67 research outputs found

    MĂ©canismes molĂ©culaires impliquĂ©s dans la rĂ©gulation de l’acide polysialique (PSA) dans le nĂ©ocortex visuel des souris durant la maturation des synapses GABAergiques

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    Le fonctionnement du cortex cĂ©rĂ©bral nĂ©cessite l’action coordonnĂ©e de deux des sous-types majeurs de neurones, soient les neurones Ă  projections glutamatergiques et les interneurones GABAergiques. Les interneurones GABAergiques ne constituent que 20 Ă  30% des cellules corticales par rapport au grand nombre de neurones glutamatergiques. Leur rĂŽle est toutefois prĂ©pondĂ©rant puisqu’ils modulent fortement la dynamique et la plasticitĂ© des rĂ©seaux nĂ©ocorticaux. Il n’est donc pas surprenant que les altĂ©rations de dĂ©veloppement des circuits GABAergiques soient associĂ©es Ă  plusieurs maladies du cerveau, incluant l’épilepsie, le syndrome de Rett et la schizophrĂ©nie. La comprĂ©hension des mĂ©canismes molĂ©culaires rĂ©gissant le dĂ©veloppement des circuits GABAergiques est une Ă©tape essentielle menant vers une meilleure comprĂ©hension de la façon dont les anormalitĂ©s se produisent. ConsĂ©quemment, nous nous intĂ©ressons au rĂŽle de l’acide polysialique (PSA) dans le dĂ©veloppement des synapses GABAergiques. PSA est un homopolymĂšre de chaĂźnons polysialylĂ©s en α-2,8, et est exclusivement liĂ© Ă  la molĂ©cule d’adhĂ©sion aux cellules neuronales (NCAM) dans les cerveaux de mammifĂšres. PSA est impliquĂ© dans plusieurs processus dĂ©veloppementaux, y compris la formation et la plasticitĂ© des synapses glutamatergiques, mais son rĂŽle dans les rĂ©seaux GABAergiques reste Ă  prĂ©ciser. Les donnĂ©es gĂ©nĂ©rĂ©es dans le laboratoire du Dr. Di Cristo dĂ©montrent que PSA est fortement exprimĂ© post- natalement dans le nĂ©ocortex des rongeurs, que son abondance diminue au cours du dĂ©veloppement, et, faits importants, que son expression dĂ©pend de l’activitĂ© visuelle i et est inversement corrĂ©lĂ©e Ă  la maturation des synapses GABAergiques. La prĂ©sente propose de caractĂ©riser les mĂ©canismes molĂ©culaires rĂ©gulant l’expression de PSA dans le nĂ©ocortex visuel de la souris. Les enzymes polysialyltransfĂ©rases ST8SiaII (STX) et ST8SiaIV (PST) sont responsables de la formation de la chaĂźne de PSA sur NCAM. En contrĂŽlant ainsi la quantitĂ© de PSA sur NCAM, ils influenceraient le dĂ©veloppement des synapses GABAergiques. Mon projet consiste Ă  dĂ©terminer comment l’expression des polysialyltransfĂ©rases est rĂ©gulĂ©e dans le nĂ©ocortex visuel des souris durant la pĂ©riode post-natale; ces donnĂ©es sont Ă  la fois inconnues, et cruciales. Nous utilisons un systĂšme de cultures organotypiques dont la maturation des synapses GABAergiques est comparable au modĂšle in vivo. L’analyse de l’expression gĂ©nique par qPCR a dĂ©montrĂ© que l’expression des polysialyltransfĂ©rases diminue au cours du dĂ©veloppement; une baisse majeure corrĂ©lant avec l’ouverture des yeux chez la souris. Nous avons de plus illustrĂ© pour la premiĂšre fois que l’expression de STX, et non celle de PST, est activitĂ©-dĂ©pendante, et que ce processus requiert l’activation du rĂ©cepteur NMDA, une augmentation du niveau de calcium intracellulaire et la protĂ©ine kinase C (PKC). Ces donnĂ©es dĂ©montrent que STX est l’enzyme rĂ©gulant prĂ©fĂ©rentiellement le niveau de PSA sur NCAM au cours de la pĂ©riode post-natale dans le cortex visuel des souris. Des donnĂ©es prĂ©liminaires d’un second volet de notre investigation suggĂšrent que l’acĂ©tylation des histones et la mĂ©thylation de l’ADN pourraient Ă©galement contribuer Ă  la rĂ©gulation de la transcription de cette enzyme durant le dĂ©veloppement. Plus d’investigations seront toutefois nĂ©cessaires afin de confirmer cette hypothĂšse. En somme, la connaissance des mĂ©canismes par lesquels l’expression des ii polysialyltransfĂ©rases est modulĂ©e est essentielle Ă  la comprĂ©hension du processus de maturation des synapses GABAergiques. Ceci permettrait de moduler pharmacologiquement