1,053 research outputs found

    Multisensory Stimulation in Stroke Rehabilitation

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    The brain has a large capacity for automatic simultaneous processing and integration of sensory information. Combining information from different sensory modalities facilitates our ability to detect, discriminate, and recognize sensory stimuli, and learning is often optimal in a multisensory environment. Currently used multisensory stimulation methods in stroke rehabilitation include motor imagery, action observation, training with a mirror or in a virtual environment, and various kinds of music therapy. Non-invasive brain stimulation has showed promising preliminary results in aphasia and neglect. Patient heterogeneity and the interaction of age, gender, genes, and environment are discussed. Randomized controlled longitudinal trials starting earlier post-stroke are needed. The advance in brain network science and neuroimaging enabling longitudinal studies of structural and functional networks are likely to have an important impact on patient selection for specific interventions in future stroke rehabilitation. It is proposed that we should pay more attention to age, gender, and laterality in clinical studies

    Methylphenidate-mediated motor control network enhancement in patients with traumatic brain injury.

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    PRIMARY OBJECTIVE: To investigate functional improvement late (>6 months) after traumatic brain injury (TBI). To this end, we conducted a double-blind, placebo-controlled experimental medicine study to test the hypothesis that a widely used cognitive enhancer would benefit patients with TBI. RESEARCH DESIGN: We focused on motor control function using a sequential finger opposition fMRI paradigm in both patients and age-matched controls. METHODS AND PROCEDURES: Patients' fMRI and DTI scans were obtained after randomised administration of methylphenidate or placebo. Controls were scanned without intervention. To assess differences in motor speed, we compared reaction times from the baseline condition of a sustained attention task. MAIN OUTCOMES AND RESULTS: Patients' reaction times correlated with wide-spread motor-related white matter abnormalities. Administration of methylphenidate resulted in faster reaction times in patients, which were not significantly different from those achieved by controls. This was also reflected in the fMRI findings in that patients on methylphenidate activated the left inferior frontal gyrus significantly more than when on placebo. Furthermore, stronger functional connections between pre-/post-central cortices and cerebellum were noted for patients on methylphenidate. CONCLUSIONS: Our findings suggest that residual functionality in patients with TBI may be enhanced by a single dose of methylphenidate.The study was funded by the Evelyn Trust- grant number 06/20. C.D. was funded by the Clinical Academic Research Awards organized by the East of England Multi Professional Deanery. B.J.S. consults for Cambridge Cognition, Otsuka, Servier and Lundbeck. She holds a grant from Janssen/J&J and has share options in Cambridge Cognition. D.K.M. is supported by the Neuroscience Theme of the NIHR Cambridge Biomedical Research Centre and NIHR Senior Investigator awards, and by Framework Program 7 funding from the European Commission (TBIcare). He has received lecture and consultancy fees and support for research from Glaxo SmithKline, Solvay and Linde. E.A.S. is funded by the Stephen Erskine Fellowship, Queens' College, Cambridge, UK

    How Does Working Memory Training Work? Transfer, Strategies, and Neural Correlates in Children Aged 9-14 Years

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    Working memory predicts children’s academic achievement at school and future prospects. Working memory training may offer generalised improvements; however, evidence has been mixed and is a source of controversial debate. Training has been shown to improve performance on working memory tasks, but it is unclear if this reflects increased capacity or a change in strategy. Training has been found to improve children’s attention, maths, and reading, but rarely in studies with appropriate control groups. Very few controlled studies have investigated the neural correlates of working memory training in children, obscuring inferences about neural mechanisms. Chapter 2 presents the most comprehensive investigation of the neural correlates of working memory training to date. Training is found to improve children’s working memory performance, increase recruitment of the middle frontal gyrus, and increase connectivity within the posterior parietal cortex, but not change grey matter volume. It is concluded that repeated coactivation of fronto-parietal regions during training may increase executive or attentional control. However, strategy change may influence task-related brain activation. Chapter 3 presents a randomised controlled trial of ‘MetaCogmed’, a novel working memory and metacognitive strategy training programme designed to facilitate transfer to academic outcomes. Working memory training alone is found to improve children’s performance on tasks of working memory and mathematical reasoning. However, only the improvements in working memory were maintained three months later. MetaCogmed did not improve academic outcomes more than working memory training alone. It is concluded that working memory training may improve children’s maths ability in the short-term when offered in addition to school, and that metacognitive training may require more time and activities to promote generalisation. Chapter 4 presents a novel neuroimaging investigation of memory strategies in children. Grouping is found to be associated with decreased recruitment of the left middle frontal gyrus and increased recruitment of the left premotor cortex. It is suggested that grouping may afford an organisational advantage and more efficient use of working memory capacity compared to sequential rehearsal

