Your search keyword '"López Farre, Antonio José"' showing total 16 results

1. FXa inhibition by rivaroxaban modifies mechanisms associated with the pathogenesis of human abdominal aortic aneurysms

Author

Moñux Ducaju, Guillermo, Zamorano León, José Javier, Marqués Pablo, Sopeña, Bernardo, García García, José Manuel, Laich de Koller, Guillermo, Calvo Rico, Bibiana, García Fernández, Miguel Ángel, Serrano, Javier, López Farre, Antonio José, Moñux Ducaju, Guillermo, Zamorano León, José Javier, Marqués Pablo, Sopeña, Bernardo, García García, José Manuel, Laich de Koller, Guillermo, Calvo Rico, Bibiana, García Fernández, Miguel Ángel, Serrano, Javier, and López Farre, Antonio José

Abstract

Aims To evaluate if rivaroxaban, an oral factor Xa (FXa) inhibitor, could modify the expression in vitro of inflammatory and oxidative stress biomarkers in abdominal aortic aneurysmal (AAA) sites showing intraluminal thrombus. Methods AAA sites with intraluminal mural thrombus were obtained from six patients undergoing elective AAA repair. In addition, control abdominal aortic samples were obtained from six organ donors. AAA sites were incubated in the presence and absence of 50 nmol l–1 rivaroxaban. Results AAA sites showing thrombus demonstrated higher content of FXa than control. Interleukin-6 levels released from AAA [Control: median: 23.45 (interquartile range: 16.17–37.15) vs. AAA: median: 153.07 (interquartile range: 100.80–210.69) pg ml–1 mg tissue–1, P < 0.05] and the expression levels of nitric oxide synthase 2 were significantly higher in AAA than in control. The protein expression level of NADPH oxidase subunits gp67-and gp91-phox, but did not gp47-phox, were also significantly higher in the AAA sites than in control. Addition of rivaroxaban to AAA sites explants significantly reduced the release of interleukin-6 [median: 51.61 (interquartile range: 30.87–74.03) pg ml–1 mg tissue–1, P < 0.05 with respect to AAA alone] and the content of nitric oxide synthase 2, gp67 and gp91-phox NADPH subunits. The content of matrix metallopeptidase 9 was significantly higher in the AAA sites as compared to control. Rivaroxaban also reduced matrix metallopeptidase 9 content in AAA sites to similar levels to control. Conclusions FXa inhibition by rivaroxaban exerted anti-inflammatory and antioxidative stress properties in human AAA sites, suggesting a role of FXa in these mechanisms associated with the pathogenesis of AAA., Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2024

2. BRCA2 gene mutations and coagulation-associated biomarkers

Author

Pérez Segura, Pedro, Zamorano León, José Javier, Acosta, Daniel, Santos Sancho, Juana María, Modrego, Javier, Caldés, Trinidad, de la Hoya, Miguel, Díaz-Rubio García, Eduardo, Díaz Millán, Isabel, Heras Jiménez, Natalia De Las, Rico Zalba, Luis, Lahera Julia, Vicente, Melander, Olle, López Farre, Antonio José, Pérez Segura, Pedro, Zamorano León, José Javier, Acosta, Daniel, Santos Sancho, Juana María, Modrego, Javier, Caldés, Trinidad, de la Hoya, Miguel, Díaz-Rubio García, Eduardo, Díaz Millán, Isabel, Heras Jiménez, Natalia De Las, Rico Zalba, Luis, Lahera Julia, Vicente, Melander, Olle, and López Farre, Antonio José

Abstract

Thromboembolic events are the second cause of death in cancer patients, although the mechanisms underlying this increased thromboembolic risk remain unclear. The aims of this study were to examine whether BRCA2 gene mutations may modify the circulating levels of thrombocoagulation biomarkers and whether breast cancer development may influence changes in such circulating biomarkers. The study was performed in 25 women with mutations in the BRCA2 gene (n=12 breast cancer, n=13 breast cancer-free) and in 13 BRCA2 non-mutant controls. Results revealed that plasma levels of fibrinogen gamma chain isotypes 2 and 3, haptoglobin isotypes 4 and 5, serotransferrin isotypes 3 and 4 and convertase C3/C5 isotypes 4 and 5 were significantly higher in BRCA2 mutation carriers compared to controls. However, plasma levels of vitamin D binding protein isotype 1 and alpha1-antitrypsin isotypes 2, 3 and 4 were significantly decreased in BRCA2 mutation carriers compared to controls. Plasma expression of PF4 and P-selectin was significantly higher in BRCA2 mutations carriers than in controls. BRCA2 truncated mutations conserving a binding region for RAD51 were associated with increased plasma levels of alpha1-antitrypsin isotypes 3 and 4 with respect to women showing BRCA2 mutations that loss the binding RD51 region to BRCA2. Only plasma levels of vitamin D binding protein isotypes 1 and 3 were significantly reduced and alpha 1-antitrypsin isotype 1 was increased in cancer-free BRCA2 mutation carriers compared to BRCA2 mutation carriers with breast cancer. The presence of BRCA2 mutations is associated with increased plasma levels of thrombo-coagulating-related proteins, which are independent to breast cancer development., Sociedad Española de Oncología, Fondo Europeo de Desarrollo Regional, Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2024

