Your search keyword '"Viguera, Enrique"' showing total 19 results

1. European first-year university students accept evolution but lack substantial knowledge about it: a standardized European cross-country assessment

Author

Kuschmierz, Paul, Beniermann, Anna, Bergmann, Alexander, Pinxten, Rianne, Aivelo, Tuomas, Berniak-Woźny, Justyna, Bohlin, Gustav, Bugallo-Rodriguez, Anxela, Cardia, Pedro, Cavadas, Bento Filipe Barreiras Pinto, Cebesoy, Umran Betul, Cvetković, Dragana D., Demarsy, Emilie, Đorđević, Mirko S., Drobniak, Szymon M., Dubchak, Liudmyla, Dvořáková, Radka M., Fančovičová, Jana, Fortin, Corinne, Futo, Momir, Geamănă, Nicoleta Adriana, Gericke, Niklas, Grasso, Donato A., Korfiatis, Konstantinos, Lendvai, Ádám Z., Mavrikaki, Evangelia, Meneganzin, Andra, Mogias, Athanasios, Möller, Andrea, Mota, Paulo G., Naciri, Yamama, Németh, Zoltán, Ożańska-Ponikwia, Katarzyna, Paolucci, Silvia, Pap, Péter László, Petersson, Maria, Pietrzak, Barbara, Pievani, Telmo, Pobric, Alma, Porozovs, Juris, Realdon, Giulia, Sá-Pinto, Xana, Savković, Uroš B., Sicard, Mathieu, Sofonea, Mircea T., Sorgo, Andrej, Stermin, Alexandru N., Tăușan, Ioan, Torkar, Gregor, Türkmen, Lütfullah, Tutnjević, Slavica, Uitto, Anna E., Varga, Máté, Varga, Mirna, Vazquez-Ben, Lucia, Viguera, Enrique, Virtbauer, Lisa Christine, Vutsova, Albena, Yruela, Inmaculada, Zandveld, Jelle, and Graf, Dittmar

Published

2021

2. DNA degradation in human teeth exposed to thermal stress

Author

Lozano-Peral, Diego, Rubio, Leticia, Santos, Ignacio, Gaitán, María Jesús, Viguera, Enrique, and Martín-de-las-Heras, Stella

Published

2021

3. España y las perspectivas financieras de la UE

Author

Navarro, Alberto and Viguera, Enrique

Published

2005

4. Reductive Genome Evolution in Buchnera aphidicola

Author

Kamerbeek, Judith, Palacios, Carmen, Rausell, Carolina, Abascal, Federico, Bastolla, Ugo, Fernández, Jose M., Jiménez, Luis, Postigo, Marina, Silva, Francisco J., Tamames, Javier, Viguera, Enrique, Latorre, Amparo, Valencia, Alfonso, Morán, Federico, and Moya, Andrés

Published

2003

5. LA DINÁMICA DE LA SOCIEDAD INTERNACIONAL. EL PAPEL DEL G20.

Author

VIGUERA, ENRIQUE

Subjects

*BALANCE of power, *GREAT powers (International relations), *DECISION making, *EMERGING markets, *PRESIDENTS, GROUP of Twenty countries, DEVELOPED countries, DEVELOPING countries, WESTERN countries

Abstract

Encompassing a diverse range of countries, including superpowers, emerging economies and developed nations, the G20's emerged during the waning years of unipolarity. Its unique composition, together with its flexible and informal working methods seems to be allowing it to adapt better than other organizations to a more multipolar landscape. Recent decisions taken in New Delhi further reinforce the G20's commitment to inclusivity and its sensitivity to the challenges faced by less developed countries. But despite the efforts of some prominent emerging countries that have recently assumed its rotating Presidency or will assume it soon, it remains to be seen how far the commitment of Western countries can go and whether it will be possible to encourage a more active engagement by China who seems lately more inclined on its own assertiveness or in promoting other competing structures such as BRICS. The US's role is crucial for the G20's effectiveness and survival as a forum for addressing global challenges. A new Trump presidency, less interested in multilateralism, could potentially hinder this progress. [ABSTRACT FROM AUTHOR]

Published

2023

6. The helicases DinG, Rep and UvrD cooperate to promote replication across transcription units in vivo

Author

Boubakri, Hasna, de Septenville, Anne Langlois, Viguera, Enrique, and Michel, Bénédicte

