Your search keyword '"Ester Díaz-Mora"' showing total 10 results

1. p38δ controls Mitogen- and Stress-activated Kinase-1 (MSK1) function in response to toll-like receptor activation in macrophages

Author

Ester Díaz-Mora, Diego González-Romero, Marta Meireles-da-Silva, Juan José Sanz-Ezquerro, and Ana Cuenda

Subjects

p38δ/p38γ, MSK1, macrophages, phosphorylation, MAPK, Biology (General), QH301-705.5

Abstract

Mitogen- and Stress-activated Kinase (MSK) 1 is a nuclear protein, activated by p38α Mitogen-Activated Kinase (MAPK) and extracellular signal-regulated kinase (ERK1/2), that modulate the production of certain cytokines in macrophages. Using knockout cells and specific kinase inhibitors, we show that, besides p38α and ERK1/2, another p38MAPK, p38δ, mediates MSK phosphorylation and activation, in LPS-stimulated macrophages. Additionally, recombinant MSK1 was phosphorylated and activated by recombinant p38δ, to the same extent than by p38α, in in vitro experiments. Moreover, the phosphorylation of the transcription factors CREB and ATF1, that are MSK physiological substrates, and the expression of the CREB-dependent gene encoding DUSP1, were impaired in p38δ-deficient macrophages. Also, the transcription of IL-1Ra mRNA, that is MSK-dependent, was reduced. Our results indicate that MSK activation can be one possible mechanism by which p38δ regulates the production of a variety of inflammatory molecules involved in immune innate response.

Published

2023

2. B Cell Development and T-Dependent Antibody Response Are Regulated by p38γ and p38δ

Author

Laura Barrio, Sara Román-García, Ester Díaz-Mora, Ana Risco, Rodrigo Jiménez-Saiz, Yolanda R. Carrasco, and Ana Cuenda

Subjects

p38MAPK, p38γ, p38δ, B cell, lymphocyte, spleen, Biology (General), QH301-705.5

Abstract

p38MAP kinase (MAPK) signal transduction pathways are important regulators of inflammation and the immune response; their involvement in immune cell development and function is still largely unknown. Here we analysed the role of the p38 MAPK isoforms p38γ and p38δ in B cell differentiation in bone marrow (BM) and spleen, using mice lacking p38γ and p38δ, or conditional knockout mice that lack both p38γ and p38δ specifically in the B cell compartment. We found that the B cell differentiation programme in the BM was not affected in p38γ/δ-deficient mice. Moreover, these mice had reduced numbers of peripheral B cells as well as altered marginal zone B cell differentiation in the spleen. Expression of co-stimulatory proteins and activation markers in p38γ/δ-deficient B cells are diminished in response to B cell receptor (BCR) and CD40 stimulation; p38γ and p38δ were necessary for B cell proliferation induced by BCR and CD40 but not by TLR4 signaling. Furthermore, p38γ/δ-null mice produced significantly lower antibody responses to T-dependent antigens. Our results identify unreported functions for p38γ and p38δ in B cells and in the T-dependent humoral response; and show that the combined activity of these kinases is needed for peripheral B cell differentiation and function.

Published

2020

3. Myeloid cell deficiency of p38γ/p38δ protects against candidiasis and regulates antifungal immunity

Author

Dayanira Alsina‐Beauchamp, Alejandra Escós, Pilar Fajardo, Diego González‐Romero, Ester Díaz‐Mora, Ana Risco, Miguel A Martín‐Serrano, Carlos del Fresno, Jorge Dominguez‐Andrés, Noelia Aparicio, Rafal Zur, Natalia Shpiro, Gordon D Brown, Carlos Ardavín, Mihai G Netea, Susana Alemany, Juan J Sanz‐Ezquerro, and Ana Cuenda

