249 research outputs found
Chronic Treatment with a Promnesiant GABA-A α5-Selective Inverse Agonist Increases Immediate Early Genes Expression during Memory Processing in Mice and Rectifies Their Expression Levels in a Down Syndrome Mouse Model
Decrease of GABAergic transmission has been proposed to improve memory functions. Indeed, inverse agonists selective for α5 GABA-A-benzodiazepine receptors (α5IA) have promnesiant activity. Interestingly, we have recently shown that α5IA can rescue cognitive deficits in Ts65Dn mice, a Down syndrome mouse model with altered GABAergic transmission. Here, we studied the impact of chronic treatment with α5IA on gene expression in the hippocampus of Ts65Dn and control euploid mice after being trained in the Morris water maze task. In euploid mice, chronic treatment with α5IA increased IEGs expression, particularly of c-Fos and Arc genes. In Ts65Dn mice, deficits of IEGs activation were completely rescued after treatment with α5IA. In addition, normalization of Sod1 overexpression in Ts65Dn mice after α5IA treatment was observed. IEG expression regulation after α5IA treatment following behavioral stimulation could be a contributing factor for both the general promnesiant activity of α5IA and its rescuing effect in Ts65Dn mice alongside signaling cascades that are critical for memory consolidation and cognition
Specific targeting of the GABA-A receptor α5 subtype by a selective inverse agonist restores cognitive deficits in Down syndrome mice
An imbalance between inhibitory and excitatory neurotransmission has been
proposed to contribute to altered brain function in individuals with Down
syndrome (DS). Gamma-aminobutyric acid (GABA) is the major inhibitory
neurotransmitter in the central nervous system and accordingly treatment with
GABA-A antagonists can efficiently restore cognitive functions of Ts65Dn mice, a
genetic model for DS. However, GABA-A antagonists are also convulsant which
preclude their use for therapeutic intervention in DS individuals. Here, we have
evaluated safer strategies to release GABAergic inhibition using a
GABA-A-benzodiazepine receptor inverse agonist selective for the α5-subtype
(α5IA). We demonstrate that α5IA restores learning and memory functions of
Ts65Dn mice in the novel-object recognition and in the Morris water maze tasks.
Furthermore, we show that following behavioural stimulation, α5IA enhances
learning-evoked immediate early gene products in specific brain regions involved
in cognition. Importantly, acute and chronic treatments with α5IA do not induce
any convulsant or anxiogenic effects that are associated with GABA-A antagonists
or non-selective inverse agonists of the GABA-A-benzodiazepine receptors.
Finally, chronic treatment with α5IA did not induce histological alterations in
the brain, liver and kidney of mice. Our results suggest that non-convulsant
α5-selective GABA-A inverse agonists could improve learning and memory deficits
in DS individuals
Radiation therapy of anal canal carcinoma
La radio(chimio)thérapie correspond au traitement de référence des carcinomes épidermoïdes du canal anal localisés qui représentent la majorité des cas. Elle a pour objectif d’obtenir une stérilisation tumorale définitive tout en conservant un sphincter anal fonctionnel. Cet article a pour objectif de préciser les indications et les modalités de la radiothérapie pelvienne dans cette situation. Il sera également question des nouvelles modalités d’irradiation (Radiothérapie Conformationnelle avec Modulation d’Intensité ; Tomothérapie hélicoïdale et irradiation avec modulation d’intensité volumétrique par Arc thérapie) qui permettent à la fois une meilleure définition des volumes cibles et une meilleure protection des organes à risque (intestin grêle, recto-sigmoïde, vessie, organes génitaux notamment). Cette dernière réduit la toxicité induite, ce qui permet d’envisager une réduction de la durée totale du traitement (réduction de la durée de la pause thérapeutique entre les 2 séquences de radiothérapie, voire suppression de cette pause avec traitement continu). La réduction de la toxicité devrait également permettre d’augmenter la dose totale délivrée dans le volume cible. L’intérêt d’une telle stratégie mérite d’être évalué.Radio(chemo)therapy is the standard treatment of localized epidermoid carcinomas of the anal canal, which represent the majority of cases. The aim of treatment is to obtain tumor sterilization while preserving functional anal sphincter. This article concerns the indications and the modalities of radiotherapy in this situation, with special attention to the new available radiation techniques (conformational static field intensity modulated radiotherapy; helicoidal tomotherapy; volumetric modulated arc therapy). These developments mainly allow to reduce the dose to normal tissues and organs at risk thereby minimizing the risk of toxicity. The reduction of the induced morbidity should allow to shorten the classical 2 to 6 weeks gap period between the two sequences of radiotherapy and therefore the total duration of treatment. It also should allow dose escalation to the tumor volume potentially leading to improved locoregional control
Gene expression signature of cerebellar hypoplasia in a mouse model of Down syndrome during postnatal development
Background Down syndrome is a chromosomal disorder caused by the presence of three copies of chromosome 21. The mechanisms by which this aneuploidy produces the complex and variable phenotype observed in people with Down syndrome are still under discussion. Recent studies have demonstrated an increased transcript level of the three-copy genes with some dosage compensation or amplification for a subset of them. The impact of this gene dosage effect on the whole transcriptome is still debated and longitudinal studies assessing the variability among samples, tissues and developmental stages are needed. Results We thus designed a large scale gene expression study in mice (the Ts1Cje Down syndrome mouse model) in which we could measure the effects of trisomy 21 on a large number of samples (74 in total) in a tissue that is affected in Down syndrome (the cerebellum) and where we could quantify the defect during postnatal development in order to correlate gene expression