Published

2010

7. Reductive genome evolution in Buchnera aphidicola

Author

van Ham, Roeland C.H.J., Kamerbeek, Judith, Palacios, Carmen, Rausell, Carolina, Abascal, Federico, Bastolla, Ugo, Fernandez, Jose M., Jimenez, Luis, Postigo, Marina, Silva, Francisco J., Tamames, Javier, Viguera, Enrique, Latorre, Amparo, Valencia, Alfonso, Moran, Federico, and Moya, Andres

Subjects

Evolution -- Research, Genetic research, Science and technology

Abstract

We have sequenced the genome of the intracellular symbiont Buchnera aphidicola from the aphid Baizongia pistacea. This strain diverged 80-150 million years ago from the common ancestor of two previously sequenced Buchnera strains. Here, a field-collected, nonclonal sample of insects was used as source material for laboratory procedures. As a consequence, the genome assembly unveiled intrapopulational variation, consisting of [approximately equal to] 1,200 polymorphic sites. Comparison of the 618-kb (kbp) genome with the two other Buchnera genomes revealed a nearly perfect gene-order conservation, indicating that the onset of genomic stasis coincided closely with establishment of the symbiosis with aphids, [approximately equal to] 200 million years ago. Extensive genome reduction also predates the synchronous diversification of Buchnera and its host; but, at a slower rate, gene loss continues among the extant lineages. A computational study of protein folding predicts that proteins in Buchnera, as well as proteins of other intracellular bacteria, are generally characterized by smaller folding efficiency compared with proteins of free living bacteria. These and other degenerative genomic features are discussed in light of compensatory processes and theoretical predictions on the long-term evolutionary fate of symbionts like Buchnera.

Published

2003

8. Replication slippage involves DNA polymerase pausing and dissociation

Author

Viguera, Enrique, Canceill, Danielle, and Ehrlich, S.Dusko

Published

2001

9. Satisfaction, Assessment and Adaptation to a Virtual Environment of the University Mentoring Programme GuíaMe-AC-UMA for Gifted High School Students.

Author

Castro-Zamudio, Serafina, Viguera, Enrique, Cortés-Ramos, Antonio, Castilla-Mesa, María Teresa, Valbuena-Díaz, Daniel, and Moreno-Madrid, Isabel

Abstract

The purpose of this study is to analyse the satisfaction levels of participants (mentees, mentors, and technical-research team) of a university mentoring programme. The GuíaMe-AC-UMA is aimed at gifted high school students. Due to the COVID-19 pandemic, the IX edition was carried out in an online format. The results were compared to those of the in-person edition (VII edition) to assess whether there were differences between the editions. For this purpose, three versions (one for each participant type) of a Likert-type questionnaire were distributed among the participants of the 22 workshops offered by the GuíaMe-AC-UMA Programme. A total of 224 responses were received: 21 from the mentors, 181 from the mentees and 22 from the technical-research team. The results indicate a high level of satisfaction with the development of the workshops by all participants. While the mentees preferred the in-person edition, the rest of the participants showed no difference in satisfaction levels between editions. A similar result was observed when correcting for the subject area of the workshop. The in-person edition was valued higher than the online version by all. The overall level of satisfaction shown by all participants and the support for continuation of the programme suggest that this type of educational offer is beneficial and satisfactory for all involved, in accordance with previous research on mentoring programmes. These results indicate that programmes focused on young pre-university students with high abilities are valued; these results encourage us to continue the programme. [ABSTRACT FROM AUTHOR]

Published

2022

10. Lethality of bypass polymerases in Escherichia coli cells with a defective clamp loader complex of DNA polymerase III

Author

Viguera, Enrique, Petranovic, Mirjana, Zahradka, Davor, Germain, Karine, Ehrlich, Dusko S., and Michel, Bénédicte

Published

2003

11. Rescue of arrested replication forks by homologous recombination

Author

Michel, Benedicte, Flores, Maria-Jose, Viguera, Enrique, Grompone, Gianfranco, Seigneur, Marie, and Bidnenko, Vladimir

Subjects

DNA, Genetic recombination -- Research, Chromosome replication -- Research, Science and technology