Subjects

Candida albicans, infection, kinase inhibitor, p38MAPK, signalling, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Candida albicans is a frequent aetiologic agent of sepsis associated with high mortality in immunocompromised patients. Developing new antifungal therapies is a medical need due to the low efficiency and resistance to current antifungal drugs. Here, we show that p38γ and p38δ regulate the innate immune response to C. albicans. We describe a new TAK1‐TPL2‐MKK1‐ERK1/2 pathway in macrophages, which is activated by Dectin‐1 engagement and positively regulated by p38γ/p38δ. In mice, p38γ/p38δ deficiency protects against C. albicans infection by increasing ROS and iNOS production and thus the antifungal capacity of neutrophils and macrophages, and by decreasing the hyper‐inflammation that leads to severe host damage. Leucocyte recruitment to infected kidneys and production of inflammatory mediators are decreased in p38γ/δ‐null mice, reducing septic shock. p38γ/p38δ in myeloid cells are critical for this effect. Moreover, pharmacological inhibition of p38γ/p38δ in mice reduces fungal burden, revealing that these p38MAPKs may be therapeutic targets for treating C. albicans infection in humans.

Published

2018

4. TPL2 kinase expression is regulated by the p38γ/p38δ-dependent association of aconitase-1 with

Author

Alejandra, Escós, José, Martín-Gómez, Diego, González-Romero, Ester, Díaz-Mora, Rosario, Francisco-Velilla, Cesar, Santiago, José M, Cuezva, Sonia, Domínguez-Zorita, Encarnación, Martínez-Salas, Nahum, Sonenberg, Juan José, Sanz-Ezquerro, Seyed Mehdi, Jafarnejad, and Ana, Cuenda

Subjects

Aconitate Hydratase, Mitogen-Activated Protein Kinase 13, Mitogen-Activated Protein Kinase 12, Gene Expression Regulation, RNA, Messenger, MAP Kinase Kinase Kinases, Immunity, Innate

Abstract

p38γ and p38δ (p38γ/p38δ) regulate inflammation, in part by controlling tumor progression locus 2 (TPL2) expression in myeloid cells. Here, we demonstrate that TPL2 protein levels are dramatically reduced in p38γ/p38δ-deficient (p38γ/δ

Published

2023

5. p38γ and p38δ modulate innate immune response by regulating MEF2D activation

Author

Alejandra Escós, Ester Díaz-Mora, Michael Pattison, Pilar Fajardo, Diego González-Romero, Ana Risco, José Martín-Gómez, Éric Bonneil, Nahum Sonenberg, Seyed Mehdi Jafarnejad, Juan José Sanz-Ezquerro, Steven C. Ley, and Ana Cuenda

Abstract

Evidence implicating p38γ and p38δ (p38γ/p38δ) in inflammation are mainly based on experiments using p38γ/p38δ deficient (p38γ/δ-/-) mice, which show low levels of TPL2, the kinase upstream of MKK1-ERK1/2 in myeloid cells. This could obscure p38γ/p38δ roles, since TPL2 is essential for regulating inflammation. Here we generated a p38γD171A/D171A/p38δ-/-(p38γ/δKIKO) mouse, expressing kinase-inactive p38γ and lacking p38δ. This mouse exhibited normal TPL2 levels, making it an excellent tool to elucidate specific p38γ/p38δ functions. p38γ/δKIKO mice showed a reduced inflammatory response and less susceptibility to LPS-induced septic shock andCandida albicansinfection than wild-type mice. Gene expression analyses in LPS-activated WT and p38γ/δKIKO macrophages revealed that p38γ/p38δ regulated numerous genes implicated in innate immune response. Additionally, phospho-proteomic analyses andin vitrokinase assays showed that the transcription factor myocyte enhancer factor-2D (MEF2D) was phosphorylated at Ser444 via p38γ/p38δ. Mutation of MEF2D Ser444 to the non-phosphorylatable residue Ala increased its transcriptional activity and the expression ofiNOSandIL-1βmRNA. These results suggest that p38γ/p38δ govern innate immune responses by regulating MEF2D phosphorylation and transcriptional activity.