3. New circulating biomarkers for predicting cardiovascular death in healthy population

Author

Olle, Melander, Modrego, Javier, Zamorano León, José Javier, Santos Sancho, Juana María, Lahera Julia, Vicente, López Farre, Antonio José, Olle, Melander, Modrego, Javier, Zamorano León, José Javier, Santos Sancho, Juana María, Lahera Julia, Vicente, and López Farre, Antonio José

Abstract

There is interest to analyse newer biomarkers to identify healthy individuals at risk to develop cardiovascular disease (CVD) incidents and death. To determine in healthy individuals new circulating protein biomarkers, whose systemic levels may be associated with the risk of future development of CVD incidents and death. The study was performed in 82 individuals from the Malm€o Diet and Cancer study cohort, free from CVD of whom 41 developed CVD and 41 did not. Plasma proteins related to inflammation and thrombo-coagulating processes were analysed. a1-antitrypsin isotype 3 plasma levels were significantly higher while apolipoprotein J plasma levels were lower in participants that developed CVD incidents than those that did not develop acute cardiovascular episode. Of 82 participants, 17 died by CVD causes. There were proteins whose expression in plasma was significantly higher in participants suffering CVD death as compared with those that did not die by CVD. These proteins included: fibrinogen b-chain isotypes 1 and 3, fibrinogen-c-chain isotype 2, vitamin D-binding protein isotypes 1, 2 and 3, a1-antitrypsin isotypes 3 and 6, haptoglobin isotypes 3,4,5 and 5, haemopexin isotypes 1 and 2, and Rho/Rac guanine nucleotide exchange factor 2. Moreover, apolipoprotein J plasma levels were found lower in participants that died by cardiovascular cause. Association between plasma levels of proteins and CVD death was independent of age, gender, conventional risk factors and plasma C-reactive protein levels. Several protein plasma levels and protein isotypes related to inflammation and thrombo-coagulating phenomena were independently associated with the risk of future CVD death., Fondo de Investigaciones de la Seguridad Social, Unión Europea, Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2024

4. Pro-apoptotic properties and mitochondrial functionality in platelet-like-particles generated from low Aspirin-incubated Meg-01 cells

Author

Freixer, Gala, Zekri-Nechar, Khaoula, Zamorano-León, José J., Butta, Nora V, Monzón, Elena, Giner, Manel, Martínez Martínez, Carlos Hugo, Recio Hoyas, María José, López Farre, Antonio José, Freixer, Gala, Zekri-Nechar, Khaoula, Zamorano-León, José J., Butta, Nora V, Monzón, Elena, Giner, Manel, Martínez Martínez, Carlos Hugo, Recio Hoyas, María José, and López Farre, Antonio José

Abstract

Long-term therapy with low Aspirin (ASA) dose is basis to prevent thrombotic acute events. However, the anti-platelet mechanisms of ASA remain not completely known. The aim was to analyze if in vitro exposure of human megakaryocytes to low ASA concentration may alter the apoptotic features of the newly formed platelets. Cultured Meg-01 cells, a human megakaryoblastic cell line, were stimulated to form platelets with 10 nmol/L phorbol 12-myristate-13-acetate (PMA) in the presence and absence of ASA (0.33 mmol/L). Results revealed that platelet-like particles (PLPs) derived from ASA-exposed Meg-01 cells, showed higher content of pro-apoptotic proteins Bax and Bak than PLPs from non-ASA incubated Meg-01 cells. It was accompanied of reduced cytochrome C oxidase activity and higher mitochondrial content of PTEN-induced putative kinase-1 in PLPs from ASA-incubated Meg-01 cells. However, only after calcium ionophore A23187 stimulation, caspase-3 activity, the cytosolic cytochrome C content, and reduction of mitochondrial membrane potential were higher in PLPs from ASA-incubated megakaryocytes than in those from Meg-01 without ASA. Nitric oxide synthase 3 content was higher in PLPs from ASA-exposed Meg-01 cells than in PLPs from non-ASA incubated Meg-01 cells. The L-arginine antagonist, NG-Nitro-L-arginine Methyl Ester, reduced caspase-3 activity in A23187-stimulated PLPs generated from ASA-incubated Meg-01 cells. As conclusions exposure of megakaryocyte to ASA promotes that the newly generated PLPs have, under stimulating condition, higher sensitivity to go into apoptosis than those PLPs generated from Meg-01 cells without ASA. It could be associated with differences in mitochondrial functionality and NO formation., FIS (Fondo de Investigación Sanitaria), GenObIA, Depto. de Inmunología, Oftalmología y ORL, Fac. de Medicina, TRUE, pub

