab-interacting lysosomal protein (RILP) and homotypic vacuole fusion and protein sorting (HOPs) components Vps41 and Vps16. The latter observations demonstrated that phagosomal Rab7 was active and capable of recruiting effectors involved in membrane fusion. Nevertheless, active Rab7 was not sufficient to bring about the delivery of lysosomal proteins to the maturing vacuole, which is shown for the first time to be dependent on a class I PI3K. [ABSTRACT FROM AUTHOR]

Published
2012
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15. Modern Lineages of Mycobacterium tuberculosis Exhibit Lineage-Specific Patterns of Growth and Cytokine Induction in Human Monocyte-Derived Macrophages.

Author

Sarkar, Rajesh, Lenders, Laura, Wilkinson, Katalin A., Wilkinson, Robert J., Nicol, Mark P., and Neyrolles, Olivier

Subjects
MYCOBACTERIUM tuberculosis, MACROPHAGES, CYTOKINES, PHENOTYPES, MICROBIAL virulence
Abstract

Background: Strains of Mycobacterium tuberculosis vary in virulence. Strains that have caused outbreaks in the United States and United Kingdom have been shown to subvert the innate immune response as a potential immune evasion mechanism. There is, however, little information available as to whether these patterns of immune subversion are features of individual strains or characteristic of broad clonal lineages of M. tuberculosis. Methods: Strains from two major modern lineages (lineage 2 [East-Asian] and lineage 4 [Euro- American]) circulating in the Western Cape in South Africa as well as a comparator modern lineage (lineage 3 [CAS/Delhi]) were identified. We assessed two virulence associated characteristics: mycobacterial growth (in liquid broth and monocyte derived macrophages) and early pro-inflammatory cytokine induction. Results: In liquid culture, Lineage 4 strains grew more rapidly and reached higher plateau levels than other strains (lineage 4 vs. lineage 2 p = 0.0024; lineage 4 vs. lineage 3 p = 0.0005). Lineage 3 strains were characterized by low and early plateau levels, while lineage 2 strains showed an intermediate growth phenotype. In monocyte-derived macrophages, lineage 2 strains grew faster than lineage 3 strains (p<0.01) with lineage 4 strains having an intermediate phenotype. Lineage 2 strains induced the lowest levels of pro-inflammatory TNF and IL-12p40 as compared to other lineages (lineage 2: median TNF 362 pg/ml, IL- 12p40 91 pg/ml; lineage 3: median TNF 1818 pg/ml, IL-12p40 123 pg/ml; lineage 4: median TNF 1207 pg/ml, IL-12p40 205 pg/ml;). In contrast, lineage 4 strains induced high levels of IL-12p40 and intermediate level of TNF. Lineage 3 strains induced high levels of TNF and intermediate levels of IL-12p40. Conclusions: Strains of M. tuberculosis from the three major modern strain lineages possess distinct patterns of growth and cytokine induction. Rapid growth and immune subversion may be key characteristics to the success of these strains in different human populations. [ABSTRACT FROM AUTHOR]

Published
2012
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16. Clonal Expansion of Both Modern and Ancient Genotypes of Mycobacterium tuberculosis in Southern Taiwan.

Author

Jia-Ru Chang, Yih-Yuan Chen, Tsi-Shu Huang, Wei-Feng Huang, Shu-Chen Kuo, Fan-Chen Tseng, Ih-Jen Su, Chien-Hsing Lin, Yao-Shen Chen, Jun-Ren Sun, Tzong-Shi Chiueh, Horng-Yunn Dou, and Neyrolles, Olivier

Subjects
MYCOBACTERIUM tuberculosis, GENETIC polymorphisms, MASS spectrometry, TUBERCULOSIS
Abstract

