Your search keyword '"Alcaraz, Luis A."' showing total 7 results

1. Neuroimaging Findings in Patients with EBF3Mutations: Report of Two Cases

Author

Jiménez de la Peña, Mar, Jiménez de Domingo, Ana, Tirado, Pilar, Calleja-Pérez, Beatriz, Alcaraz, Luis A., Álvarez, Sara, Williams, Jonathan, Hagman, James R., Németh, Andrea H., and Fernández-Jaén, Alberto

Abstract

Early B cell factor 3 (EBF3) is a transcription factor involved in brain development. Heterozygous, loss-of-function mutations in EBF3have been reported in an autosomal dominant neurodevelopmental syndrome characterized by hypotonia, ataxia, and developmental delay (sometimes described as “HADD”s). We report 2 unrelated cases with novel de novo EBF3mutations: c.455G>T (p.Arg152Leu) and c.962dup (p.Tyr321*) to expand the genotype/phenotype correlations of this disorder; clinical, neuropsychological, and MRI studies were used to define the phenotype. IQ was in the normal range and diffusion tensor imaging revealed asymmetric alterations of the longitudinal fasciculus in both cases. Our results demonstrate that EBF3mutations can underlie neurodevelopmental disorders without intellectual disability. Long tract abnormalities have not been previously recognized and suggest that they may be an unrecognized and characteristic feature in this syndrome.

Published

2021

2. ¿Es útil el uso del índice tobillo-brazo en pacientes con diabetes en atención primaria?

Author

Cervilla Suárez, Francisco José, Muñoz Cobos, Francisca, García Ruiz, Antonio, and Gálvez Alcaraz, Luis Federico

Published

2024

3. Consumo de ansiolíticos e hipnóticos y factores asociados en las personas mayores

Author

Téllez-Lapeira, Juan M., López-Torres Hidalgo, Jesús, Gálvez-Alcaraz, Luis, Párraga-Martínez, Ignacio, Boix-Gras, Clotilde, and García-Ruiz, Antonio

Abstract

Estimar la prevalencia del consumo de ansiolíticos e hipnóticos referido por los mayores de 65 años e identificar posibles factores condicionantes del citado uso.

Published

2017

4. Development of a novel analytical approach combining the quantification of amino acids, organic acids and glucose using HPLC-UV-Vis and HPLC-MS with screening via NMR

Author

Gómez-Mingot, Maria, Alcaraz, Luis A., MacIntyre, David A., Jiménez, Beatriz, Pineda-Lucena, Antonio, Montiel, Vicente, Banks, Craig E., and Iniesta, Jesús

Abstract

A simple, rapid, sensitive and selective procedure based on the combination of HPLC-UV-Vis and HPLC-MS has been developed and single laboratory partially validated for the determination of a set of 13 analytes present in a commercially available IVF medium utilising small sample volumes (20–30 μL). The composition fingerprint of the complex sample obtained by NMR spectroscopy in 11 minutes provided identification based on a screening of the metabolomic profile. HPLC-MS allowed the glucose–sodium adduct to be measured accurately and the working and linear ranges achieved were 0.028–0.389 mmol L−1with a detection limit of 13 μM. HPLC-UV-Vis allowed accurate concentrations of pyruvic and lactic acids with linear ranges over 0.005–0.1 mmol L−1with a limit of detection of 28 μM for pyruvic acid to be determined in 8 minutes, while lactic acid presented a linear range over 0.1–2 mmol L−1with a limit of detection of 1.2 mM possible. The use of HPLC-UV-Vis allowed the chromatographic separation of 8 amino acids (aspartate, glutamate, serine, glycine, asparagine, glutamine, alanine, and proline), the dipeptide alanyl-glutamine and taurine previous to a chemical derivatization, providing a total run time of 40 minutes. The method was partially validated to show a linear range of 0.028–0.280 mmol L−1with detection limits ranging between 1 and 30 μM. Development of the analytical approach provided determination and quantification of a set of 13 analytes from a very complex sample. Although well established analytical techniques were used here, combinatory methodologies were partially validated for the first time to this purpose. The novelty of the combination of techniques relies on a screening tool and a strategy to the future evaluation and an improved assessment of human embryo viability.

Published

2012

5. Into the Lipid Realm: Stability and Thermodynamics of Membrane Proteins

Author

Barrera, Francisco, Alcaraz, Luis, Hurtado-Gomez, Estefania, and Neira, Jose

Abstract

The first comprehensive studies on the structure and thermodynamics of membrane proteins have started revealing the exact architecture of these macromolecules and the physical-chemical rules behind their structures. In this review, the stabilities of several families of membrane proteins, obtained by using spectroscopic, calorimetric and single molecule techniques are surveyed. The data on the stability of membrane proteins are compared with those obtained in soluble proteins. The comparison indicates that although the number of particular atomic interactions is larger in membrane proteins than in soluble ones, the overall values are similar. The consensus is that some intrinsic properties of membrane proteins resemble those of soluble ones, but there are critical differences arising form the inter-molecular contacts with the surrounding membrane. Taken together, all these efforts improve our understanding of the universal forces governing protein folding, and will help in the design of membrane proteins in the near future.

