164 results on '"Marta Valle"'
Search Results
2. Mujer con hipertiroidismo y piernas en piel de naranja
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Salvador Labrador-Descalzo, Marta Valle-Coca, and Daniel Mata-Cano
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Medicine (General) ,R5-920 - Published
- 2025
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3. SERVICE-LEARNING IN NEUROSCIENCE TEACHING AND DISSEMINATION OF RESEARCH
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Marc López-Cano, Josep Argerich, Marta Valle-León, Alejandro Fernández-Solanas, and Víctor Fernández-Dueñas
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Neurosciences. Biological psychiatry. Neuropsychiatry ,RC321-571 - Published
- 2023
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4. Genetic diversification patterns in swine influenza A virus (H1N2) in vaccinated and nonvaccinated animals
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Álvaro López-Valiñas, Marta Valle, Marta Pérez, Ayub Darji, Chiara Chiapponi, Llilianne Ganges, Joaquim. Segalés, and José I. Núñez
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swine influenza virus ,viral evolution ,vaccination ,NGS ,quasispecies ,Microbiology ,QR1-502 - Abstract
Influenza A viruses (IAVs) are characterized by having a segmented genome, low proofreading polymerases, and a wide host range. Consequently, IAVs are constantly evolving in nature causing a threat to animal and human health. In 2009 a new human pandemic IAV strain arose in Mexico because of a reassortment between two strains previously circulating in pigs; Eurasian “avian-like” (EA) swine H1N1 and “human-like” H1N2, highlighting the importance of swine as adaptation host of avian to human IAVs. Nowadays, although of limited use, a trivalent vaccine, which include in its formulation H1N1, H3N2, and, H1N2 swine IAV (SIAV) subtypes, is one of the most applied strategies to reduce SIAV circulation in farms. Protection provided by vaccines is not complete, allowing virus circulation, potentially favoring viral evolution. The evolutionary dynamics of SIAV quasispecies were studied in samples collected at different times from 8 vaccinated and 8 nonvaccinated pigs, challenged with H1N2 SIAV. In total, 32 SIAV genomes were sequenced by next-generation sequencing, and subsequent variant-calling genomic analysis was carried out. Herein, a total of 364 de novo single nucleotide variants (SNV) were found along all genetic segments in both experimental groups. The nonsynonymous substitutions proportion found was greater in vaccinated animals suggesting that H1N2 SIAV was under positive selection in this scenario. The impact of each substitution with an allele frequency greater than 5% was hypothesized according to previous literature, particularly in the surface glycoproteins hemagglutinin and neuraminidase. The H1N2 SIAV quasispecies evolution capacity was evidenced, observing different evolutionary trends in vaccinated and nonvaccinated animals.
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- 2023
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5. Unique effect of clozapine on adenosine A2A-dopamine D2 receptor heteromerization
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Marta Valle-León, Nil Casajuana-Martin, Claudia Llinas del Torrent, Josep Argerich, Laura Gómez-Acero, Kristoffer Sahlholm, Sergi Ferré, Leonardo Pardo, and Francisco Ciruela
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Clozapine ,Haloperidol ,Aripiprazole ,Dopamine D2 receptor ,Adenosine A2A receptor ,Receptor heteromerization ,Therapeutics. Pharmacology ,RM1-950 - Abstract
The striatal dopamine D2 receptor (D2R) is generally accepted to be involved in positive symptoms of schizophrenia and is a main target for clinically used antipsychotics. D2R are highly expressed in the striatum, where they form heteromers with the adenosine A2A receptor (A2AR). Changes in the density of A2AR-D2R heteromers have been reported in postmortem tissue from patients with schizophrenia, but the degree to which A2R are involved in schizophrenia and the effect of antipsychotic drugs is unknown. Here, we examine the effect of exposure to three prototypical antipsychotic drugs on A2AR-D2R heteromerization in mammalian cells using a NanoBiT assay. After 16 h of exposure, a significant increase in the density of A2AR-D2R heteromers was found with haloperidol and aripiprazole, but not with clozapine. On the other hand, clozapine, but not haloperidol or aripiprazole, was associated with a significant decrease in A2AR-D2R heteromerization after 2 h of treatment. Computational binding models of these compounds revealed distinctive molecular signatures that explain their different influence on heteromerization. The bulky tricyclic moiety of clozapine displaces TM 5 of D2R, inducing a clash with A2AR, while the extended binding mode of haloperidol and aripiprazole stabilizes a specific conformation of the second extracellular loop of D2R that enhances the interaction with A2AR. It is proposed that an increase in A2AR-D2R heteromerization is involved in the extrapyramidal side effects (EPS) of antipsychotics and that the specific clozapine-mediated destabilization of A2AR-D2R heteromerization can explain its low EPS liability.
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- 2023
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6. Vaccination against swine influenza in pigs causes different drift evolutionary patterns upon swine influenza virus experimental infection and reduces the likelihood of genomic reassortments
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Álvaro López-Valiñas, Marta Valle, Miaomiao Wang, Ayub Darji, Guillermo Cantero, Chiara Chiapponi, Joaquim Segalés, Llilianne Ganges, and José I. Núñez
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swine influenza virus ,vaccination ,coinfection ,virus evolution ,reassortant ,Microbiology ,QR1-502 - Abstract
Influenza A viruses (IAVs) can infect a wide variety of bird and mammal species. Their genome is characterized by 8 RNA single stranded segments. The low proofreading activity of their polymerases and the genomic reassortment between different IAVs subtypes allow them to continuously evolve, constituting a constant threat to human and animal health. In 2009, a pandemic of an IAV highlighted the importance of the swine host in IAVs adaptation between humans and birds. The swine population and the incidence of swine IAV is constantly growing. In previous studies, despite vaccination, swine IAV growth and evolution were proven in vaccinated and challenged animals. However, how vaccination can drive the evolutionary dynamics of swine IAV after coinfection with two subtypes is poorly studied. In the present study, vaccinated and nonvaccinated pigs were challenged by direct contact with H1N1 and H3N2 independent swine IAVs seeder pigs. Nasal swab samples were daily recovered and broncho-alveolar lavage fluid (BALF) was also collected at necropsy day from each pig for swine IAV detection and whole genome sequencing. In total, 39 swine IAV whole genome sequences were obtained by next generation sequencing from samples collected from both experimental groups. Subsequently, genomic, and evolutionary analyses were carried out to detect both, genomic reassortments and single nucleotide variants (SNV). Regarding the segments found per sample, the simultaneous presence of segments from both subtypes was much lower in vaccinated animals, indicating that the vaccine reduced the likelihood of genomic reassortment events. In relation to swine IAV intra-host diversity, a total of 239 and 74 SNV were detected within H1N1 and H3N2 subtypes, respectively. Different proportions of synonymous and nonsynonymous substitutions were found, indicating that vaccine may be influencing the main mechanism that shape swine IAV evolution, detecting natural, neutral, and purifying selection in the different analyzed scenarios. SNV were detected along the whole swine IAV genome with important nonsynonymous substitutions on polymerases, surface glycoproteins and nonstructural proteins, which may have an impact on virus replication, immune system escaping and virulence of virus, respectively. The present study further emphasized the vast evolutionary capacity of swine IAV, under natural infection and vaccination pressure scenarios.
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- 2023
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7. Torus palatinus en 2 hermanas
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Salvador Labrador-Descalzo, Nerea Cortina-Garmendia, and Marta Valle-Coca
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Torus palatinus ,Gender ,Inheritance ,Biopsy ,Cranial CT scan with contrast ,Surgery or Conservative Treatment ,Medicine - Abstract
Resumen: Una mujer joven de 40 años acude a nuestra consulta por padecer de un nódulo de consistencia dura en el paladar de 3 meses de evolución. Destaca que tiene una hermana recién diagnosticada de torus palatinus. Ante esta sospecha y con el fin de descartar otras enfermedades tumorales, se deriva a la paciente a la consulta de maxilofacial donde, tras ser valorada, se decide realizar una biopsia de la lesión, con el resultado de hiperplasia, papilomatosis e inflamación, descartándose malignidad. Un TAC con contraste realizado en la cabeza y el cuello, permite el diagnostico de torus palatinus central. Abstract: A young female 40 years of age, presented to our Health center complaining of hard nodule in the hard palate for a period of 3 months. She has a sister with a recent Diagnosis of Torus palatinus. With the aim of ruling out a Malignant condition, the patient was referred to Maxillofacial specialist and after assessment a Biopsy of the lesion was taken and described as hyperplasia, papillomatosis and inflammatory cells with abscence of histological malignancy. A CT scan of the head and neck with contrast material was performed shortly after, with the diagnosis of central Torus Palatinus.
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- 2023
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8. Dopamine-induced arrestin recruitment and desensitization of the dopamine D4 receptor is regulated by G protein-coupled receptor kinase-2
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Viktor Burström, Richard Ågren, Nibal Betari, Marta Valle-León, Emilio Garro-Martínez, Francisco Ciruela, and Kristoffer Sahlholm
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luminescence measurements ,luciferase ,electrophysiology ,HEK 293 cells ,Xenopus laevis ,G protein-coupled inwardly rectifying potassium channels ,Therapeutics. Pharmacology ,RM1-950 - Abstract
The dopamine D4 receptor (D4R) is expressed in the retina, prefrontal cortex, and autonomic nervous system and has been implicated in attention deficit hyperactivity disorder (ADHD), substance use disorders, and erectile dysfunction. D4R has also been investigated as a target for antipsychotics due to its high affinity for clozapine. As opposed to the closely related dopamine D2 receptor (D2R), dopamine-induced arrestin recruitment and desensitization at the D4R have not been studied in detail. Indeed, some earlier investigations could not detect arrestin recruitment and desensitization of this receptor upon its activation by agonist. Here, we used a novel nanoluciferase complementation assay to study dopamine-induced recruitment of β-arrestin2 (βarr2; also known as arrestin3) and G protein-coupled receptor kinase-2 (GRK2) to the D4R in HEK293T cells. We also studied desensitization of D4R-evoked G protein-coupled inward rectifier potassium (GIRK; also known as Kir3) current responses in Xenopus oocytes. Furthermore, the effect of coexpression of GRK2 on βarr2 recruitment and GIRK response desensitization was examined. The results suggest that coexpression of GRK2 enhanced the potency of dopamine to induce βarr2 recruitment to the D4R and accelerated the rate of desensitization of D4R-evoked GIRK responses. The present study reveals new details about the regulation of arrestin recruitment to the D4R and thus increases our understanding of the signaling and desensitization of this receptor.
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- 2023
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9. Corrigendum: Striatal dopamine D2-muscarinic acetylcholine M1 receptor-receptor interaction in a model of movement disorders
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René A. J. Crans, Elise Wouters, Marta Valle-León, Jaume Taura, Caio M. Massari, Víctor Fernández-Dueñas, Christophe P. Stove, and Francisco Ciruela
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D2R ,M1R ,sumanirole ,VU0255035 ,striatum ,Parkinson’s disease ,Therapeutics. Pharmacology ,RM1-950 - Published
- 2022
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10. HIVconsv Vaccines and Romidepsin in Early-Treated HIV-1-Infected Individuals: Safety, Immunogenicity and Effect on the Viral Reservoir (Study BCN02)
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Beatriz Mothe, Miriam Rosás-Umbert, Pep Coll, Christian Manzardo, Maria C. Puertas, Sara Morón-López, Anuska Llano, Cristina Miranda, Samandhy Cedeño, Miriam López, Yovaninna Alarcón-Soto, Guadalupe Gómez Melis, Klaus Langohr, Ana M. Barriocanal, Jessica Toro, Irene Ruiz, Cristina Rovira, Antonio Carrillo, Michael Meulbroek, Alison Crook, Edmund G. Wee, Jose M. Miró, Bonaventura Clotet, Marta Valle, Javier Martinez-Picado, Tomáš Hanke, Christian Brander, José Moltó, and The BCN02 Study Investigators
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romidepsin ,HDAC inhibitor ,kick&kill strategy ,HIVconsv ,early-treatment ,Immunologic diseases. Allergy ,RC581-607 - Abstract
Kick&kill strategies combining drugs aiming to reactivate the viral reservoir with therapeutic vaccines to induce effective cytotoxic immune responses hold potential to achieve a functional cure for HIV-1 infection. Here, we report on an open-label, single-arm, phase I clinical trial, enrolling 15 early-treated HIV-1-infected individuals, testing the combination of the histone deacetylase inhibitor romidepsin as a latency-reversing agent and the MVA.HIVconsv vaccine. Romidepsin treatment resulted in increased histone acetylation, cell-associated HIV-1 RNA, and T-cell activation, which were associated with a marginally significant reduction of the viral reservoir. Vaccinations boosted robust and broad HIVconsv-specific T cells, which were strongly refocused toward conserved regions of the HIV-1 proteome. During a monitored ART interruption phase using plasma viral load over 2,000 copies/ml as a criterium for ART resumption, 23% of individuals showed sustained suppression of viremia up to 32 weeks without evidence for reseeding the viral reservoir. Results from this pilot study show that the combined kick&kill intervention was safe and suggest a role for this strategy in achieving an immune-driven durable viremic control.