We present the first comprehensive analysis of Mycobacterium tuberculosis isolates circulating in the Kaohsiung region of southern Taiwan. The major spoligotypes found in the 224 isolates studied were Beijing lineages (n = 97; 43.3%), EAI lineages (n = 72; 32.1%) and Haarlem lineages (n = 18; 8.0%). By 24 MIRU-VNTR typing, 174 patterns were identified, including 24 clusters of 74 isolates and 150 unique patterns. The combination of spoligotyping and 12-MIRU- VNTR revealed that 129 (57.6%) of the 224 isolates were clustered in 18 genotypes. Moreover, 63.6% (7/11) of infected persons younger than 30 years had a Beijing strain, which could suggest recent spread among younger persons by this family of TB strains in Kaohsiung. Among the 94 Beijing family (SIT1, SIT250 and SIT1674) isolates further analyzed for SNPs by mass spectrometry, the most frequent strain found was ST10 (n = 49; 52%), followed by ST22 (n = 17; 18%) and ST19 (n = 11; 12%). Among the EAI-Manila family isolates analyzed by region deletion-based subtyping, the most frequent strain found was RD type 1 (n = 63; 87.5%), followed by RD type 2 (n = 9; 12.5%). In our previous study, the proportion of modern Beijing strains (52.5%) in northern Taiwan was significantly higher than the proportion of EAI strains (11%). In contrast, in the present study, EAI strains comprised up to 32% of Beijing strains in southern Taiwan. In conclusion, both 'modern' (Beijing) and 'ancient' (EAI) M. tuberculosis strains are prevalent in the Kaohsiung region, perhaps suggesting that both strains are somehow more adapted to southern Taiwan. It will be interesting to investigate the dynamics of the lineage composition by different selection pressures. [ABSTRACT FROM AUTHOR]

Published
2012
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17. How Did the TB Patients Reach DOTS Services in Delhi? A Study of Patient Treatment Seeking Behavior.

Author

Kapoor, Sunil K., Raman, A. Venkat, Sachdeva, Kuldeep Singh, Satyanarayana, Srinath, and Neyrolles, Olivier

Subjects
TUBERCULOSIS research, TUBERCULOSIS patients, MEDICAL care, LUNG diseases
Abstract

Setting: Revised National Tuberculosis Control Programme (RNTCP), Delhi, India. Objective: To ascertain the number and sequence of providers visited by TB patients before availing treatment services from DOTS; to describe the duration between onset of symptoms to treatment. Study design: A cross sectional, qualitative study. Information was gathered through in-depth interviews of TB patients registered during the month of Oct, 2012 for availing TB treatment under the Revised National TB Control Programme from four tuberculosis diagnosis and treatment centers in Delhi. Results: Out of the 114 patients who registered, 108 participated in the study. The study showed that informal providers and retail chemists were the first point of contact and source of clinical advice for two-third of the patients, while the rest sought medical care from qualified providers directly. Most patients sought medical care from more than two providers, before being diagnosed as TB. Female TB patients and patients with extra-pulmonary TB had long mean duration between onset of symptoms to initiation of treatment (6.3 months and 8.4 months respectively). Conclusion: The pathways followed by TB patients, illustrated in this study, provide valuable lessons on the importance of different types of providers (both formal and informal) in the health system in a society like India and the delays in the diagnosis and treatment of tuberculosis. [ABSTRACT FROM AUTHOR]

Published
2012
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18. An Interferon-Related Signature in the Transcriptional Core Response of Human Macrophages to Mycobacterium tuberculosis Infection.

Author

Kang Wu, Dandan Dong, Hai Fang, Levillain, Florence, Wen Jin, Jian Mei, Gicquel, Brigitte, Yanzhi Du, Kankan Wang, Qian Gao, Neyrolles, Olivier, and Ji Zhang

Subjects
INTERFERONS, ANTINEOPLASTIC agents, ANTIVIRAL agents, LYMPHOKINES, GLYCOPROTEINS
Abstract