Published

2024

5. Serum biomarkers in uncontrolled no heart-beating donors may identify kidneys that will never work after transplantation

Author

López Farre, Antonio José, Santos Sancho, Juana María, Modrego, Javier, Zamorano León, José Javier, Martín, Leyre, Sánchez Fructuoso, Ana Isabel, Rodríguez Sierra, Pablo, Herrero Calvo, José Antonio, Río Gallegos, Francisco José Del, Barrientos Alberto, Barrientos Guzmán, Alberto, López Farre, Antonio José, Santos Sancho, Juana María, Modrego, Javier, Zamorano León, José Javier, Martín, Leyre, Sánchez Fructuoso, Ana Isabel, Rodríguez Sierra, Pablo, Herrero Calvo, José Antonio, Río Gallegos, Francisco José Del, Barrientos Alberto, and Barrientos Guzmán, Alberto

Abstract

Background/aims Kidneys from uncontrolled non heart-beating donors achieve a good level of renal function after transplantation. However, a number of them will never function in the recipient. Our aim was to determine if serum biomarkers associated with platelet activity, inflammation and the nitric oxide system in uncontrolled non heart-beating donors may help to predict no renal function recovery after renal transplantation. Methods Serum levels of interleukin (IL)-6, IL-10, intercellular cell adhesion molecule-1 (ICAM-1), cyclic guanosine monophosphate (cGMP), nitrite + nitrate and platelet factor-4 (PF4) were measured using enzyme-linked immunosorbent assay (ELISA) kits in 88 uncontrolled non heart-beating donors divided according to the renal functionality achieved in the recipients into functional (n = 76) and non functional (n = 12). Results Kidneys from donors with higher IL-6 levels (>900 pg/ml) were functional after transplantation. Serum cGMP levels below 372.3 fmol/l were also associated with kidneys that recovered the renal function. However, serum levels of PF4 showed the best correlation with recovery of renal functional in the recipients since they were significantly lower in the donors whose kidneys functioned after transplantation. Conclusions Serum PF4 levels in uncontrolled non heart-beating donors may be a good predictor for kidneys that never will reach functional recovery. Some serum cGMP, IL-6 and IL-10 levels may simply help identify kidneys that will function after transplantation., Fondo de Investigaciones de la Seguridad Social, Fondo Europeo de Desarrollo Regional, Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2024

6. Nitric oxide blocks hKv1.5 channels by S-nitrosylation and by a cyclic GMP-dependent mechanism

Author

Núñez Fernández, Lucía, Vaquero González, Luis Miguel, Gómez García, Ricardo, Caballero Collado, Ricardo, Mateos Cáceres, Petra, Macaya Miguel, Carlos, Iriepa Canalda, Isabel, Gálvez Ruano, Enrique, López Farre, Antonio José, Tamargo Menéndez, Juan, Delpón Mosquera, María Eva, Núñez Fernández, Lucía, Vaquero González, Luis Miguel, Gómez García, Ricardo, Caballero Collado, Ricardo, Mateos Cáceres, Petra, Macaya Miguel, Carlos, Iriepa Canalda, Isabel, Gálvez Ruano, Enrique, López Farre, Antonio José, Tamargo Menéndez, Juan, and Delpón Mosquera, María Eva