l’expression de ces enzymes; la sur-expression de STX et/ou PST pourrait produire une plus grande quantitĂ© de PSA, dĂ©stabiliser les synapses GABAergiques, et consĂ©quemment, rĂ©-induire la plasticitĂ© cĂ©rĂ©brale.The functioning of the cerebral cortex requires coordinated action of two major neuronal subtypes - the glutamatergic projection neurons and the GABAergic interneurons. GABAergic interneurons represent 20 to 30% of all cortical cells. Even though they are a minor cell population in the cerebral cortex compared to glutamatergic neurons, they are key modulators of network dynamics and plasticity of neocortical circuits. It is therefore not surprising that aberrant development of GABAergic circuits is implicated in many neurodevelopmental disorders including epilepsy, Rett syndrome and schizophrenia. Understanding the molecular mechanisms governing the development of GABAergic inhibitory synapses in neocortex is important towards a better comprehension of how abnormalities in this developmental process can occur. Therefore, we focus specifically on the role of polysialic acid (PSA) in the development of GABAergic synapses. PSA is a α-2,8 polysialylated homopolymer, which is exclusively linked to the Neural Cell Adhesion Molecule (NCAM) in the mammalian brain. It is involved in several developmental processes including formation and plasticity of glutamatergic synapses; however its role in GABAergic circuit formation has not been explored so far. Previously in Dr Di Cristo’s lab, we showed that PSA is strongly expressed post-natally and its expression steadily declines during development in mice neocortex. We also showed that the developmental and activity-dependant regulation of PSA expression is inversely correlated with the maturation of perisomatic GABAergic innervation. Our aim is to characterize the molecular mechanisms regulating PSA expression in mouse iv visual cortex during post-natal development. Two polysialyltransferases, ST8SiaII (STX) and ST8SiaIV (PST), are responsible for PSA attachment to NCAM. By controlling the amount of PSA on NCAM, they can influence GABAergic synapses development. The mechanisms regulating STX and PST expression is crucial but remain still unknown. My research project focused on the mechanisms regulating STX and PST transcription in the mouse postnatal cortex. We used an organotypic culture system, which recapitulates many aspects of GABAergic synapse maturation as observed in vivo. Polysialyltransferases transcript levels were measured by qPCR and showed that STX and PST mRNA levels steadily decline during post-natal development in the mouse cortex; the sharpest reduction in the expression of both enzymes correlate with eye opening. We further demonstrate for the first time that STX mRNA levels is activity-dependant, requires the activation of NMDA receptors, an increase in intracellular Calcium levels and is PKC-dependent. Altogether, we show that the regulation of the expression of STX is the main mechanism responsible for PSA expression levels in the cortex around eyes opening. We next investigated whether epigenetic mechanisms regulate STX transcription and preliminary data suggest that histone acetylation and DNA methylation may contribute to STX expression during development. However, further experiments are required to confirm this hypothesis. In summary, understanding the mechanisms modulating STX and PST expression in the neocortex is essential for the comprehension of their precise role in GABAergic synapse maturation. This knowledge could allow us to modulate pharmacologically the expression of these enzymes; in turn overexpression of STX and PST may re-induce PSA expression, thereby destabilizing GABAergic synapses, and ultimately facilitating cortical plasticity in the adult

    Comparison of peak flow velocity through the left ventricular outflow tract and effective orifice area indexed to body surface area in Golden Retriever puppies to predict development of subaortic stenosis in adult dogs.

