Your search keyword '"Cuevas, Víctor D. [0000-0002-2816-8070]"' showing total 4 results

1. The gene signature of activated M-CSF-primed human monocyte-derived macrophages is IL-10-dependent

Author

Ministerio de Economía y Competitividad (España), Fundación BBVA, Fundació La Marató de TV3, Red de Investigación en Inflamación y Enfermedades Reumáticas (España), European Commission, Cuevas, Víctor D. [0000-0002-2816-8070], Simón-Fuentes, Miriam [0000-0002-8503-0174], Samaniego, Rafael [0000-0002-3081-7332], Sánchez-Mateos, Paloma [0000-0001-6589-4445], Escribese, María M. [0000-0001-5057-5150], Bustos, Matilde [0000-0003-2306-9548], Ocaña, Alberto [0000-0002-1067-9630], Domínguez-Soto, Ángeles [0000-0003-1299-5992], Vega, Miguel A. [0000-0001-6151-4193], Corbí, Angel L. [0000-0003-1980-5733], Cuevas, Víctor D., Simón-Fuentes, Miriam, Orta-Zavalza, Emmanuel, Samaniego, Rafael, Sánchez-Mateos, Paloma, Escribese, María M., Cimas, Francisco J., Bustos, Matilde, Pérez-Diego, Mario, Ocaña, Alberto, Domínguez-Soto, Ángeles, Vega Palacios, Miguel A., Corbí, Angel L., Ministerio de Economía y Competitividad (España), Fundación BBVA, Fundació La Marató de TV3, Red de Investigación en Inflamación y Enfermedades Reumáticas (España), European Commission, Cuevas, Víctor D. [0000-0002-2816-8070], Simón-Fuentes, Miriam [0000-0002-8503-0174], Samaniego, Rafael [0000-0002-3081-7332], Sánchez-Mateos, Paloma [0000-0001-6589-4445], Escribese, María M. [0000-0001-5057-5150], Bustos, Matilde [0000-0003-2306-9548], Ocaña, Alberto [0000-0002-1067-9630], Domínguez-Soto, Ángeles [0000-0003-1299-5992], Vega, Miguel A. [0000-0001-6151-4193], Corbí, Angel L. [0000-0003-1980-5733], Cuevas, Víctor D., Simón-Fuentes, Miriam, Orta-Zavalza, Emmanuel, Samaniego, Rafael, Sánchez-Mateos, Paloma, Escribese, María M., Cimas, Francisco J., Bustos, Matilde, Pérez-Diego, Mario, Ocaña, Alberto, Domínguez-Soto, Ángeles, Vega Palacios, Miguel A., and Corbí, Angel L.

Abstract

During inflammatory responses, monocytes are recruited into inflamed tissues, where they become monocyte-derived macrophages and acquire pro-inflammatory and tissue-damaging effects in response to the surrounding environment. In fact, monocyte-derived macrophage subsets are major pathogenic cells in inflammatory pathologies. Strikingly, the transcriptome of pathogenic monocyte-derived macrophage subsets resembles the gene profile of macrophage colony-stimulating factor (M-CSF)-primed monocyte-derived human macrophages (M-MØ). As M-MØ display a characteristic cytokine profile after activation (IL10high TNFlow IL23low IL6low), we sought to determine the transcriptional signature of M-MØ upon exposure to pathogenic stimuli. Activation of M-MØ led to the acquisition of a distinctive transcriptional profile characterized by the induction of a group of genes (Gene set 1) highly expressed by pathogenic monocyte-derived macrophages in COVID-19 and whose presence in tumor-associated macrophages (TAM) correlates with the expression of macrophage-specific markers (CD163, SPI1) and IL10. Indeed, Gene set 1 expression was primarily dependent on ERK/p38 and STAT3 activation, and transcriptional analysis and neutralization experiments revealed that IL-10 is not only required for the expression of a subset of genes within Gene set 1 but also significantly contributes to the idiosyncratic gene signature of activated M-MØ. Our results indicate that activation of M-CSF-dependent monocyte-derived macrophages induces a distinctive gene expression profile, which is partially dependent on IL-10, and identifies a gene set potentially helpful for macrophage-centered therapeutic strategies.

