Your search keyword '"Pulito-Cueto, Verónica"' showing total 4 results

1. Inflammasome-Related Genetic Polymorphisms as Severity Biomarkers of COVID-19.

Author

Pulito-Cueto, Verónica, Sebastián Mora-Gil, María, Ferrer-Pargada, Diego, Remuzgo-Martínez, Sara, Genre, Fernanda, Lera-Gómez, Leticia, Alonso-Lecue, Pilar, Batista-Liz, Joao Carlos, Tello-Mena, Sandra, Abascal-Bolado, Beatriz, Izquierdo, Sheila, Ruiz-Cubillán, Juan José, Armiñanzas-Castillo, Carlos, Blanco, Ricardo, González-Gay, Miguel A., López-Mejías, Raquel, and Cifrián, José M.

Subjects

*COVID-19, *GENETIC polymorphisms, *BIOMARKERS

Abstract

The most critical forms of coronavirus disease 2019 (COVID-19) are associated with excessive activation of the inflammasome. Despite the COVID-19 impact on public health, we still do not fully understand the mechanisms by which the inflammatory response influences disease prognosis. Accordingly, we aimed to elucidate the role of polymorphisms in the key genes of the formation and signaling of the inflammasome as biomarkers of COVID-19 severity. For this purpose, a large and well-defined cohort of 377 COVID-19 patients with mild (n = 72), moderate (n = 84), severe (n = 100), and critical (n = 121) infections were included. A total of 24 polymorphisms located in inflammasome-related genes (NLRP3, NLRC4, NLRP1, CARD8, CASP1, IL1B, IL18, NFKB1, ATG16L1, and MIF) were genotyped in all of the patients and in the 192 healthy controls (HCs) (who were without COVID-19 at the time of and before the study) by RT-qPCR. Our results showed that patients with mild, moderate, severe, and critical COVID-19 presented similar allelic and genotypic distribution in all the variants studied. No statistically significant differences in the haplotypic distribution of NLRP3, NLRC4, NLRP1, CARD8, CASP1, IL1B, and ATG16L1 were observed between COVID-19 patients, who were stratified by disease severity. Each stratified group of patients presented a similar genetic distribution to the HCs. In conclusion, our results suggest that the inflammasome polymorphisms studied are not associated with the worsening of COVID-19. [ABSTRACT FROM AUTHOR]

Published

2024

2. IgA Vasculitis: Influence of CD40, BLK and BANK1 Gene Polymorphisms.

Author

Batista Liz, Joao Carlos, Genre, Fernanda, Pulito-Cueto, Verónica, Remuzgo-Martínez, Sara, Prieto-Peña, Diana, Márquez, Ana, Ortego-Centeno, Norberto, Leonardo, María Teresa, Peñalba, Ana, Narváez, Javier, Martín-Penagos, Luis, Belmar-Vega, Lara, Gómez-Fernández, Cristina, Miranda-Filloy, José A., Caminal-Montero, Luis, Collado, Paz, De Árgila, Diego, Quiroga-Colina, Patricia, Vicente-Rabaneda, Esther F., and Triguero-Martínez, Ana

Subjects

GENETIC polymorphisms, IMMUNOGLOBULIN A, VASCULITIS, GENETIC variation, HAPLOTYPES, DELAYED onset of disease, MUCOCUTANEOUS lymph node syndrome, SCHOENLEIN-Henoch purpura

Abstract

CD40, BLK and BANK1 genes involved in the development and signaling of B-cells are identified as susceptibility loci for numerous inflammatory diseases. Accordingly, we assessed the potential influence of CD40, BLK and BANK1 on the pathogenesis of immunoglobulin-A vasculitis (IgAV), predominantly a B-lymphocyte inflammatory condition. Three genetic variants within CD40 (rs1883832, rs1535045, rs4813003) and BLK (rs2254546, rs2736340, rs2618476) as well as two BANK1 polymorphisms (rs10516487, rs3733197), previously associated with inflammatory diseases, were genotyped in 382 Caucasian patients with IgAV and 955 sex- and ethnically matched healthy controls. No statistically significant differences were observed in the genotype and allele frequencies of CD40, BLK and BANK1 when IgAV patients and healthy controls were compared. Similar results were found when CD40, BLK and BANK1 genotypes or alleles frequencies were compared between patients with IgAV stratified according to the age at disease onset or to the presence/absence of gastrointestinal or renal manifestations. Moreover, no CD40, BLK and BANK1 haplotype differences were disclosed between patients with IgAV and healthy controls and between patients with IgAV stratified according to the clinical characteristics mentioned above. Our findings indicate that CD40, BLK and BANK1 do not contribute to the genetic background of IgAV. [ABSTRACT FROM AUTHOR]