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- 2020
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11. Striatal Dopamine D2-Muscarinic Acetylcholine M1 Receptor–Receptor Interaction in a Model of Movement Disorders
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René A. J. Crans, Elise Wouters, Marta Valle-León, Jaume Taura, Caio M. Massari, Víctor Fernández-Dueñas, Christophe P. Stove, and Francisco Ciruela
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D2R ,M1R ,sumanirole ,VU0255035 ,striatum ,Parkinson’s disease ,Therapeutics. Pharmacology ,RM1-950 - Abstract
Parkinson’s disease (PD) is a neurodegenerative disorder characterized by motor control deficits, which is associated with the loss of striatal dopaminergic neurons from the substantia nigra. In parallel to dopaminergic denervation, there is an increase of acetylcholine within the striatum, resulting in a striatal dopaminergic–cholinergic neurotransmission imbalance. Currently, available PD pharmacotherapy (e.g., prodopaminergic drugs) does not reinstate the altered dopaminergic–cholinergic balance. In addition, it can eventually elicit cholinergic-related adverse effects. Here, we investigated the interplay between dopaminergic and cholinergic systems by assessing the physical and functional interaction of dopamine D2 and muscarinic acetylcholine M1 receptors (D2R and M1R, respectively), both expressed at striatopallidal medium spiny neurons. First, we provided evidence for the existence of D2R–M1R complexes via biochemical (i.e., co-immunoprecipitation) and biophysical (i.e., BRET1 and NanoBiT®) assays, performed in transiently transfected HEK293T cells. Subsequently, a D2R–M1R co-distribution in the mouse striatum was observed through double-immunofluorescence staining and AlphaLISA® immunoassay. Finally, we evaluated the functional interplay between both receptors via behavioral studies, by implementing the classical acute reserpine pharmacological animal model of experimental parkinsonism. Reserpinized mice were administered with a D2R-selective agonist (sumanirole) and/or an M1R-selective antagonist (VU0255035), and alterations in PD-related behavioral tasks (i.e., locomotor activity) were evaluated. Importantly, VU0255035 (10 mg/kg) potentiated the antiparkinsonian-like effects (i.e., increased locomotor activity and decreased catalepsy) of an ineffective sumanirole dose (3 mg/kg). Altogether, our data suggest the existence of putative striatal D2R/M1R heteromers, which might be a relevant target to manage PD motor impairments with fewer adverse effects.
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- 2020
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12. In vivo Effects of Romidepsin on T-Cell Activation, Apoptosis and Function in the BCN02 HIV-1 Kick&Kill Clinical Trial
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Miriam Rosás-Umbert, Marta Ruiz-Riol, Marco A. Fernández, Marta Marszalek, Pep Coll, Christian Manzardo, Samandhy Cedeño, José M. Miró, Bonaventura Clotet, Tomáš Hanke, José Moltó, Beatriz Mothe, Christian Brander, the BCN02 study group, Susana Benet, Anuksa Llano, Javier Martinez-Picado, Sara Morón-López, Roger Paredes, Maria C. Puertas, Roser Escrig, Silvia Gel, Miriam López, Cristina Miranda, Jose Muñoz, Nuria Perez-Alvarez, Jordi Puig, Boris Revollo, Jessica Toro, Ana Maria Barriocanal, Magi Farré, Cristina Perez-Reche, Marta Valle, Juan Ambrosioni, Irene Ruiz, Cristina Rovira, Carmen Ligero, Jose M. Miro, Antonio Carrillo, Michael Meulbroek, Ferran Pujol, Jorge Saz, Nicola Borthwick, Alison Crook, and Edmund G. Wee
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romidepsin ,HDAC inhibitor ,kick&kill strategy ,therapeutic vaccine ,latency reversing agent (LRA) ,Immunologic diseases. Allergy ,RC581-607 - Abstract
Romidepsin (RMD) is a well-characterized histone deacetylase inhibitor approved for the treatment of cutaneous T-cell lymphoma. in vitro and in vivo studies have demonstrated that it is able to induce HIV-1 gene expression in latently infected CD4+ T cells from HIV-1+ individuals on suppressive antiretroviral therapy. However, in vitro experiments suggested that RMD could also impair T-cell functionality, particularly of activated T cells. Thus, the usefulness of RMD in HIV-1 kick&kill strategies, that aim to enhance the immune system elimination of infected cells after inducing HIV-1 viral reactivation, may be limited. In order to address whether the in vitro observations are replicated in vivo, we determined the effects of RMD on the total and HIV-1-specific T-cell populations in longitudinal samples from the BCN02 kick&kill clinical trial (NCT02616874). BCN02 was a proof-of-concept study in 15 early treated HIV-1+ individuals that combined MVA.HIVconsv vaccination with three weekly infusions of RMD given as a latency reversing agent. Our results show that RMD induced a transient increase in the frequency of apoptotic T cells and an enhanced activation of vaccine-induced T cells. Although RMD reduced the number of vaccine-elicited T cells secreting multiple cytokines, viral suppressive capacity of CD8+ T cells was preserved over the RMD treatment. These observations have important implications for the design of effective kick&kill strategies for the HIV-1 cure.
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- 2020
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13. Intrinsically regulated learning is modulated by synaptic dopamine signaling
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Pablo Ripollés, Laura Ferreri, Ernest Mas-Herrero, Helena Alicart, Alba Gómez-Andrés, Josep Marco-Pallares, Rosa Maria Antonijoan, Toemme Noesselt, Marta Valle, Jordi Riba, and Antoni Rodriguez-Fornells
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learning ,reward ,memory ,dopamine ,word learning ,language ,Medicine ,Science ,Biology (General) ,QH301-705.5 - Abstract
We recently provided evidence that an intrinsic reward-related signal—triggered by successful learning in absence of any external feedback—modulated the entrance of new information into long-term memory via the activation of the dopaminergic midbrain, hippocampus, and ventral striatum (the SN/VTA-Hippocampal loop; Ripollés et al., 2016). Here, we used a double-blind, within-subject randomized pharmacological intervention to test whether this learning process is indeed dopamine-dependent. A group of healthy individuals completed three behavioral sessions of a language-learning task after the intake of different pharmacological treatments: a dopaminergic precursor, a dopamine receptor antagonist or a placebo. Results show that the pharmacological intervention modulated behavioral measures of both learning and pleasantness, inducing memory benefits after 24 hr only for those participants with a high sensitivity to reward. These results provide causal evidence for a dopamine-dependent mechanism instrumental in intrinsically regulated learning and further suggest that subject-specific reward sensitivity drastically alters learning success.
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- 2018
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14. Pridopidine Reverses Phencyclidine-Induced Memory Impairment
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Kristoffer Sahlholm, Marta Valle-León, Víctor Fernández-Dueñas, and Francisco Ciruela
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dopamine stabilizers ,cognition ,mice ,sigma-1 receptor ,phencyclidine ,Therapeutics. Pharmacology ,RM1-950 - Abstract
Pridopidine is in clinical trials for Huntington's disease treatment. Originally developed as a dopamine D2 receptor (D2R) ligand, pridopidine displays about 100-fold higher affinity for the sigma-1 receptor (sigma-1R). Interestingly, pridopidine slows disease progression and improves motor function in Huntington's disease model mice and, in preliminarily reports, Huntington's disease patients. The present study examined the anti-amnesic potential of pridopidine. Thus, memory impairment was produced in mice by administration of phencyclidine (PCP, 10 mg/kg/day) for 10 days, followed by 14 days' treatment with pridopidine (6 mg/kg/day), or saline. Finally, novel object recognition performance was assessed in the animals. Mice receiving PCP and saline exhibited deficits in novel object recognition, as expected, while pridopidine treatment counteracted PCP-induced memory impairment. The effect of pridopidine was attenuated by co-administration of the sigma receptor antagonist, NE-100 (10 mg/kg). Our results suggest that pridopidine exerts anti-amnesic and potentially neuroprotective actions. These data provide new insights into the therapeutic potential of pridopidine as a pro-cognitive drug.
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- 2018
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15. Population pharmacokinetic modelling of rupatadine solution in 6-11 year olds and optimisation of the experimental design in younger children.
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Eva Santamaría, Javier Alejandro Estévez, Jordi Riba, Iñaki Izquierdo, and Marta Valle
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Medicine ,Science - Abstract
AIMS:To optimise a pharmacokinetic (PK) study design of rupatadine for 2-5 year olds by using a population PK model developed with data from a study in 6-11 year olds. The design optimisation was driven by the need to avoid children's discomfort in the study. METHODS:PK data from 6-11 year olds with allergic rhinitis available from a previous study were used to construct a population PK model which we used in simulations to assess the dose to administer in a study in 2-5 year olds. In addition, an optimal design approach was used to determine the most appropriate number of sampling groups, sampling days, total samples and sampling times. RESULTS:A two-compartmental model with first-order absorption and elimination, with clearance dependent on weight adequately described the PK of rupatadine for 6-11 year olds. The dose selected for a trial in 2-5 year olds was 2.5 mg, as it provided a Cmax below the 3 ng/ml threshold. The optimal study design consisted of four groups of children (10 children each), a maximum sampling window of 2 hours in two clinic visits for drawing three samples on day 14 and one on day 28 coinciding with the final examination of the study. CONCLUSIONS:A PK study design was optimised in order to prioritise avoidance of discomfort for enrolled 2-5 year olds by taking only four blood samples from each child and minimising the length of hospital stays.
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- 2017
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16. Revealing Adenosine A2A-Dopamine D2 Receptor Heteromers in Parkinson’s Disease Post-Mortem Brain through a New AlphaScreen-Based Assay
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Víctor Fernández-Dueñas, Maricel Gómez-Soler, Marta Valle-León, Masahiko Watanabe, Isidre Ferrer, and Francisco Ciruela
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AlphaScreen ,GPCR oligomerization ,Parkinson’s disease ,Adenosine A2A receptor ,Dopamine D2 receptor ,Biology (General) ,QH301-705.5 ,Chemistry ,QD1-999 - Abstract
Background: Several biophysical techniques have been successfully implemented to detect G protein-coupled receptors (GPCRs) heteromerization. Although these approaches have made it possible to ascertain the presence of GPCR heteromers in animal models of disease, no success has been accomplished in pathological human post-mortem brains. The AlphaScreen technology has been consistently used to quantify small analyte accumulation or depletion, bimolecular interactions, and post-translational modifications. The high signal-to-background, dynamic range and sensitivity exhibited by this technology support that it may be suitable to detect GPCR heteromers even under non-optimal conditions. Methods: Here, we describe the development of a new AlphaScreen assay to detect GPCR oligomers in human post-mortem brain. Results: Adenosine A2A-dopamine D2 receptor (A2AR/D2R) heteromer formation was monitored in caudate from healthy and Parkinson’s disease (PD) subjects. The approach was first validated using striatal membranes from wild type and A2AR deficient mice. Secondly, we took advantage of the 6-hydroxydopamine hemiparkinsonian rat model to validate previous results. In addition, finally, A2AR/D2R heteromer formation was assessed in caudate membranes from human post-mortem brains. Importantly, our preliminary results revealed an increase in A2AR/D2R heteromer formation in PD brains. Conclusions: The new AlphaScreen assay allowed assessing GPCR heteromers in human post-mortem brains with high sensitivity.
