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1. Killer‐cell immunoglobulin‐like receptor polymorphism is associated with COVID‐19 outcome: Results of a pilot observational study.

Author

Niño‐Ramírez, J. E., Alcoceba, M., Gutiérrez‐Zufiaurre, M. N., Marcos, M., Gil‐Etayo, F. J., Bartol‐Sánchez, M. R., Eiros, R., Chillón, M. C., García‐Álvarez, M., Terradillos‐Sánchez, P., Presa, D., Muñoz, J. L., López‐Bernús, A., López‐Sánchez, E., González‐Calle, D., Sánchez, P. L., Compán‐Fernández, O., González, M., García‐Sanz, R., and Boix, F.

Subjects
LOGISTIC regression analysis, GENETIC polymorphisms, TREATMENT effectiveness, IMMUNOGENETICS
Abstract

The pathogenesis of COVID‐19 warrants unravelling. Genetic polymorphism analysis may help answer the variability in disease outcome. To determine the role of KIR and HLA polymorphisms in susceptibility, progression, and severity of SARS‐CoV‐2 infection, 458 patients and 667 controls enrolled in this retrospective observational study from April to December 2020. Mild/moderate and severe/death study groups were established. HLA‐A, ‐B, ‐C, and KIR genotyping were performed using the Lifecodes® HLA‐SSO and KIR‐SSO kits on the Luminex® 200™ xMAP fluoroanalyser. A probability score using multivariate binary logistic regression analysis was calculated to estimate the likelihood of severe COVID‐19. ROC analysis was used to calculate the best cut‐off point for predicting a worse clinical outcome with high sensitivity and specificity. A p ≤ 0.05 was considered statistically significant. KIR AA genotype protected positively against severity/death from COVID‐19. Furthermore, KIR3DL1, KIR2DL3 and KIR2DS4 genes protected patients from severe forms of COVID‐19. KIR Bx genotype, as well as KIR2DL2, KIR2DS2, KIR2DS3 and KIR3DS1 were identified as biomarkers of severe COVID‐19. Our logistic regression model, which included clinical and KIR/HLA variables, categorised our cohort of patients as high/low risk for severe COVID‐19 disease with high sensitivity and specificity (Se = 94.29%, 95% CI [80.84–99.30]; Sp = 84.55%, 95% CI [79.26–88.94]; OR = 47.58, 95%CI [11.73–193.12], p < 0.0001). These results illustrate an association between KIR/HLA ligand polymorphism and different COVID‐19 outcomes and remarks the possibility of use them as a surrogate biomarkers to detect severe patients in possible future infectious outbreaks. [ABSTRACT FROM AUTHOR]

Published
2024
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5. VP33.15: MicroRNAs profile from plasma of pregnant women with intrauterine fetal growth restriction

Author

Muntion, S., primary, Boix, F., additional, Caro, M. Rodrigo, additional, Moruno, M. Huélamo, additional, de la Torre, A. Gómez, additional, Herrera, R. Ortega, additional, Antúnez, M. García, additional, Sánchez, P. Terradillos, additional, Alvarez, M. García, additional, Fraile, F., additional, Sánchez‐Guijo, F., additional, and Nava, A.M. Cubo, additional

Published
2021
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6. VP37.14: Pregnant women with pre‐eclampsia show increased serum levels of implantation and differentiation trophoblast factors

Author

Boix, F., primary, Muntion, S., additional, Moruno, M. Huélamo, additional, Caro, M. Rodrigo, additional, Sánchez, P. Terradillos, additional, Alvarez, M. García, additional, de la Torre, A. Gómez, additional, Herrera, R. Ortega, additional, Antúnez, M. García, additional, Fraile, F., additional, Sánchez‐Guijo, F., additional, and Nava, A.M. Cubo, additional

Published
2021
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11. Identification of peripheral CD154+ T cells and HLA-DRB1 as biomarkers of acute cellular rejection in adult liver transplant recipients

Author

Boix, F, primary, Legaz, I, additional, Minhas, A, additional, Alfaro, R, additional, Jiménez–Coll, V, additional, Mrowiec, A, additional, Martínez–Banaclocha, H, additional, Galián, J A, additional, Botella, C, additional, Moya–Quiles, M R, additional, Sanchez–Bueno, F, additional, Robles, R, additional, de la Peña–Moral, J, additional, Ramirez, P, additional, Pons, J A, additional, Minguela, A, additional, and Muro, M, additional

Published
2020
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12. EXPERIMENTAL CAVITATION INVESTIGATION OF THE ELECTROMAGNETIC PbBi PUMP WITH ROTATING PERMANENT MAGNETS.

