Your search keyword '"Ugalde‐Triviño, Lola"' showing total 6 results

1. Proton pump inhibitor effect on esophageal protein signature of eosinophilic esophagitis, prediction, and evaluation of treatment response.

Author

Molina‐Jiménez, Francisca, Ugalde‐Triviño, Lola, Arias‐González, Laura, Armenteros, Elisa, Relaño‐Rupérez, Carlos, Casabona, Sergio, Moreno‐Monteagudo, José Andrés, Pérez‐Fernández, María Teresa, Martín‐Domínguez, Verónica, Fernández‐Pacheco, Jennifer, Laserna‐Mendieta, Emilio José, Muñoz‐Hernández, Patricia, García‐Martínez, Jorge, Muñoz, Javier, Lucendo, Alfredo J., Santander, Cecilio, and Majano, Pedro

Subjects

*PROTON pump inhibitors, *EOSINOPHILS, *SIGNAL processing, *EOSINOPHILIC esophagitis, *PROTEOMICS, *INFLAMMATION

Abstract

Background Methods Results Conclusion Recently, we have identified a dysregulated protein signature in the esophageal epithelium of eosinophilic esophagitis (EoE) patients including proteins associated with inflammation and epithelial barrier function; however, the effect of proton pump inhibitor (PPI) treatment on this signature is unknown. Herein, we used a proteomic approach to investigate: (1) whether PPI treatment alters the esophageal epithelium protein profile observed in EoE patients and (2) whether the protein signature at baseline predicts PPI response.We evaluated the protein signature of esophageal biopsies using a cohort of adult EoE (n = 25) patients and healthy controls (C) (n = 10). In EoE patients, esophageal biopsies were taken before (pre) and after (post) an 8‐week PPI treatment, determining the histologic response. Eosinophil count PostPPI was used to classify the patients: ≥15 eosinophils/hpf as non‐responders (non‐responder) and < 15 eosinophils/hpf as responders (R). Protein signature was determined and differentially accumulated proteins were characterized to identify altered biological processes and signaling pathways.Comparative analysis of differentially accumulated proteins between groups revealed common signatures between three groups of patients with inflammation (responder‐PrePPI, non‐responder‐PrePPI, and non‐responder‐PostPPI) and without inflammation (controls and responder‐PostPPI). PPI therapy almost reversed the EoE specific esophageal protein signature, which is enriched in pathways associated with inflammation and epithelial barrier function, in responder‐PostPPI. Furthermore, we identified a set of candidate proteins to differentiate responder‐PrePPI and non‐responder‐PrePPI EoE patients before treatment.These findings provide evidence that PPI therapy reverses the alterations in esophageal inflammatory and epithelial proteins characterizing EoE, thereby providing new insights into the mechanism of PPI clinical response. Interestingly, our results also suggest that PPI response could be predicted at baseline in EoE. [ABSTRACT FROM AUTHOR]

Published

2024

2. Circulating immunome fingerprint in eosinophilic esophagitis is associated with clinical response to proton pump inhibitor treatment.

Author

Ugalde-Triviño, Lola, Molina-Jiménez, Francisca, H.-Vázquez, Juan, Relaño-Rupérez, Carlos, Arias-González, Laura, Casabona, Sergio, Pérez-Fernandez, Maria Teresa, Martín-Domínguez, Verónica, Fernández-Pacheco, Jennifer, Lucendo, Alfredo J., Bernardo, David, Santander, Cecilio, and Majano, Pedro

Subjects

EOSINOPHILIC esophagitis, PROTON pump inhibitors, DENDRITIC cells

Abstract

Objectives: The aim of the study was to characterize the circulating immunome of patients with EoE before and after proton pump inhibitor (PPI) treatment in order to identify potential non-invasive biomarkers of treatment response. Methods: PBMCs from 19 healthy controls and 24 EoE patients were studied using a 39-plex spectral cytometry panel. The plasmacytoid dendritic cell (pDC) population was differentially characterized by spectral cytometry analysis and immunofluorescence assays in esophageal biopsies from 7 healthy controls and 13 EoE patients. Results: Interestingly, EoE patients at baseline had lower levels of circulating pDC compared with controls. Before treatment, patients with EoE who responded to PPI therapy had higher levels of circulating pDC and classical monocytes, compared with non-responders. Moreover, following PPI therapy pDC levels were increased in all EoE patients, while normal levels were only restored in PPIresponding patients. Finally, circulating pDC levels inversely correlated with peak eosinophil count and pDC count in esophageal biopsies. The number of tissue pDCs significantly increased during active EoE, being even higher in nonresponder patients when compared to responder patients pre-PPI. pDC levels decreased after PPI intake, being further restored almost to control levels in responder patients post-PPI. Conclusions: We hereby describe a unique immune fingerprint of EoE patients at diagnosis. Moreover, circulating pDC may be also used as a novel non-invasive biomarker to predict subsequent response to PPI treatment. [ABSTRACT FROM AUTHOR]