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    Objective — To evaluate the usefulness of Doppler-derived peak flow velocity through the left ventricular outflow tract (LVOT Vmax) and effective orifice area indexed to body surface area (EOAi) in puppies to predict development of subaortic stenosis (SAS) in the same dogs as adults. Design — Prospective, longitudinal, observational study. Animals — 38 Golden Retrievers. Procedures — Cardiac auscultation and echocardiography were performed on 2- to 6-monthold puppies, then repeated at 12 to 18 months. Subaortic stenosis was diagnosed when LVOT Vmax was = 2.3 m/s in adult dogs with left basilar systolic murmurs. Results—All puppies with EOAi < 1.46 cm2/m2 had SAS as adults. All adults with EOAi <1.29 cm2/m2 had SAS. An LVOT Vmax > 2.3 m/s in puppyhood was 63% sensitive and 100% specific for SAS in adulthood. In puppies, LVOT Vmax was more strongly associated with a future diagnosis of SAS (area under the curve [AUC], 0.89) than was EOAi (AUC, 0.80). In puppies, the combination of LVOT Vmax and EOAi yielded slightly higher sensitivity (69%) and specificity (100%) for adult SAS than did LVOT Vmax alone. In unaffected and affected dogs, LVOT Vmax increased significantly from puppyhood to adulthood but EOAi did not. Conclusions and Clinical Relevance — In Golden Retriever puppies, LVOT Vmax > 2.3 m/s and EOAi < 1.46 cm2/m2 were both associated with a diagnosis of SAS at adulthood. The combination of these 2 criteria may result in higher sensitivity for SAS screening. Unlike LVOT Vmax, EOAi did not change during growth in either unaffected Golden Retrievers or those with SAS. (J Am Vet Med Assoc 2014;245:1367–1374

    The effect of mere-measurement of cognitions on physical activity behavior: a randomized controlled trial among overweight and obese individuals

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    <p>Abstract</p> <p>Background</p> <p>The promotion of physical activity among an overweight/obese population is an important challenge for clinical practitioners and researchers. In this regard, completing a questionnaire on cognitions could be a simple and easy strategy to increase levels of physical activity. Thus, the aim of the present study was to test the effect of completing a questionnaire based on the Theory of Planned Behavior (TPB) on the level of physical activity.</p> <p>Methods</p> <p>Overall, 452 overweight/obese adults were recruited and randomized to the experimental or control group. At baseline, participants completed a questionnaire on cognitions regarding their participation in leisure-time physical activity (experimental condition) versus a questionnaire on fruit and vegetable consumption (control condition). The questionnaires assessed the TPB variables that are beliefs, attitude, norm, perception of control, intention and a few additional variables from other theories. At three-month follow-up, leisure-time physical activity was self-reported by means of a short questionnaire. An analysis of covariance with baseline physical activity level as covariate was used to verify the effect of the intervention.</p> <p>Results</p> <p>At follow-up, 373 participants completed the leisure-time physical activity questionnaire. The statistical analysis showed that physical activity participation was greater among participants in the experimental condition than those in the control condition (<it>F</it>(1,370) = 6.85, <it>p </it>= .009, <it>d </it>= 0.20).</p> <p>Conclusions</p> <p>Findings indicate that completing a TPB questionnaire has a significant positive impact on subsequent participation in physical activity. Consequently, asking individuals to complete such a questionnaire is a simple, inexpensive and easy strategy to increase the level of physical activity among overweight/obese adults.</p