Published

2022

6. TPL2 kinase expression is regulated by the p38γ/p38δ-dependent association of aconitase-1 with TPL2 mRNA

Author

Alejandra Escós, José Martín-Gómez, Diego González-Romero, Ester Díaz-Mora, Rosario Francisco-Velilla, Cesar Santiago, José M. Cuezva, Sonia Domínguez-Zorita, Encarnación Martínez-Salas, Nahum Sonenberg, Juan José Sanz-Ezquerro, Seyed Mehdi Jafarnejad, Ana Cuenda, and UAM. Departamento de Biología Molecular

Subjects

Aconitate Hydratase, Multidisciplinary, Messenger RNA, Nuclear Factor Kappa B 1p10, Aconitate 1, Phosphotransferase, Biología y Biomedicina / Biología

Abstract

p38γ and p38δ (p38γ/p38δ) regulate inflammation, in part by controlling tumor progression locus 2 (TPL2) expression in myeloid cells. Here, we demonstrate that TPL2 protein levels are dramatically reduced in p38γ/p38δ-deficient (p38γ/δ2/2) cells and tissues without affecting TPL2 messenger ribonucleic acid (mRNA) expression. We show that p38γ/p38δ posttranscriptionally regulates the TPL2 amount at two different levels. p38γ/p38δ interacts with the TPL2/A20 Binding Inhibitor of NF-κB2 (ABIN2)/Nuclear Factor κB1p105 (NF-κB1p105) complex, increasing TPL2 protein stability. Additionally, p38γ/p38δ regulates TPL2 mRNA translation by modulating the repressor function of TPL2 30 Untranslated region (UTR) mediated by its association with aconitase-1 (ACO1). ACO1 overexpression in wild-type cells increases the translational repression induced by TPL2 30UTR and severely decreases TPL2 protein levels. p38δ binds to ACO1, and p38δ expression in p38γ/δ2/2 cells fully restores TPL2 protein to wild-type levels by reducing the translational repression of TPL2 mRNA. This study reveals a unique mechanism of posttranscriptional regulation of TPL2 expression, which given its central role in innate immune response, likely has great relevance in physiopathology, MCIN/AEI/10.13039/501100011033 Grants PID2019-108349RB-100 (to J.J.S.-E. and A.C.) and SAF2016-79792R (to J.J.S.-E. and A.C.)

Published

2022

7. B Cell Development and T-Dependent Antibody Response Are Regulated by p38γ and p38δ

Author

Ana Risco, Sara Roman-Garcia, Rodrigo Jiménez-Saiz, Yolanda R. Carrasco, Ana Cuenda, Ester Díaz-Mora, Laura Barrio, Ministerio de Ciencia e Innovación (España), Risco, Cristina, and Risco, Cristina [0000-0001-7501-5934]

Subjects

0301 basic medicine, MAPK/ERK pathway, p38γ, Lymphocyte, B-cell receptor, lymphocyte, p38δ, 03 medical and health sciences, Cell and Developmental Biology, 0302 clinical medicine, medicine, lcsh:QH301-705.5, B cell, Original Research, CD40, Marginal zone B cell differentiation, biology, Cell growth, Cell Biology, Cell biology, 030104 developmental biology, medicine.anatomical_structure, lcsh:Biology (General), 030220 oncology & carcinogenesis, biology.protein, p38MAPK, spleen, Signal transduction, Developmental Biology

Abstract

p38MAP kinase (MAPK) signal transduction pathways are important regulators of inflammation and the immune response; their involvement in immune cell development and function is still largely unknown. Here we analysed the role of the p38 MAPK isoforms p38γ and p38δ in B cell differentiation in bone marrow (BM) and spleen, using mice lacking p38γ and p38δ, or conditional knockout mice that lack both p38γ and p38δ specifically in the B cell compartment. We found that the B cell differentiation programme in the BM was not affected in p38γ/δ-deficient mice. Moreover, these mice had reduced numbers of peripheral B cells as well as altered marginal zone B cell differentiation in the spleen. Expression of co-stimulatory proteins and activation markers in p38γ/δ-deficient B cells are diminished in response to B cell receptor (BCR) and CD40 stimulation; p38γ and p38δ were necessary for B cell proliferation induced by BCR and CD40 but not by TLR4 signaling. Furthermore, p38γ/δ-null mice produced significantly lower antibody responses to T-dependent antigens. Our results identify unreported functions for p38γ and p38δ in B cells and in the T-dependent humoral response; and show that the combined activity of these kinases is needed for peripheral B cell differentiation and function., This work was supported by grants from the Spanish Ministry of Science and Innovation (SAF2013-45331-R and SAF2016-79792RtoAC; BFU2011-30097, BFU2013-48828-P,andRTI2018-101345-B-I00/MCIU/AEI/FEDER, UE to YC).