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- 2019
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17. The role of opioid transmission in music-induced pleasure
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Ernest Mas‐Herrero, Laura Ferreri, Gemma Cardona, Robert J. Zatorre, Francesc Pla‐Juncà, Rosa María Antonijoan, Jordi Riba, Marta Valle, Antoni Rodriguez‐Fornells, RS: FPN NPPP II, and Section Psychopharmacology
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History and Philosophy of Science ,General Neuroscience ,General Biochemistry, Genetics and Molecular Biology - Abstract
Studies conducted in rodents indicate a crucial role of the opioid circuit in mediating objective hedonic reactions to primary rewards. However, it remains unclear whether opioid transmission is also essential to experience pleasure with more abstract rewards, such as music. We addressed this question using a double-blind within-subject pharmacological design in which opioid levels were up- and downregulated by administering an opioid agonist (oxycodone) and antagonist (naltrexone), respectively, before healthy participants (n = 21) listened to music. Participants also performed a monetary incentive delay (MID) task to control for the effectiveness of the treatment and the specificity of the effects. Our results revealed that the pharmacological intervention did not modulate subjective reports of pleasure, nor the occurrence of chills. On the contrary, psychophysiological (objective) measures of emotional arousal, such as skin conductance responses (SCRs), were bidirectionally modulated in both the music and MID tasks. This modulation specifically occurred during reward consumption, with greater pleasure-related SCR following oxycodone than naltrexone. These findings indicate that opioid transmission does not modulate subjective evaluations but rather affects objective reward-related psychophysiological responses. These findings raise new caveats about the role of the opioidergic system in the modulation of pleasure for more abstract or cognitive forms of rewarding experiences, such as music.
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- 2023
18. Development of a Novel σ1 Receptor Biosensor Based on Its Heterodimerization with Binding Immunoglobulin Protein in Living Cells
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Xavier Morató, Víctor Fernández-Dueñas, Pilar Pérez-Villamor, Marta Valle-León, José Miguel Vela, Manuel Merlos, Javier Burgueño, and Francisco Ciruela
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Oligòmers ,Disseny de medicaments ,Biosensors ,Proteïnes portadores ,Carrier proteins ,Physiology ,Oligomers ,Cognitive Neuroscience ,Cell Biology ,General Medicine ,Biochemistry ,Drug design - Abstract
The σ1 receptor (S1R) is a ligand-regulated non-opioid intracellular receptor involved in several pathological conditions. The development of S1R-based drugs as therapeutic agents is a challenge due to the lack of simple functional assays to identify and classify S1R ligands. We have developed a novel nanoluciferase binary technology (NanoBiT) assay based on the ability of S1R to heteromerize with the binding immunoglobulin protein (BiP) in living cells. The S1R-BiP heterodimerization biosensor allows for rapid and accurate identification of S1R ligands by monitoring the dynamics of association-dissociation of S1R and BiP. Acute treatment of cells with the S1R agonist PRE-084 produced rapid and transient dissociation of the S1R-BiP heterodimer, which was blocked by haloperidol. The effect of PRE-084 was enhanced by calcium depletion, leading to a higher reduction in heterodimerization even in the presence of haloperidol. Prolonged incubation of cells with S1R antagonists (haloperidol, NE-100, BD-1047, and PD-144418) increased the formation of S1R-BiP heteromers, while agonists (PRE-084, 4-IBP, and pentazocine) did not alter heterodimerization under the same experimental conditions. The newly developed S1R-BiP biosensor is a simple and effective tool for exploring S1R pharmacology in an easy cellular setting. This biosensor is suitable for high-throughput applications and a valuable resource in the researcher's toolkit.
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- 2023
19. Un caso clínico neurológico en atención primaria: síndrome de Miller-Fisher
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Descalzo, Salvador Labrador, primary, Garmendia, Nerea Cortina, additional, Coca, Marta Valle, additional, and García, José Nicanor Valle, additional
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- 2022
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20. Population Pharmacokinetics of Intra-articular and Intravenous Administration of Tranexamic Acid in Patients Undergoing Total Knee Replacement
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Ma José Martínez-Zapata, Xavier Aguilera Roig, Aránzazu González Osuna, Francesc Pla-Junca, Luisa Fernanda Rojas, Marta Valle, Sebastián Videla, and C. Lamas
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Antifibrinolytic ,Dose ,medicine.drug_class ,medicine.medical_treatment ,Population ,Blood Loss, Surgical ,Renal function ,Injections, Intra-Articular ,Pharmacokinetics ,Fibrinolysis ,Humans ,Medicine ,Blood Transfusion ,Pharmacology (medical) ,Arthroplasty, Replacement, Knee ,Adverse effect ,education ,Aged ,Pharmacology ,education.field_of_study ,business.industry ,Antifibrinolytic Agents ,Tranexamic Acid ,Anesthesia ,Administration, Intravenous ,Female ,business ,Tranexamic acid ,medicine.drug - Abstract
Tranexamic acid (TXA), an antifibrinolytic drug, is usually administered intravenously; however, intra-articular administration has recently been proven to be as effective as intravenous administration. Limited information regarding the pharmacokinetics (PK) of TXA after intra-articular administration has been reported. The aim of this study was to develop a population PK model of TXA administered as a single intra-articular dose and as two intravenous doses, and to study the sources of interindividual variability (IIV) in the PK processes of TXA. The developed model was used to simulate PK profiles of TXA at different dosage regimens and in patients with renal impairment. Patients who underwent primary unilateral total knee replacement (TKR) received 1 g/10 mL (concentration of 100 mg/mL) of TXA applied directly to the surgical field before wound closure, or 2 g (two doses of 1 g) of intravenous TXA. A population PK model was developed using a nonlinear mixed-effects approach and sources of IIV, such as sex, age, body weight, height, body mass index (BMI), preoperative haemoglobin, preoperative haematocrit, and creatinine clearance. Twenty-four patients were included, 12 in each group. Twenty patients were female, mean age (standard deviation) was 73.7 years (5.6). The disposition of TXA was best described as a two-compartment model with clearance dependent on creatinine clearance. Bootstrap results indicated that the model was stable and robust. The estimated bioavailability for intra-articular administration was 81%. Simulations indicated that 100% of patients would have plasma concentrations associated with partial fibrinolysis at 8 h post-administration with the dosages and routes of administration used in the present study. Intra-articular administration would produce complete inhibition of fibrinolysis in only 12% of patients compared with 72.5% with intravenous administration. No adverse events were reported. This population PK model demonstrated that a single dose of high-concentration, low-volume intra-articular TXA can achieve antifibrinolytic plasma concentrations of the drug for 8 h, providing both local and systemic effects in patients undergoing TKR. TXA administration to the surgical field could be an alternative to the intravenous; route for patients undergoing TKR; however, clinical studies are needed to assess the toxic local effects of TXA. Spanish Clinical Studies Registry Number: 2017-004059-22. Date of registration: 12 April 2018.
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- 2021
21. Dopamine modulations of reward‐driven music memory consolidation
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Robert J. Zatorre, Laura Ferreri, Jordi Riba, Gemma Cardona, Pablo Ripollés, Antoni Rodríguez-Fornells, Ernest Mas-Herrero, Marta Valle, Rosa M. Antonijoan, RS: FPN NPPP II, and Section Psychopharmacology
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Adult ,ENHANCES EXPLICIT ,media_common.quotation_subject ,EPISODIC MEMORY ,pleasure ,INDIVIDUAL-DIFFERENCES ,behavioral disciplines and activities ,General Biochemistry, Genetics and Molecular Biology ,CAPACITY ,Pleasure ,ACTIVATION ,memory ,Young Adult ,History and Philosophy of Science ,CONNECTIVITY ,Humans ,music ,Active listening ,Episodic memory ,reward ,Memory Consolidation ,media_common ,Analysis of Variance ,Recall ,General Neuroscience ,PERSISTENCE ,Dopaminergic ,Brain ,Flexibility (personality) ,PERFORMANCE ,humanities ,Mental Recall ,Auditory Perception ,Memory consolidation ,SENSITIVITY ,dopamine ,Psychology ,psychological phenomena and processes ,Period (music) ,RESPONSES ,Cognitive psychology - Abstract
Music listening provides one of the most significant abstract rewards for humans because hearing music activates the dopaminergic mesolimbic system. Given the strong link between reward, dopamine, and memory, we aimed here to investigate the hypothesis that dopamine-dependent musical reward can drive memory improvements. Twenty-nine healthy participants of both sexes provided reward ratings of unfamiliar musical excerpts that had to be remembered following a consolidation period under three separate conditions: after the ingestion of a dopaminergic antagonist, a dopaminergic precursor, or a placebo. Linear mixed modeling of the intervention data showed that the effect of reward on memory-i.e., the greater the reward experienced while listening to the musical excerpts, the better the memory recollection performance-was modulated by both dopaminergic signaling and individual differences in reward processing. Greater pleasure was consistently associated with better memory outcomes in participants with high sensitivity to musical reward, but this effect was lost when dopaminergic signaling was disrupted in participants with average or low musical hedonia. Our work highlights the flexibility of the human dopaminergic system, which can enhance memory formation not only through explicit and/or primary reinforcers but also via abstract and aesthetic rewards such as music.
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- 2021
22. Rupatadine Oral Solution Titration by Body Weight in Paediatric Patients Suffering from Allergic Rhinitis: A Population Pharmacokinetic Study
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Marta Valle, Eva Santamaria, and Iñaki Izquierdo
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medicine.medical_specialty ,medicine.medical_treatment ,Rupatadine ,Population ,Cmax ,rupatadine ,Body weight ,Gastroenterology ,children ,Pharmacokinetics ,population pharmacokinetics ,Internal medicine ,Medicine ,Pharmacology (medical) ,Advances and Applications [Clinical Pharmacology] ,Population pharmacokinetics ,education ,Children ,Original Research ,Paediatric patients ,education.field_of_study ,business.industry ,Antihistamine ,business ,medicine.drug ,Blood sampling - Abstract
Eva Santamaria,1,2 Iñaki Izquierdo,2 Marta Valle1,3 1Departament de Farmacologia, de Terapèutica i de Toxicologia, Universitat Autònoma de Barcelona, Barcelona, Spain; 2Clinical Development, Porfolio & Strategy, Biorhom SL Grupo Uriach, Barcelona, Spain; 3Pharmacokinetic/Pharmacodynamic Modeling and Simulation. Institut de Recerca de l’Hospital de la Santa Creu i Sant Pau-IIB Sant Pau, Barcelona, SpainCorrespondence: Iñaki IzquierdoManager of Clinical Development & Medical Advise; Porfolio & Strategy Area, Biorhom, S.L. (Grupo Uriach) Polígon Ind. Riera de Caldes, Avinguda Camí Reial, 51-57, Palau-solità i Plegamans, Barcelona, 08184, SpainEmail Inaki.izquierdo@uriach.comBackground: Allergic rhinitis (AR) and chronic urticaria, both are treated in children with doses of second generation of antihistamines that have been mostly based on extrapolation of data obtained in adults. The objectives of this work were to develop a model to explain the pharmacokinetics (PK) of rupatadine, a second generation antihistamine, administered to children 2− 11 years old and to calculate the non-compartmental PK parameters for two groups of age (2– 5 and 6– 11 years old) based on the individual Bayesian estimates from the selected model.Methods: Data from two PK studies with rupatadine oral solution (1 mg/mL) were pooled: Study A, an extensive blood sampling study performed in 11 children (6– 11 years old) who received a single oral dose of rupatadine; and Study B, a sparse blood sampling study in 40 children (2– 5 years old) receiving multiple oral doses. A simultaneous population PK model was developed using data available for all children. Using individual Bayesian estimates from the selected model, steady-state plasma concentrations for both studies were simulated and the non-parametric PK parameters were calculated for two age groups: 2– 5 years (subgroup I) and 6– 11 years (subgroup II).Results: A two-compartment model with first-order absorption and elimination with clearance depending on body weight, better described the PK of rupatadine for 2– 11 year old children. The plasma clearance dependence on weight was linear. The mean (SD) non-compartment PK parameters calculated using simulated plasma profiles at steady state were: Cmax, 2.54 (1.26) vs 1.96 (0.52) ng/mL; AUC0-24h, 10.74 (3.09) vs 10.38 (4.31) ng/mL/h; and t1/2, 12.28 (3.09) vs 15.94 (4.09) h, for children 6– 11 and 2– 5 years old, respectively.Conclusions: The PK of rupatadine depends on the weight of paediatric patients but not on their age. The dosage strategy adjusted by body weight in children 2– 11 years old (2.5 mL if weight 10– 25 kg, and 5 mL if ≥ 25 kg) provides similar exposure between the two groups of age, and to that obtained in adults with the 10 mg dose tablet formulation.Keywords: rupatadine, children, population pharmacokinetics
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- 2021
23. Pharmacokinetic/pharmacodynamic analysis of romidepsin used as an HIV latency reversing agent
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Christian Manzardo, Cristina Miranda, Christian Brander, Miriam Rosás-Umbert, Miriam López, José Moltó, Bonaventura Clotet, Marta Ruiz-Riol, Maria C. Puertas, Marta Valle, Beatriz Mothe, Javier Martinez-Picado, and José M. Miró
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CD4-Positive T-Lymphocytes ,0301 basic medicine ,Microbiology (medical) ,030106 microbiology ,Population ,HIV Infections ,Pharmacology ,Romidepsin ,03 medical and health sciences ,Pharmacokinetics ,In vivo ,Depsipeptides ,Humans ,Medicine ,Pharmacology (medical) ,Dosing ,education ,education.field_of_study ,business.industry ,Bayes Theorem ,Virus Latency ,030104 developmental biology ,Infectious Diseases ,Apoptosis ,Pharmacodynamics ,HIV-1 ,business ,CD8 ,medicine.drug - Abstract
ObjectivesTo develop a population pharmacokinetic model for romidepsin given as an HIV latency reversing agent (LRA) and to explore the relationship between romidepsin exposure and its in vivo effects on viral gene expression and antiviral immunity.MethodsA population pharmacokinetic analysis was performed in 15 HIV-1-infected patients who received three weekly infusions of romidepsin (5 mg/m2) within the BCN02 clinical trial. A full pharmacokinetic profile was obtained for each participant at the first dose, and additional samples thereafter. A population pharmacokinetic model was developed. Bayesian estimates of the individual pharmacokinetic parameters of romidepsin were used to simulate individual time–concentration curves on each occasion. The relationship between romidepsin AUC0–∞ and its in vivo effects was assessed.ResultsRomidepsin pharmacokinetics were best described by a three-compartment model with linear kinetics. Body weight influenced romidepsin disposition. A significant relationship was observed between romidepsin AUC0–∞ and increases in expression of exhaustion markers by CD4+ and CD8+ T cells and apoptosis markers in CD4+, but not with histone acetylation levels or HIV-1 cell-associated RNA in CD4+ T cells. For each increase of 100 ng·h/mL in romidepsin AUC0–∞, CD4+ counts decreased by a mean (95% CI) of 74 (42–94) cells/mm3 after dosing.ConclusionsA population model describing the pharmacokinetics of romidepsin as an HIV LRA was developed. Higher exposure to romidepsin resulted in higher expression of apoptosis markers and declines in CD4+ count but did not increase viral reactivation levels. These observations have important implications for the optimization of effective kick-and-kill strategies for an HIV-1 cure.