Abstract

Objective: This study was undertaken to analyze whether nitric oxide (NO) modulates the human potassium channel hKv1.5, which generates the ultrarapid delayed rectifier current (IKur) that determines the height and duration of atrial action potentials. Methods: Currents were recorded using the whole-cell patch-clamp in Ltk- cells expressing hKv1.5 channels. Results: The NO donors (+/-)-S-Nitroso-N-acetylpenicillamine (SNAP) and sodium nitroprusside, a NO solution, and l-Arginine inhibited hKv1.5 currents in a concentration-dependent manner. The NO concentration in the cell chamber was monitored using a sensor, and the IC50 for NO-induced hKv1.5 block was 340+/-70 nM. SNAP also inhibited the IKur recorded in mouse ventricular myocytes. The NO effects were partially mediated by the activation of the soluble guanylate cyclase (sGC)/cGMP/cGMP-dependent protein kinase (PKG) pathway. The biotin-switch assay demonstrated the presence of S-nitrosylated cysteines (Cys) on the hKv1.5 protein in SNAP-treated cells. Molecular modeling of hKv1.5 channel structure suggests that S-nitrosylation of Cys331 (segment 2, S2) and Cys346 (S2) would be stabilized by hydrogen bridge bonds with Ile262 (S1) and Arg342 (S2), respectively. Conclusions: NO inhibits the hKv1.5 current by a cGMP-dependent mechanism and by the S-nitrosylation of the hKv1.5 protein, an effect that contributes to shaping the human atrial action potentials., Mutua Madrileña Foundation, Red HERACLES, Depto. de Farmacología y Toxicología, Fac. de Medicina, TRUE, pub

Published

2024

7. Endothelial damage in major depression patients is modulated by SSRI treatment, as demonstrated by circulating biomarkers and an in vitro cell model

Author

Lopez Vilchez, Irene, Diaz Ricart, M, Navarro, V, Zamorano León, José Javier, López Farre, Antonio José, Galán, A. M., Gasto C, Escolar G, Lopez Vilchez, Irene, Diaz Ricart, M, Navarro, V, Zamorano León, José Javier, López Farre, Antonio José, Galán, A. M., Gasto C, and Escolar G

Abstract

There is a link between depression, cardiovascular events and inflammation. We have explored this connection through endothelial dysfunction, using in vivo and in vitro approaches. We evaluated circulating biomarkers of endothelial dysfunction in patients with major depression at their diagnosis (MD-0) and during antidepressant treatment with the selective serotonin reuptake inhibitor escitalopram, for 8 and 24 weeks (MD-8 and MD-24). Results were always compared with matched healthy controls (CON). We measured in vivo circulating endothelial cells (CECs) and endothelial progenitor cells (EPCs) in blood samples, and assessed plasma levels of soluble von Willebrand factor (VWF) and vascular cell adhesion molecule-1 (VCAM-1). CEC counts, soluble VWF and VCAM-1 were statistically elevated in MD-0 (P<0.01 versus CON) and gradually decreased during treatment. Conversely, EPC levels were lower in MD-0, tending to increase throughout treatment. In vitro studies were performed in human endothelial cells cultured in the presence of sera from each study group. Elevated expression of the inflammation marker intercellular adhesion molecule-1 and oxidative stress, with lower presence of endothelial nitric oxide synthase and higher reactive oxygen species production, were found in cells exposed to MD-0 sera (P<0.05 versus CON). These results were normalized in cells exposed to MD-24 sera. Thrombogenicity of extracellular matrices generated by these cells, measured as expression of VWF, tissue factor and platelet reactivity, showed non-significant differences. We provide a model of cultured endothelial cells reproducing endothelial dysfunction in naive patients with major depression, demonstrating endothelial damage and inflammation at diagnosis, and recovering with selective serotonin reuptake inhibitor treatment for 24 weeks., Instituto de Salud Carlos III, Cardiovascular Research Net, Health Institutes, Ministerio de Economía y Competitividad, Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2024

8. Nitric oxide inhibits Kv4.3 and human cardiac transient outward potassium current (Ito1)

Author

Gómez García, Ricardo, Macaya Miguel, Carlos, Caballero Collado, Ricardo, López Farre, Antonio José, Tamargo Menéndez, Juan, Delpón Mosquera, María Eva, Gómez García, Ricardo, Macaya Miguel, Carlos, Caballero Collado, Ricardo, López Farre, Antonio José, Tamargo Menéndez, Juan, and Delpón Mosquera, María Eva

