Your search keyword '"Báfica A"' showing total 11 results

1. Neuraminidase inhibitors rewire neutrophil function in vivo in murine sepsis and ex vivo in COVID-19

Author

Rodrigo de Oliveira Formiga, Flávia C. Amaral, Camila F. Souza, Daniel A. G. B. Mendes, Carlos W. S. Wanderley, Cristina B. Lorenzini, Adara A. Santos, Juliana Antônia, Lucas F. Faria, Caio C. Natale, Nicholas M. Paula, Priscila C. S. Silva, Fernanda R. Fonseca, Luan Aires, Nicoli Heck, Márick R. Starick, Celso M. Queiroz-Junior, Felipe R. S. Santos, Filipe R. O. de Souza, Vivian V. Costa, Shana P. C. Barroso, Alexandre Morrot, Johan Van Weyenbergh, Regina Sordi, Frederico Alisson-Silva, Fernando Q. Cunha, Edroaldo L. Rocha, Sylvie Chollet-Martin, Maria Margarita Hurtado-Nedelec, Clémence Martin, Pierre-Régis Burgel, Daniel S. Mansur, Rosemeri Maurici, Matthew S. Macauley, André Báfica, Véronique Witko-Sarsat, and Fernando Spiller

Subjects

Oseltamivir, biology, business.industry, ANTIVIRAIS, medicine.disease, Article, Sepsis, NEU1, chemistry.chemical_compound, Zanamivir, chemistry, In vivo, Immunology, medicine, Viral neuraminidase, biology.protein, business, Neuraminidase, Ex vivo, medicine.drug

Abstract

Neutrophil overstimulation plays a crucial role in tissue damage during severe infections. Neuraminidase (NEU)-mediated cleavage of surface sialic acid has been demonstrated to regulate leukocyte responses. Here, we report that antiviral NEU inhibitors constrain host NEU activity, surface sialic acid release, ROS production, and NETs released by microbial-activated human neutrophils.In vivo, treatment with Oseltamivir results in infection control and host survival in peritonitis and pneumonia models of sepsis. Single-cell RNA sequencing re-analysis of publicly data sets of respiratory tract samples from critical COVID-19 patients revealed an overexpression of NEU1 in infiltrated neutrophils. Moreover, Oseltamivir or Zanamivir treatment of whole blood cells from severe COVID-19 patients reduces host NEU-mediated shedding of cell surface sialic acid and neutrophil overactivation. These findings suggest that neuraminidase inhibitors can serve as host-directed interventions to dampen neutrophil dysfunction in severe infections.At a GlanceIn a severe systemic inflammatory response, such as sepsis and COVID-19, neutrophils play a central role in organ damage. Thus, finding new ways to inhibit the exacerbated response of these cells is greatly needed. Here, we demonstrate thatin vitrotreatment of whole blood with the viral neuraminidase inhibitors Oseltamivir or Zanamivir, inhibits the activity of human neuraminidases as well as the exacerbated response of neutrophils. In experimental models of severe sepsis, oseltamivir decreased neutrophil activation and increased the survival rate of mice. Moreover, Oseltamivir or Zanamivirex vivotreatment of whole blood cells from severe COVID-19 patients rewire neutrophil function.

Published

2022

2. Neuraminidase inhibitors rewire neutrophil function in murine sepsis and COVID-19 patients’ cells

Author

Formiga, Rodrigo O., Amaral, Flávia C., Souza, Camila F., Mendes, Daniel A. G. B., Wanderley, Carlos W. S., Lorenzini, Cristina B., Santos, Adara A., Antônia, Juliana, Faria, Lucas F., Natale, Caio C., Paula, Nicholas M., Silva, Priscila C. S., Fonseca, Fernanda R., Aires, Luan, Heck, Nicoli, Barroso, Shana P. C., Morrot, Alexandre, Sordi, Regina, Alisson-Silva, Frederico, Mansur, Daniel S., Cunha, Fernando Q., Maurici, Rosemeri, Báfica, André, Macauley, Matthew S., and Spiller, Fernando

Subjects

sepsis, Oseltamivir, sialic acid, SARS-CoV-2, neutrophil, COVID-19, neuraminidase, Zanamivir, Article

Abstract

Neutrophils overstimulation plays a crucial role in tissue damage during severe infections. Neuraminidase-mediated cleavage of surface sialic acid has been demonstrated to regulate leukocyte responses. Here, we report that antiviral neuraminidase inhibitors constrain host neuraminidase activity, surface sialic acid release, ROS production, and NETs released by microbial-activated human neutrophils. In vivo , treatment with Oseltamivir results in infection control and host survival in murine models of sepsis. Moreover, Oseltamivir or Zanamivir treatment of whole blood cells from severe COVID-19 patients reduces host NEU-mediated shedding of surface sialic acid and neutrophil overactivation. These findings suggest that neuraminidase inhibitors are host-directed interventions to dampen neutrophil dysfunction in severe infections.