Abstract

DNA synthesis is an accurate and very processive phenomenon; nevertheless, replication fork progression on chromosomes can be impeded by DNA lesions, DNA secondary structures, or DNA-bound proteins. Elements interfering with the progression of replication forks have been reported to induce rearrangements and/or render homologous recombination essential for viability, in all organisms from bacteria to human. Arrested replication forks may be the target of nucleases, thereby providing a substrate for double-strand break repair enzyme. For example in bacteria, direct fork breakage was proposed to occur at replication forks blocked by a bona fide replication terminator sequence, a specific site that arrests bacterial chromosome replication. Alternatively, an arrested replication fork may be transformed into a recombination substrate by reversal of the forked structures. In reversed forks, the last duplicated portions of the template strands reanneal, allowing the newly synthesized strands to pair. In bacteria, this reaction was proposed to occur in replication mutants, in which fork arrest is caused by a defect in a replication protein, and in UV irradiated cells. Recent studies suggest that it may also occur in eukaryote organisms. We will review here observations that link replication hindrance with DNA rearrangements and the possible underlying molecular processes.

Published

2001

12. Pharmacogenomics of Prostaglandin and Leukotriene Receptors.

Author

Cornejo-García, José A., Perkins, James R., Jurado-Escobar, Raquel, García-Martín, Elena, Agúndez, José A., Viguera, Enrique, Pérez-Sánchez, Natalia, Blanca-López, Natalia, Rauch, Bernhard H., and Roviezzo, Fiorentina

Subjects

SINGLE nucleotide polymorphisms, PHARMACOGENOMICS, PROSTAGLANDINS

Abstract

Individual genetic background together with environmental effects are thought to be behind many human complex diseases. A number of genetic variants, mainly single nucleotide polymorphisms (SNPs), have been shown to be associated with various pathological and inflammatory conditions, representing potential therapeutic targets. Prostaglandins (PTGs) and leukotrienes (LTs) are eicosanoids derived from arachidonic acid and related polyunsaturated fatty acids that participate in both normal homeostasis and inflammatory conditions. These bioactive lipid mediators are synthesized through two major multistep enzymatic pathways: PTGs by cyclooxygenase and LTs by 5-lipoxygenase. The main physiological effects of PTGs include vasodilation and vascular leakage (PTGE2); mast cell maturation, eosinophil recruitment, and allergic responses (PTGD2); vascular and respiratory smooth muscle contraction (PTGF2), and inhibition of platelet aggregation (PTGI2). LTB4 is mainly involved in neutrophil recruitment, vascular leakage, and epithelial barrier function, whereas cysteinyl LTs (CysLTs) (LTC4, LTD4, and LTE4) induce bronchoconstriction and neutrophil extravasation, and also participate in vascular leakage. PTGs and LTs exert their biological functions by binding to cognate receptors, which belong to the seven transmembrane, G protein-coupled receptor superfamily. SNPs in genes encoding these receptors may influence their functionality and have a role in disease susceptibility and drug treatment response. In this review we summarize SNPs in PTGs and LTs receptors and their relevance in human diseases. We also provide information on gene expression. Finally, we speculate on future directions for this topic. [ABSTRACT FROM AUTHOR]

Published

2016

13. Mammalian L-amino acid decarboxylases producing 1,4-diamines: analogies among differences

Author

Viguera, Enrique, Trelles, Oswaldo, Urdiales, Jose Luis, Mates, Jose Manuel, and Sanchez-Jimenez, Francisca

Subjects

Amines -- Research, Decarboxylases -- Research, Proteins -- Research, Biological sciences, Chemistry

Abstract

Mammalian mRNAs encoding histidine decarboxylase and aromatic-L-amino-acid decarboxylase were analyzed using a computer-based algorithm to determine the existence of PEST regions in hydrophilic protein sequences. The overlapping of the PEST regions of HDCs and DDCs indicate that some protein sequences found in HDCs were also present in DDCs. This suggests that HDCs share common structural features with DDCs.

Published

1994

14. ssb Gene Duplication Restores the Viability of ΔholC and ΔholD Escherichia coli Mutants.