Author

Kravalis, K., Boix, F., Bucenieks, I., Buligins, L., Delonca, M., Goldšteins, L., and Stora, T.

Subjects
*ELECTROMAGNETIC induction, *ELECTROMAGNETIC pumps, *PERMANENT magnets, *FLUID flow, *CAVITATION
Abstract

Electromagnetic induction pumps with rotating permanent magnets (EMP) are used mostly in experimental setups, where operation safety and reliability are crucial. Such pumps can face flow parameter decrease when operating at a low inlet pressure compared with those gained at higher inlet pressure values. The pump's developed flow rate increase does not correspond to the magnetic rotor rotation rate increase at the lower inlet pressure caused by the cavitation process at the pumps inlet tract. The study focuses on critical cavitation numbers at several inlet tract sections under severe cavitation conditions which prevent the flow rate increase. The current study is an experimental approach to characterize the pump operation parameters using cavitation numbers and comparing them with the literature data. [ABSTRACT FROM AUTHOR]

Published
2022
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15. Management of mixed acute rejection driven by a de novodonor-specific complement-binding anti-DQB1*03:01 antibody and intraepithelial CD8 T-cells in a kidney recipient: a case report

Author

Boix, F, Feito, J, Rodríguez-Campón, A, Chillón, MC, García-Sánchez, S, Tabernero, G, Fraile, P, and García-Sanz, R

Abstract

ABSTRACTMixed acute rejection is a clinicopathological entity that is difficult to accurately diagnose, and so may be under-reported. Allografts are lost more often than in either humoral or cellular rejection. The diagnosis requires both histological and immunological studies on renal biopsy and blood specimens from the transplant recipient to provide the required rescue therapy to abolish the allogeneic response against the graft. We present a clinical case report of an active mixed acute rejection driven by a de novodonor-specific complement-binding anti-DQB1*03:01 antibody and intraepithelial CD8 T-cells in a patient with a kidney transplant. The patient was diagnosed, treated, and followed up as per the local institution’s procedure with a full recovery of graft function. Our case emphasises the challenge of a mixed acute rejection and supports the need to improve the post-transplant outcome of recipients and their grafts.

Published
2021
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16. Identification of peripheral CD154+ T cells and HLA‐DRB1 as biomarkers of acute cellular rejection in adult liver transplant recipients.

Author

Boix, F., Legaz, I., Minhas, A., Alfaro, R., Jiménez–Coll, V., Mrowiec, A., Martínez–Banaclocha, H., Galián, J. A., Botella, C., Moya–Quiles, M. R., Sanchez–Bueno, F., Robles, R., Peña–Moral, J., Ramirez, P., Pons, J. A., Minguela, A., and Muro, M.

Subjects
*T cells, *LIVER transplantation, *HLA histocompatibility antigens, *CELL surface antigens, *RECEIVER operating characteristic curves, *ALLOIMMUNITY, *CD3 antigen
Abstract

Summary: Decreasing graft rejection and increasing graft and patient survival are great challenges facing liver transplantation (LT). Different T cell subsets participate in the acute cellular rejection (ACR) of the allograft. Cell‐mediated immunity markers of the recipient could help to understand the mechanisms underlying acute rejection. This study aimed to analyse different surface antigens on T cells in a cohort of adult liver patients undergoing LT to determine the influence on ACR using multi‐parametric flow cytometry functional assay. Thirty patients were monitored at baseline and during 1 year post‐transplant. Two groups were established, with (ACR) and without (NACR) acute cellular rejection. Leukocyte, total lymphocyte, percentages of CD4+CD154+ and CD8+CD154+ T cells, human leukocyte antigen (HLA) mismatch between recipient–donor and their relation with ACR as well as the acute rejection frequencies were analysed. T cells were stimulated with concanavalin A (Con‐A) and surface antigens were analysed by fluorescence activated cell sorter (FACS) analysis. A high percentage of CD4+CD154+ T cells (P = 0·001) and a low percentage of CD8+CD154+ T cells (P = 0·002) at baseline were statistically significant in ACR. A receiver operating characteristic analysis determined the cut‐off values capable to stratify patients at high risk of ACR with high sensitivity and specificity for CD4+CD154+ (P = 0·001) and CD8+CD154+ T cells (P = 0·002). In logistic regression analysis, CD4+CD154+, CD8+CD154+ and HLA mismatch were confirmed as independent risk factors to ACR. Post‐transplant percentages of both T cell subsets were significantly higher in ACR, despite variations compared to pretransplant. These findings support the selection of candidates for LT based on the pretransplant percentages of CD4+CD154+ and CD8+CD154+ T cells in parallel with other transplant factors. [ABSTRACT FROM AUTHOR]