    The Role of Expectations in Treatment Outcome and Symptom Development in Anxiety Disorders

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    For more than 60 years, researchers have been interested in determining the impact of expectations on treatment outcome. Earlier studies mostly focused on two types of expectations: prognostic and process expectations. Aims: To review how four different types of expectations (prognostic, process, anxiety expectancy and anxiety sensitivity) contribute to psychotherapy outcome, and to the development of clinical disorders, especially anxiety. Conclusions: First, the role of process and prognostic expectancies in clinical disorders and psychotherapy outcome should be clarified by addressing the methodological flaws of the earlier expectancy studies. Second, studies, especially those on anxiety disorders, may benefit from evaluating the four different types of expectations to determine their relative impact on outcome, and on the development and maintenance of these disorders. Third, possible links with other clinical disorders should be further explored. Finally, expectancies should be assessed prior to treatment and after several sessions to determine the extent to which the treatment\u27s failure in modifying initial low expectancies contribute to a poor outcome

    Priority interventions to improve the management of chronic non-cancer pain in primary care: a participatory research of the ACCORD program

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    Purpose: There is evidence that the management of chronic non-cancer pain (CNCP) in primary care is far from being optimal. A 1-day workshop was held to explore the perceptions of key actors regarding the challenges and priority interventions to improve CNCP management in primary care. Methods: Using the Chronic Care Model as a conceptual framework, physicians (n=6), pharmacists (n=6), nurses (n=6), physiotherapists (n=6), psychologists (n=6), pain specialists (n=6), patients (n=3), family members (n=3), decision makers and managers (n=4), and pain researchers (n=7) took part in seven focus groups and five nominal groups. Results: Challenges identified in focus group discussions were related to five dimensions: knowledge gap, “work in silos”, lack of awareness that CNCP represents an important clinical problem, difficulties in access to health professionals and services, and patient empowerment needs. Based on the nominal group discussions, the following priority interventions were identified: interdisciplinary continuing education, interdisciplinary treatment approach, regional expert leadership, creation and definition of care paths, and patient education programs. Conclusion: Barriers to optimal management of CNCP in primary care are numerous. Improving its management cannot be envisioned without considering multifaceted interventions targeting several dimensions of the Chronic Care Model and focusing on both clinicians and patients

    Clinical correlates identify ProBDNF and thrombo-inflammatory markers as key predictors of circulating p75NTR extracellular domain levels in older adults

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    The p75NTR receptor binds all neurotrophins and is mostly known for its role in neuronal survival and apoptosis. Recently, the extracellular domain (ECD) of p75NTR has been reported in plasma, its levels being dysregulated in numerous neurological diseases. However, the factors associated with p75NTR ECD levels remain unknown. We investigated clinical correlates of plasma p75NTR ECD levels in older adults without clinically manifested neurological disorders. Circulating p75NTR levels were measured by enzyme-linked immunosorbent assay in plasma obtained from participants in the BEL-AGE cohort (n = 1,280). Determinants of plasma p75NTR ECD levels were explored using linear and non-linear statistical models. Plasma p75NTR ECD levels were higher in male participants; were positively correlated with circulating concentrations of pro-brain-derived neurotrophic factor, and inflammatory markers interleukin-6 and CD40 Ligand; and were negatively correlated with the platelet activation marker P-selectin. While most individuals had p75NTR levels ranging from 43 to 358 pg/ml, high p75NTR levels reaching up to 9,000 pg/ml were detectable in a subgroup representing 15% of the individuals studied. In this cohort of older adults without clinically manifested neurological disorders, there was no association between plasma p75NTR ECD levels and cognitive performance, as assessed by the Montreal Cognitive Assessment score. The physiological relevance of high p75NTR ECD levels in plasma warrants further investigation. Further research assessing the source of circulating p75NTR is needed for a deeper understanding of the direction of effect, and to investigate whether high p75NTR ECD levels are predictive biomarkers or consequences of neuropathology