    Interventional programmes to improve cognition during healthy and pathological ageing: Cortical modulations and evidence for brain plasticity

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    Available online 06 March 2018A growing body of evidence suggests that healthy elderly individuals and patients with Alzheimer’s disease retain an important potential for neuroplasticity. This review summarizes studies investigating the modulation of neural activity and structural brain integrity in response to interventions involving cognitive training, physical exercise and non-invasive brain stimulation in healthy elderly and cognitively impaired subjects (including patients with mild cognitive impairment (MCI) and Alzheimer’s disease). Moreover, given the clinical relevance of neuroplasticity, we discuss how evidence for neuroplasticity can be inferred from the functional and structural brain changes observed after implementing these interventions. We emphasize that multimodal programmes, which combine several types of interventions, improve cognitive function to a greater extent than programmes that use a single interventional approach. We suggest specific methods for weighting the relative importance of cognitive training, physical exercise and non-invasive brain stimulation according to the functional and structural state of the brain of the targeted subject to maximize the cognitive improvements induced by multimodal programmes.This study was funded by the European Commission Marie-Skłodowska Curie Actions, Individual Fellowships; 655423-NIBSAD, Italian Ministry of HealthGR-2011-02349998, and Galician government (Postdoctoral Grants Plan I2C 2011-2015)

    Facilitatory stimulation of the pre-SMA in healthy aging has distinct effects on task-based activity and connectivity

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    Semantic cognition is central to communication and our understanding of the world. It is usually well preserved in healthy aging. However, semantic control processes, which guide semantic access and retrieval, decline with age. The present study explored the potential of intermittent theta burst stimulation (iTBS) to enhance semantic cognition in healthy middle-aged to older adults. Using an individualized stimulation approach, we applied iTBS to the pre-supplementary motor area (pre-SMA) and assessed task-specific effects on semantic judgments in functional neuroimaging. We found increased activation after effective relative to sham stimulation only for the semantic task in visual and dorsal attention networks. Further, iTBS increased functional connectivity in domain-general executive networks. Notably, stimulation-induced changes in activation and connectivity related differently to behavior: While increased activation of the parietal dorsal attention network was linked to poorer semantic performance, its enhanced coupling with the pre-SMA was associated with more efficient semantic processing. Our findings indicate differential effects of iTBS on activity and connectivity. We show that iTBS modulates networks in a task-dependent manner and generates remote network effects. Stimulating the pre-SMA was linked to more efficient but not better performance, indicating a role in domain-general semantic control processes distinct to domain-specific semantic control

    Exploring visual verbal working memory

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    Investigating the neural substrates of gambling disorder using multiple neuromodulation and neuroimaging approaches