The W-Beijing family of Mycobacterium tuberculosis (Mtb) strains is known for its high-prevalence and -virulence, as well as for its genetic diversity, as recently reported by our laboratories and others. However, little is known about how the immune system responds to these strains. To explore this issue, here we used reverse engineering and genome-wide expression profiling of human macrophage-like THP-1 cells infected by different Mtb strains of the W-Beijing family, as well as by the reference laboratory strain H37Rv. Detailed data mining revealed that host cell transcriptome responses to H37Rv and to different strains of the W-Beijing family are similar and overwhelmingly induced during Mtb infections, collectively typifying a robust gene expression signature ("THP1r2Mtb-induced signature"). Analysis of the putative transcription factor binding sites in promoter regions of genes in this signature identified several key regulators, namely STATs, IRF-1, IRF-7, and Oct-1, commonly involved in interferon-related immune responses. The THP1r2Mtb-induced signature appeared to be highly relevant to the interferon-inducible signature recently reported in active pulmonary tuberculosis patients, as revealed by cross-signature and cross-module comparisons. Further analysis of the publicly available transcriptome data from human patients showed that the signature appears to be relevant to active pulmonary tuberculosis patients and their clinical therapy, and be tuberculosis specific. Thus, our results provide an additional layer of information at the transcriptome level on mechanisms involved in host macrophage response to Mtb, which may also implicate the robustness of the cellular defense system that can effectively fight against genetic heterogeneity in this pathogen. [ABSTRACT FROM AUTHOR]

Published
2012
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19. Comparative miRNA Expression Profiles in Individuals with Latent and Active Tuberculosis.

Author

Chuan Wang, Shunyao Yang, Gang Sun, Xuying Tang, Shuihua Lu, Neyrolles, Olivier, and Qian Gao

Subjects
MICRORNA, TUBERCULOSIS, MYCOBACTERIAL diseases, LUNG diseases, BIOMARKERS, GENE expression
Abstract

The mechanism of latent tuberculosis (TB) infection remains elusive. Several host factors that are involved in this complex process were previously identified. Micro RNAs (miRNAs) are endogenous ∼ 22 nt RNAs that play important regulatory roles in a wide range of biological processes. Several studies demonstrated the clinical usefulness of miRNAs as diagnostic or prognostic biomarkers in various malignancies and in a few nonmalignant diseases. To study the role of miRNAs in the transition from latent to active TB and to discover candidate biomarkers of this transition, we used human miRNA microarrays to probe the transcriptome of peripheral blood mononuclear cells (PBMCs) in patients with active TB, latent TB infection (LTBI), and healthy controls. Using the software package BRB Array Tools for data analyses, 17 miRNAs were differentially expressed between the three groups (P<0.01). Hierarchical clustering of the 17 miRNAs expression profiles showed that individuals with active TB clustered independently of individuals with LTBI or from healthy controls. Using the predicted target genes and previously published genome-wide transcriptional profiles, we constructed the regulatory networks of miRNAs that were differentially expressed between active TB and LTBI. The regulatory network revealed that several miRNAs, with previously established functions in hematopoietic cell differentiation and their target genes may be involved in the transition from latent to active TB. These results increase the understanding of the molecular basis of LTBI and confirm that some miRNAs may control gene expression of pathways that are important for the pathogenesis of this infectious disease. [ABSTRACT FROM AUTHOR]

Published
2011
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20. Innate Immune Response to Mycobacterium tuberculosis Beijing and Other Genotypes.

Author

Chongzhen Wang, Peyron, Pascale, Mestre, Olga, Kaplan, Gilla, van Soolingen, Dick, Qian Gao, Gicquel, Brigitte, and Neyrolles, Olivier

Subjects
IMMUNE response, MYCOBACTERIUM tuberculosis, PUBLIC health, CYTOKINES, PHAGOCYTES, MACROPHAGES, DENDRITIC cells
Abstract