    Social support, but not perceived food environment, is associated with diet quality in French-speaking Canadians from the PREDISE study

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    The objectives were to assess whether social support for healthy eating and perceived food environment are associated with diet quality, and to investigate if sociodemographic characteristics moderate these associations. A probability sample of French-speaking adults from the Province of QuĂ©bec, Canada, was recruited in the context of the PREDISE study. Participants reported their perceptions of supportive and non-supportive actions related to healthy eating from close others at home and outside of home (n = 952), and of the accessibility to healthy foods (n = 1035). The Canadian Healthy Eating Index (C-HEI) was calculated based on three Web-based 24 h food recalls. Multiple linear regression models showed that supportive (B = 1.50 (95% CI 0.46, 2.54)) and non-supportive (B = −3.06 (95% CI −4.94, −1.18)) actions related to healthy eating from close others at home were positively and negatively associated with C-HEI, respectively, whereas actions from close others outside of home were not. The negative association between non-supportive actions occurring at home and C-HEI was stronger among participants with lower (vs. higher) levels of education (p interaction = 0.03). Perceived accessibility to healthy foods was not associated with C-HEI (p > 0.05). These results suggest that the social environment may have a stronger influence on healthy eating than the perceived physical environment. This adds support for healthy eating promotion programs involving entire families, especially for more socioeconomically disadvantaged individuals, whose efforts to eat healthily may be more easily thwarted by non-supportive household

    Approaches to considering sex and gender in continuous professional development for health and social care professionals : an emerging paradigm

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    Consideration of sex and gender in research and clinical practice is necessary to redress health inequities and reduce knowledge gaps. As all health professionals must maintain and update their skills throughout their career, developing innovative continuing professional education programs that integrate sex and gender issues holds great promise for reducing these gaps. This article proposes new approaches to partnership, team development, pedagogical theory, content development, evaluation and data management that will advance the integration of sex and gender in continuing professional development (CPD). Our perspectives build on an intersectoral and interprofessional research team that includes several perspectives, including those of CPD, health systems, knowledge translation and sex and gender

    Sensory Experience Differentially Modulates the mRNA Expression of the Polysialyltransferases ST8SiaII and ST8SiaIV in Postnatal Mouse Visual Cortex

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    Polysialic acid (PSA) is a unique carbohydrate composed of a linear homopolymer of α-2,8 linked sialic acid, and is mainly attached to the fifth immunoglobulin-like domain of the neural cell adhesion molecule (NCAM) in vertebrate neural system. In the brain, PSA is exclusively synthesized by the two polysialyltransferases ST8SiaII (also known as STX) and ST8SiaIV (also known as PST). By modulating adhesive property of NCAM, PSA plays a critical role in several neural development processes such as cell migration, neurite outgrowth, axon pathfinding, synaptogenesis and activity-dependent plasticity. The expression of PSA is temporally and spatially regulated during neural development and a tight regulation of PSA expression is essential to its biological function. In mouse visual cortex, PSA is downregulated following eye opening and its decrease allows the maturation of GABAergic synapses and the opening of the critical period for ocular dominance plasticity. Relatively little is known about how PSA levels are regulated by sensory experience and neuronal activity. Here, we demonstrate that while both ST8SiaII and ST8SiaIV mRNA levels decrease around the time of eye opening in mouse visual cortex, only ST8SiaII mRNA level reduction is regulated by sensory experience. Using an organotypic culture system from mouse visual cortex, we further show that ST8SiaII gene expression is regulated by spiking activity and NMDA-mediated excitation. Further, we show that both ST8SiaII and ST8SiaIV mRNA levels are positively regulated by PKC-mediated signaling. Therefore, sensory experience-dependent ST8SiaII gene expression regulates PSA levels in postnatal visual cortex, thus acting as molecular link between visual activity and PSA expression
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