Abstract

Aims: Chronic atrial fibrillation (CAF) is characterized by a shortening of the plateau phase of the action potentials (AP) and a decrease in the bioavailability of nitric oxide (NO). In this study, we analysed the effects of NO on Kv4.3 (I(Kv4.3)) and on human transient outward K(+) (I(to1)) currents as well as the signalling pathways responsible for them. We also analysed the expression of NO synthase 3 (NOS3) in patients with CAF. Methods and results: I(Kv4.3) and I(to1) currents were recorded in Chinese hamster ovary cells and in human atrial and mouse ventricular dissociated myocytes using the whole-cell patch clamp. The expression of NOS3 was analysed by western blotting. AP were recorded using conventional microelectrode techniques in mouse atrial preparations. NO and NO donors inhibited I(Kv4.3) and human I(to1) in a concentration- and voltage-dependent manner (IC(50) for NO: 375.0 +/- 48 nM) as a consequence of the activation of adenylate cyclase and the subsequent activation of the cAMP-dependent protein kinase and the serine-threonine phosphatase 2A. The density of the I(to1) recorded in ventricular myocytes from wild-type (WT) and NOS3-deficient mice (NOS3(-/-)) was not significantly different. Furthermore, the duration of atrial AP repolarization in WT and NOS3(-/-) mice was not different. The increase in NO levels to 200 nM prolonged the plateau phase of the mouse atrial AP and lengthened the AP duration measured at 20 and 50% of repolarization of the human atrial CAF-remodelled AP as determined using a mathematical model. However, the expression of NOS3 was not modified in left atrial appendages from CAF patients. Conclusion: Our results suggested that the increase in the atrial NO bioavailability could partially restore the duration of the plateau phase of CAF-remodelled AP by inhibiting the I(to1) as a result of the activation of non-canonical enzymatic pathways., Ministerio de Educación y Ciencia, Ministerio de Sanidad y Consumo, Instituto de Salud Carlos III, Sociedad Española de Cardiología, Fundación LILLY, Depto. de Farmacología y Toxicología, Fac. de Medicina, TRUE, pub

Published

2024

9. Platelet Content of Nitric Oxide Synthase 3 Phosphorylated At Serine1177 Is Associated with the Functional Response of Platelets to Aspirin

Author

Modrego, Javier, Azcona, Luis, Martín Palacios, Naiara, Zamorano León, José Javier, Segura, Antonio, Rodriguez, Pablo, Guerra, Reddy, Tamargo Menéndez, Juan, Macaya Miguel, Carlos, López Farre, Antonio José, Modrego, Javier, Azcona, Luis, Martín Palacios, Naiara, Zamorano León, José Javier, Segura, Antonio, Rodriguez, Pablo, Guerra, Reddy, Tamargo Menéndez, Juan, Macaya Miguel, Carlos, and López Farre, Antonio José

Abstract

Objective: To analyse if platelet responsiveness to aspirin (ASA) may be associated with a different ability of platelets to generate nitric oxide (NO). Patients/methods: Platelets were obtained from 50 patients with stable coronary ischemia and were divided into ASA-sensitive (n = 26) and ASA-resistant (n = 24) using a platelet functionality test (PFA-100). Results: ASA-sensitive platelets tended to release more NO (determined as nitrite + nitrate) than ASA-resistant platelets but it did not reach statistical significance. Protein expression of nitric oxide synthase 3 (NOS3) was higher in ASA-sensitive than in ASA-resistant platelets but there were no differences in the platelet expression of nitric oxide synthase 2 (NOS2) isoform. The highest NOS3 expression in ASA-sensitive platelets was independent of the presence of T-to-C mutation at nucleotide position -786 (T(-786) → C) in the NOS3-coding gene. However, platelet content of phosphorylated NOS3 at Serine (Ser)(1177), an active form of NOS3, was higher in ASA-sensitive than in ASA-resistant platelets. The level of platelet NOS3 Ser(1177) phosphorylation was positively associated with the closure time in the PFA-100 test. In vitro, collagen failed to stimulate the aggregation of ASA-sensitive platelets, determined by lumiaggregometry, and it was associated with a significant increase (p = 0.018) of NOS3 phosphorylation at Ser(1177). On the contrary, collagen stimulated the aggregation of ASA-resistant platelets but did not significantly modify the platelet content of phosphorylated NOS3 Ser(1177). During collagen stimulation the release of NO from ASA-sensitive platelets was significantly enhanced but it was not modified in ASA-resistant platelets. Conclusions: Functional platelet responsiveness to ASA was associated with the platelet content of phosphorylated NOS3 at Ser(1177)., Instituto de Salud Carlos III, Unión Europea, Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2024

10. Escitalopram Impairs Thrombin-Induced Platelet Response, Cytoskeletal Assembly and Activation of Associated Signalling Pathways

Author

López Víchez, Irene, Jerez Dolz, Didac, Díaz Ricart, Maribel, Navarro, Víctor, Urooj Zafar, M, Zamorano León, José Javier, López Farre, Antonio José, Badimon, Juan, Gasto, Cristóbal, Escolar, Ginés, López Víchez, Irene, Jerez Dolz, Didac, Díaz Ricart, Maribel, Navarro, Víctor, Urooj Zafar, M, Zamorano León, José Javier, López Farre, Antonio José, Badimon, Juan, Gasto, Cristóbal, and Escolar, Ginés