Published

2021

2. IVIg promote cross-tolerance against inflammatory stimuli in vitro and in vivo

Author

Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Comunidad de Madrid, Cuevas, Víctor D. [0000-0002-2816-8070], Domínguez-Andrés, Jorge [0000-0002-9091-1961], Saz-Leal, Paula [0000-0002-6263-4709], Sancho, David [0000-0003-2890-3984], Ochoa-Grullón, Juliana [0000-0002-5218-7108], Sánchez-Ramón, Silvia [0000-0001-9585-6167], Vega, Miguel A. [0000-0001-6151-4193], Corbí, Angel L. [0000-0003-1980-5733], Domínguez-Soto, Ángeles, Simón-Fuentes, Miriam, Casas-Engel, Mateo de las, Cuevas, Víctor D., López-Bravo, María, Domínguez-Andrés, Jorge, Saz-Leal, Paula, Sancho, David, Ardavín, Carlos, Ochoa-Grullón, Juliana, Sánchez-Ramón, Silvia, Vega Palacios, Miguel A., Corbí, Angel L., Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Comunidad de Madrid, Cuevas, Víctor D. [0000-0002-2816-8070], Domínguez-Andrés, Jorge [0000-0002-9091-1961], Saz-Leal, Paula [0000-0002-6263-4709], Sancho, David [0000-0003-2890-3984], Ochoa-Grullón, Juliana [0000-0002-5218-7108], Sánchez-Ramón, Silvia [0000-0001-9585-6167], Vega, Miguel A. [0000-0001-6151-4193], Corbí, Angel L. [0000-0003-1980-5733], Domínguez-Soto, Ángeles, Simón-Fuentes, Miriam, Casas-Engel, Mateo de las, Cuevas, Víctor D., López-Bravo, María, Domínguez-Andrés, Jorge, Saz-Leal, Paula, Sancho, David, Ardavín, Carlos, Ochoa-Grullón, Juliana, Sánchez-Ramón, Silvia, Vega Palacios, Miguel A., and Corbí, Angel L.

Abstract

IVIg is an approved therapy for immunodeficiency and for several autoimmune and inflammatory diseases. However, the molecular basis for the IVIg anti-inflammatory activity remains to be fully explained and cannot be extrapolated from studies on animal models of disease. We now report that IVIg impairs the generation of human monocyte-derived anti-inflammatory macrophages by inducing JNK activation and activin A production and limits proinflammatory macrophage differentiation by inhibiting GM-CSF-driven STAT5 activation. In vivo, IVIg provokes a rapid increase in peripheral blood activin A, CCL2, and IL-6 levels, an effect that can be recapitulated in vitro on human monocytes. On differentiating monocytes, IVIg promotes the acquisition of altered transcriptional and cytokine profiles, reduces TLR expression and signaling, and upregulates negative regulators of TLR-initiated intracellular signaling. In line with these effects, in vivo IVIg infusion induces a state tolerant toward subsequent stimuli that results in reduced inflammatory cytokine production after LPS challenge in human peripheral blood and significant protection from LPS-induced death in mice. Therefore, IVIg conditions human macrophages toward the acquisition of a state of cross-tolerance against inflammatory stimuli, an effect that correlates with the net anti-inflammatory action of IVIg in vivo.