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- 2020
24. Involvement of adenosine A1 and A2A receptors on guanosine-mediated anti-tremor effects in reserpinized mice
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Luisa Bandeira Binder, Caio M. Massari, Marc López-Cano, Francisco Ciruela, Leandra C. Constantino, Marta Valle-León, Víctor Fernández-Dueñas, Carla I. Tasca, and Naiani Ferreira Marques
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0301 basic medicine ,chemistry.chemical_classification ,Reactive oxygen species ,Antagonist ,Guanosine ,Cell Biology ,Pharmacology ,Adenosine ,Adenosine receptor ,03 medical and health sciences ,Cellular and Molecular Neuroscience ,chemistry.chemical_compound ,030104 developmental biology ,0302 clinical medicine ,chemistry ,medicine ,Receptor ,Molecular Biology ,Nucleoside ,030217 neurology & neurosurgery ,Ex vivo ,medicine.drug - Abstract
Parkinson’s disease (PD) signs and symptoms regularly include tremor. Interestingly, the nucleoside guanosine (GUO) has already proven to be effective in reducing reserpine-induced tremulous jaw movements (TJMs) in rodent models, thus becoming a promising antiparkinsonian drug. Here, we aimed at revealing the mechanism behind GUO antiparkinsonian efficacy by assessing the role of adenosine A1 and A2A receptors (A1R and A2AR) on GUO-mediated anti-tremor effects in the reserpinized mouse model of PD. Reserpinized mice showed elevated reactive oxygen species (ROS) production and cellular membrane damage in striatal slices assessed ex vivo and GUO treatment reversed ROS production. Interestingly, while the simultaneous administration of sub-effective doses of GUO (5 mg/kg) and SCH58261 (0.01 mg/kg), an A2AR antagonist, precluded reserpine-induced TJMs, these were ineffective on reverting ROS production in ex vivo experiments. Importantly, GUO was able to reduce TJM and ROS production in reserpinized mouse lacking the A2AR, thus suggesting an A2AR-independent mechanism of GUO-mediated effects. Conversely, the administration of DPCPX (0.75 mg/kg), an A1R antagonist, completely abolished both GUO-mediated anti-tremor effects and blockade of ROS production. Overall, these results indicated that GUO anti-tremor and antioxidant effects in reserpinized mice were A1R dependent but A2AR independent, thus suggesting a differential participation of adenosine receptors in GUO-mediated effects.
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- 2020
25. In-vivo range verification analysis with in-beam PET data for patients treated with proton therapy at CNAO
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Martina Moglioni, Aafke Christine Kraan, Guido Baroni, Giuseppe Battistoni, Nicola Belcari, Andrea Berti, Pietro Carra, Piergiorgio Cerello, Mario Ciocca, Angelica De Gregorio, Micol De Simoni, Damiano Del Sarto, Marco Donetti, Yunsheng Dong, Alessia Embriaco, Maria Evelina Fantacci, Veronica Ferrero, Elisa Fiorina, Marta Fischetti, Gaia Franciosini, Giuseppe Giraudo, Francesco Laruina, Davide Maestri, Marco Magi, Giuseppe Magro, Etesam Malekzadeh, Michela Marafini, Ilaria Mattei, Enrico Mazzoni, Paolo Mereu, Alfredo Mirandola, Matteo Morrocchi, Silvia Muraro, Ester Orlandi, Vincenzo Patera, Francesco Pennazio, Marco Pullia, Alessandra Retico, Angelo Rivetti, Manuel Dionisio Da Rocha Rolo, Valeria Rosso, Alessio Sarti, Angelo Schiavi, Adalberto Sciubba, Giancarlo Sportelli, Sara Tampellini, Marco Toppi, Giacomo Traini, Antonio Trigilio, Serena Marta Valle, Francesca Valvo, Barbara Vischioni, Viviana Vitolo, Richard Wheadon, and Maria Giuseppina Bisogni
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Cancer Research ,Inter-fractional range differences ,In-vivo treatment verification ,In-beam PET imaging ,inter-fractional range differences ,clinical trial ,in-vivo treatment verification ,Proton therapy ,Morphological changes ,Clinical trial ,Oncology ,in-beam PET imaging ,morphological changes ,proton therapy - Abstract
Morphological changes that may arise through a treatment course are probably one of the most significant sources of range uncertainty in proton therapy. Non-invasive in-vivo treatment monitoring is useful to increase treatment quality. The INSIDE in-beam Positron Emission Tomography (PET) scanner performs in-vivo range monitoring in proton and carbon therapy treatments at the National Center of Oncological Hadrontherapy (CNAO). It is currently in a clinical trial (ID: NCT03662373) and has acquired in-beam PET data during the treatment of various patients. In this work we analyze the in-beam PET (IB-PET) data of eight patients treated with proton therapy at CNAO. The goal of the analysis is twofold. First, we assess the level of experimental fluctuations in inter-fractional range differences (sensitivity) of the INSIDE PET system by studying patients without morphological changes. Second, we use the obtained results to see whether we can observe anomalously large range variations in patients where morphological changes have occurred. The sensitivity of the INSIDE IB-PET scanner was quantified as the standard deviation of the range difference distributions observed for six patients that did not show morphological changes. Inter-fractional range variations with respect to a reference distribution were estimated using the Most-Likely-Shift (MLS) method. To establish the efficacy of this method, we made a comparison with the Beam’s Eye View (BEV) method. For patients showing no morphological changes in the control CT the average range variation standard deviation was found to be 2.5 mm with the MLS method and 2.3 mm with the BEV method. On the other hand, for patients where some small anatomical changes occurred, we found larger standard deviation values. In these patients we evaluated where anomalous range differences were found and compared them with the CT. We found that the identified regions were mostly in agreement with the morphological changes seen in the CT scan.
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- 2022
26. Un caso clínico neurológico en atención primaria: síndrome de Miller-Fisher
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Salvador Labrador Descalzo, Nerea Cortina Garmendia, Marta Valle Coca, and José Nicanor Valle García
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Community and Home Care ,Gastroenterology - Published
- 2022
27. C677T and A1298C MTHFR gene polymorphisms and response to fluoropyrimidine-based chemotherapy in Mestizo patients with metastatic colorectal cancer
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Ricardo Chinchilla-Monge, Marta Valle, Jad Abbas, and Allan Ramos-Esquivel
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Costa Rica ,medicine.medical_specialty ,Genotype ,Colorectal cancer ,Single-nucleotide polymorphism ,Gastroenterology ,Polymorphism, Single Nucleotide ,Colorectal neoplasms ,Internal medicine ,Genetics ,medicine ,Humans ,Genetic Predisposition to Disease ,General Pharmacology, Toxicology and Pharmaceutics ,Molecular Biology ,Genetics (clinical) ,Methylenetetrahydrofolate Reductase (NADPH2) ,biology ,Proportional hazards model ,business.industry ,Methylenetetrahydrofolate reductase ,Hazard ratio ,Odds ratio ,medicine.disease ,digestive system diseases ,Oxaliplatin ,Irinotecan ,Case-Control Studies ,Colonic Neoplasms ,biology.protein ,Molecular Medicine ,Fluorouracil ,business ,Colorectal Neoplasms ,medicine.drug - Abstract
Objective: To assess the association between C677T and A1298C methylenetetrahydrofolate reductase (MTHFR) single-nucleotide polymorphisms (SNPs) and response to first-line fluoropyrimidine-based chemotherapy for metastatic colorectal adenocarcinoma. Methods: A total of 68 patients were prospectively followed up in San Juan de Dios Hospital (San José, Costa Rica) from January 2019 to November 2020. Patients received first-line therapy with capecitabine or 5-fluorouracil in combination with oxaliplatin or irinotecan. Germline and somatic DNA was extracted from blood samples and paraffin-embedded tissue, respectively. Overall response rate (partial response + complete response) was assessed according to RECIST 1.1 criteria. Cox regression models were performed to identify the effect of MTHFR C677T and A1298C SNPs on progression-free survival (PFS) and overall survival (OS) (NCT registration number: 03852290). Results: Patients harboring one or both T alleles of the MTHFR C677T SNP had better overall response than homozygous wild-type individuals [odds ratio (OR): 3.21; 95% confidence interval (CI), 1.05–9.81; P = 0.03]. No association was found between the MTHFR A1298C genotypes and overall response (OR: 0.75; 95% CI, 0.26–2.20; P = 0.60). Patients with the MTHFR 677 TT and CT genotypes had longer PFS than CC individuals (hazard ratio: 0.53; 95% CI, 0.28–0.98; P = 0.045), even after adjustment for confounders (hazard ratio: 0.50; 95% CI, 0.25–0.98; P = 0.04). We found no association between the MTHFR A1298C SNP and PFS (hazard ratio: 1.35; 95% CI, 0.72–2.55; P = 0.34). None of the SNPs was associated with OS. Conclusion: Patients carrying at least one mutant allele of the MTHFR C677T SNP had a better overall response and longer PFS than wild-type homozygous patients. UCR::Vicerrectoría de Investigación::Unidades de Investigación::Ciencias de la Salud::Centro de Investigación en Hematología y Trastornos Afines (CIHATA)
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- 2021
28. Dopamine modulates the reward experiences elicited by music
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Helena Alicart, Jordi Riba, Pablo Ripollés, Rosa M. Antonijoan, Alba Gomez-Andres, Robert J. Zatorre, Marta Valle, Laura Ferreri, Antoni Rodríguez-Fornells, Ernest Mas-Herrero, Josep Marco-Pallarés, Guillem Olivé, RS: FPN NPPP II, and Section Psychopharmacology
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Adult ,Male ,Levodopa ,media_common.quotation_subject ,Emotions ,NUCLEUS-ACCUMBENS ,Administration, Oral ,pleasure ,Placebo ,Pleasure ,Young Adult ,motivation ,Dopamine ,Commentaries ,medicine ,Humans ,music ,EMOTIONAL RESPONSES ,BRAIN ,ANTICIPATION ,reward ,media_common ,Multidisciplinary ,Risperidone ,CORRELATE ,LEVODOPA ,Dopaminergic ,Dopamine antagonist ,Cognition ,Placebo Effect ,humanities ,RECEPTOR OCCUPANCY ,SEMANTIC ACTIVATION ,LIKING ,Dopamine Agonists ,Auditory Perception ,Female ,dopamine ,Psychology ,Neuroscience ,medicine.drug - Abstract
Understanding how the brain translates a structured sequence of sounds, such as music, into a pleasant and rewarding experience is a fascinating question which may be crucial to better understand the processing of abstract rewards in humans. Previous neuroimaging findings point to a challenging role of the dopaminergic system in music-evoked pleasure. However, there is a lack of direct evidence showing that dopamine function is causally related to the pleasure we experience from music. We addressed this problem through a double blind within-subject pharmacological design in which we directly manipulated dopaminergic synaptic availability while healthy participants (n = 27) were engaged in music listening. We orally administrated to each participant a dopamine precursor (levodopa), a dopamine antagonist (risperidone), and a placebo (lactose) in three different sessions. We demonstrate that levodopa and risperidone led to opposite effects in measures of musical pleasure and motivation: while the dopamine precursor levodopa, compared with placebo, increased the hedonic experience and music-related motivational responses, risperidone led to a reduction of both. This study shows a causal role of dopamine in musical pleasure and indicates that dopaminergic transmission might play different or additive roles than the ones postulated in affective processing so far, particularly in abstract cognitive activities.
