316 research outputs found
Constructing a New Body Politic: Institutional Design and Education in Simón Bolívar, Simón Rodríguez, and Andrés Bello
Santiago de Chile, September 18, 1845: General Diego José Benavente (1790-1867) read a speech about his involvement in the independence movement at the University of Chile. The attendants to his address included Manuel Bulnes, President of the Republic; Manuel Montt, Minister of Education; Andrés Bello, Rector of the University; and heads of the state institutions. In front of them, Benavente asserted that if independence heroes were alive, “cuánta ser[ía] su satisfacción y complacencia al ver la nación independiente [. . .] gozando profunda paz bajo la égida de sus instituciones [y marchando] hacia la realización de los altos fines que ellos se propusieron” (122-23). An independence figure himself, Benavente linked the emancipatory goals in the country to the consolidation of a republican state apparatus. With respect to the University of Chile, he stated that a specific aim of the founding fathers was “la erección de este templo para que sus hijos vinieran a iniciarse en los sublimes misterios de aquellas ciencias que forman, conservan, y enriquecen a los Estados” (123)
Changes in the expression of the type 2 diabetes-associated gene VPS13C in the β cell are associated with glucose intolerance in humans and mice
Single nucleotide polymorphisms (SNPs) close to the VPS13C, C2CD4A and C2CD4B genes on chromosome 15q are associated with impaired fasting glucose and increased risk of type 2 diabetes. eQTL analysis revealed an association between possession of risk (C) alleles at a previously implicated causal SNP, rs7163757, and lowered VPS13C and C2CD4A levels in islets from female (n = 40, P < 0.041) but not from male subjects. Explored using promoter-reporter assays in β-cells and other cell lines, the risk variant at rs7163757 lowered enhancer activity. Mice deleted for Vps13c selectively in the β-cell were generated by crossing animals bearing a floxed allele at exon 1 to mice expressing Cre recombinase under Ins1 promoter control (Ins1Cre). Whereas Vps13cfl/fl:Ins1Cre (βVps13cKO) mice displayed normal weight gain compared with control littermates, deletion of Vps13c had little effect on glucose tolerance. Pancreatic histology revealed no significant change in β-cell mass in KO mice vs. controls, and glucose-stimulated insulin secretion from isolated islets was not altered in vitro between control and βVps13cKO mice. However, a tendency was observed in female null mice for lower insulin levels and β-cell function (HOMA-B) in vivo. Furthermore, glucose-stimulated increases in intracellular free Ca2+ were significantly increased in islets from female KO mice, suggesting impaired Ca2+ sensitivity of the secretory machinery. The present data thus provide evidence for a limited role for changes in VPS13C expression in conferring altered disease risk at this locus, particularly in females, and suggest that C2CD4A may also be involved
Anatomical basis of sleep
El sueño es un estado biológico activo, periódico,
en el que se distinguen las etapas NREM y REM, que se
alternan sucesivamente durante la noche. Intervienen
los relojes biológicos en la modulación del sistema, así
como neurotransmisores específicos. Se trata de una
red neuronal compleja, en la que intervienen diversas
zonas del sistema nervioso central. Los procesos oníricos
están controlados además de forma neural.
Se resume la historia de las investigaciones sobre
el tema, desde el siglo XIX hasta nuestra época. Hay
que destacar los recientes descubrimientos de Lugaresi
y su equipo, que, al describir el insomnio familiar
grave, dieron importancia al núcleo dorsomedial del
tálamo en la instauración de la fase de sueño profundo.
Al grupo de Reinoso se debe el hallazgo de que el
“director de orquesta” en la instauración del sueño
REM es la zona ventral paramediana del núcleo reticular
pontino ora
El consumo de la información científico-técnica por las empresas
The use of information of the Spanish industrial firms located at the Autonomous Community of Madrid is analyzed through the bibliographic searches and copies of original documents requested to CINDOC. Subject distribution of requested
documents is shown as well as the age-dependent decrease of the demand.
Journal articles account for 95% of requests, their scattering, distribution by countries and obsolescence according to subjects is also determined. Industrial firms in
the Biomedical and Chemical sectors are the biggest users of information , as contained in United States and Western European journals and the Spanish journals are
also heavily used. More of 60% of requested articles has been published in the 90s, while only 5% were published before 1970. Highest degree obsolescence appears in
Medicine, Pharmacy and BiologyEstudio del consumo de información de las empresas españolas a través de la demanda de consultas bibliográficas y copias de documentos recibida en el CINDOC, procedente de las empresas de la Comunidad de Madrid. Para los diferentes tipos de documentos solicitados se determina la distribución por materias y su antigüedad, y para los artículos de revistas que constituyen más del 95% de los documentos
requeridos se determina también la dispersión por títulos de las revistas y la procedencia de éstas por países de edición. Los datos ponen de manifiesto que las empresas de los sectores biomédico (Medicina, Farmacia y Biología) y químico
son las que más información externa utilizan, publicada sobre todo en revistas de Estados Unidos y de los países europeos occidentales, y que las revistas españolas tienen también una alta utilización. Más del 60% de la información solicitada es de
la década actual y sólo un 5% de los trabajos solicitados es anterior a 1970. De las materias más demandadas, Medicina, Farmacia y Biología son las que muestran mayor obsolescenci
High Levels of Proinflammatory Cytokines, but Not Markers of Tissue Injury, in Unaffected Intestinal Areas from Patients with IBD
