168 research outputs found
Spectral ergodicity and normal modes in ensembles of sparse matrices
We investigate the properties of sparse matrix ensembles with particular
regard for the spectral ergodicity hypothesis, which claims the identity of
ensemble and spectral averages of spectral correlators. An apparent violation
of the spectral ergodicity is observed. This effect is studied with the aid of
the normal modes of the random matrix spectrum, which describe fluctuations of
the eigenvalues around their average positions. This analysis reveals that
spectral ergodicity is not broken, but that different energy scales of the
spectra are examined by the two averaging techniques. Normal modes are shown to
provide a useful complement to traditional spectral analysis with possible
applications to a wide range of physical systems.Comment: 22 pages, 15 figure
The Intrinsic Quantum Excitations of Low Temperature Glasses
Several puzzling regularities concerning the low temperature excitations of
glasses are quantitatively explained by quantizing domain wall motions of the
random first order glass transition theory. The density of excitations agrees
with experiment and scales with the size of a dynamically coherent region at
, being about 200 molecules. The phonon coupling depends on the Lindemann
ratio for vitrification yielding the observed universal relation between phonon wavelength and mean free path .
Multilevel behavior is predicted to occur in the temperature range of the
thermal conductivity plateau.Comment: 4 pages, submitted to PR
Modeling neurocognitive and neurobiological recovery in addiction
This book focuses on "what to know" and "how to apply" information, prioritizing novel principles and delineating cutting-edge assessment, phenotyping and treatment tools
Flux Pinning and Phase Transitions in Model High-Temperature Superconductors with Columnar Defects
We calculate the degree of flux pinning by defects in model high-temperature
superconductors (HTSC's). The HTSC is modeled as a three-dimensional network of
resistively-shunted Josephson junctions in an external magnetic field,
corresponding to a HTSC in the extreme Type-II limit. Disorder is introduced
either by randomizing the coupling between grains (Model A disorder) or by
removing grains (Model B disorder). Three types of defects are considered:
point disorder, random line disorder, and periodic line disorder; but the
emphasis is on random line disorder. Static and dynamic properties of the
models are determined by Monte Carlo simulations and by solution of the
analogous coupled overdamped Josephson equations in the presence of thermal
noise. Random line defects considerably raise the superconducting transition
temperature T, and increase the apparent critical current density
J, in comparison to the defect-free crystal. They are more effective
in these respects than a comparable volume density of point defects, in
agreement with the experiments of Civale {\it et al}. Periodic line defects
commensurate with the flux lattice are found to raise T even more than
do random line defects. Random line defects are most effective when their
density approximately equals the flux density. Near T, our static and
dynamic results appear consistent with the anisotropic Bose glass scaling
hypotheses of Nelson and Vinokur, but with possibly different critical indices:Comment: 10 pages, LaTeX(REVTeX v3.0, twocolumn), 11 figures (not included
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Gaze-grasp coordination in obstacle avoidance: differences between binocular and monocular viewing
Most adults can skillfully avoid potential obstacles when acting in everyday cluttered scenes. We examined how gaze and hand movements are normally coordinated for obstacle avoidance and whether these are altered when binocular depth information is unavailable. Visual fixations and hand movement kinematics were simultaneously recorded, while 13 right-handed subjects reached-to-precision grasp a cylindrical household object presented alone or with a potential obstacle (wine glass) located to its left (thumb's grasp side), right or just behind it (both closer to the finger's grasp side) using binocular or monocular vision. Gaze and hand movement strategies differed significantly by view and obstacle location. With binocular vision, initial fixations were near the target's centre of mass (COM) around the time of hand movement onset, but usually shifted to end just above the thumb's grasp site at initial object contact, this mainly being made by the thumb, consistent with selecting this digit for guiding the grasp. This strategy was associated with faster binocular hand movements and improved end-point grip precision across all trials than with monocular viewing, during which subjects usually continued to fixate the target closer to its COM despite a similar prevalence of thumb-first contacts. While subjects looked directly at the obstacle at each location on a minority of trials and