Published

2019

8. Myeloid cell deficiency of p38 gamma/p38 delta protects against candidiasis and regulates antifungal immunity

Author

Pilar Fajardo, Susana Alemany, Alejandra Escós, Mihai G. Netea, Dayanira Alsina-Beauchamp, Juan Jose Sanz-Ezquerro, Carlos del Fresno, Jorge Domínguez-Andrés, Noelia Aparicio, Natalia Shpiro, Diego Gonzalez‐Romero, Ana Cuenda, Miguel A. Martín-Serrano, Ana Risco, Carlos Ardavín, Ester Díaz-Mora, Rafal Zur, Gordon D. Brown, Ministerio de Economía y Competitividad (España), Fundación La Marató TV3, European Research Council, Dutch Research Council (Holanda), Wellcome Trust, Medical Research Council (Reino Unido), Fundació La Marató de TV3, Netherlands Organization for Scientific Research, Medical Research Council (UK), University of Aberdeen, Fundación 'la Caixa', and European Commission

Subjects

0301 basic medicine, Medicine (General), Myeloid, Neutrophils, Cell, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Nitric Oxide Synthase Type II, QH426-470, Mitogen-Activated Protein Kinase 13, Mitogen-Activated Protein Kinase 12, Candida albicans, Medicine, Myeloid Cells, signalling, Research Articles, IN-VIVO, Mice, Knockout, P38-DELTA, biology, INVASIVE CANDIDIASIS, Candidiasis, Microbiology, Virology & Host Pathogen Interaction, 3. Good health, medicine.anatomical_structure, Host-Pathogen Interactions, p38MAPK, Molecular Medicine, Female, Infection, Research Article, Signal Transduction, Antifungal, medicine.drug_class, kinase inhibitor, Immunology, CROSS-TALK, TNF-ALPHA PRODUCTION, Signalling, Sepsis, 03 medical and health sciences, R5-920, All institutes and research themes of the Radboud University Medical Center, INFLAMMATION, Immunity, Genetics, Animals, PATTERN-RECOGNITION RECEPTORS, Pharmacology & Drug Discovery, Kinase inhibitor, Innate immune system, business.industry, Septic shock, Macrophages, P38-GAMMA, LOCI-2 TPL2 KINASE, medicine.disease, biology.organism_classification, infection, Mice, Inbred C57BL, 030104 developmental biology, INNATE IMMUNITY, business, Reactive Oxygen Species

Abstract

Candida albicans is a frequent aetiologic agent of sepsis associated with high mortality in immunocompromised patients. Developing new antifungal therapies is a medical need due to the low efficiency and resistance to current antifungal drugs. Here, we show that p38γ and p38δ regulate the innate immune response to C. albicans. We describe a new TAK1‐TPL2‐MKK1‐ERK1/2 pathway in macrophages, which is activated by Dectin‐1 engagement and positively regulated by p38γ/p38δ. In mice, p38γ/p38δ deficiency protects against C. albicans infection by increasing ROS and iNOS production and thus the antifungal capacity of neutrophils and macrophages, and by decreasing the hyper‐inflammation that leads to severe host damage. Leucocyte recruitment to infected kidneys and production of inflammatory mediators are decreased in p38γ/δ‐null mice, reducing septic shock. p38γ/p38δ in myeloid cells are critical for this effect. Moreover, pharmacological inhibition of p38γ/p38δ in mice reduces fungal burden, revealing that these p38MAPKs may be therapeutic targets for treating C. albicans infection in humans., This work was supported by grants from the MINECO [SAF2013‐45331‐R and SAF2016‐79792‐R (AEI/FEDER, UE)] to AC and JJS‐E, La Marató TV3 Foundation (20133431) to AC and (SAF2014‐52009‐R) to SA. ERC Consolidator Grant (#310372) and a Spinoza grant of the Netherlands Organization for Scientific Research to MGN, and Wellcome Trust, the Medical Research Council (MRC; UK), the MRC Centre for Medical Mycology at the University of Aberdeen to GDB. DAB and AE receive MINECO FPI fellowships, AR a MINECO Juan de la Cierva award and JD‐A a La Caixa Foundation PhD fellowship.