Intestinal alterations in IBD are triggered and maintained by an overexpression of proinflammatory cytokines. Additionally, increased immune activation has been found in the adjacent intestinal areas without displaying any apparent histological alterations, however, the regulatory environment is not well established. Biopsy specimens from patients with ulcerative colitis (UC) and Crohn's disease (CD), from both affected and unaffected areas, and also from a group of colonic biopsies from healthy controls, were included in our study. Cytokines and markers of mucosal damage were analyzed by real-time PCR, and some of the results confirmed by western-blot and ELISA. Levels of IFNγ, TNFα, IL-6, IL-15, IL-18, and IL-23 were increased (above healthy controls) in both affected and unaffected areas from IBD. IL-1β, IL-6, IL-12, and IL-27 were higher in affected areas compared to unaffected ones in UC but not CD. In general, a correlation was observed between mRNA levels of these cytokines and both iNOS and Granzyme B. SOCS-2 and SOCS-3 were also increased in the affected areas. In conclusion, the unaffected areas from IBD show increased levels of a restricted set of cytokines that may exert immune activating roles in these areas without being able to trigger tissue damage
Functional Analysis of the Phycomyces carRA Gene Encoding the Enzymes Phytoene Synthase and Lycopene Cyclase
Phycomyces carRA gene encodes a protein with two domains. Domain R is characterized by red carR mutants that accumulate lycopene. Domain A is characterized by white carA mutants that do not accumulate significant amounts of carotenoids. The carRA-encoded protein was identified as the lycopene cyclase and phytoene synthase enzyme by sequence homology with other proteins. However, no direct data showing the function of this protein have been reported so far. Different Mucor circinelloides mutants altered at the phytoene synthase, the lycopene cyclase or both activities were transformed with the Phycomyces carRA gene. Fully transcribed carRA mRNA molecules were detected by Northern assays in the transformants and the correct processing of the carRA messenger was verified by RT-PCR. These results showed that Phycomyces carRA gene was correctly expressed in Mucor. Carotenoids analysis in these transformants showed the presence of ß-carotene, absent in the untransformed strains, providing functional evidence that the Phycomyces carRA gene complements the M. circinelloides mutations. Co-transformation of the carRA cDNA in E. coli with different combinations of the carotenoid structural genes from Erwinia uredovora was also performed. Newly formed carotenoids were accumulated showing that the Phycomyces CarRA protein does contain lycopene cyclase and phytoene synthase activities. The heterologous expression of the carRA gene and the functional complementation of the mentioned activities are not very efficient in E. coli. However, the simultaneous presence of both carRA and carB gene products from Phycomyces increases the efficiency of these enzymes, presumably due to an interaction mechanism
Normal radial migration and lamination are maintained in dyslexia-susceptibility candidate gene homolog Kiaa0319 knockout mice
AbstractDevelopmental dyslexia is a common disorder with a strong genetic component, but the underlying molecular mechanisms are still unknown. Several candidate dyslexia-susceptibility genes, including KIAA0319, DYX1C1, and DCDC2, have been identified in humans. RNA interference experiments targeting these genes in rat embryos have shown impairments in neuronal migration, suggesting that defects in radial cortical migration could be involved in the disease mechanism of dyslexia. Here we present the first characterisation of a Kiaa0319 knockout mouse line. Animals lacking KIAA0319 protein do not show anatomical abnormalities in any of the layered structures of the brain. Neurogenesis and radial migration of cortical projection neurons are not altered, and the intrinsic electrophysiological properties of Kiaa0319-deficient neurons do not differ from those of wild-type neurons. Kiaa0319 overexpression in cortex delays radial migration, but does not affect final neuronal position. However, knockout animals show subtle differences suggesting possible alterations in anxiety-related behaviour and in sensorimotor gating. Our results do not reveal a migration disorder in the mouse model, adding to the body of evidence available for Dcdc2 and Dyx1c1 that, unlike in the rat in utero knockdown models, the dyslexia-susceptibility candidate mouse homolog genes do not play an evident role in neuronal migration. However, KIAA0319 protein expression seems to be restricted to the brain, not only in early developmental stages but also in adult mice, indicative of a role of this protein in brain function. The constitutive and conditional knockout lines reported here will be useful tools for further functional analyses of Kiaa0319
Effects of Genetic Variants in ADCY5, GIPR, GCKR and VPS13C on Early Impairment of Glucose and Insulin Metabolism in Children
OBJECTIVE: Recent genome-wide association studies identified novel candidate genes for fasting and 2 h blood glucose and insulin levels in adults. We investigated the role of four of these loci (ADCY5, GIPR, GCKR and VPS13C) in early impairment of glucose and insulin metabolism in children. RESEARCH DESIGN AND METHODS: We genotyped four variants (rs2877716; rs1260326; rs10423928; rs17271305) in 638 Caucasian children with detailed metabolic testing including an oGTT and assessed associations with measures of glucose and insulin metabolism (including fasting blood glucose, insulin levels and insulin sensitivity/secretion indices) by linear regression analyses adjusted for age, sex, BMI-SDS and pubertal stage. RESULTS: The major allele (C) of rs2877716 (ADCY5) was nominally associated with decreased fasting plasma insulin (P = 0.008), peak insulin (P = 0.009) and increased QUICKI (P = 0.016) and Matsuda insulin sensitivity index (P = 0.013). rs17271305 (VPS13C) was nominally associated with 2 h blood glucose (P = 0.009), but not with any of the insulin or insulin sensitivity parameters. We found no association of the GIPR and GCKR variants with parameters of glucose and insulin metabolism. None of the variants correlated with anthropometric traits such as height, WHR or BMI-SDS, which excluded potential underlying associations with obesity. CONCLUSIONS: Our data on obese children indicate effects of genetic variation within ADCY5 in early impairment of insulin metabolism and VPS13C in early impairment of blood glucose homeostasis
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