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- 2019
29. Ayahuasca improves emotion dysregulation in a community sample and in individuals with borderline-like traits
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Marta Valle, Juan C. Pascual, Matilde Elices, Jordi Riba, Alba Franquesa, Joaquim Soler, Enric Álvarez, Elisabet Domínguez-Clavé, RS: FPN NPPP II, and Section Psychopharmacology
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Adult ,Male ,HUMAN PHARMACOLOGY ,mindfulness ,Mindfulness ,EXPERIENCES QUESTIONNAIRE ,media_common.quotation_subject ,Emotions ,Psychological intervention ,Five Facet Mindfulness Questionnaire ,BEHAVIOR-THERAPY SKILLS ,Emotional dysregulation ,altered states ,psychometric properties ,VALIDATION ,Self-Control ,03 medical and health sciences ,0302 clinical medicine ,Surveys and Questionnaires ,medicine ,Humans ,RECURRENT DEPRESSION ,MCLEAN SCREENING INSTRUMENT ,Meditation ,Borderline personality disorder ,media_common ,Pharmacology ,personality-disorder ,Banisteriopsis ,Ayahuasca ,Awareness ,Middle Aged ,medicine.disease ,030227 psychiatry ,Female ,Observational study ,Plant Preparations ,Self Report ,Psychology ,030217 neurology & neurosurgery ,Clinical psychology - Abstract
BackgroundResearch suggests that mindfulness-based interventions may improve mindfulness-related capacities (e.g., decentering, non-judging, and non-reacting) and emotion regulation. Previously, our group reported that ayahuasca could be a potential analogue of mindfulness practice. The main aim of the current study was to examine the effects of ayahuasca on emotional regulation and mindfulness-related capacities. Secondarily, we sought to explore the effects of ayahuasca on individuals with borderline personality disorder (BPD) traits.MethodThis is an observational study of 45 volunteers who participated in an ayahuasca session. The volunteers completed various self-report instruments designed to measure emotional dysregulation (Difficulties in Emotion Regulation Scale (DERS)) and mindfulness traits (Five Facet Mindfulness Questionnaire (FFMQ)-Short Form and Experiences Questionnaire (EQ)) prior to and 24h after the ayahuasca session. The volunteers were divided into two subgroups based on their score on the McLean Screening Instrument for BPD (MSI-BPD). Twelve participants were grouped into the BPD-like traits subgroup while the rest of them were included in the non-BPD-like subgroup. We performed within-subjects and between-group analyses.ResultsOverall, the participants showed significant improvements on the FFMQ subscales observing, acting with awareness, non-judging, and non-reacting and also significantly improved on decentering (EQ scale) and on the DERS subscales emotional non-acceptance, emotional interference, and lack of control. The BPD-like subgroup also showed significant improvements on the DERS subscales emotional interference and lack of control but not in mindfulness capacities.ConclusionsThese findings suggest a potential therapeutic effect for ayahuasca in emotion regulation and mindfulness capacities (including decentering, acceptance, awareness, and sensitivity to meditation practice). Based on these results, we believe that ayahuasca therapy could be of value in clinical populations, such as individuals with BPD, affected by emotion dysregulation.
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- 2018
30. The Kappa Opioid Receptor and the Sleep of Reason: Cortico-Subcortical Imbalance Following Salvinorin-A
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Frederic Sampedro, Jordi Riba, Jimena Coimbra, Maite Garrido, Rosa M. Antonijoan, Genís Ona, Valle Camacho, Marta Valle, Carolina Migliorelli, Montserrat Puntes, Miguel Angel Mañanas, Maria Rosa Ballester, Sergio Romero, Universitat Politècnica de Catalunya. Departament d'Enginyeria de Sistemes, Automàtica i Informàtica Industrial, Universitat Politècnica de Catalunya. BIOART - BIOsignal Analysis for Rehabilitation and Therapy, RS: FPN NPPP II, and Section Psychopharmacology
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Male ,AYAHUASCA ,Electroencephalography ,Regular Research Articles ,CONNECTIVITY ,Ciències de la salut::Medicina::Neurologia [Àrees temàtiques de la UPC] ,Pharmacology (medical) ,EEG ,Cervell ,Child ,salvinorin-A ,opioids ,medicine.diagnostic_test ,AcademicSubjects/SCI01870 ,Enginyeria biomèdica [Àrees temàtiques de la UPC] ,Salvinorin-A ,Brain ,Psychotomimetic ,Middle Aged ,STATE ,Psychiatry and Mental health ,medicine.anatomical_structure ,Neurology ,Cerebral cortex ,FMRI ,SPECT ,Female ,medicine.drug ,Agonist ,Gamma wave ,Adult ,Psychotropic drugs ,Adolescent ,AcademicSubjects/MED00415 ,hallucinogens ,medicine.drug_class ,Psychotomimetic drug ,Kappa opioid receptor ,κ-opioid receptor ,Psicofàrmacs ,MECHANISMS ,Temporal lobe ,Diterpenes, Clerodane ,Neurologia ,Young Adult ,PSYCHOSIS ,Double-Blind Method ,TOMOGRAPHY ,medicine ,Humans ,Opiacis ,Pharmacology ,business.industry ,Receptors, Opioid, kappa ,AMYGDALA ,MODEL ,Opioids ,Hallucinogens ,business ,Neuroscience - Abstract
Background The mechanisms through which kappa opioid receptor (KOR) agonists induce psychotomimetic effects are largely unknown, although the modulation of this receptor has attracted attention for its clinical use. In this work, we characterize the neuropharmacological effects of salvinorin-A, a highly selective KOR agonist. Methods Changes in multimodal electroencephalography, single-photon emission computed tomography, and subjective effects following the acute administration of salvinorin-A are reported. The study included 2 sub-studies that employed a double-blind, crossover, randomized, placebo-controlled design. Results The electroencephalography measures showed a marked increase in delta and gamma waves and a decrease in alpha waves while subjects were under the effect of salvinorin-A. Regarding single-photon emission computed tomography measures, significant decreases in regional cerebral blood flow were detected in multiple regions of the frontal, temporal, parietal, and occipital cortices. Significant regional cerebral blood flow increases were observed in some regions of the medial temporal lobe, including the amygdala, the hippocampal gyrus, and the cerebellum. The pattern of subjective effects induced by salvinorin-A was similar to those observed in relation to other psychotomimetic drugs but with an evidently dissociative nature. No dysphoric effects were reported. Conclusion The salvinorin-A–mediated KOR agonism induced dramatic psychotomimetic effects along with a generalized decrease in cerebral blood flow and electric activity within the cerebral cortex.
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- 2021
31. Perovskite Thin Single Crystal for a High Performance and Long Endurance Memristor
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Ismael Fernandez‐Guillen, Clara A. Aranda, Pablo F. Betancur, Marta Vallés‐Pelarda, Cristina Momblona, Teresa S. Ripolles, Rafael Abargues, and Pablo P. Boix
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electroforming ,endurance ,impedance spectroscopy ,memristors ,perovskite ,Electric apparatus and materials. Electric circuits. Electric networks ,TK452-454.4 ,Physics ,QC1-999 - Abstract
Abstract Metal halide perovskites (MHPs) exhibit electronic and ionic characteristics suitable for memristors. However, polycrystalline thin film perovskite memristors often suffer from reliability issues due to grain boundaries, while bulk single‐crystal perovskite memristors struggle to achieve high LRS/HRS ratios. In this study, a single crystal memristive device utilizing a wide bandgap perovskite is introduced, MAPbBr3, in a high surface/thickness configuration. This thin single crystal overcomes these challenges, exhibiting a remarkable LRS/HRS ratio of up to 50 and endurance of 103 cycles, representing one of the highest reported values to date. This exceptional stability enables to analyze the electroforming process and LRS through impedance spectroscopy, providing insights into the underlying operational mechanism. As far as it is known, this is the first reported thin single‐crystal MHP memristor device and the first time that the electroforming process is recorded through impedance spectroscopy. This device's outstanding stability and performance position it as a promising candidate for high‐density data storage and neuromorphic applications.
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- 2024
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32. Detection of Interfractional Morphological Changes in Proton Therapy: A Simulation and In Vivo Study With the INSIDE In-Beam PET
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Elisa Fiorina, Veronica Ferrero, Guido Baroni, Giuseppe Battistoni, Nicola Belcari, Niccolo Camarlinghi, Piergiorgio Cerello, Mario Ciocca, Micol De Simoni, Marco Donetti, Yunsheng Dong, Alessia Embriaco, Marta Fischetti, Gaia Franciosini, Giuseppe Giraudo, Aafke Kraan, Francesco Laruina, Carmela Luongo, Davide Maestri, Marco Magi, Giuseppe Magro, Etesam Malekzadeh, Carlo Mancini Terracciano, Michela Marafini, Ilaria Mattei, Enrico Mazzoni, Paolo Mereu, Riccardo Mirabelli, Alfredo Mirandola, Matteo Morrocchi, Silvia Muraro, Alessandra Patera, Vincenzo Patera, Francesco Pennazio, Alessandra Retico, Angelo Rivetti, Manuel Dionisio Da Rocha Rolo, Valeria Rosso, Alessio Sarti, Angelo Schiavi, Adalberto Sciubba, Elena Solfaroli Camillocci, Giancarlo Sportelli, Sara Tampellini, Marco Toppi, Giacomo Traini, Serena Marta Valle, Francesca Valvo, Barbara Vischioni, Viviana Vitolo, Richard Wheadon, and Maria Giuseppina Bisogni
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adaptive therapy ,Computer science ,Materials Science (miscellaneous) ,medicine.medical_treatment ,Monte Carlo method ,Biophysics ,General Physics and Astronomy ,030218 nuclear medicine & medical imaging ,in vivo treatment verification ,03 medical and health sciences ,0302 clinical medicine ,In vivo ,Robustness (computer science) ,in-beam pet ,medicine ,proton therapy ,range monitoring ,Physical and Theoretical Chemistry ,Radiation treatment planning ,Proton therapy ,Mathematical Physics ,Monte Carlo simulation ,Particle therapy ,medicine.diagnostic_test ,business.industry ,clinical trial ,lcsh:QC1-999 ,Positron emission tomography ,030220 oncology & carcinogenesis ,Nuclear medicine ,business ,Beam (structure) ,lcsh:Physics - Abstract
In particle therapy, the uncertainty of the delivered particle range during the patient irradiation limits the optimization of the treatment planning. Therefore, an in vivo treatment verification device is required, not only to improve the plan robustness, but also to detect significant interfractional morphological changes during the treatment itself. In this article, an effective and robust analysis to detect regions with a significant range discrepancy is proposed. This study relies on an in vivo treatment verification by means of in-beam Positron Emission Tomography (PET) and was carried out with the INSIDE system installed at the National Center of Oncological Hadrontherapy (CNAO) in Pavia, which is under clinical testing since July 2019. Patients affected by head-and-neck tumors treated with protons have been considered. First, in order to tune the analysis parameters, a Monte Carlo (MC) simulation was carried out to reproduce a patient who required a replanning because of significant morphological changes found during the treatment. Then, the developed approach was validated on the experimental measurements of three patients recruited for the INSIDE clinical trial (ClinicalTrials.govID: NCT03662373), showing the capability to estimate the treatment compliance with the prescription both when no morphological changes occurred and when a morphological change did occur, thus proving to be a promising tool for clinicians to detect variations in the patients treatments.