Published

2018

9. p38γ and p38δ modulate innate immune response by regulating MEF2D activation

Author

Alejandra Escós, Ester Diaz-Mora, Michael Pattison, Pilar Fajardo, Diego González-Romero, Ana Risco, José Martín-Gómez, Éric Bonneil, Nahum Sonenberg, Seyed Mehdi Jafarnejad, Juan José Sanz-Ezquerro, Steven C Ley, and Ana Cuenda

Subjects

p38γ, phosphorylation, inflammation, MEF2D, p38δ, MAPK, Medicine, Science, Biology (General), QH301-705.5

Abstract

Evidence implicating p38γ and p38δ (p38γ/p38δ) in inflammation are mainly based on experiments using Mapk12/Mapk13-deficient (p38γ/δKO) mice, which show low levels of TPL2, the kinase upstream of MKK1–ERK1/2 in myeloid cells. This could obscure p38γ/p38δ roles, since TPL2 is essential for regulating inflammation. Here, we generated a Mapk12D171A/D171A/Mapk13−/− (p38γ/δKIKO) mouse, expressing kinase-inactive p38γ and lacking p38δ. This mouse exhibited normal TPL2 levels, making it an excellent tool to elucidate specific p38γ/p38δ functions. p38γ/δKIKO mice showed a reduced inflammatory response and less susceptibility to lipopolysaccharide (LPS)-induced septic shock and Candida albicans infection than wild-type (WT) mice. Gene expression analyses in LPS-activated wild-type and p38γ/δKIKO macrophages revealed that p38γ/p38δ-regulated numerous genes implicated in innate immune response. Additionally, phospho-proteomic analyses and in vitro kinase assays showed that the transcription factor myocyte enhancer factor-2D (MEF2D) was phosphorylated at Ser444 via p38γ/p38δ. Mutation of MEF2D Ser444 to the non-phosphorylatable residue Ala increased its transcriptional activity and the expression of Nos2 and Il1b mRNA. These results suggest that p38γ/p38δ govern innate immune responses by regulating MEF2D phosphorylation and transcriptional activity.

Published

2023

10. Evolutionary analysis of p38 stress-activated kinases in unicellular relatives of animals suggests an ancestral function in osmotic stress

Author

Victoria Shabardina, Pedro Romero Charria, Gonzalo Bercedo Saborido, Ester Diaz-Mora, Ana Cuenda, Iñaki Ruiz-Trillo, and Juan Jose Sanz-Ezquerro

Subjects

p38 kinases, paralog fate, origin of animals, p38 evolution, Biology (General), QH301-705.5

Abstract

p38 kinases are key elements of the cellular stress response in animals. They mediate the cell response to a multitude of stress stimuli, from osmotic shock to inflammation and oncogenes. However, it is unknown how such diversity of function in stress evolved in this kinase subfamily. Here, we show that the p38 kinase was already present in a common ancestor of animals and fungi. Later, in animals, it diversified into three JNK kinases and four p38 kinases. Moreover, we identified a fifth p38 paralog in fishes and amphibians. Our analysis shows that each p38 paralog has specific amino acid substitutions around the hinge point, a region between the N-terminal and C-terminal protein domains. We showed that this region can be used to distinguish between individual paralogs and predict their specificity. Finally, we showed that the response to hyperosmotic stress in Capsaspora owczarzaki, a close unicellular relative of animals, follows a phosphorylation–dephosphorylation pattern typical of p38 kinases. At the same time, Capsaspora's cells upregulate the expression of GPD1 protein resembling an osmotic stress response in yeasts. Overall, our results show that the ancestral p38 stress pathway originated in the root of opisthokonts, most likely as a cell's reaction to salinity change in the environment. In animals, the pathway became more complex and incorporated more stimuli and downstream targets due to the p38 sequence evolution in the docking and substrate binding sites around the hinge region. This study improves our understanding of p38 evolution and opens new perspectives for p38 research.

Published

2023