Published

2022

3. BAFF, APRIL and BAFFR on the pathogenesis of Immunoglobulin-A vasculitis.

Author

Prieto-Peña, Diana, Genre, Fernanda, Remuzgo-Martínez, Sara, Pulito-Cueto, Verónica, Atienza-Mateo, Belén, Llorca, Javier, Sevilla-Pérez, Belén, Ortego-Centeno, Norberto, Lera-Gómez, Leticia, Leonardo, María Teresa, Peñalba, Ana, Narváez, Javier, Martín-Penagos, Luis, Rodrigo, Emilio, Miranda-Filloy, José A., Caminal-Montero, Luis, Collado, Paz, Pérez, Javier Sánchez, de Argila, Diego, and Rubio, Esteban

Subjects

VASCULITIS, IMMUNOGLOBULIN A, B cells, GENETIC polymorphisms, AUTOIMMUNE diseases

Abstract

BAFF, APRIL and BAFF-R are key proteins involved in the development of B-lymphocytes and autoimmunity. Additionally, BAFF, APRIL and BAFFR polymorphisms were associated with immune-mediated conditions, being BAFF GCTGT>A a shared insertion-deletion genetic variant for several autoimmune diseases. Accordingly, we assessed whether BAFF, APRIL and BAFFR represent novel genetic risk factors for Immunoglobulin-A vasculitis (IgAV), a predominantly B-lymphocyte inflammatory condition. BAFF rs374039502, which colocalizes with BAFF GCTGT>A, and two tag variants within APRIL (rs11552708 and rs6608) and BAFFR (rs7290134 and rs77874543) were genotyped in 386 Caucasian IgAV patients and 806 matched healthy controls. No genotypes or alleles differences were observed between IgAV patients and controls when BAFF, APRIL and BAFFR variants were analysed independently. Likewise, no statistically significant differences were found in the genotype and allele frequencies of BAFF, APRIL or BAFFR when IgAV patients were stratified according to the age at disease onset or to the presence/absence of gastrointestinal (GI) or renal manifestations. Similar results were disclosed when APRIL and BAFFR haplotypes were compared between IgAV patients and controls and between IgAV patients stratified according to the clinical characteristics mentioned above. Our results suggest that BAFF, APRIL and BAFFR do not contribute to the genetic network underlying IgAV. [ABSTRACT FROM AUTHOR]

Published

2021

4. Identification of a 3′‐Untranslated Genetic Variant of RARB Associated With Carotid Intima‐Media Thickness in Rheumatoid Arthritis: A Genome‐Wide Association Study.

Author

López‐Mejías, Raquel, Carmona, F. David, Genre, Fernanda, Remuzgo‐Martínez, Sara, González‐Juanatey, Carlos, Corrales, Alfonso, Vicente, Esther F., Pulito‐Cueto, Verónica, Miranda‐Filloy, José A., Ramírez Huaranga, Marco A., Blanco, Ricardo, Robustillo‐Villarino, Montserrat, Rodríguez‐Carrio, Javier, Alperi‐López, Mercedes, Alegre‐Sancho, Juan J., Mijares, Verónica, Lera‐Gómez, Leticia, Pérez‐Pampín, Eva, González, Antonio, and Ortega‐Castro, Rafaela

Subjects

ATHEROSCLEROSIS risk factors, ALLELES, CARDIOVASCULAR diseases, CARDIOVASCULAR diseases risk factors, CELL receptors, CELLULAR signal transduction, COLLAGEN, COMPARATIVE studies, GENETIC polymorphisms, GENOMES, IMMUNE system, RHEUMATOID arthritis, CAROTID artery stenosis, ONTOLOGIES (Information retrieval), CAROTID intima-media thickness, METABOLISM

Abstract

Objective: To investigate the genetic background influencing the development of cardiovascular (CV) disease in patients with rheumatoid arthritis (RA). Methods: We performed a genome‐wide association study (GWAS) in which, after quality control and imputation, a total of 6,308,944 polymorphisms across the whole genome were analyzed in 2,989 RA patients of European origin. Data on subclinical atherosclerosis, obtained through assessment of carotid intima‐media thickness (CIMT) and presence/absence of carotid plaques by carotid ultrasonography, were available for 1,355 individuals. Results: A genetic variant of the RARB gene (rs116199914) was associated with CIMT values at the genome‐wide level of significance (minor allele [G] β coefficient 0.142, P = 1.86 × 10−8). Interestingly, rs116199914 overlapped with regulatory elements in tissues related to CV pathophysiology and immune cells. In addition, biologic pathway enrichment and predictive protein–protein relationship analyses, including suggestive GWAS signals of potential relevance, revealed a functional enrichment of the collagen biosynthesis network related to the presence/absence of carotid plaques (Gene Ontology no. 0032964; false discovery rate–adjusted P = 4.01 × 10−3). Furthermore, our data suggest potential influences of the previously described candidate CV risk loci NFKB1,MSRA, and ZC3HC1 (P = 8.12 × 10−4, P = 5.94 × 10−4, and P = 2.46 × 10−4, respectively). Conclusion: The present findings strongly suggest that genetic variation within RARB contributes to the development of subclinical atherosclerosis in patients with RA. [ABSTRACT FROM AUTHOR]

Published

2019