Abstract

Background Serotonin reuptake inhibitors (SSRIs) may impair platelet function. Thrombin is a strong platelet agonist causing irreversible aggregation, release of granules' contents, cytoskeletal rearrangement and activation of signalling pathways. We investigated the effects of the SSRI escitalopram (SCIT) on thrombin-induced platelet response. Methods Isolated platelets were exposed to SCIT and activated with thrombin. We evaluated (1) platelet response by aggregometry and flow cytometry; (2) modifications in cytoskeleton proteins and signalling pathways by electrophoresis and Western blot; and (3) ultrastructural changes in platelets by electron microscopy. Results SCIT inhibited platelet response to thrombin, measured as platelet aggregation and expression of activation markers CD62-P and CD63 from platelet granules. Platelet aggregation decreased in a dose-dependent manner, reaching statistical significance with SCIT ≥32 µg/mL (65.4 ± 6.8% vs. 77.7 ± 2.5% for controls; p < 0.05). Expression of activation markers was statistically reduced with SCIT ≥20 µg/mL (p < 0.05). SCIT impaired the polymerization of the actin cytoskeleton and association of contractile proteins during activation with thrombin (p < 0.05 with SCIT ≥50 µg/mL). Resting platelets incubated with SCIT became most spherical, with increased platelet roundness (p < 0.01, SCIT 50 µg/mL vs. control). SCIT interfered with signalling pathways modulated by thrombin (RhoA, PKC, Erk1/2 and PI3K/AKT). Conclusions Our data indicate that SCIT inhibits thrombin-induced platelet response and interferes with cytoskeletal assembly and related signalling pathways, thus resulting in compromised release of granules' contents, reduced platelet activation and aggregation. These mechanisms may explain the antithrombotic benefits observed in patients treated with this SSRI, and could become new therapeutic targets for future antithrombotic strategies., Instituto de Salud Carlos III, Red de Investigación Cardiovascular, European Regional Development Fund, Ministerio de Economía y Competitividad, Technology Development Projects in Health, CIBERSAM, Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2024

11. Impact of Clopidogrel and Aspirin Treatment on the Expression of Proteins in Platelets from Type-2 Diabetic Patients with Stable Coronary Ischemia

Author

Azcona, Luis, López Farre, Antonio José, Jiménez Mateos Cáceres, Petra, Segura, Antonio, Rodríguez Sierra, Pablo, Modrego, Javier, Zamorano León, José Javier, Macaya Miguel, Carlos, Azcona, Luis, López Farre, Antonio José, Jiménez Mateos Cáceres, Petra, Segura, Antonio, Rodríguez Sierra, Pablo, Modrego, Javier, Zamorano León, José Javier, and Macaya Miguel, Carlos

Abstract

The purpose of this study was to compare the effect of dual antiplatelet therapy [clopidogrel + aspirin (ASA)] with respect to ASA on the protein expression of platelets from controlled type-2 diabetic patients with stable coronary ischemia. Patients had been taking ASA (100 mg day) and they were randomized to receive (n = 29) or not (n = 28) 75 mg day clopidogrel for 12 ± 2 weeks in a blind form. Protein expression was analyzed by two-dimensional electrophoresis and mass spectrometry. The protein expression of a limited number of proteins such as actin-binding protein isotypes 2 and 5, lactate dehydrogenase, serotransferrin isotype 4, protein disulfide isomerase-A3 isotype 1, fibrinogen beta chain isotype 5, Ras-related protein Rab-7b isotypes 1 and 6, and immunoglobulin heavy chain was changed after dual antiplatelet therapy. Plasma level of platelet factor 4 (PF4), an in vivo marker of platelet activity, was not different between both groups. These changes suggest lower platelet reactivity after dual antiplatelet therapy in the studied patients. However, the variation in platelet proteome was lower than it would be initially expected, taking into account the apparent clinical beneficial effects of dual antiplatelet therapy. PF4 plasma level was not further decreased in the platelets treated for a longer time than 9-12 months with ASA + clopidogrel, as compared with ASA alone., Fondo de Investigacion de la Seguridad Social, Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2024

12. Nitric oxide from mononuclear cells may be involved in platelet responsiveness to aspirin

Author

López Farre, Antonio José, Modrego Javier, Azcona, Luis, Guerra, Redy, Segura, Antonio, Rodríguez Sierra, Pablo, Zamorano León, José Javier, Lahera Julia, Vicente, Macaya Miguel, Carlos, López Farre, Antonio José, Modrego Javier, Azcona, Luis, Guerra, Redy, Segura, Antonio, Rodríguez Sierra, Pablo, Zamorano León, José Javier, Lahera Julia, Vicente, and Macaya Miguel, Carlos