Published

2008

6. Flexibility in HIV-1 Assembly Subunits: Solution Structure of the Monomeric C-Terminal Domain of the Capsid Protein

Author

Alcaraz, Luis A., del Álamo, Marta, Barrera, Francisco N., Mateu, Mauricio G., and Neira, José L.

Abstract

The protein CA forms the mature capsid of human immunodeficiency virus. Hexamerization of the N-terminal domain and dimerization of the C-terminal domain, CAC, occur during capsid assembly, and both domains constitute potential targets for anti-HIV inhibitors. CAC homodimerization occurs mainly through its second helix, and is abolished when its sole tryptophan is mutated to alanine. Previous thermodynamic data obtained with the dimeric and monomeric forms of CAC indicate that the structure of the mutant resembles that of a monomeric intermediate found in the folding and association reactions of CAC. We have solved the three-dimensional structure in aqueous solution of the monomeric mutant. The structure is similar to that of the subunits in the dimeric, nonmutated CAC, except the segment corresponding to the second helix, which is highly dynamic. At the end of this region, the polypeptide chain is bent to bury several hydrophobic residues and, as a consequence, the last two helices are rotated 90° when compared to their position in dimeric CAC. The previously obtained thermodynamic data are consistent with the determined structure of the monomeric mutant. This extraordinary ability of CAC to change its structure may contribute to the different modes of association of CA during HIV assembly, and should be taken into account in the design of new drugs against this virus.

Published

2007

7. Comparative genome sequence analysis underscores mycoparasitism as the ancestral life style of Trichoderma

Author

Kubicek, Christian P, Herrera-Estrella, Alfredo, Seidl-Seiboth, Verena, Martinez, Diego A, Druzhinina, Irina S, Thon, Michael, Zeilinger, Susanne, Casas-Flores, Sergio, Horwitz, Benjamin A, Mukherjee, Prasun K, Mukherjee, Mala, Kredics, László, Alcaraz, Luis D, Aerts, Andrea, Antal, Zsuzsanna, Atanasova, Lea, Cervantes-Badillo, Mayte G, Challacombe, Jean, Chertkov, Olga, McCluskey, Kevin, Coulpier, Fanny, Deshpande, Nandan, von Döhren, Hans, Ebbole, Daniel J, Esquivel-Naranjo, Edgardo U, Fekete, Erzsébet, Flipphi, Michel, Glaser, Fabian, Gómez-Rodríguez, Elida Y, Gruber, Sabine, Han, Cliff, Henrissat, Bernard, Hermosa, Rosa, Hernández-Oñate, Miguel, Karaffa, Levente, Kosti, Idit, Le Crom, Stéphane, Lindquist, Erika, Lucas, Susan, Lübeck, Mette, Lübeck, Peter S, Margeot, Antoine, Metz, Benjamin, Misra, Monica, Nevalainen, Helena, Omann, Markus, Packer, Nicolle, Perrone, Giancarlo, Uresti-Rivera, Edith E, Salamov, Asaf, Schmoll, Monika, Seiboth, Bernhard, Shapiro, Harris, Sukno, Serenella, Tamayo-Ramos, Juan Antonio, Tisch, Doris, Wiest, Aric, Wilkinson, Heather H, Zhang, Michael, Coutinho, Pedro M, Kenerley, Charles M, Monte, Enrique, Baker, Scott E, and Grigoriev, Igor V

Abstract

Background: Mycoparasitism, a lifestyle where one fungus is parasitic on another fungus, has special relevance when the prey is a plant pathogen, providing a strategy for biological control of pests for plant protection. Probably, the most studied biocontrol agents are species of the genus Hypocrea/Trichoderma. Results: Here we report an analysis of the genome sequences of the two biocontrol species Trichoderma atroviride(teleomorph Hypocrea atroviridis) and Trichoderma virens(formerly Gliocladium virens, teleomorph Hypocrea virens), and a comparison with Trichoderma reesei(teleomorph Hypocrea jecorina). These three Trichodermaspecies display a remarkable conservation of gene order (78 to 96%), and a lack of active mobile elements probably due to repeat-induced point mutation. Several gene families are expanded in the two mycoparasitic species relative to T. reeseior other ascomycetes, and are overrepresented in non-syntenic genome regions. A phylogenetic analysis shows that T. reeseiand T. virensare derived relative to T. atroviride. The mycoparasitism-specific genes thus arose in a common Trichodermaancestor but were subsequently lost in T. reesei. Conclusions: The data offer a better understanding of mycoparasitism, and thus enforce the development of improved biocontrol strains for efficient and environmentally friendly protection of plants.

Published

2011