Background: As a species, Mycobacterium tuberculosis is more diverse than previously thought. In particular, the Beijing family of M. tuberculosis strains is spreading and evoluating throughout the world and this is giving rise to public health concerns. Genetic diversity within this family has recently been delineated further and a specific genotype, called Bmyc10, has been shown to represent over 60% of all Beijing clinical isolates in several parts of the world. How the host immune system senses and responds to various M. tuberculosis strains may profoundly influence clinical outcome and the relative epidemiological success of the different mycobacterial lineages. We hypothesised that the success of the Bmyc10 group may, at least in part, rely upon its ability to alter innate immune responses and the secretion of cytokines and chemokines by host phagocytes. Methodology/Principal Findings: We infected human macrophages and dendritic cells with a collection of genetically well-defined M. tuberculosis clinical isolates belonging to various mycobacterial families, including Beijing. We analyzed cytokine and chemokine secretion on a semi-global level using antibody arrays allowing the detection of sixty-five immunity-related soluble molecules. Our data indicate that Beijing strains induce significantly less interleukin (IL)-6, tumor necrosis factor (TNF), IL-10 and GRO-α than the H37Rv reference strain, a feature that is variously shared by other modern and ancient M. tuberculosis families and which constitutes a signature of the Beijing family as a whole. However, Beijing strains did not differ relative to each other in their ability to modulate cytokine secretion. Conclusions/Significance: Our results confirm and expand upon previous reports showing that M. tuberculosis Beijing strains in general are poor in vitro cytokine inducers in human phagocytes. The results suggest that the epidemiological success of the Beijing Bmyc10 is unlikely to rely upon any specific ability of this group of strains to impair anti-mycobacterial innate immunity. [ABSTRACT FROM AUTHOR]

Published
2010
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21. Ultra-rapid near universal TB drug regimen identified via parabolic response surface platform cures mice of both conventional and high susceptibility

Author

Daniel L. Clemens, Saša Masleša-Galić, Barbara Jane Dillon, Aleidy Silva, Chih-Ming Ho, Bai-Yu Lee, Marcus A. Horwitz, Susana Nava, and Neyrolles, Olivier

Subjects
Bacterial Diseases, 0301 basic medicine, Extensively Drug-Resistant Tuberculosis, Antitubercular Agents, SQ109, lcsh:Medicine, Adamantane, Clofazimine, Gastroenterology, Mice, chemistry.chemical_compound, Medicine and Health Sciences, Drug Interactions, Diarylquinolines, lcsh:Science, Lung, Materials, Multidisciplinary, biology, Pharmaceutics, Animal Models, Ethylenediamines, Actinobacteria, Drug Combinations, Infectious Diseases, Experimental Organism Systems, 5.1 Pharmaceuticals, 6.1 Pharmaceuticals, Physical Sciences, Development of treatments and therapeutic interventions, Infection, Research Article, medicine.drug, medicine.medical_specialty, Tuberculosis, General Science & Technology, Materials Science, 030106 microbiology, Mouse Models, Drug-Drug Interactions, Research and Analysis Methods, Mycobacterium tuberculosis, 03 medical and health sciences, Rare Diseases, Model Organisms, Drug Therapy, Internal medicine, medicine, Animals, Humans, Pharmacology, Aerosols, Bacteria, Animal, Euthanasia, business.industry, lcsh:R, Organisms, Evaluation of treatments and therapeutic interventions, Biology and Life Sciences, Extensively drug-resistant tuberculosis, Pyrazinamide, Tropical Diseases, medicine.disease, biology.organism_classification, Disease Models, Animal, Regimen, Emerging Infectious Diseases, Orphan Drug, 030104 developmental biology, chemistry, Mixtures, Disease Models, Animal Studies, lcsh:Q, Antimicrobial Resistance, Bedaquiline, business
Abstract

As current treatment of tuberculosis is burdensomely long, provoking non-adherence and drug resistance, effective short-course treatments are needed. Using the output-driven parabolic response surface (PRS) platform, we have identified drug regimens that treat tuberculosis more rapidly in mice than the current Standard Regimen used in humans. We show that PRS Regimen III, comprising clofazimine, SQ109, bedaquiline and pyrazinamide, rapidly sterilizes the lung both in conventionally studied BALB/c mice and in C3HeB/FeJ mice, highly susceptible mice that develop massive necrotic granulomatous lung lesions akin to those in humans, achieving relapse-free cure in only 4 weeks (p

Published
2018
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22. Interplay of strain and race/ethnicity in the innate immune response to M. tuberculosis

Author

David M. Lewinsohn, Philip C. Hopewell, Dennis Osmond, Leah G. Jarlsberg, Mark R. Segal, Michael A. Gold, Midori Kato-Maeda, Sebastien Gagneux, Payam Nahid, Karen M. Dobos, and Neyrolles, Olivier