Abstract

Background Several mechanisms have been proposed to explain why some platelets have a reduced response to aspirin (ASA). Among them, it was reported an increased circulating level of vitamin-D-binding protein (DBP). In addition, nitric oxide (NO) released from mononuclear cells was involved in the antiplatelet effects of ASA. The aim was to analyse the relationship between platelet response to ASA and both NO generation and vitamin-D-binding protein content in mononuclear cells. Materials and methods Mononuclear cells were obtained from patients with stable coronary artery disease that were divided by a platelet functionality test (PFA-100) as ASA-sensitive (n = 23) and ASA resistant (n = 27). Results Both the release of NO (determined by nitrite + nitrate concentration) and the expression of endothelial-type NO synthase (eNOS) were higher in mononuclear cells from ASA sensitive as compared with those from ASA-resistant patients. There was a positive correlation between either the release of NO and the expression of eNOS protein in mononuclear cells with the ability of ASA to inhibit platelet activity. DBP content in mononuclear cells was higher in ASA resistant than in ASA sensitive. The level of DBP content in mononuclear cells was negatively associated with the ability of ASA to inhibit platelets. However, in vitro experiments suggested that there was no association between DBP and NO production by mononuclear cells. Conclusions Mononuclear cells from patients with platelets with lower responsiveness to ASA showed a reduced ability to produce NO., Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, FALSE, pub

Published

2024

13. Plasma desmoplakin I biomarker of vascular recurrence after ischemic stroke

Author

López Farre, Antonio José, Zamorano León, José Javier, Segura, Antonio, Jiménez Mateos Cáceres, Petra, Modrego, Javier, Rodriguez Sierra, Pablo, Calatrava, Laura, Tamargo Menéndez, Juan, Macaya Miguel, Carlos, López Farre, Antonio José, Zamorano León, José Javier, Segura, Antonio, Jiménez Mateos Cáceres, Petra, Modrego, Javier, Rodriguez Sierra, Pablo, Calatrava, Laura, Tamargo Menéndez, Juan, and Macaya Miguel, Carlos

Abstract

Stroke patients have a high risk of vascular recurrence. Biomarkers related to vascular recurrence, however, remain to be identified. The aim of the study was to identify, through proteomic analysis, plasma biomarkers associated with vascular recurrence within one year after the first ischemic stroke. This is a substudy (n = 134) of a large prospective multicenter study of post-stroke patients with an ischemic stroke. Plasma samples were obtained at inclusion. Among the identified proteins, only plasma levels of desmoplakin I were associated with protection against a new vascular event (Odds ratio: 0.64; 95% CI: 0.46-0.89; p = 0.009) after adjustment for hypercholesterolemia, statins and previous atherothrombotic stroke subtype. A greater number of patients without vascular recurrence had been treated with statins within three months of the recent ischemic stroke. Only patients who had been taking statins for 3 months after the ischemic stroke and did not suffer vascular recurrence over a follow-up year, have higher levels of desmoplakin I at the time of inclusion (Odds ratio 0.49; 95% CI: 0.28-0.86; p = 0.013). Increased desmoplakin I levels, determined within 1-3 months of the first ischemic stroke, could be a biomarker for statin responsiveness against a new vascular event in post-ischemic stroke patients taking statins early (1-3 months) after the ischemic stroke., Brystol-Myers Squibb, Fondo de Investigaciones de la Seguridad Social, Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2024

14. Trends and Predictors for the Uptake of Colon Cancer Screening Using the Fecal Occult Blood Test in Spain from 2011 to 2017

Author

Zamorano León, José Javier, López De Andrés, Ana Isabel, Alvarez-Gonzalez A, Maestre-Miquel C, Astasio Arbiza, Paloma, López Farre, Antonio José, Miguel Díez, Javier De, Jiménez García, Rodrigo, Albaladejo-Vicente R, Zamorano León, José Javier, López De Andrés, Ana Isabel, Alvarez-Gonzalez A, Maestre-Miquel C, Astasio Arbiza, Paloma, López Farre, Antonio José, Miguel Díez, Javier De, Jiménez García, Rodrigo, and Albaladejo-Vicente R