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    Introduction : Le trouble du jeu de hasard et d'argent (GD) est caractérisé par un comportement de jeu inadapté qui interfère avec les activités personnelles ou professionnelles. Ce trouble psychiatrique est difficile à traiter avec les thérapies actuelles et les rechutes sont fréquentes. Les symptômes dépressifs et cognitifs (e.g., l'impulsivité), ainsi que le "craving" (désir intense de jouer) sont des facteurs prédictifs de rechutes. Une meilleure compréhension des substrats neuronaux et leurs significations cliniques pourraient mener au développement de nouveaux traitements. La stimulation transcrânienne à courant direct (tDCS) pourrait être l'un de ceux-ci car elle permet de cibler des circuits neuronaux spécifiques. De plus, la tDCS ciblant le cortex dorsolatéral préfrontal (DLPFC) pourrait améliorer les symptômes dépressifs et cognitifs et réduire le craving. Cependant, les effets précis de la tDCS sur la fonction cérébrale, ainsi que leurs significations cliniques, demeurent à être élucidés. Par ailleurs, étant donné que les patients avec GD présentent souvent des différences morphométriques par rapport aux individus en santé, il est possible de faire l'hypothèse que la morphométrie cérébrale influence les effets de la tDCS. Objectifs : Ce travail avait trois objectifs principaux. Le premier objectif était d'explorer s'il y avait des associations entre les substrats neuronaux et les symptômes cliniques et cognitifs. Le deuxième objectif était d'examiner les effets de la tDCS sur la fonction cérébrale. Le troisième objectif était d'explorer si la morphométrie du site de stimulation (DLPFC) pouvait influencer les effets de la tDCS sur les substrats neuronaux. Méthode : Nous avons réalisé quatre études différentes. Dans la première étude, nous avons mesuré la morphométrie cérébrale en utilisant l'imagerie par résonance magnétique (IRM) structurelle. Nous avons mesuré les corrélations entre la morphométrie et les symptômes cliniques (dépression, sévérité et durée du GD) et cognitifs (impulsivité). De plus, nous avons comparé la morphométrie des patients à celui d'une base de données normative (individus en santé) en contrôlant pour plusieurs facteurs comme l'âge. Dans la deuxième étude, nous avons mesuré la fonction cérébrale (connectivité fonctionnelle) des patients avec l'IRM fonctionnelle. Nous avons examiné s'il y avait des liens entre la connectivité fonctionnelle et les symptômes cognitifs (impulsivité et prise de risque) et cliniques (sévérité et durée du GD). Dans la troisième étude, nous avons étudié les effets de la tDCS sur la connectivité fonctionnelle et si la morphométrie du DLPFC pouvait influencer ces effets. Dernièrement, dans la quatrième étude, nous avons examiné si la morphométrie du DLPFC pouvait influencer les effets de la tDCS sur la neurochimie (avec la spectroscopie par résonance magnétique). Résultats : Nous avons démontré deux corrélations positives entre la superficie du cortex occipital et les symptômes dépressifs (étude I). Nous avons également mis en évidence une corrélation positive entre la connectivité fonctionnelle d'un réseau occipital et l'impulsivité (étude II). De plus, il y avait une corrélation positive entre la connectivité fonctionnelle de ce réseau et la sévérité du GD. Par ailleurs, il y avait des corrélations positives entre la connectivité fonctionnelle de l'opercule frontal droit et la prise de risque (étude II). En outre, la connectivité fonctionnelle d'un réseau cérébelleux était corrélée avec les symptômes dépressifs (étude II). Les patients avaient aussi plusieurs différences morphométriques par rapport aux individus en santé (cortex occipital, préfrontal, etc.). Nous avons démontré également que la tDCS appliquée sur le DLPFC a augmenté la connectivité fonctionnelle d'un réseau fronto-pariétal (étude III). Finalement, cette thèse a montré que la morphométrie du DLPFC influence les augmentations induites par la tDCS sur la connectivité fonctionnelle du réseau fronto-pariétal (étude III) et le niveau de GABA frontal (étude IV). Conclusions : Cette thèse démontre une importance clinique potentielle pour les régions occipitales, frontales et cérébelleuses, particulièrement pour les patients ayant des symptômes dépressifs ou cognitifs. De plus, elle montre que la tDCS peut renforcer le fonctionnement d'un réseau fronto-pariétal connu pour son rôle dans les fonctions exécutives. Il reste à déterminer si un plus grand nombre de sessions pourrait apporter des bénéfices cliniques additionnels afin d'aider les patients à résister le jeu. Finalement, les résultats de cette thèse suggèrent que la morphométrie des régions sous les électrodes pourrait aider à identifier les meilleurs candidats pour la tDCS et pourrait être considéré pour la sélection des cibles de stimulation.Introduction: Gambling disorder (GD) is characterised by maladaptive gambling behaviour that interferes with personal or professional activities. This psychiatric disorder is difficult to treat with currently available treatments and relapse rates are high. Several factors can predict relapse, including depressive and cognitive (e.g., impulsivity, risk taking) symptoms, in addition to craving (strong desire to gamble). A better understanding of neural substrates and their clinical significance could help develop new treatments. Transcranial direct current stimulation (tDCS) might be one of these since it can target specific neural circuits. In addition, tDCS targeting the dorsolateral prefrontal cortex (DLPFC) could improve depressive and cognitive symptoms as well as reduce craving. However, the precise effects of tDCS on brain function, as well as their clinical significance, remain to be elucidated. Furthermore, considering that patients with GD often display morphometric differences as compared to healthy individuals, it may be worth investigating whether brain morphometry influences the effects of tDCS. Objectives: This work had three main objectives. The first objective was to explore whether there were associations between neural substrates and clinical and cognitive symptoms. The second objective was to examine the effects of tDCS on brain function. The third objective was to explore whether morphometry of the stimulation site (DLPFC) influenced the effects of tDCS on neural substrates. Methods: We carried out four different studies. In the first study, we investigated brain morphometry using structural magnetic resonance imaging (MRI). We tested for correlations between morphometry and clinical symptoms (depression, GD severity, GD duration) and cognitive symptoms (impulsivity). In addition, we compared the morphometry of patients with GD to that of a normative database (healthy individuals) while controlling for several factors such as age. In a second study, we assessed brain function (functional connectivity) in patients with functional MRI (fMRI). We examined whether there were associations between brain function and cognitive symptoms (impulsivity and risk taking) as well as clinical symptoms (GD severity and duration). In the third study, we examined tDCS-induced effects on brain function and whether morphometry of the DLPFC influenced these effects. Lastly, in the fourth study, we examined whether DLPFC morphometry influenced tDCS-induced effects on neurochemistry (using magnetic resonance spectroscopy imaging). Results: Firstly, we found two positive correlations between surface area of the occipital cortex and depressive symptoms (study I). We also showed a positive correlation between functional connectivity of an occipital network and impulsivity (study II). In addition, there was a positive correlation between functional connectivity of this network and GD severity (study II). In addition, there were positive correlations between functional connectivity of the right frontal operculum and risk-taking (study II). Also, functional connectivity of a cerebellar network was positively correlated with depressive symptoms (study II). Moreover, patients with GD had several morphometric differences as compared to healthy individuals (occipital and prefrontal cortices, etc.). Furthermore, we observed that tDCS over the DLPFC increased functional connectivity of a fronto-parietal circuit during stimulation (study III). Lastly, this thesis indicated that DLPFC morphometry influenced tDCS-induced elevations on fronto-parietal functional connectivity (study III) and frontal GABA levels (study IV). Conclusions: This thesis suggests the potential clinical relevance of occipital, frontal, and cerebellar regions, particularly for those with depressive and cognitive symptoms. It also indicates that tDCS can strengthen the functioning of a fronto-parietal network known to be implicated in executive functions. It remains to be seen whether a greater number of tDCS sessions could lead to clinical benefits to help patients resist gambling. Finally, the results of this thesis suggest that morphometry of the regions under the electrodes might help predict better candidates for tDCS and could be considered to select stimulation targets

