Difusión del consumo de leche en España (1865- 1981)

La aproximación habitual en el estudio de la difusión del consumo de un alimento, además de descomponer su aportación nutricional, consiste en estudiar la evolución de sus consumos medios. Pero en todo proceso de difusión de un nuevo producto, establecer el consumo promedio es tan importante como conocer el número de consumidores. Este artículo propone un análisis de la recepción del consumo de leche entre la población española atendiendo a ambas dimensiones entre finales del siglo XIX y 1981. Esto es, se combinará el conocimiento de la evolución del número de consumidores con el de sus niveles medios de consumo. Adoptar este planteamiento supone enfrentarse con el problema de la ausencia de datos sobre la magnitud de consumidores en las fuentes estadísticas disponibles. Este artículo propone una estrategia metodológica diseñada para reconstruir la evolución de esa población tanto en una escala temporal como espacial.

El programa Biodiversitat Micològica de les terres de Ponent. Notícia i primers resultats.

La tardor de 1994 ha presentat unes condicions molt favorables de pluviositat, humitat i temperatura, que han permès un estudi intensiu (59 excursions, 64 localitats) de la part occidental, baixa i seca, de Catalunya, de la qual es tenien molt poques dades micològiques. E1 catàleg preliminar que oferim, amb tot i l'absència de moltes espècies pendents d'estudi o confirmació, i també de les més eurioiques, considerades poc característiques, conté 170 espècies, i permet fer-se una idea de la flora fúngica xero-termòfila mediterrània, especialment, la de les brolles, pinedes i espais oberts. Al costat d'algunes espècies poc citades, com Eutryblidiella hysterina, Helvella villosa, Agaricus pilatianus, Amanita boudieri, Calyptella capula, Ceriporia bresadolae, Coprinus vosoustii, Henningsomyces puber, Hygrophorus carneogriseus, Marasmius corbariensis, Phellinus punctatus, Ramicola iberica, Skeletocutis percandida, Tulostoma nanum, T. occidentale, T. xerophilum, Typhula setipes, Xerocomus ichnusanus, d'altres han mostrat una abundància inusitada, com Mycocalicium minutellum, Amanita ovoidea, Clitocybe alexandrí, C. umbilicata, Entoloma rusticoides, Hebeloma edurum, Inocybe roseipes, Lepista rickenii, Lopharia spadicea, Omphalotus olearius, Phaeotellus rickenii, Polyporus meridionalis, Suillus bellinii, S. collinitus, Volvariella speciosa, Mucilago crustacea. És previst continuar les prospeccions, per a completar aquesta primera visió.

Hog1 bypasses stress-mediated down-regulation of transcription by RNA polymerase II redistribution and chromatin remodeling

Cells are subjected to dramatic changes of gene expression upon environmental changes. Stresscauses a general down-regulation of gene expression together with the induction of a set of stress-responsivegenes. The p38-related stress-activated protein kinase Hog1 is an important regulator of transcription uponosmostress in yeast. Genome-wide localization studies of RNA polymerase II (RNA Pol II) and Hog1 showed that stress induced major changes in RNA Pol II localization, with a shift toward stress-responsive genes relative to housekeeping genes. RNA Pol II relocalization required Hog1, which was also localized to stress-responsive loci. In addition to RNA Pol II-bound genes, Hog1 also localized to RNA polymerase III-bound genes, pointing to a wider role for Hog1 in transcriptional control than initially expected. Interestingly, an increasing association of Hog1 with stressresponsive genes was strongly correlated with chromatin remodeling and increased gene expression. Remarkably, MNase-Seq analysis showed that although chromatin structure was not significantly altered at a genome-wide level in response to stress, there was pronounced chromatin remodeling for those genes that displayed Hog1 association. Hog1 serves to bypass the general down-regulation of gene expression that occurs in response to osmostress, and does so both by targeting RNA Pol II machinery and by inducing chromatin remodeling at stressresponsive loci.

A nuclear defect in the 4p16 region predisposes to multiple mitochondrial DNA deletions in families with Wolfram syndrome.

Wolfram syndrome is a progressive neurodegenerative disorder transmitted in an autosomal recessive mode. We report two Wolfram syndrome families harboring multiple deletions of mitochondrial DNA. The deletions reached percentages as high as 85-90% in affected tissues such as the central nervous system of one patient, while in other tissues from the same patient and from other members of the family, the percentages of deleted mitochondrial DNA genomes were only 1-10%. Recently, a Wolfram syndrome gene has been linked to markers on 4p16. In both families linkage between the disease locus and 4p16 markers gave a maximum multipoint lod score of 3.79 at theta = 0 (Pi<0.03) with respect to D4S431. In these families, the syndrome was caused by mutations in this nucleus-encoded gene which deleteriously interacts with the mitochondrial genome. This is the first evidence of the implication of both genomes in a recessive disease.