Published

2020

3. Neuraminidase inhibitors rewire neutrophil functionin vivoin murine sepsis andex vivoin COVID-19

Author

de Oliveira Formiga, Rodrigo, primary, Amaral, Flávia C., additional, Souza, Camila F., additional, Mendes, Daniel A. G. B., additional, Wanderley, Carlos W. S., additional, Lorenzini, Cristina B., additional, Santos, Adara A., additional, Antônia, Juliana, additional, Faria, Lucas F., additional, Natale, Caio C., additional, Paula, Nicholas M., additional, Silva, Priscila C. S., additional, Fonseca, Fernanda R., additional, Aires, Luan, additional, Heck, Nicoli, additional, Starick, Márick R., additional, Queiroz-Junior, Celso M., additional, Santos, Felipe R. S., additional, de Souza, Filipe R. O., additional, Costa, Vivian V., additional, Barroso, Shana P. C., additional, Morrot, Alexandre, additional, Van Weyenbergh, Johan, additional, Sordi, Regina, additional, Alisson-Silva, Frederico, additional, Cunha, Fernando Q., additional, Rocha, Edroaldo L., additional, Chollet-Martin, Sylvie, additional, Hurtado-Nedelec, Maria Margarita, additional, Martin, Clémence, additional, Burgel, Pierre-Régis, additional, Mansur, Daniel S., additional, Maurici, Rosemeri, additional, Macauley, Matthew S., additional, Báfica, André, additional, Witko-Sarsat, Véronique, additional, and Spiller, Fernando, additional

Published

2020

4. ISG15/USP18/STAT2 is a molecular hub regulating autocrine IFN I-mediated control of Dengue and Zika virus replication

Author

G. Malaquias, Teodoro Fajardo, E.L. da Rocha, P. F. dos Santos, Trevor R. Sweeney, Edgar Kozlova, A. A. dos Santos, Thomas J Sanford, Daniel O. Patricio, Z. G. Soares, André Báfica, C. E. Espada, Juliano Bordignon, and Daniel S. Mansur

Subjects

0303 health sciences, biology, viruses, 030302 biochemistry & molecular biology, biology.organism_classification, ISG15, Virus, 3. Good health, Cell biology, 03 medical and health sciences, Flavivirus, Paracrine signalling, Immune system, Viral replication, Interferon, medicine, Autocrine signalling, 030304 developmental biology, medicine.drug

Abstract

SUMMARYThe establishment of a virus infection is the result of the pathogen’s ability to replicate in a hostile environment generated by the host’s immune system. Here, we found that ISG15 restricts Dengue and Zika viruses’ replication through the stabilization of its binding partner USP18. ISG15 expression was necessary to control DV replication driven by both autocrine and paracrine type one interferon (IFN-I) signaling. Moreover, USP18 competes with NS5-mediated STAT2 degradation, a major mechanism for establishment of flavivirus infection. Strikingly, reconstitution of USP18 in ISG15-deficient cells was sufficient to restore the cells’ immune response and restrict virus growth, suggesting that the IFNAR-mediated ISG15 activity is also antiviral. Our results add a novel layer of complexity in the virus/host interaction interface and suggest that NS5 has a narrow window of opportunity to degrade STAT2, therefore suppressing host’s IFN-I mediated response and promoting virus replication.