Published
2021
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18. Pretransplant CD28 Biomarker (Levels of Expression and Quantification of Molecules per Cell) in Peripheral CD4+ T Cells Predicts Acute Rejection Episodes in Liver and Kidney Recipients

Author

Boix, F., primary, Bolarín, J.M., additional, Eguía, J., additional, Gonzalez-Martinez, G., additional, De La Peña, J., additional, Galian, J.A., additional, Hernández-Martínez, A.M., additional, Moya-Quiles, M.R., additional, Legaz, I., additional, Campillo, J.A., additional, Ramirez, P., additional, Sanchez-Bueno, F., additional, García-Alonso, A.M., additional, Pons, J.A., additional, Minguela, A., additional, Llorente, S., additional, and Muro, M., additional

Published
2016
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20. Activated Regulatory T Cells Expressing CD4+CD25highCD45RO+CD62L+ Biomarkers Could Be a Risk Factor in Liver Allograft Rejection

Author

Boix, F., primary, Millan, O., additional, San Segundo, D., additional, Mancebo, E., additional, Miras, M., additional, Rimola, A., additional, Fábrega, E., additional, Allende, L., additional, Minguela, A., additional, Paz-Artal, E., additional, López-Hoyos, M., additional, Brunet, M., additional, and Muro, M., additional

Published
2015
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23. Genetic polymorphisms of tumour necrosis factor alpha (TNF‐α) promoter gene and response to TNF‐α inhibitors in Spanish patients with inflammatory bowel disease

Author

López‐Hernández, R., primary, Valdés, M., additional, Campillo, J. A., additional, Martínez‐Garcia, P., additional, Salama, H., additional, Salgado, G., additional, Boix, F., additional, Moya‐Quiles, M. R., additional, Minguela, A., additional, Sánchez‐Torres, A., additional, Miras, M., additional, Garcia, A., additional, Carballo, F., additional, Álvarez‐López, M. R., additional, and Muro, M., additional

Published
2013
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24. C1q-Fixing Human Leukocyte Antigen Assay in Immunized Renal Patients: Correlation Between Luminex SAB-C1q and SAB-IgG

Author

Llorente, S., primary, Boix, F., additional, Eguia, J., additional, López, M., additional, Bosch, A., additional, Martinez, H., additional, Gonzalez, M.J., additional, López-Hernández, R., additional, Salgado, G., additional, Moya-Quiles, M.R., additional, Campillo, J.A., additional, García-Alonso, A.M., additional, Minguela, A., additional, Jimeno, L., additional, Álvarez-López, M.R., additional, and Muro, M., additional

Published
2012
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26. Arrêt des extraits «poussière de maison: indications pour réorienter l'immunothérapie

Author

De Feytaud, M., primary, Etienne, V., additional, Suard-Boix, F., additional, Michel, G., additional, Roche, J.C., additional, Vast, C., additional, Lang, A., additional, Chehowah, J., additional, Busy, M.F., additional, Guilloux, L., additional, Leynadier, F., additional, Didierlaurent, A., additional, Fadel, R., additional, and André, C., additional

Published
1999
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27. Profil de sensibilisation des patients désensibilisés à la poussière de maison. Indications pour réorienter l'immunothérapie

Author

De Feytaud, M., primary, Etienne, V., additional, Suard-Boix, F., additional, Michel, G., additional, Roche, J.C., additional, Vast, C., additional, Lang, A., additional, Chehowah, J., additional, Busy, M.F., additional, Guilloux, L., additional, Leynadier, F., additional, Didierlaurent, A., additional, Fadel, R., additional, and Andre, C., additional

Published
1999
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28. Tolérance, compliance et efficacité de l'immunothérapie spécifique par des extraits allergéniques aqueux ou adsorbés sur phosphate de calcium

Author

Fadel, R., primary, Andre, C., additional, Bellanger, M., additional, Bonardel, N., additional, Brunet-Moret, M.J., additional, Castelain, C., additional, Caubet, Y., additional, Dollois, B., additional, Guinnepain, M.T., additional, Larchevesque, M., additional, Leynadier, F., additional, Nicolas, P., additional, Raffard, M., additional, Saada-Buisson, F., additional, and Suard-Boix, F., additional

Published
1998
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