A nuclear defect in the 4p16 region predisposes to multiple mitochondrial DNA deletions in families with Wolfram syndrome.

Wolfram syndrome is a progressive neurodegenerative disorder transmitted in an autosomal recessive mode. We report two Wolfram syndrome families harboring multiple deletions of mitochondrial DNA. The deletions reached percentages as high as 85-90% in affected tissues such as the central nervous system of one patient, while in other tissues from the same patient and from other members of the family, the percentages of deleted mitochondrial DNA genomes were only 1-10%. Recently, a Wolfram syndrome gene has been linked to markers on 4p16. In both families linkage between the disease locus and 4p16 markers gave a maximum multipoint lod score of 3.79 at theta = 0 (Pi<0.03) with respect to D4S431. In these families, the syndrome was caused by mutations in this nucleus-encoded gene which deleteriously interacts with the mitochondrial genome. This is the first evidence of the implication of both genomes in a recessive disease.

Effect of drift on segregation in two-component diffusion-limited aggregation

An effect of drift is investigated on the segregation pattern in diffusion-limited aggregation (DLA) with two components (A and B species). The sticking probability PAB (=PBA) between the different species is introduced into the DLA model with drift, where the sticking probability PAA (=PBB) between the same species equals 1. By using computer simulation it is found that the drift has an important effect on not only the morphology but also the segregation pattern. Under the drift and the small sticking probability, a characteristic pattern appears where elongated clusters of A species and of B species are periodically dispersed. The period decreases with increasing drift. The periodic structure of the deposits is characterized by an autocorrelation function. The shape of the cluster consisting of only A species (or B species) shows a vertically elongated filamentlike structure. Each cluster becomes vertically longer with decreasing sticking probability PAB. The segregation pattern is distinctly different from that with no drift and a small sticking probability PAA. The effect of the concentration on the segregation pattern is also shown.

Aggregation under a forced convective flow

Morphological transitions are analyzed for a radial multiparticle diffusion-limited aggregation process grown under a convective drift. The introduction of a tangential flow changes the morphology of the diffusion-limited structure, into multiarm structures, inclined opposite to the flow, whose limit consists of single arms, when decreasing density. The case of shear flow is also considered. The anisotropy of the patterns is characterized in terms of a tangential correlation function based analysis. Comparison between the simulation results and preliminary experimental results has been done.

A semi-grand canonical Monte Carlo simulation model for ion binding to ionizable surfaces: proton binding of carboxylated latex particles as a case study

In this paper, we present a computer simulation study of the ion binding process at an ionizable surface using a semi-grand canonical Monte Carlo method that models the surface as a discrete distribution of charged and neutral functional groups in equilibrium with explicit ions modelled in the context of the primitive model. The parameters of the simulation model were tuned and checked by comparison with experimental titrations of carboxylated latex particles in the presence of different ionic strengths of monovalent ions. The titration of these particles was analysed by calculating the degree of dissociation of the latex functional groups vs. pH curves at different background salt concentrations. As the charge of the titrated surface changes during the simulation, a procedure to keep the electroneutrality of the system is required. Here, two approaches are used with the choice depending on the ion selected to maintain electroneutrality: counterion or coion procedures. We compare and discuss the difference between the procedures. The simulations also provided a microscopic description of the electrostatic double layer (EDL) structure as a function of p H and ionic strength. The results allow us to quantify the effect of the size of the background salt ions and of the surface functional groups on the degree of dissociation. The non-homogeneous structure of the EDL was revealed by plotting the counterion density profiles around charged and neutral surface functional groups.

Contribution of S6K1/MAPK signaling pathways in the response to oxidative stress: activation of RSK and MSK by hydrogen peroxide

Cells respond to different kind of stress through the coordinated activation of signaling pathways such as MAPK or p53. To find which molecular mechanisms are involved, we need to understand their cell adaptation. The ribosomal protein, S6 kinase 1 (S6K1), is a common downstream target of signaling by hormonal or nutritional stress. Here, we investigated the initial contribution of S6K1/MAPK signaling pathways in the cell response to oxidative stress produced by hydrogen peroxide (H2O2). To analyze S6K1 activation, we used the commercial anti-phospho-Thr389-S6K1 antibody most frequently mentioned in the bibliography. We found that this antibody detected an 80-90 kDa protein that was rapidly phosphorylated in response to H2O2 in several human cells. Unexpectedly, this phosphorylation was insensitive to both mTOR and PI3K inhibitors, and knock-down experiments showed that this protein was not S6K1. RSK and MSK proteins were candidate targets of this phosphorylation. We demonstrated that H2O2 stimulated phosphorylation of RSK and MSK kinases at residues that are homologous to Thr389 in S6K1. This phosphorylation required the activity of either p38 or ERK MAP kinases. Kinase assays showed activation of RSK and MSK by H2O2. Experiments with mouse embryonic fibroblasts from p38 animals" knockout confirmed these observations. Altogether, these findings show that the S6K1 signaling pathway is not activated under these conditions, clarify previous observations probably misinterpreted by non-specific detection of proteins RSK and MSK by the anti-phospho-Thr389-S6K1 antibody, and demonstrate the specific activation of MAPK signaling pathways through ERK/p38/RSK/MSK by H2O2.