Published

2019

5. Vasculature-associated adipose tissue macrophages dynamically adapt to inflammatory and metabolic challenges

Author

Daniel Augusto Gasparin Bueno Mendes, Bernardo S. Reis, Jingyi Chi, Paul Cohen, Hernandez Moura Silva, Juan J. Lafaille, Daniel S. Mansur, Gabriela F. Rodrigues-Luiz, Daniel Mucida, Audrey Crane, David P. Hoytema van Konijnenburg, Patricia Martin, Raquel Duque Nascimento Arifa, Ken Cadwell, Victor J. Torres, Patricia d’Emery Alves Santos, and André Báfica

Subjects

0303 health sciences, education.field_of_study, Adipose tissue macrophages, Population, Adipose tissue, CD11c, Inflammation, White adipose tissue, Biology, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, Macrophage, medicine.symptom, education, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Tissue-resident macrophages comprise the most abundant immune cell population in healthy adipose tissue. Adipose tissue macrophage populations change during metabolic stress and ageing, and are thought to contribute to the pathogenesis of obesity. Here, we studied adipose tissue macrophage subpopulations in the steady state, and in response to nutritional and infectious challenges.Using comprehensive cell-surface-based and gene expression analyses, we found that tissue-resident macrophages from healthy epididymal white adipose tissue (eWAT) tightly associate with blood vessels, displaying a very high endocytic capacity. We refer to these cells as Vasculature-associated Adipose tissue Macrophages (VAMs). Chronic high fat diet (HFD) feeding results in the accumulation of a monocyte-derived CD11c+CD64+double positive (DP) macrophage eWAT population with a predominant anti-inflammatory gene profile, but reduced endocytic function. In contrast, fasting rapidly and reversibly leads to VAM depletion, while acute inflammatory stress induced by pathogens transiently depletes VAMs and simultaneously boosts DP macrophage accumulation. Our results indicate that adipose tissue macrophage populations adapt to metabolic stress and inflammation, suggesting an important role for these cells in restoring homeostasis.

Published

2018

6. ISG15/USP18/STAT2 is a molecular hub regulating autocrine IFN I-mediated control of Dengue and Zika virus replication

Author

Espada, Constanza Eleonora, primary, da Rocha, Edroaldo Lummertz, additional, dos Santos, Adara Aurea, additional, Soares, Zamira Guerra, additional, Malaquias, Greicy, additional, Patrício, Daniel Oliveira, additional, Kozlova, Edgar Gonzalez, additional, dos Santos, Paula Fernandes, additional, Bordignon, Juliano, additional, Sanford, Thomas J., additional, Fajardo, Teodoro, additional, Sweeney, Trevor R., additional, Báfica, André, additional, and Mansur, Daniel Santos, additional

Published

2019

7. An evolutionary recent IFN-IL-6-CEBP axis is linked to monocyte expansion and tuberculosis severity in humans

Author

Delgobo, Murilo, primary, Mendes, Daniel A. G. B., additional, Kozlova, Edgar, additional, Rocha, Edroaldo Lummertz, additional, Rodrigues-Luiz, Gabriela F., additional, Mascarin, Lucas, additional, Dias, Greicy, additional, Patrício, Daniel O., additional, Dierckx, Tim, additional, Bicca, Maíra A., additional, Breton, Gaëlle, additional, de Menezes, Yonne Karoline Tenório, additional, Starick, Márick R., additional, Rovaris, Darcita, additional, Del Moral, Joanita, additional, Mansur, Daniel S., additional, Van Weyenbergh, Johan, additional, and Báfica, André, additional

Published

2019

8. RSV Downregulates IL-21/IL-21R On TFH Cells Via PD-L1 Induction In APCs Impairing Protective Humoral Responses

Author

Ana Paula de Souza, Thiago J. Borges, Tiago Fazolo, Luiz Carlos Rodrigues, Cristina Bonorino, Daniel Augusto Gasparin Bueno Mendes, André Báfica, Fábio Luiz Dal Moro Maito, Rodrigo Benedetti Gassen, and Deise Nascimento de Freitas

Subjects

education.field_of_study, viruses, Population, Germinal center, Inflammation, Biology, Virology, Affinity maturation, medicine.anatomical_structure, Immune system, Immunology, medicine, biology.protein, Avidity, medicine.symptom, Antibody, education, B cell