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- 2021
33. Monitoring Carbon Ion Beams Transverse Position Detecting Charged Secondary Fragments: Results From Patient Treatment Performed at CNAO
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Marco Toppi, Guido Baroni, Giuseppe Battistoni, Maria Giuseppina Bisogni, Piergiorgio Cerello, Mario Ciocca, Patrizia De Maria, Micol De Simoni, Marco Donetti, Yunsheng Dong, Alessia Embriaco, Veronica Ferrero, Elisa Fiorina, Marta Fischetti, Gaia Franciosini, Aafke Christine Kraan, Carmela Luongo, Etesam Malekzadeh, Marco Magi, Carlo Mancini-Terracciano, Michela Marafini, Ilaria Mattei, Enrico Mazzoni, Riccardo Mirabelli, Alfredo Mirandola, Matteo Morrocchi, Silvia Muraro, Vincenzo Patera, Francesco Pennazio, Angelo Schiavi, Adalberto Sciubba, Elena Solfaroli-Camillocci, Giancarlo Sportelli, Sara Tampellini, Giacomo Traini, Serena Marta Valle, Barbara Vischioni, Viviana Vitolo, and Alessio Sarti
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Cancer Research ,Materials science ,medicine.medical_treatment ,030218 nuclear medicine & medical imaging ,03 medical and health sciences ,0302 clinical medicine ,Optics ,Relative biological effectiveness ,medicine ,charged particles ,RC254-282 ,Original Research ,Range (particle radiation) ,Particle therapy ,carbon ions ,fibre detectors ,online monitoring ,particle therapy ,business.industry ,Detector ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,Charged particle ,Transverse plane ,Oncology ,030220 oncology & carcinogenesis ,Ionization chamber ,business ,Beam (structure) - Abstract
Particle therapy in which deep seated tumours are treated using 12C ions (Carbon Ions RadioTherapy or CIRT) exploits the high conformity in the dose release, the high relative biological effectiveness and low oxygen enhancement ratio of such projectiles. The advantages of CIRT are driving a rapid increase in the number of centres that are trying to implement such technique. To fully profit from the ballistic precision achievable in delivering the dose to the target volume an online range verification system would be needed, but currently missing. The 12C ions beams range could only be monitored by looking at the secondary radiation emitted by the primary beam interaction with the patient tissues and no technical solution capable of the needed precision has been adopted in the clinical centres yet. The detection of charged secondary fragments, mainly protons, emitted by the patient is a promising approach, and is currently being explored in clinical trials at CNAO. Charged particles are easy to detect and can be back-tracked to the emission point with high efficiency in an almost background-free environment. These fragments are the product of projectiles fragmentation, and are hence mainly produced along the beam path inside the patient. This experimental signature can be used to monitor the beam position in the plane orthogonal to its flight direction, providing an online feedback to the beam transverse position monitor chambers used in the clinical centres. This information could be used to cross-check, validate and calibrate, whenever needed, the information provided by the ion chambers already implemented in most clinical centres as beam control detectors. In this paper we study the feasibility of such strategy in the clinical routine, analysing the data collected during the clinical trial performed at the CNAO facility on patients treated using 12C ions and monitored using the Dose Profiler (DP) detector developed within the INSIDE project. On the basis of the data collected monitoring three patients, the technique potential and limitations will be discussed.
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- 2021
34. Ayahuasca as a Versatile Therapeutic Agent: From Molecules to Metacognition and Back
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José A. Morales-García, Ana Perez-Castillo, Matilde Elices, Juan Carlos Pascual, Marta Valle, Joaquim Soler, Jordi Riba, and Elisabet Domínguez-Clavé
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Metacognition ,Cellular level ,Ayahuasca ,Psychology ,Neuroscience - Abstract
In this chapter, we review the latest research on the neuroscience and therapeutic potential of ayahuasca. Currently, the type of research available ranges from in vitro experiments to clinical studies performed to assess the modulation of neural and psychological processes. We also discuss the most recently reported findings, including (a) the neurobiological effects of ayahuasca, (b) the psychological mechanisms underlying the potential therapeutic effects of ayahuasca, (c) ayahuasca-induced metabolic and connectivity changes, and (d) the possible link with mindfulness-related capacities and emotion regulation. We also examine the effects of ayahuasca at the cellular level to better explore the role of β-carbolines and the neurogenetic properties of these alkaloids. These important findings indicate that these compounds, which still play a minor role in the overall pharmacology of ayahuasca, merit greater attention. Our aim is to show the remarkable versatility of ayahuasca as a therapeutic agent. Ayahuasca interacts with the brain–mind complex on multiple levels, and could be a powerful tool to help patients with neuropsychiatric disorders who are unable to find relief through currently available treatments.
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- 2021
35. Older Age is Associated with Higher Dolutegravir Exposure in Plasma and Cerebrospinal Fluid of People Living with HIV
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Antonio D'Avolio, Simona Di Giambenedetto, Mattia Trunfio, José Moltó, Maurizio Milesi, Cristina Gervasoni, Stefano Bonora, Francesc Pla-Junca, Marta Valle, Alberto Borghetti, Valeria Avataneo, Chiara Alcantarini, Dario Cattaneo, Giovanni Di Perri, and Andrea Calcagno
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0301 basic medicine ,Male ,medicine.medical_specialty ,Pyridones ,030106 microbiology ,Human immunodeficiency virus (HIV) ,HIV Infections ,medicine.disease_cause ,3-Ring ,Settore MED/17 - MALATTIE INFETTIVE ,Gastroenterology ,Piperazines ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Pharmacotherapy ,Cerebrospinal fluid ,Heterocyclic Compounds ,Internal medicine ,Oxazines ,medicine ,Humans ,Pharmacology (medical) ,Trough Concentration ,030212 general & internal medicine ,HIV Integrase Inhibitors ,Retrospective Studies ,Pharmacology ,medicine.diagnostic_test ,business.industry ,Age Factors ,Middle Aged ,chemistry ,Ageing ,Therapeutic drug monitoring ,Concomitant ,Dolutegravir ,Female ,business ,Heterocyclic Compounds, 3-Ring - Abstract
Background People living with human immunodeficiency virus are ageing under combination antiretroviral treatments but data on drug exposure in serum and cerebrospinal fluid are limited. Dolutegravir is a widely used second-generation integrase strand transfer inhibitor: conflicting data suggest that neuropsychiatric side effects may present at a higher frequency in patients with higher dolutegravir serum concentrations. Methods We performed a retrospective analysis of our therapeutic drug monitoring registry identifying patients receiving once-daily dolutegravir without concomitant interacting drugs and significant clinical conditions. Data were analysed stratifying time after drug dose intake (maximum concentration 0.5-4 and trough concentration 21-27 h). Cerebrospinal fluid samples from patients enrolled in neurological studies and receiving dolutegravir were analysed for dolutegravir cerebrospinal fluid concentrations and cerebrospinal fluid-to-plasma ratios. Serum and cerebrospinal fluid concentrations were measured through validated chromatographic methods. Results We included 207 (providing 457 serum samples) and 41 patients (providing 41 cerebrospinal fluid samples). Participants were mostly male (68.2-72.8%) of median age of 50 years (50-53 years). Non-significant changes in dolutegravir maximum concentration and trough concentration were observed with age at Spearman's test (pvalues > 0.05); linear logistic regression showed a significant effect of age on dolutegravir trough concentration (p = 0.0013) (Fig. 1). Dolutegravir maximum concentration [3830 ng/mL (2311-5057) vs 4230 ng/mL (2919-5272),p = 0.311] and trough concentration [838 ng/mL (362-1587) vs 966 ng/mL (460-2085),p = 0.056] were non-significantly or borderline higher in patients aged > 50 years. Cerebrospinal dolutegravir concentrations were associated with plasma concentrations (rho = 0.374,p = 0.016) and age (rho = 0.537,p = 0.003); cerebrospinal fluid dolutegravir concentrations (13.8 vs 7.3 ng/mL,p = 0.015) and cerebrospinal fluid-to-plasma ratios (0.57 vs 0.32%,p = 0.017] were higher in participants aged > 50 years. Conclusions We observed an increase in dolutegravir exposure in serum and in cerebrospinal fluid in older patients living with human immunodeficiency virus.
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- 2021
36. Amplified Luminescent Proximity Homogeneous Assay (Alpha)-Based Technique to Detect GPCR Oligomers in Human Postmortem Brain
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Francisco Ciruela, Víctor Fernández-Dueñas, and Marta Valle-León
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Postmortem brain ,Homogeneous ,Chemistry ,Biophysics ,Alpha (ethology) ,Luminescence ,G protein-coupled receptor - Published
- 2021
37. Association of C677T and A1298C
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Allan, Ramos-Esquivel, Ricardo, Chinchilla, and Marta, Valle
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Costa Rica ,Male ,Antimetabolites, Antineoplastic ,Organoplatinum Compounds ,Leucovorin ,Middle Aged ,Polymorphism, Single Nucleotide ,Antineoplastic Combined Chemotherapy Protocols ,Ethnicity ,Humans ,Female ,Fluorouracil ,Prospective Studies ,Neoplasm Metastasis ,Colorectal Neoplasms ,Methylenetetrahydrofolate Reductase (NADPH2) ,Aged - Abstract
Enzymatic variants involved in fluoropyrimidine metabolism have been associated with adverse events (AEs). We assessed the association between C677T (rs1801133) and A1298 (rs1801131) methylenetetrahydrofolate reductase (MTHFR) polymorphisms and AEs in patients with first-line fluoropyrimidine-based chemotherapy.Fifty patients with metastatic colorectal cancer were prospectively followed-up during the first 4 cycles of fluoropyrimidine-based treatment to assess AEs. Germline DNA was analyzed to determine the C677T and A1298C MTHFR polymorphisms. The associations between MTHFR polymorphisms and toxicity were examined.Individuals carrying at least one mutant allele of the MTHFR C677T polymorphism had increased risk to experience anemia (OR=1.69, 95% CI=1.13-2.53, p=0.005), neutropenia (OR=2.27, 95% CI=1.47-3.42, p0.001) thrombocytopenia (OR=1.91, 95% CI=1.30-2.70, p0.001), neuropathy (OR=1.77, 95% CI=1.16-2.70, p=0.02), diarrhea (OR=1.69, 95% CI=1.13-2.53, p=0.005), and hand-foot syndrome (OR=1.56, 95% CI=1.08-2.27, p=0.013), compared to patients carrying the wild type alleles. The presence of the mutant allele C of the MTHFR A1298C polymorphism was associated with increased risk of anemia (OR=2.75, 95% CI=1.01-7.48, p=0.02) and thrombocytopenia (OR=3.14, 95% CI=1.01-9.78, p=0.03); however, the prevalence of this allele in the sample was quite low (20%).MTHFR C677T and A1298C polymorphisms predicted toxicity in a subset of Mestizo patients with colorectal adenocarcinoma.
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- 2020
38. Decreased striatal adenosine A
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Marta, Valle-León, Luis F, Callado, Ester, Aso, María M, Cajiao-Manrique, Kristoffer, Sahlholm, Marc, López-Cano, Concepció, Soler, Xavier, Altafaj, Masahiko, Watanabe, Sergi, Ferré, Víctor, Fernández-Dueñas, José M, Menchón, and Francisco, Ciruela
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Mice ,Adenosine ,Receptor, Adenosine A2A ,Receptors, Dopamine D2 ,Dopamine ,Schizophrenia ,Animals ,Neurochemistry ,Corpus Striatum ,Article - Abstract
According to the adenosine hypothesis of schizophrenia, the classically associated hyperdopaminergic state may be secondary to a loss of function of the adenosinergic system. Such a hypoadenosinergic state might either be due to a reduction of the extracellular levels of adenosine or alterations in the density of adenosine A2A receptors (A2ARs) or their degree of functional heteromerization with dopamine D2 receptors (D2R). In the present study, we provide preclinical and clinical evidences for this latter mechanism. Two animal models for the study of schizophrenia endophenotypes, namely the phencyclidine (PCP) mouse model and the A2AR knockout mice, were used to establish correlations between behavioural and molecular studies. In addition, a new AlphaLISA-based method was implemented to detect native A2AR-D2R heteromers in mouse and human brain. First, we observed a reduction of prepulse inhibition in A2AR knockout mice, similar to that observed in the PCP animal model of sensory gating impairment of schizophrenia, as well as a significant upregulation of striatal D2R without changes in A2AR expression in PCP-treated animals. In addition, PCP-treated animals showed a significant reduction of striatal A2AR-D2R heteromers, as demonstrated by the AlphaLISA-based method. A significant and pronounced reduction of A2AR-D2R heteromers was next demonstrated in postmortem caudate nucleus from schizophrenic subjects, even though both D2R and A2AR were upregulated. Finally, in PCP-treated animals, sub-chronic administration of haloperidol or clozapine counteracted the reduction of striatal A2AR-D2R heteromers. The degree of A2AR-D2R heteromer formation in schizophrenia might constitute a hallmark of the illness, which indeed should be further studied to establish possible correlations with chronic antipsychotic treatments.