Published

2018

3. The gene signature of activated M-CSF-primed human monocyte-derived macrophages is IL-10-dependent

Author

Víctor D. Cuevas, Miriam Simón-Fuentes, Matilde Bustos, Miguel A. Vega, María M. Escribese, Ángeles Domínguez-Soto, Mario Pérez-Diego, Rafael Samaniego, Angel L. Corbí, Francisco J. Cimas, Paloma Sánchez-Mateos, Alberto Ocaña, Emmanuel Orta-Zavalza, Ministerio de Economía y Competitividad (España), Fundación BBVA, Fundació La Marató de TV3, Red de Investigación en Inflamación y Enfermedades Reumáticas (España), European Commission, Cuevas, Víctor D., Simón-Fuentes, Miriam, Samaniego, Rafael, Sánchez-Mateos, Paloma, Escribese, María M., Bustos, Matilde, Ocaña, Alberto, Domínguez-Soto, Ángeles, Vega, Miguel A., Corbí, Angel L., Cuevas, Víctor D. [0000-0002-2816-8070], Simón-Fuentes, Miriam [0000-0002-8503-0174], Samaniego, Rafael [0000-0002-3081-7332], Sánchez-Mateos, Paloma [0000-0001-6589-4445], Escribese, María M. [0000-0001-5057-5150], Bustos, Matilde [0000-0003-2306-9548], Ocaña, Alberto [0000-0002-1067-9630], Domínguez-Soto, Ángeles [0000-0003-1299-5992], Vega, Miguel A. [0000-0001-6151-4193], and Corbí, Angel L. [0000-0003-1980-5733]

Subjects

Macrophage, Macrophage polarization, Biology, Monocytes, Transcriptome, Gene expression, Humans, Immunology and Allergy, Internal medicine, Cells, Cultured, Inflammation, SPI1, Macrophage Colony-Stimulating Factor, Macrophages, COVID-19, Granulocyte-Macrophage Colony-Stimulating Factor, Cell Differentiation, Gene signature, RC31-1245, Cell biology, Interleukin-10, Interleukin 10, Medicine, CD163, Research Article

Abstract

14 p.-5 fig., During inflammatory responses, monocytes are recruited into inflamed tissues, where they become monocyte-derived macrophages and acquire pro-inflammatory and tissue-damaging effects in response to the surrounding environment. In fact, monocyte-derived macrophage subsets are major pathogenic cells in inflammatory pathologies. Strikingly, the transcriptome of pathogenic monocyte-derived macrophage subsets resembles the gene profile of macrophage colony-stimulating factor (M-CSF)-primed monocyte-derived human macrophages (M-MØ). As M-MØ display a characteristic cytokine profile after activation (IL10high TNFlow IL23low IL6low), we sought to determine the transcriptional signature of M-MØ upon exposure to pathogenic stimuli. Activation of M-MØ led to the acquisition of a distinctive transcriptional profile characterized by the induction of a group of genes (Gene set 1) highly expressed by pathogenic monocyte-derived macrophages in COVID-19 and whose presence in tumor-associated macrophages (TAM) correlates with the expression of macrophage-specific markers (CD163, SPI1) and IL10. Indeed, Gene set 1 expression was primarily dependent on ERK/p38 and STAT3 activation, and transcriptional analysis and neutralization experiments revealed that IL-10 is not only required for the expression of a subset of genes within Gene set 1 but also significantly contributes to the idiosyncratic gene signature of activated M-MØ. Our results indicate that activation of M-CSF-dependent monocyte-derived macrophages induces a distinctive gene expression profile, which is partially dependent on IL-10, and identifies a gene set potentially helpful for macrophage-centered therapeutic strategies., This work was supported by grants from Ministerio de Economía y Competitividad (SAF2017-83785-R) to M.A.V. and A.L.C., “Ayudas FUNDACIÓN BBVA a equipos de investigación científica SARS-CoV-2 y COVID-19” to M.A.V. and A.L.C., Grant 201619.31 from Fundació La Marató/TV3 to A.L.C., and Red de Investigación en Enfermedades Reumáticas (RIER, RD16/0012/0007), and cofinanced by the European Regional Development Fund “A way to achieve Europe” (ERDF), to A.L.C. V.D.C. was funded by a Formación de Personal Investigador predoctoral fellowship from MINECO (Grant BES-2012-053864).