changes to the phenotype observed. Statistical analysis of microarray data revealed a major gene dosage effect: for the three-copy genes as well as for a 2 Mb segment from mouse chromosome 12 that we show for the first time as being deleted in the Ts1Cje mice. This gene dosage effect impacts moderately on the expression of euploid genes (2.4 to 7.5% differentially expressed). Only 13 genes were significantly dysregulated in Ts1Cje mice at all four postnatal development stages studied from birth to 10 days after birth, and among them are 6 three-copy genes. The decrease in granule cell proliferation demonstrated in newborn Ts1Cje cerebellum was correlated with a major gene dosage effect on the transcriptome in dissected cerebellar external granule cell layer. Conclusion High throughput gene expression analysis in the cerebellum of a large number of samples of Ts1Cje and euploid mice has revealed a prevailing gene dosage effect on triplicated genes. Moreover using an enriched cell population that is thought responsible for the cerebellar hypoplasia in Down syndrome, a global destabilization of gene expression was not detected. Altogether these results strongly suggest that the three-copy genes are directly responsible for the phenotype present in cerebellum. We provide here a short list of candidate genes
The cerebellar transcriptome during postnatal development of the Ts1Cje mouse, a segmental trisomy model for Down syndrome
The central nervous system of persons with Down syndrome presents cytoarchitectural abnormalities that likely result from gene-dosage effects affecting the expression of key developmental genes. To test this hypothesis, we have investigated the transcriptome of the cerebellum of the Ts1Cje mouse model of Down syndrome during postnatal development using microarrays and quantitative PCR (qPCR). Genes present in three copies were consistently overexpressed, with a mean ratio relative to euploid of 1.52 as determined by qPCR. Out of 63 three-copy genes tested, only five, nine and seven genes had ratios >2 or <1.2 at postnatal days 0 (P0), P15 and P30, respectively. This gene-dosage effect was associated with a dysregulation of the expression of some two-copy genes. Out of 8258 genes examined, the Ts1Cje/euploid ratios differed significantly from 1.0 for 406 (80 and 154 with ratios above 1.5 and below 0.7, respectively), 333 (11 above 1.5 and 55 below 0.7) and 246 genes (59 above 1.5 and 69 below 0.7) at P0, P15 and P30, respectively. Among the two-copy genes differentially expressed in the trisomic cerebellum, six homeobox genes, two belonging to the Notch pathway, were severely repressed. Overall, at P0, transcripts involved in cell differentiation and development were over-represented among the dysregulated genes, suggesting that cell differentiation and migration might be more altered than cell proliferation. Finally, global gene profiling revealed that transcription in Ts1Cje mice is more affected by the developmental changes than by the trisomic state, and that there is no apparent detectable delay in the postnatal development of the cerebellum of Ts1Cje mic
International differences in self-reported health measures in 33 major metropolitan areas in Europe.
The increasing concentration of populations into large conurbations in recent decades has not been matched by international health assessments, which remain largely focused at the country level. We aimed to demonstrate the use of routine survey data to compare the health of large metropolitan centres across Europe and determine the extent to which differences are due to socio-economic factors
Apoptosis screening of human chromosome 21 proteins reveals novel cell death regulators
The functional analysis of chromosome 21 (Chr21) proteins is of great medical relevance. This refers, in particular, to the trisomy of human Chr21, which results in Down’s syndrome, a complex developmental and neurodegenerative disease. In a previous study we analyzed 89 human Chr21 genes for the subcellular localization of their encoded proteins using a transfected-cell array technique. In the present study, the results of the follow-up investigation are presented in which 52 human Chr21 genes were over-expressed in HEK cells using the transfected-cell array platform, and the effect of this protein over-expression on the induction of apoptosis has been analyzed. We found that the over-expression of two Chr21 proteins (claudin-14 and -8) induced cell death independent of the classic caspase-mediated apoptosis. Our results strongly suggest the functional involvement of claudins in the control of the cell cycle and regulation of the cell death induction mechanism
Modifications of the endosomal compartment in peripheral blood mononuclear cells and fibroblasts from Alzheimer’s disease patients
International audienceIdentification of blood-based biomarkers of Alzheimer’s disease (AD) remains a challenge. Neuropathological studies have identified enlarged endosomes in post-mortem brains as the earliest cellular change associated to AD. Here the presence of enlarged endosomes was investigated in peripheral blood mononuclear cells from 48 biologically defined AD patients (25 with mild cognitive impairment and 23 with dementia (AD-D)), and 23 age-matched healthy controls using immunocytochemistry and confocal microscopy. The volume and number of endosomes were not significantly different between AD and controls. However, the percentage of cells containing enlarged endosomes was significantly higher in the AD-D group as compared with controls. Furthermore, endosomal volumes significantly correlated to [C11]PiB cortical index measured by positron emission tomography in the AD group, independently of the APOE genotype, but not to the levels of amyloid-beta, tau and phosphorylated tau measured in the cerebrospinal fluid. Importantly, we confirmed the presence of enlarged endosomes in fibroblasts from six unrelated AD-D patients as compared with five cognitively normal controls. This study is the first, to our knowledge, to report morphological alterations of the endosomal compartment in peripheral cells from AD patients correlated to amyloid load that will now be evaluated as a possible biomarker
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