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- 2020
39. Dopaminergic signalling modulates reward-driven music memory consolidation
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Ernest Mas-Herrero, Robert J. Zatorre, Laura Ferreri, Marta Valle, Gemma Cardona, Jordi Riba, Rosa M. Antonijoan, Antoni Rodríguez-Fornells, and Pablo Ripollés
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Signalling ,Dopaminergic ,Memory formation ,Flexibility (personality) ,Memory consolidation ,Psychology ,behavioral disciplines and activities ,psychological phenomena and processes ,Cognitive psychology ,Memory recognition - Abstract
Previously, we provided causal evidence for a dopamine-dependent effect of intrinsic reward on memory during self-regulated learning (Ripollés et al., 2016; Ripollés et al., 2018). Here, we further investigated the dopamine-dependent link between reward and memory by focusing on one of the most iconic abstract rewards in humans: music. Twenty-nine healthy participants listened to unfamiliar excerpts—which had to be remembered following a consolidation period—after the intake of a dopaminergic antagonist, a dopaminergic precursor, and a placebo across three separated sessions. The intervention modulated the pleasantness experienced during music-listening and memory recognition of the presented songs (i.e., lower with the antagonist, higher with the precursor) in individuals with higher sensitivity to musical reward. Our work highlights the flexibility of the human dopaminergic system, which is able to enhance memory formation not only through explicit and/or primary reinforcers but also via intrinsic, abstract, or aesthetic rewards of different natures.
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- 2020
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40. Decreased Striatal Adenosine A(2A)-Dopamine D(2)Receptor Heteromerization in Schizophrenia
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Kristoffer Sahlholm, Masahiko Watanabe, Xavier Altafaj, Luis F. Callado, Víctor Fernández-Dueñas, Francisco Ciruela, Marc López-Cano, Marta Valle-León, José M. Menchón, Concepció Soler, María M. Cajiao-Manrique, Sergi Ferré, and Ester Aso
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dopamine D2 receptors ,Adenosine A2A receptor ,phencyclidine ,Adenosinergic ,Biology ,haloperidol ,03 medical and health sciences ,0302 clinical medicine ,Dopamine ,Dopamine receptor D2 ,medicine ,Haloperidol ,mice lacking ,Prepulse inhibition ,Pharmacology ,A(2A) receptors ,Neurosciences ,Adenosine ,030227 psychiatry ,Psychiatry and Mental health ,Knockout mouse ,hypothesis ,agonists ,cognitive impairments ,Neuroscience ,Neurovetenskaper ,030217 neurology & neurosurgery ,medicine.drug - Abstract
According to the adenosine hypothesis of schizophrenia, the classically associated hyperdopaminergic state may be secondary to a loss of function of the adenosinergic system. Such a hypoadenosinergic state might either be due to a reduction of the extracellular levels of adenosine or alterations in the density of adenosine A(2A)receptors (A(2A)Rs) or their degree of functional heteromerization with dopamine D(2)receptors (D2R). In the present study, we provide preclinical and clinical evidences for this latter mechanism. Two animal models for the study of schizophrenia endophenotypes, namely the phencyclidine (PCP) mouse model and the A(2A)R knockout mice, were used to establish correlations between behavioural and molecular studies. In addition, a new AlphaLISA-based method was implemented to detect native A(2A)R-D2R heteromers in mouse and human brain. First, we observed a reduction of prepulse inhibition in A(2A)R knockout mice, similar to that observed in the PCP animal model of sensory gating impairment of schizophrenia, as well as a significant upregulation of striatal D2R without changes in A(2A)R expression in PCP-treated animals. In addition, PCP-treated animals showed a significant reduction of striatal A(2A)R-D2R heteromers, as demonstrated by the AlphaLISA-based method. A significant and pronounced reduction of A(2A)R-D2R heteromers was next demonstrated in postmortem caudate nucleus from schizophrenic subjects, even though both D2R and A(2A)R were upregulated. Finally, in PCP-treated animals, sub-chronic administration of haloperidol or clozapine counteracted the reduction of striatal A(2A)R-D2R heteromers. The degree of A(2A)R-D2R heteromer formation in schizophrenia might constitute a hallmark of the illness, which indeed should be further studied to establish possible correlations with chronic antipsychotic treatments. This work was supported by FEDER/Ministerio de Ciencia, Innovacion y Universidades-Agencia Estatal de Investigacion (SAF2017-87349-R and MDM-2017-0729) and ISCIII (PIE14/00034), the Catalan government (2017 SGR 1604), Fundacio la Marato de TV3 (Grant 20152031), FWO (SBO-140028) to FC, the Basque Government (IT616/13 and IT-1211-19) and the intramural funds of the National Institute on Drug Addiction. The authors declare no conflict of interest.
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- 2020
41. Association of C677T and A1298C MTHFR Polymorphisms and Fluoropyrimidine-induced Toxicity in Mestizo Patients With Metastatic Colorectal Cancer
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Allan Ramos-Esquivel, Ricardo Chinchilla, and Marta Valle
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Cancer Research ,medicine.medical_specialty ,Anemia ,Colorectal cancer ,medicine.medical_treatment ,Single-nucleotide polymorphism ,Neutropenia ,Gastroenterology ,Mestizo population ,fluoropyrimidine-based chemotherapy ,03 medical and health sciences ,0302 clinical medicine ,cáncer ,Internal medicine ,medicine ,Allele ,Adverse effect ,Chemotherapy ,biology ,business.industry ,Metastatic colorectal cancer ,General Medicine ,medicine.disease ,methylenetetrahydrofolate reductase ,side effects ,Oncology ,030220 oncology & carcinogenesis ,Methylenetetrahydrofolate reductase ,biology.protein ,business ,SNPs - Abstract
Background/aim: Enzymatic variants involved in fluoropyrimidine metabolism have been associated with adverse events (AEs). We assessed the association between C677T (rs1801133) and A1298 (rs1801131) methylenetetrahydrofolate reductase (MTHFR) polymorphisms and AEs in patients with first-line fluoropyrimidine-based chemotherapy. Patients and methods: Fifty patients with metastatic colorectal cancer were prospectively followed-up during the first 4 cycles of fluoropyrimidine-based treatment to assess AEs. Germline DNA was analyzed to determine the C677T and A1298C MTHFR polymorphisms. The associations between MTHFR polymorphisms and toxicity were examined. Results: Individuals carrying at least one mutant allele of the MTHFR C677T polymorphism had increased risk to experience anemia (OR=1.69, 95% CI=1.13-2.53, p=0.005), neutropenia (OR=2.27, 95% CI=1.47-3.42, p
- Published
- 2020
42. Electrochemical Study of Quantum Dots-Labeled Oligonucleotide Probes for Detecting Nucleic Acid of African Swine Fever Virus
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Aksu, Davut Ahmet, Kizek, Rene, Hosnedlova, Bozena, Pay, Mert, Noguera, Marta Valle, and Banas, Dominik
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Banas D., Aksu D. A. , Noguera M. V. , Pay M., Hosnedlova B., Kizek R., -Electrochemical Study of Quantum Dots-Labeled Oligonucleotide Probes for Detecting Nucleic Acid of African Swine Fever Virus-, CHEMICKE LISTY, cilt.114, ss.778-783, 2020 ,food and beverages - Abstract
The study presents the cornerstone of the design of a biosensor for rapid detection of African swine fever virus (ASFV), affecting members of the Suidae family, in meat and meat products. Due to the widespread and serious socio-economic impact of this virus, there is an effort to prevent its spread by using a rapid detection, which can also be done by unprofessional operators (e.g., farmers). There are several methodological approaches utilizing nucleic acid amplification, e.g. PCR or RT-PCR, which require several technical steps or a high concentration of pathogen in the sample. Another technique that could overcome the above problems is the electrochemical nucleic acid detection. In this experimental work, the adsorptive transfer technique was used when the nucleic acid was accumulated on the electrode and a non-specifically linked oligonucleotide was washed away. To verify the stability of the ODN CA signal, the signals for King F and King R were measured for 15 days and control charts were generated. No measurement exceeded the 2 SD limit. The results show good reproducibility of measurements among individual days. QDs of 5 nm, with an excitation maximum at 327 nm and an emission maximum at 607 nm with an absorption maximum at 550 nm interacted with ODN. The adsorptive transfer technique was used in which the oligonucleotide was first bound to the electrode and then quantum dots was bound to the oligonucleotide, which was detected by measuring the signal of the separate oligonucleotide probes (King F and King R) (n = 10) and measuring the cadmium signal (n = 10). The oligonucleotide signals were King F 33 +/- 5 nA, King R 22 +/- 3 nA, King F/QDs 16 +/- 9 nA and King R/QDs 16 +/- 5 nA (oligonucleotide signal) and King F/QDs 62 +/- 16 nA and King R/QDs 89 +/- 18 nA (cadmium signal). These findings can be used for further experimental work in hybridizing oligonucleotide probes to viral DNA.
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- 2020
43. The MONDO tracker: characterisation and study of secondary ultrafast neutrons production in carbon ion radiotherapy
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Marco Toppi, Giuseppe Battistoni, Alessandro Bochetti, Patrizia De Maria, Micol De Simoni, Yunsheng Dong, Marta Fischetti, Gaia Franciosini, Leonardo Gasparini, Marco Magi, Enrico Manuzzato, Ilaria Mattei, Riccardo Mirabelli, Silvia Muraro, Luca Parmesan, Vincenzo Patera, Matteo Perenzoni, Alessio Sarti, Angelo Schiavi, Adalberto Sciubba, Giacomo Traini, Serena Marta Valle, and Michela Marafini
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Photon ,Physics::Instrumentation and Detectors ,medicine.medical_treatment ,Materials Science (miscellaneous) ,Monte Carlo method ,Biophysics ,General Physics and Astronomy ,Context (language use) ,Tracking (particle physics) ,01 natural sciences ,Optics ,SPAD technology ,0103 physical sciences ,medicine ,Neutron ,Physical and Theoretical Chemistry ,010306 general physics ,neutron tracker ,Mathematical Physics ,Physics ,Elastic scattering ,Particle therapy ,business.industry ,Detector ,neutron tracker, particle therapy, scintillating fibers ,neutron tracking ,lcsh:QC1-999 ,particle therapy ,carbon ions radiotherapy ,scintillating fibers ,secondary radiation monitoring ,business ,lcsh:Physics - Abstract
Secondary neutrons produced in Particle Therapy (PT) treatments are responsible for the delivery of a large fraction of the out-of-target dose as they feebly interact with the patient body. To properly account for their contribution to the total dose delivered to the patient, a high precision experimental characterisation of their production energy and angular distributions is eagerly needed. The experimental challenge posed by the detection and tracking of such neutrons will be addressed by the MONDO tracker: a compact scintillating fibres detector exploiting single and double elastic scattering interactions allowing for a complete neutron four momentum reconstruction. To achieve a high detection efficiency while matching the fibres (squared, 250 $\mu$m side) high granularity, a single photon sensitive readout has been developed using the CMOS based SPAD technology. The readout sensor, with pixels of $125\times250\ \micro\meter^2$ size, will be organised in tiles covering the full detector surface and will implement an auto-trigger strategy to identify the events of interest. The expected detector performance in the context of neutron component characterisation in PT treatments delivered using carbon ions has been evaluated using a Monte Carlo simulation accounting for the detector response and the neutrons production spectra.