Author

Duigou, Stéphane, Silvain, Maud, Viguera, Enrique, and Michel, Bénédicte

Subjects

CHROMOSOME duplication, BACTERIAL genetics, ESCHERICHIA coli, GENETIC mutation, GENES, GENETIC code

Abstract

The HolC-HolD (χψ) complex is part of the DNA polymerase III holoenzyme (Pol III HE) clamp-loader. Several lines of evidence indicate that both leading- and lagging-strand synthesis are affected in the absence of this complex. The Escherichia coli ΔholD mutant grows poorly and suppressor mutations that restore growth appear spontaneously. Here we show that duplication of the ssb gene, encoding the single-stranded DNA binding protein (SSB), restores ΔholD mutant growth at all temperatures on both minimal and rich medium. RecFOR-dependent SOS induction, previously shown to occur in the ΔholD mutant, is unaffected by ssb gene duplication, suggesting that lagging-strand synthesis remains perturbed. The C-terminal SSB disordered tail, which interacts with several E. coli repair, recombination and replication proteins, must be intact in both copies of the gene in order to restore normal growth. This suggests that SSB-mediated ΔholD suppression involves interaction with one or more partner proteins. ssb gene duplication also suppresses ΔholC single mutant and ΔholC ΔholD double mutant growth defects, indicating that it bypasses the need for the entire χψ complex. We propose that doubling the amount of SSB stabilizes HolCD-less Pol III HE DNA binding through interactions between SSB and a replisome component, possibly DnaE. Given that SSB binds DNA in vitro via different binding modes depending on experimental conditions, including SSB protein concentration and SSB interactions with partner proteins, our results support the idea that controlling the balance between SSB binding modes is critical for DNA Pol III HE stability in vivo, with important implications for DNA replication and genome stability. [ABSTRACT FROM AUTHOR]

Published

2014

15. Sma3s: A Three-Step Modular Annotator for Large Sequence Datasets.

Author

Muñoz-Mérida, Antonio, Viguera, Enrique, Claros, M. Gonzalo, Trelles, Oswaldo, and Pérez-Pulido, Antonio J.

Abstract

Automatic sequence annotation is an essential component of modern ‘omics’ studies, which aim to extract information from large collections of sequence data. Most existing tools use sequence homology to establish evolutionary relationships and assign putative functions to sequences. However, it can be difficult to define a similarity threshold that achieves sufficient coverage without sacrificing annotation quality. Defining the correct configuration is critical and can be challenging for non-specialist users. Thus, the development of robust automatic annotation techniques that generate high-quality annotations without needing expert knowledge would be very valuable for the research community. We present Sma3s, a tool for automatically annotating very large collections of biological sequences from any kind of gene library or genome. Sma3s is composed of three modules that progressively annotate query sequences using either: (i) very similar homologues, (ii) orthologous sequences or (iii) terms enriched in groups of homologous sequences. We trained the system using several random sets of known sequences, demonstrating average sensitivity and specificity values of ∼85%. In conclusion, Sma3s is a versatile tool for high-throughput annotation of a wide variety of sequence datasets that outperforms the accuracy of other well-established annotation algorithms, and it can enrich existing database annotations and uncover previously hidden features. Importantly, Sma3s has already been used in the functional annotation of two published transcriptomes. [ABSTRACT FROM PUBLISHER]

Published

2014

16. Rifampicin suppresses thymineless death by blocking the transcription-dependent step of chromosome initiation.

Author

Martín, Carmen Mata, Viguera, Enrique, and Guzmán, Elena C.

Subjects

*RIFAMPIN, *THYMINE, *GENETIC transcription, *CELL death, *DNA replication, *CHROMOSOMES

Abstract

Highlights: [•] This study aims to identify how rifampicin suppresses Thymineless death (TLD). [•] Rifampicin concentration during thymine starvation inversely correlates with TLD. [•] Replication intermediates accumulate during thymine starvation at oriC. [•] Altering transcription in cis in the oriC region alleviates TLD. [•] Data shows that rifampicin suppresses TLD by inhibiting replication initiation. [ABSTRACT FROM AUTHOR]

Published

2014

17. A microRNA Signature Associated with Early Recurrence in Breast Cancer.

Author

Pérez-Rivas, Luis G., Jerez, José M., Carmona, Rosario, de Luque, Vanessa, Vicioso, Luis, Claros, M. Gonzalo, Viguera, Enrique, Pajares, Bella, Sánchez, Alfonso, Ribelles, Nuria, Alba, Emilio, and Lozano, José

Subjects

MICRORNA, DISEASE relapse, BREAST cancer treatment, HEALTH outcome assessment, METASTASIS, RNA interference