Published

2024

3. Proteomic analysis of the esophageal epithelium reveals key features of eosinophilic esophagitis pathophysiology

Author

Lucendo, Alfredo J., Santander, Cecilio, Majano Rodríguez, Pedro Lorenzo, Molina Jiménez, Francisca, Ugalde Triviño, Lola, Arias González, Laura, Relaño Rupérez, Carlos, Casabona, Sergio, Pérez Fernández, María Teresa, Martín Domínguez, Verónica, Fernández Pacheco, Jennifer, Laserna Mendieta, Emilio José, Muñoz Hernández, Patricia, Arias Arias, Ángel, Cano, Ainara, Muñoz, Javier, Majano, Pedro, Lucendo, Alfredo J., Santander, Cecilio, Majano Rodríguez, Pedro Lorenzo, Molina Jiménez, Francisca, Ugalde Triviño, Lola, Arias González, Laura, Relaño Rupérez, Carlos, Casabona, Sergio, Pérez Fernández, María Teresa, Martín Domínguez, Verónica, Fernández Pacheco, Jennifer, Laserna Mendieta, Emilio José, Muñoz Hernández, Patricia, Arias Arias, Ángel, Cano, Ainara, Muñoz, Javier, and Majano, Pedro

Abstract

Background Eosinophilic esophagitis (EoE) is a chronic non-IgE-mediated allergic disease of the esophagus. An unbiased proteomics approach was performed to investigate pathophysiological changes in esophageal epithelium. Additionally, an RNAseq-based transcriptomic analysis in paired samples was also carried out. Methods Total proteins were purified from esophageal endoscopic biopsies in a cohort of adult EoE patients (n = 25) and healthy esophagus controls (n = 10). Differentially accumulated (DA) proteins in EoE patients compared to control tissues were characterized to identify altered biological processes and signaling pathways. Results were also compared with a quantitative proteome dataset of the human esophageal mucosa. Next, results were contrasted with those obtained after RNAseq analysis in paired samples. Finally, we matched up protein expression with two EoE-specific mRNA panels (EDP and Eso-EoE panel). Results A total of 1667 proteins were identified, of which 363 were DA in EoE. RNA sequencing in paired samples identified 1993 differentially expressed (DE) genes. Total RNA and protein levels positively correlated, especially in DE mRNA-proteins pairs. Pathway analysis of these proteins in EoE showed alterations in immune and inflammatory responses for the upregulated proteins, and in epithelial differentiation, cornification and keratinization in those downregulated. Interestingly, a set of DA proteins, including eosinophil-related and secreted proteins, were not detected at the mRNA level. Protein expression positively correlated with EDP and Eso-EoE, and corresponded with the most abundant proteins of the human esophageal proteome. Conclusions We unraveled for the first time key proteomic features involved in EoE pathogenesis. An integrative analysis of transcriptomic and proteomic datasets provides a deeper insight than transcriptomic alone into understanding complex disease mechanisms., European Regional Development Fund, Ministerio de Ciencia e Innovación (MCIN), Ministerio de Trabajo y Economía Social, Comunidad de Madrid, Asociacion Española de Gastroenterología, Instituto de Salud Carlos III, Depto. de Biología Celular, Fac. de Ciencias Biológicas, TRUE, pub

Published

2023

4. Proteomic analysis of the esophageal epithelium reveals key features of eosinophilic esophagitis pathophysiology.

Author

Molina‐Jiménez, Francisca, Ugalde‐Triviño, Lola, Arias‐González, Laura, Relaño‐Rupérez, Carlos, Casabona, Sergio, Pérez‐Fernández, María Teresa, Martín‐Domínguez, Verónica, Fernández‐Pacheco, Jennifer, Laserna‐Mendieta, Emilio José, Muñoz‐Hernández, Patricia, Arias‐Arias, Ángel, Cano, Ainara, Muñoz, Javier, Lucendo, Alfredo J., Santander, Cecilio, and Majano, Pedro