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- 2020
44. Striatal Dopamine D
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René A. J. Crans, Elise Wouters, Marta Valle-León, Jaume Taura, Caio M. Massari, Víctor Fernández-Dueñas, Christophe P. Stove, and Francisco Ciruela
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0301 basic medicine ,M1R ,CHOLINERGIC INTERNEURONS ,striatum ,Parkinson's disease ,M1 ,SUMANIROLE ,Substantia nigra ,Pharmacology ,Medium spiny neuron ,03 medical and health sciences ,0302 clinical medicine ,PARKINSONS-DISEASE ,Dopamine receptor D2 ,Malaltia de Parkinson ,Muscarinic acetylcholine receptor ,medicine ,Pharmacology (medical) ,MODULATION ,VU0255035 ,Receptors neurals ,IN-VIVO ,Original Research ,D2R ,Chemistry ,Dopaminergic ,lcsh:RM1-950 ,Malalties neurodegeneratives ,Neurodegenerative Diseases ,Muscarinic acetylcholine receptor M1 ,Sumanirole ,030104 developmental biology ,lcsh:Therapeutics. Pharmacology ,ANIMAL-MODELS ,030220 oncology & carcinogenesis ,MOTOR SYMPTOMS ,Parkinson’s disease ,HETEROMERS ,SUBTYPE ,Neural receptor ,Acetylcholine ,sumanirole ,medicine.drug - Abstract
A corrigendum was published at https://doi.org/10.3389/fphar.2022.1075433, Parkinson's disease (PD) is a neurodegenerative disorder characterized by motor control deficits, which is associated with the loss of striatal dopaminergic neurons from the substantia nigra. In parallel to dopaminergic denervation, there is an increase of acetylcholine within the striatum, resulting in a striatal dopaminergic-cholinergic neurotransmission imbalance. Currently, available PD pharmacotherapy (e.g., prodopaminergic drugs) does not reinstate the altered dopaminergic-cholinergic balance. In addition, it can eventually elicit cholinergic-related adverse effects. Here, we investigated the interplay between dopaminergic and cholinergic systems by assessing the physical and functional interaction of dopamine D2 and muscarinic acetylcholine M1 receptors (D2R and M1R, respectively), both expressed at striatopallidal medium spiny neurons. First, we provided evidence for the existence of D2R-M1R complexes via biochemical (i.e., co-immunoprecipitation) and biophysical (i.e., BRET1 and NanoBiT®) assays, performed in transiently transfected HEK293T cells. Subsequently, a D2R-M1R co-distribution in the mouse striatum was observed through double-immunofluorescence staining and AlphaLISA® immunoassay. Finally, we evaluated the functional interplay between both receptors via behavioral studies, by implementing the classical acute reserpine pharmacological animal model of experimental parkinsonism. Reserpinized mice were administered with a D2R-selective agonist (sumanirole) and/or an M1R-selective antagonist (VU0255035), and alterations in PD-related behavioral tasks (i.e., locomotor activity) were evaluated. Importantly, VU0255035 (10 mg/kg) potentiated the antiparkinsonian-like effects (i.e., increased locomotor activity and decreased catalepsy) of an ineffective sumanirole dose (3 mg/kg). Altogether, our data suggest the existence of putative striatal D2R/M1R heteromers, which might be a relevant target to manage PD motor impairments with fewer adverse effects.
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- 2019
45. Effects of the Dopamine Stabilizer, Pridopidine, on Basal and Phencyclidine-Induced Locomotion: Role of Dopamine D2 and Sigma-1 Receptors
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Kristoffer Sahlholm, Jaume Taura, Francisco Ciruela, Víctor Fernández-Dueñas, and Marta Valle-León
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0301 basic medicine ,Time Factors ,Dopamine Agents ,Phencyclidine ,Pharmacology ,Open field ,Mice ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Piperidines ,Dopamine ,Dopamine receptor D2 ,medicine ,Animals ,Receptors, sigma ,Prepulse inhibition ,Mice, Knockout ,Analysis of Variance ,Sigma-1 receptor ,Dose-Response Relationship, Drug ,Prepulse Inhibition ,Receptors, Dopamine D2 ,General Neuroscience ,Pridopidine ,030104 developmental biology ,Acoustic Stimulation ,chemistry ,Dopamine receptor ,Exploratory Behavior ,Excitatory Amino Acid Antagonists ,Locomotion ,030217 neurology & neurosurgery ,medicine.drug - Abstract
Background: Pridopidine, a compound in clinical trials for Huntington's disease treatment, was originally synthesized as a dopamine D2 receptor (D2R) ligand, but later found to possess higher affinity for the sigma-1 receptor (S1R). However, the putative contributions of D2R and S1R to the behavioral profile of acutely administered pridopidine have not been investigated. Objective: The present study sought to compare the effects of acute pridopidine on wild-type vs. D2R and S1R knockout mice, at high (60 mg/kg) and low (6 mg/kg) doses. Method: Pridopidine effects on basal and phencyclidine-induced locomotor activity was measured in the open field test. Additionally, the actions of pridopidine on prepulse inhibition was measured in animals treated with saline or phencyclidine. Results: Whereas inhibition of spontaneous and phencyclidine-induced locomotion was readily observed at 60 mg/kg pridopidine, neither locomotor stimulation in habituated mice, nor any effects on prepulse inhibition were detected upon pridopidine treatment. Surprisingly, inhibition of spontaneous locomotion was unaffected by both D2R and S1R deletion. Conclusion: The present results suggest the involvement of additional targets, besides D2R and S1R, in mediating locomotor inhibition by pridopidine.
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- 2018
46. Impact of clinical pharmacist intervention on antimicrobial use in a small 164-bed hospital
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Pedro Mas-Morey, Marta Valle, Alfonso Ballesteros-Fernández, and Elisabet Sanmartin-Mestre
- Subjects
0301 basic medicine ,medicine.medical_specialty ,030106 microbiology ,infectious diseases ,law.invention ,pharmacotherapy ,03 medical and health sciences ,Pharmacotherapy ,law ,clinical pharmacy ,therapeutics ,medicine ,Antimicrobial stewardship ,General Pharmacology, Toxicology and Pharmaceutics ,Medical prescription ,Adverse effect ,Intensive care medicine ,medicine.diagnostic_test ,business.industry ,biochemical phenomena, metabolism, and nutrition ,Antimicrobial ,Intensive care unit ,adverse events ,Clinical pharmacy ,Therapeutic drug monitoring ,Original Article ,business - Abstract
Objectives To study the impact of clinical pharmacist interventions (PIs) on antimicrobial prescriptions in terms of physician acceptance rates, clinical benefits and antimicrobial use/cost outcomes. Methods This study retrospectively analysed the impact of antimicrobial PIs over a 2-year period (October 2012 to October 2014) in a private non-teaching 164-bed hospital without a formal antimicrobial stewardship programme. Excluded from the study were outpatients and patients admitted to the intensive care unit or the emergency department. The PIs focused on appropriate indication and appropriate dosage; drug adverse events, allergies, intolerance and interactions; sequential therapy; therapeutic de-escalation; excessive duration of treatment and therapeutic drug monitoring. Carbapenems and linezolid were classified as special-vigilance drugs. Amoxicillin-clavulanic, piperacillin-tazobactam and vancomycin were classified as preferred drugs. Clinical benefits evaluated in accordance with internal guidelines, were classified as enhancing appropriate antimicrobial prescription or potentially reducing toxicity. Antimicrobial use and expenditure were compared with that of the previous 2-year period. Results 386 PIs were implemented in 303 patients. The overall acceptance rate was 83.4%. The acceptance rate for appropriate prescription PIs was significantly lower than for toxicity PIs (73.7% vs 90.9%; p
- Published
- 2017
47. P-43 C677T and A1298C MTHFR gene polymorphisms and response to fluoropyrimidine-based chemotherapy in mestizo patients with metastatic colorectal cancer
- Author
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Marta Valle, R. Chinchilla-Monge, and A. Ramos-Esquivel
- Subjects
Oncology ,Chemotherapy ,medicine.medical_specialty ,biology ,Colorectal cancer ,business.industry ,medicine.medical_treatment ,Hematology ,medicine.disease ,Methylenetetrahydrofolate reductase ,Internal medicine ,medicine ,biology.protein ,business - Published
- 2021
48. Revealing Adenosine A
- Author
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Víctor, Fernández-Dueñas, Maricel, Gómez-Soler, Marta, Valle-León, Masahiko, Watanabe, Isidre, Ferrer, and Francisco, Ciruela
- Subjects
Male ,Receptor, Adenosine A2A ,GPCR oligomerization ,Gene Expression ,Adenosine A2A receptor ,Article ,Rats, Sprague-Dawley ,Mice ,AlphaScreen ,Animals ,Humans ,Parkinson Disease, Secondary ,Oxidopamine ,Aged ,Aged, 80 and over ,Mice, Knockout ,Parkinson Disease ,Dopamine D2 receptor ,Corpus Striatum ,High-Throughput Screening Assays ,Rats ,Disease Models, Animal ,Case-Control Studies ,Parkinson’s disease ,Female ,Autopsy ,Protein Multimerization - Abstract
Background: Several biophysical techniques have been successfully implemented to detect G protein-coupled receptors (GPCRs) heteromerization. Although these approaches have made it possible to ascertain the presence of GPCR heteromers in animal models of disease, no success has been accomplished in pathological human post-mortem brains. The AlphaScreen technology has been consistently used to quantify small analyte accumulation or depletion, bimolecular interactions, and post-translational modifications. The high signal-to-background, dynamic range and sensitivity exhibited by this technology support that it may be suitable to detect GPCR heteromers even under non-optimal conditions. Methods: Here, we describe the development of a new AlphaScreen assay to detect GPCR oligomers in human post-mortem brain. Results: Adenosine A2A-dopamine D2 receptor (A2AR/D2R) heteromer formation was monitored in caudate from healthy and Parkinson’s disease (PD) subjects. The approach was first validated using striatal membranes from wild type and A2AR deficient mice. Secondly, we took advantage of the 6-hydroxydopamine hemiparkinsonian rat model to validate previous results. In addition, finally, A2AR/D2R heteromer formation was assessed in caudate membranes from human post-mortem brains. Importantly, our preliminary results revealed an increase in A2AR/D2R heteromer formation in PD brains. Conclusions: The new AlphaScreen assay allowed assessing GPCR heteromers in human post-mortem brains with high sensitivity.
- Published
- 2019
49. Revealing Adenosine A2A-Dopamine D2 Receptor Heteromers in Parkinson's Disease Post-Mortem Brain through a New AlphaScreen-Based Assay
- Author
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Maricel Gómez-Soler, Marta Valle-León, Francisco Ciruela, Víctor Fernández-Dueñas, Masahiko Watanabe, Isidre Ferrer, and Universitat de Barcelona
- Subjects
Parkinson's disease ,Adenosine ,GPCR oligomerization ,Dopamine ,Adenosina ,Heteromer ,Adenosine A2A receptor ,Dopamina ,Catalysis ,Inorganic Chemistry ,lcsh:Chemistry ,AlphaScreen ,Dopamine receptor D2 ,Malaltia de Parkinson ,medicine ,Physical and Theoretical Chemistry ,Receptor ,Molecular Biology ,lcsh:QH301-705.5 ,Spectroscopy ,G protein-coupled receptor ,Dopamine D2 receptor ,Chemistry ,Organic Chemistry ,Wild type ,General Medicine ,medicine.disease ,Computer Science Applications ,lcsh:Biology (General) ,lcsh:QD1-999 ,Parkinson’s disease ,Neuroscience ,medicine.drug - Abstract
Background: Several biophysical techniques have been successfully implemented to detect G protein-coupled receptors (GPCRs) heteromerization. Although these approaches have made it possible to ascertain the presence of GPCR heteromers in animal models of disease, no success has been accomplished in pathological human post-mortem brains. The AlphaScreen technology has been consistently used to quantify small analyte accumulation or depletion, bimolecular interactions, and post-translational modifications. The high signal-to-background, dynamic range and sensitivity exhibited by this technology support that it may be suitable to detect GPCR heteromers even under non-optimal conditions. Methods: Here, we describe the development of a new AlphaScreen assay to detect GPCR oligomers in human post-mortem brain. Results: Adenosine A2A-dopamine D2 receptor (A2AR/D2R) heteromer formation was monitored in caudate from healthy and Parkinson&rsquo, s disease (PD) subjects. The approach was first validated using striatal membranes from wild type and A2AR deficient mice. Secondly, we took advantage of the 6-hydroxydopamine hemiparkinsonian rat model to validate previous results. In addition, finally, A2AR/D2R heteromer formation was assessed in caudate membranes from human post-mortem brains. Importantly, our preliminary results revealed an increase in A2AR/D2R heteromer formation in PD brains. Conclusions: The new AlphaScreen assay allowed assessing GPCR heteromers in human post-mortem brains with high sensitivity.
- Published
- 2019
50. Dopamine receptor heteromers: biasing antipsychotics
- Author
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Francisco Ciruela, Kristoffer Sahlholm, Marta Valle-León, and Víctor Fernández-Dueñas
- Subjects
0301 basic medicine ,Pharmacology ,business.industry ,Receptors, Dopamine D2 ,medicine.medical_treatment ,Biasing ,03 medical and health sciences ,Dopamine D2 Receptor Antagonists ,030104 developmental biology ,0302 clinical medicine ,Dopamine receptor ,Dopamine receptor D2 ,Drug Discovery ,Schizophrenia ,Molecular Medicine ,Medicine ,Animals ,Humans ,Protein Multimerization ,business ,Antipsychotic ,Neuroscience ,030217 neurology & neurosurgery ,Antipsychotic Agents ,Signal Transduction - Published
- 2018
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