Abstract

Respiratory syncytial virus (RSV) is the major cause of hospitalization for children under two years of age. RSV vaccines are currently unavailable, and children suffering from multiple reinfections by the same viral strain, fail to develop protective memory responses. Follicular helper T (TFH) cells specialize in providing B cell help to antibody production and affinity maturation, mainly via IL-21 secretion. Although RSV-specific antibodies can be detected upon infection, how they are generated and their relevance against disease protection has not been fully examined. Here, we observed that RSV expands a functionally impaired murine TFH cell population in vitro and vivo, with downregulated IL-21R expression and IL-21 production. IL-21 treatment of RSV-infected mice, however, increased TFH cells frequency, enhanced the germinal center reaction and improved protective humoral immune responses by increasing viral protein F specific antibody avidity and neutralization capacity. In vivo, it protected from RSV infection, decreasing lung inflammation. Passive immunization with purified IgG from IL-21 treated RSV-infected mice protected against RSV infection. Both viable and UV-inactivated RSV induced PD-L1 expression on B cells and DCs, however, only in DCs a direct effect of RSV was detected. Blocking PD-L1 during infection recovered IL-21R expression in TFH and B cells and increased secretion of IL-21 by TFH cells in a DC-dependent manner. Our results unveil a novel pathway by which RSV affects TFH cells activity, reducing levels of IL-21 and its receptor, by increasing PD-L1 expression on APCs. These results highlight the PD-L1/IL-21 axis importance for the generation of protective responses to RSV infection.

Published

2017

9. ISG15 induces IL-10 production in human monocytes and is a biomarker of disease severity during active tuberculosis

Author

dos Santos, Paula Fernandes, Van Weyenbergh, Johan, Delgobo, Murilo, de Oliveira Patricio, Daniel, Ferguson, Brian J., Guabiraba, Rodrigo, Dierckx, Tim, Menezes, Soraya Maria, Báfica, André, Mansur, Daniel Santos, Van Weyenbergh, Johan [0000-0003-3234-8426], Ferguson, Brian [0000-0002-6873-1032], Dierckx, Tim [0000-0002-1969-7974], Mansur, Daniel [0000-0001-6773-9334], and Apollo - University of Cambridge Repository

Subjects

2 Aetiology, 0303 health sciences, Prevention, education, 32 Biomedical and Clinical Sciences, 3 Good Health and Well Being, FOS: Health sciences, 3214 Pharmacology and Pharmaceutical Sciences, 3. Good health, 03 medical and health sciences, Rare Diseases, Infectious Diseases, 0302 clinical medicine, Clinical Research, Tuberculosis, 2.1 Biological and endogenous factors, Infection, Lung, 030304 developmental biology, 030215 immunology

Abstract

Interferon stimulated gene 15 (ISG15) deficiency in humans leads to severe interferonopathies and mycobacterial disease, the latter being previously attributed to its extracellular cytokine-like activity. Here, we demonstrate a novel role for secreted ISG15 as an IL-10 inducer, unique to primary human monocytes. Employingex vivosystems analysis of human transcriptome datasets, we observed a significant correlation of ISG15-induced monocyte IL-10 and lymphocyte IFNγ expression. This effect was associated with p38 MAPK and PI3K signalling in healthy volunteers. The specificity and MAPK/PI3K-dependence of ISG15-induced monocyte IL-10 production was confirmedin vitrousing CRISPR/Cas9 knockout and pharmacological inhibitors. Moreover, thisISG15/IL10axis was amplified in leprosy but disrupted in human active tuberculosis (TB) patients. Importantly, ISG15 strongly correlated with inflammation and disease severity during active TB. In conclusion, this study identifies a novel anti-inflammatory ISG15/IL-10 myeloid axis that is disrupted in active TB, revealing a potential biomarker for disease severity in this major human disease.

Published

2017

10. Vasculature-associated adipose tissue macrophages dynamically adapt to inflammatory and metabolic challenges

Author

Silva, Hernandez Moura, primary, Báfica, André, additional, Rodrigues-Luiz, Gabriela Flavia, additional, Chi, Jingyi, additional, Alves Santos, Patricia d’Emery, additional, Reis, Bernardo S., additional, Hoytema van Konijnenburg, David P., additional, Crane, Audrey, additional, Nascimento Arifa, Raquel Duque, additional, Martin, Patricia, additional, Mendes, Daniel Augusto G.B., additional, Mansur, Daniel Santos, additional, Torres, Victor, additional, Cadwell, Ken, additional, Cohen, Paul, additional, Mucida, Daniel, additional, and Lafaille, Juan José, additional

Published

2018

11. ISG15 induces IL-10 production in human monocytes and is a biomarker of disease severity during active tuberculosis

Author

dos Santos, Paula Fernandes, primary, Van Weyenbergh, Johan, additional, Delgobo, Murilo, additional, de Oliveira Patricio, Daniel, additional, Ferguson, Brian J., additional, Guabiraba, Rodrigo, additional, Dierckx, Tim, additional, Menezes, Soraya Maria, additional, Báfica, André, additional, and Mansur, Daniel Santos, additional

Published

2017