Subjects
Male, Bacterial Diseases, 0301 basic medicine, Lipopolysaccharide, Physiology, Epidemiology, Philippines, lcsh:Medicine, Immune Receptors, Biochemistry, White Blood Cells, chemistry.chemical_compound, Animal Cells, Immune Physiology, Ethnicity, Medicine and Health Sciences, Innate, 2.1 Biological and endogenous factors, Ethnicities, Aetiology, lcsh:Science, Toll-like Receptors, Immune Response, Innate Immune System, Immune System Proteins, Multidisciplinary, Continental Population Groups, biology, Middle Aged, 3. Good health, Actinobacteria, Infectious Diseases, Beijing, Cytokines, Female, Tumor necrosis factor alpha, Lipoteichoic acid, Cellular Types, Infection, Research Article, Signal Transduction, Adult, Adolescent, General Science & Technology, Immune Cells, Immunology, 030106 microbiology, Ethnic Groups, Ethnic Epidemiology, Mycobacterium tuberculosis, Young Adult, 03 medical and health sciences, Rare Diseases, Immune system, Humans, Tuberculosis, Blood Cells, Innate immune system, Bacteria, Prevention, Inflammatory and immune system, Macrophages, Racial Groups, lcsh:R, Immunity, Organisms, Biology and Life Sciences, Proteins, Cell Biology, Molecular Development, Tropical Diseases, biology.organism_classification, Immunity, Innate, TLR2, Emerging Infectious Diseases, Good Health and Well Being, 030104 developmental biology, chemistry, Immune System, People and Places, TLR4, Population Groupings, lcsh:Q, Chinese People, Developmental Biology
Abstract

Author(s): Nahid, P; Jarlsberg, LG; Kato-Maeda, M; Segal, MR; Osmond, DH; Gagneux, S; Dobos, K; Gold, M; Hopewell, PC; Lewinsohn, DM | Abstract: BackgroundThe roles of host and pathogen factors in determining innate immune responses to M. tuberculosis are not fully understood. In this study, we examined host macrophage immune responses of 3 race/ethnic groups to 3 genetically and geographically diverse M. tuberculosis lineages.MethodsMonocyte-derived macrophages from healthy Filipinos, Chinese and non-Hispanic White study participants (approximately 45 individuals/group) were challenged with M. tuberculosis whole cell lysates of clinical strains Beijing HN878 (lineage 2), Manila T31 (lineage 1), CDC1551 (lineage 4), the reference strain H37Rv (lineage 4), as well as with Toll-like receptor 2 agonist lipoteichoic acid (TLR2/LTA) and TLR4 agonist lipopolysaccharide (TLR4/LPS). Following overnight incubation, multiplex assays for nine cytokines: IL-1β, IL-2, IL-6, IL-8, IL-10, IL-12p70, IFNγ, TNFα, and GM-CSF, were batch applied to supernatants.ResultsFilipino macrophages produced less IL-1, IL-6, and more IL-8, compared to macrophages from Chinese and Whites. Race/ethnicity had only subtle effects or no impact on the levels of IL-10, IL-12p70, TNFα and GM-CSF. In response to the Toll-like receptor 2 agonist lipoteichoic acid (TLR2/LTA), Filipino macrophages again had lower IL-1 and IL-6 responses and a higher IL-8 response, compared to Chinese and Whites. The TLR2/LTA-stimulated Filipino macrophages also produced lower amounts of IL-10, TNFα and GM-CSF. Race/ethnicity had no impact on IL-12p70 levels released in response to TLR2/LTA. The responses to TLR4 agonist lipopolysaccharide (TLR4/LPS) were similar to the TLR2/LTA responses, for IL-1, IL-6, IL-8, and IL-10. However, TLR4/LPS triggered the release of less IL-12p70 from Filipino macrophages, and less TNFα from White macrophages.ConclusionsBoth host race/ethnicity and pathogen strain influence the innate immune response. Such variation may have implications for the development of new tools across TB therapeutics, immunodiagnostics and vaccines.

Published
2018
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