Subjects

*EOSINOPHILIC esophagitis, *PROTEOMICS, *EPITHELIUM, *ESOPHAGUS diseases, *PROTEIN expression, *PATHOLOGICAL physiology

Abstract

Background: Eosinophilic esophagitis (EoE) is a chronic non‐IgE‐mediated allergic disease of the esophagus. An unbiased proteomics approach was performed to investigate pathophysiological changes in esophageal epithelium. Additionally, an RNAseq‐based transcriptomic analysis in paired samples was also carried out. Methods: Total proteins were purified from esophageal endoscopic biopsies in a cohort of adult EoE patients (n = 25) and healthy esophagus controls (n = 10). Differentially accumulated (DA) proteins in EoE patients compared to control tissues were characterized to identify altered biological processes and signaling pathways. Results were also compared with a quantitative proteome dataset of the human esophageal mucosa. Next, results were contrasted with those obtained after RNAseq analysis in paired samples. Finally, we matched up protein expression with two EoE‐specific mRNA panels (EDP and Eso‐EoE panel). Results: A total of 1667 proteins were identified, of which 363 were DA in EoE. RNA sequencing in paired samples identified 1993 differentially expressed (DE) genes. Total RNA and protein levels positively correlated, especially in DE mRNA‐proteins pairs. Pathway analysis of these proteins in EoE showed alterations in immune and inflammatory responses for the upregulated proteins, and in epithelial differentiation, cornification and keratinization in those downregulated. Interestingly, a set of DA proteins, including eosinophil‐related and secreted proteins, were not detected at the mRNA level. Protein expression positively correlated with EDP and Eso‐EoE, and corresponded with the most abundant proteins of the human esophageal proteome. Conclusions: We unraveled for the first time key proteomic features involved in EoE pathogenesis. An integrative analysis of transcriptomic and proteomic datasets provides a deeper insight than transcriptomic alone into understanding complex disease mechanisms. [ABSTRACT FROM AUTHOR]

Published

2023

5. PSD-95: An Effective Target for Stroke Therapy Using Neuroprotective Peptides

Author

Ugalde-Triviño, Lola, primary and Díaz-Guerra, Margarita, additional

Published

2021

6. PSD-95: An effective target for stroke therapy using neuroprotective peptides

Author

Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Ugalde-Triviño, Lola, Díaz-Guerra, Margarita, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Ugalde-Triviño, Lola, and Díaz-Guerra, Margarita

Abstract

Therapies for stroke have remained elusive in the past despite the great relevance of this pathology. However, recent results have provided strong evidence that postsynaptic density protein-95 (PSD-95) can be exploited as an efficient target for stroke neuroprotection by strategies able to counteract excitotoxicity, a major mechanism of neuronal death after ischemic stroke. This scaffold protein is key to the maintenance of a complex framework of protein interactions established at the postsynaptic density (PSD) of excitatory neurons, relevant to neuronal function and survival. Using cell penetrating peptides (CPPs) as therapeutic tools, two different approaches have been devised and advanced to different levels of clinical development. First, nerinetide (Phase 3) and AVLX-144 (Phase 1) were designed to interfere with the coupling of the ternary complex formed by PSD-95 with GluN2B subunits of the N-methyl-D-aspartate type of glutamate receptors (NMDARs) and neuronal nitric oxide synthase (nNOS). These peptides reduced neurotoxicity derived from NMDAR overactivation, decreased infarct volume and improved neurobehavioral results in different models of ischemic stroke. However, an important caveat to this approach was PSD-95 processing by calpain, a pathological mechanism specifically induced by excitotoxicity that results in a profound alteration of survival signaling. Thus, a third peptide (TP95) has been recently developed to interfere with PSD-95 cleavage and reduce neuronal death, which also improves neurological outcome in a preclinical mouse model of permanent ischemia. Here, we review recent advancements in the development and characterization of PSD-95-targeted CPPs and propose the combination of these two approaches to improve treatment of stroke and other excitotoxicity-associated disorders.

Published

2021