Abstract

Background: In Spain, colorectal cancer screening using the fecal occult blood test, targeted towards the 50–69 age bracket, was implemented on different dates. We aim to assess the temporal trend of colorectal cancer (CRC) screening uptake according to the year of screening implementation in each region and to identify predictors for the uptake of CRC screening. Methods: A cross-sectional study with 12,657 participants from the Spanish National Health Surveys 2011 and 2017 was used. Uptake rates were analyzed according to the date that the screening program was implemented. Results: For regions with programs implemented before 2011, the uptake rate increased 3.34-fold from 2011 to 2017 (9.8% vs. 32.7%; p < 0.001). For regions that implemented screening within the 2011–2016 period, the uptake rose from 4.3% to 13.2% (3.07-fold; p < 0.001), and for regions that implemented screening after 2016, the uptake increased from 3.4% to 8.8% (2.59-fold; p < 0.001). For the entire Spanish population, the uptake increased 3.21-fold (6.8% vs. 21.8%; p < 0.001). Positive predictors for uptake were older age, Spanish nationality, middle-to-high educational level, suffering chronic diseases, non-smoking and living in regions where screening programs were implemented earlier. Conclusions: The different periods for the implementation of CRC screening as well as sociodemographic and health inequalities may have limited the improvement in the screening uptake from 2011 to 2017 in Spain., Depto. de Salud Pública y Materno - Infantil, Fac. de Medicina, TRUE, pub

Published

2020

15. Case report of a Spanish patient with arrhythmogenic right ventricular cardiomyopathy and palmoplantar keratoderma without plakoglobin and desmoplakin gene modifications

Author

Alonso Orgaz, S, Zamorano León, José Javier, Fernández Arquero, Miguel, Pérez Villacastín Domínguez, Julián, Perez-Castellano, N, García Torrent, María Jesús, Macaya Miguel, Carlos, López Farre, Antonio José, Alonso Orgaz, S, Zamorano León, José Javier, Fernández Arquero, Miguel, Pérez Villacastín Domínguez, Julián, Perez-Castellano, N, García Torrent, María Jesús, Macaya Miguel, Carlos, and López Farre, Antonio José

Abstract

We report a case of a 43 year old man from Spain, who has been diagnosed with Naxos disease. It is a hereditary disorder characterized by palmoplantar keratoderma, woolly hair and cardiomyopathy, which has been associated with a mutation in plakoglobin encoding gene in chromosome 17q21. In the patient, the direct sequencing of the plakoglobin gene discarded TG deletion at 2157 characteristic of Naxos disease. Analysis of the reported desmoplakin mutations associated with Carvajal Syndrome, another ARVC disease, that it is also accompanied with a skin and hair disorder, also failed to reveal mutations in desmoplakin gene. These results suggest the existence of other causative genes and/or other putative sites in desmoplakin/plakoglobin encoding genes than those recently published., Depto. de Medicina, Fac. de Medicina, TRUE, pub

Published

2007

16. Expression of endothelial nitric oxide synthase in human peritoneal tissue: regulation by escherichia coli lipopolysaccharide

Author

Arriero, María M., Rodríguez-Feo, Juan A., Celdrán, Ángel, Sánchez de Miguel, Lourdes, González Fernández, Fernando, Fortes, José, Reyero, Ana, Frieyro, Octavio, Pinta, Juan C de la, Franco, Ángeles, Casado, Santos, López Farre, Antonio José, Pastor Vargas, Carlos, Arriero, María M., Rodríguez-Feo, Juan A., Celdrán, Ángel, Sánchez de Miguel, Lourdes, González Fernández, Fernando, Fortes, José, Reyero, Ana, Frieyro, Octavio, Pinta, Juan C de la, Franco, Ángeles, Casado, Santos, López Farre, Antonio José, and Pastor Vargas, Carlos

Abstract

Changes in the expression of endothelial nitric oxide synthase (eNOS) in the peritoneum could be involved in the peritoneal dysfunction associated with peritoneal inflammation. Demonstrated recently in bovine endothelial cells was the existence of cytosolic proteins that bind to the 3′-untranslated region (3′-UTR) of eNOS mRNA and could be implicated in eNOS mRNA stabilization. The present work demonstrates that eNOS protein is expressed in human endothelial and mesothelial peritoneal cells. Escherichia coli lipopolysaccharide shortened the half-life of eNOS message, reducing eNOS protein expression in peritoneal mesothelial and endothelial cells. Moreover, under basal conditions, human peritoneal samples expressed cytosolic proteins that bind to the 3′-UTR of eNOS mRNA. The cytosolic proteins that directly bind to 3′-UTR were identified as a 60-kD protein. After incubation of human peritoneal samples with lipopolysaccharide, the binding activity of the cytosolic 60-kD protein increased in a time-dependent manner. Studies are now necessary to determine the involvement of this 60-kD protein in the regulation of eNOS expression in peritoneal cells and particularly its involvement in the peritoneal dysfunction associated with inflammatory reactions., Depto. de Bioquímica y Biología Molecular, Fac. de Ciencias Químicas, TRUE, pub

Published

2000