Abstract

Recurrent breast cancer occurring after the initial treatment is associated with poor outcome. A bimodal relapse pattern after surgery for primary tumor has been described with peaks of early and late recurrence occurring at about 2 and 5 years, respectively. Although several clinical and pathological features have been used to discriminate between low- and high-risk patients, the identification of molecular biomarkers with prognostic value remains an unmet need in the current management of breast cancer. Using microarray-based technology, we have performed a microRNA expression analysis in 71 primary breast tumors from patients that either remained disease-free at 5 years post-surgery (group A) or developed early (group B) or late (group C) recurrence. Unsupervised hierarchical clustering of microRNA expression data segregated tumors in two groups, mainly corresponding to patients with early recurrence and those with no recurrence. Microarray data analysis and RT-qPCR validation led to the identification of a set of 5 microRNAs (the 5-miRNA signature) differentially expressed between these two groups: miR-149, miR-10a, miR-20b, miR-30a-3p and miR-342-5p. All five microRNAs were down-regulated in tumors from patients with early recurrence. We show here that the 5-miRNA signature defines a high-risk group of patients with shorter relapse-free survival and has predictive value to discriminate non-relapsing versus early-relapsing patients (AUC = 0.993, p-value<0.05). Network analysis based on miRNA-target interactions curated by public databases suggests that down-regulation of the 5-miRNA signature in the subset of early-relapsing tumors would result in an overall increased proliferative and angiogenic capacity. In summary, we have identified a set of recurrence-related microRNAs with potential prognostic value to identify patients who will likely develop metastasis early after primary breast surgery. [ABSTRACT FROM AUTHOR]

Published

2014

18. Multitissue array review: A chronological description of tissue array techniques, applications and procedures

Author

Eguíluz, Cesar, Viguera, Enrique, Millán, Lucinio, and Pérez, Josefa

Subjects

*LITERATURE, *IMMUNOHISTOCHEMISTRY, *HISTOPATHOLOGY, *TRANSPLANTATION of organs, tissues, etc.

Abstract

Abstract: We performed a systematic search for literature dealing with tissue microarray technology. During the last two decades, these procedures have developed into a powerful tool for the high-throughput analysis of tissue specimens. This technology offers the following advantages: amplification of a scarce resource, experimental uniformity (tissue of multiple patients are treated in an identical manner), decreased assay volume, preservation of original blocks, amenability to a wide range of techniques and evaluation of tissue from multiple patients on the same slide. Depending on the shape of the tissue sample and the method used to obtain it, multitissue array techniques may be classified into two different groups: rod-shaped tissue techniques and core tissue techniques. These techniques have been used for quality control, diagnosis, and teaching and screening purposes. Some technical aspects should be considered when deciding which technique should be used: the number, size and origin of tissue samples; the quality of paraffin wax, the distance between samples and the depth in the receptor block; antigenicity preservation and block sectioning. This review shows different techniques, the use of which is dependent on the requirements of the arrays and the technical possibilities. [Copyright &y& Elsevier]

Published

2006

19. Genomic Determinants of Protein Folding Thermodynamics in Prokaryotic Organisms

Author

Bastolla, Ugo, Moya, Andrés, Viguera, Enrique, and van Ham, Roeland C.H.J.

Subjects

*PROTEIN conformation, *GENOMES, *NATURAL selection, *NUCLEOTIDE sequence

Abstract

Here we investigate how thermodynamic properties of orthologous proteins are influenced by the genomic environment in which they evolve. We performed a comparative computational study of 21 protein families in 73 prokaryotic species and obtained the following main results. (i) Protein stability with respect to the unfolded state and with respect to misfolding are anticorrelated. There appears to be a trade-off between these two properties, which cannot be optimized simultaneously. (ii) Folding thermodynamic parameters are strongly correlated with two genomic features, genome size and G+C composition. In particular, the normalized energy gap, an indicator of folding efficiency in statistical mechanical models of protein folding, is smaller in proteins of organisms with a small genome size and a compositional bias towards A+T. Such genomic features are characteristic for bacteria with an intracellular lifestyle. We interpret these correlations in light of mutation pressure and natural selection. A mutational bias toward A+T at the DNA level translates into a mutational bias toward more hydrophobic (and in general more interactive) proteins, a consequence of the structure of the genetic code. Increased hydrophobicity renders proteins more stable against unfolding but less stable against misfolding. Proteins with high hydrophobicity and low stability against misfolding occur in organisms with reduced genomes, like obligate intracellular bacteria. We argue that they are fixed because these organisms experience weaker purifying selection due to their small effective population sizes. This interpretation is supported by the observation of a high expression level of chaperones in these bacteria. Our results indicate that the mutational spectrum of a genome and the strength of selection significantly influence protein folding thermodynamics. [Copyright &y& Elsevier]

Published

2004