Membrane interaction of polymyxin B and synthetic analogues studied in biomimetic systems: implications for antibacterial action

Membrane-active antimicrobial peptides, such as polymyxin B (PxB), are currently in the spotlight as potential candidates toovercome bacterial resistance. We have designed synthetic analogs ofPxB in order to determine the structural requirements for membraneaction. Since the mechanism of action of PxB involves interaction withboth the outer membrane and the cytoplasmic membrane of Gramnegative bacteria, we have used an approach based on mimicking theouter layers of these membranes using monolayers, Langmuir-Blodgettfilms and unilamelar vesicles, and applying a battery of biophysicalmethods in order to dissect the different events of membraneinteraction. Collectively, results indicate that the PxB analogues act inthe bacterial membrane by the same mechanism than PxB, and that cationic amphipathicity determines peptide activity.

New strategies in the modulation of fatty acid oxidation as a treatment for obesity

Strategies that enhance fat degradation or reduce caloricfood intake could be considered therapeutic interventions to reduce notonly obesity, but also its associated disorders. The enzyme carnitinepalmitoyltransferase 1 (CPT1) is the critical rate-determining regulatorof fatty acid oxidation (FAO) and might play a key role in increasingenergy expenditure and controlling food intake. Our group has shownthat mice overexpressing CPT1 in liver are protected from weight gain,the development of obesity and insulin resistance. Regarding foodintake control, we observed that the pharmacological inhibition ofCPT1 in rat hypothalamus decreased food intake and body weight.This suggests that modulation of CPT1 activity and the oxidation offatty acids in various tissues can be crucial for the potential treatmentof obesity and associated pathologies.

La regulació dels gestors de fons d'inversió alternativa a la UE : canvi de paradigma regulatiu?

En aquest treball es fa una aproximació al procés de policy making darrere de la regulació europea dels Gestors de Fons d’Inversió Alternativa (GFIA). S’ha tractat de respondre la qüestió de perquè la UE ha regulat durament aquesta indústria respecte de la regulació duta a terme als Estats Units i dels compromisos adquirits al G20. En primer lloc s’han reconstruït les etapes d’agenda setting, formació de polítiques i presa de decisions. A continuació s’ha testat la teoria des de la qual s’ha tractat d’explicar aquest fenomen de forma majoritària, la del canvi de paradigma regulatiu, que atorga una enorme importància al rol de les idees. Tot seguit es proposa una aproximació alternativa per a explicar el perquè aquest outcome regulatiu es va produir. L’aproximació es fa des de l’Institucionalisme Històric de Pierson, tot i que no es tanca exclusivament a aquesta. El model explicatiu consisteix en 4 elements, 1) Els constrenyiments institucionals específics de la UE, 2) Una asimetria en els costos regulatius, lligat a aquest, 3) Les preferències dels principals Estats membre i altres actors rellevants i finalment 4) La crisi financera com una finestra d’oportunitat.

Treball experimental en mitjans propis: UPF.RÃ dio

Aquesta memòria recull el projecte experimental que quatre estudiants del grau en Periodisme de la Universitat Pompeu Fabra han portat a terme al mitjà UPF.Ràdio, durant el curs 2012-2013. Aquesta investigació neix de la voluntat de modernitzar i dinamitzarl’emissora universitària, a partir d’un estudi de camp inicial i del treball pràctic al mitjà. En aquest document s’exposen els objectius executats, les tasques desenvolupades i una autoavaluació final del projecte. Queda com la primera investigació sobre la naturalesa d’UPF.Ràdio i com a base per a ajudar a consolidar un projecte radiofònic solvent en el futur.

Registre telemà tic per administracions públiques

El projecte neix amb la finalitat de reduir aquests costos, creant una infraestructura que permeti realitzar els tràmits amb les Administracions Públiques per via telemàtica. D'aquesta forma se suprimeix la necessitat d'acudir presencialment a una oficina de l'Administració, suposant una gran avantatge per ambdues parts, especialment en quant al cost temporal.