    Structural and functional neural correlates of a mind-body connection.

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    The human brain underlies the complex cognitive processes of the mind, however, this is dependent upon the physiological processes of the body in order to receive adequate energy, oxygen, and blood flow. Therefore, physical measurements such as body mass index (BMI) and indices of cognitive functioning, such as intelligence, may be related via common neural features. Current analyses assessed morphometric differences in cortical and subcortical grey matter regions, white matter structural integrity, and resting-state functional activation in order to determine what combinations of neural variables predict BMI and intelligence (Wechsler Abbreviated Scale of Intelligence; WASI) with the best degree of accuracy. Data for eighty-five subjects was obtained from the Nathan Kline Institute, in connection with the 1000 Functional Connectomes neuroimaging database. Behavioral results indicated a negative correlation between BMI and WASI scores. Neural analyses revealed that increased BMI predicted changes in a frontolimbic network comprised of the anterior cingulate cortex, amygdala, and uncinate fasciculus, as well as increased cortical surface area of the left fusiform gyrus. These results indicate a relationship of BMI with emotional decision-making and visual recognition processes. Whereas, increased WASI scores predicted increased thickness and volume of prefrontal and parietal cortices, which reflect brain regions involved in the fronto-parietal attentional network. As well, increased WASI scores also related to a functional network that included increased activation of the postcentral gyrus and posterior hippocampal complex, regions involved with attention and memory. Taken together, these results indicate that BMI and intelligence are behaviorally anticorrelated, yet mediated by separate neuroanatomical substrates that associate with a variety of cognitive functioning measures
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