Published

2021

4. IVIg promote cross-tolerance against inflammatory stimuli in vitro and in vivo

Author

Carlos Ardavín, María López-Bravo, Ángeles Domínguez-Soto, Jorge Domínguez-Andrés, Paula Saz-Leal, Miriam Simón-Fuentes, Angel L. Corbí, Miguel A. Vega, David Sancho, Víctor D. Cuevas, Mateo de las Casas-Engel, Silvia Sánchez-Ramón, Juliana Ochoa-Grullón, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Comunidad de Madrid, Cuevas, Víctor D. [0000-0002-2816-8070], Domínguez-Andrés, Jorge [0000-0002-9091-1961], Saz-Leal, Paula [0000-0002-6263-4709], Sancho, David [0000-0003-2890-3984], Ochoa-Grullón, Juliana [0000-0002-5218-7108], Sánchez-Ramón, Silvia [0000-0001-9585-6167], Vega, Miguel A. [0000-0001-6151-4193], Corbí, Angel L. [0000-0003-1980-5733], Cuevas, Víctor D., Domínguez-Andrés, Jorge, Saz-Leal, Paula, Sancho, David, Ochoa-Grullón, Juliana, Sánchez-Ramón, Silvia, Vega, Miguel A., and Corbí, Angel L.

Subjects

0301 basic medicine, Lipopolysaccharides, medicine.medical_treatment, Anti-Inflammatory Agents, Endotoxin tolerance, Dendritic cells, Monocytes, Mice, hemic and lymphatic diseases, STAT5 Transcription Factor, Mechanisms, Immunology and Allergy, Medicine, Activin-A, STAT5, Immunodeficiency, Cells, Cultured, Chemokine CCL2, biology, Intravenous immune globulin, Monocyte-derived macrophages, Immunoglobulins, Intravenous, Activins, Cytokine, Intracellular, Antiinflammatory actions, Immunology, CCL2, Proinflammatory cytokine, 03 medical and health sciences, In vivo, Immune Tolerance, Immunoglobulin, Animals, Humans, Inflammation, business.industry, Interleukin-6, Macrophages, JNK Mitogen-Activated Protein Kinases, Granulocyte-Macrophage Colony-Stimulating Factor, GM-CSF, medicine.disease, In vitro, Enzyme Activation, 030104 developmental biology, biology.protein, Therapy, business

Abstract

12 p.-7 fig., IVIg is an approved therapy for immunodeficiency and for several autoimmune and inflammatory diseases. However, the molecular basis for the IVIg anti-inflammatory activity remains to be fully explained and cannot be extrapolated from studies on animal models of disease. We now report that IVIg impairs the generation of human monocyte-derived anti-inflammatory macrophages by inducing JNK activation and activin A production and limits proinflammatory macrophage differentiation by inhibiting GM-CSF-driven STAT5 activation. In vivo, IVIg provokes a rapid increase in peripheral blood activin A, CCL2, and IL-6 levels, an effect that can be recapitulated in vitro on human monocytes. On differentiating monocytes, IVIg promotes the acquisition of altered transcriptional and cytokine profiles, reduces TLR expression and signaling, and upregulates negative regulators of TLR-initiated intracellular signaling. In line with these effects, in vivo IVIg infusion induces a state tolerant toward subsequent stimuli that results in reduced inflammatory cytokine production after LPS challenge in human peripheral blood and significant protection from LPS-induced death in mice. Therefore, IVIg conditions human macrophages toward the acquisition of a state of cross-tolerance against inflammatory stimuli, an effect that correlates with the net anti-inflammatory action of IVIg in vivo., This work was supported by grants from the Ministerio de Economía y Competitividad (SAF2014-23801), the Instituto de Salud Carlos III (La Red de Investigación en Inflamación y Enfermedades Reumáticas, RIER RD12/009), and the Comunidad Autónoma de Madrid/FEDER (S2010/BMD-2350, RAPHYME Program) to A.L.C. and M.A.V. and by Instituto de Salud Carlos III Grant PI16/01428 to S.S.-R.

Published

2018