their overall fixations on the target were somewhat biased towards the grasp side nearest to it, these gaze behaviours were particularly marked on monocular vision-obstacle behind trials which also commonly ended in finger-first contact. Subjects avoided colliding with the wine glass under both views when on the right (finger side) of the workspace by producing slower and straighter reaches, with this and the behind obstacle location also resulting in 'safer' (i.e. narrower) peak grip apertures and longer deceleration times than when the goal object was alone or the obstacle was on its thumb side. But monocular reach paths were more variable and deceleration times were selectively prolonged on finger-side and behind obstacle trials, with this latter condition further resulting in selectively increased grip closure times and corrections. Binocular vision thus provided added advantages for collision avoidance, known to require intact dorsal cortical stream processing mechanisms, particularly when the target of the grasp and potential obstacle to it were fairly closely separated in depth. Different accounts of the altered monocular gaze behaviour converged on the conclusion that additional perceptual and/or attentional resources are likely engaged compared to when continuous binocular depth information is available. Implications for people lacking binocular stereopsis are briefly considered
Random Matrix Theories in Quantum Physics: Common Concepts
We review the development of random-matrix theory (RMT) during the last
decade. We emphasize both the theoretical aspects, and the application of the
theory to a number of fields. These comprise chaotic and disordered systems,
the localization problem, many-body quantum systems, the Calogero-Sutherland
model, chiral symmetry breaking in QCD, and quantum gravity in two dimensions.
The review is preceded by a brief historical survey of the developments of RMT
and of localization theory since their inception. We emphasize the concepts
common to the above-mentioned fields as well as the great diversity of RMT. In
view of the universality of RMT, we suggest that the current development
signals the emergence of a new "statistical mechanics": Stochasticity and
general symmetry requirements lead to universal laws not based on dynamical
principles.Comment: 178 pages, Revtex, 45 figures, submitted to Physics Report
Impaired peripheral reaching and on-line corrections in patient DF: optic ataxia with visual form agnosia
An influential model of vision suggests the presence of two visual streams within the brain: a dorsal occipito-parietal stream which mediates action and a ventral occipito-temporal stream which mediates perception. One of the cornerstones of this model is DF, a patient with visual form agnosia following bilateral ventral stream lesions. Despite her inability to identify and distinguish visual stimuli, DF can still use visual information to control her hand actions towards these stimuli. These observations have been widely interpreted as demonstrating a double dissociation from optic ataxia, a condition observed after bilateral dorsal stream damage in which patients are unable to act towards objects that they can recognize. In Experiment 1, we investigated how patient DF performed on the classical diagnostic task for optic ataxia, reaching in central and peripheral vision. We replicated recent findings that DF is remarkably inaccurate when reaching to peripheral targets, but not when reaching in free vision. In addition we present new evidence that her peripheral reaching errors follow the optic ataxia pattern increasing with target eccentricity and being biased towards fixation. In Experiments 2 and 3, for the first time we examined DF’s on-line control of reaching using a double-step paradigm in fixation-controlled and free-vision versions of the task. DF was impaired when performing fast on-line corrections on all conditions tested, similarly to optic ataxia patients. Our findings question the long-standing assumption that DF’s dorsal visual stream is functionally intact and that her on-line visuomotor control is spared. In contrast, in addition to visual form agnosia, DF also has visuomotor symptoms of optic ataxia which are most likely explained by bilateral damage to the superior parietal occipital cortex. We thus conclude that patient DF can no longer be considered as an appropriate single-case model for testing the neural basis of perception and action dissociations
Grasping isoluminant stimuli
We used a virtual reality setup to let participants grasp discs, which differed in luminance, chromaticity and size. Current theories on perception and action propose a division of labor in the brain into a color proficient perception pathway and a less color-capable action pathway. In this study, we addressed the question whether isoluminant stimuli, which provide only a chromatic but no luminance contrast for action planning, are harder to grasp than stimuli providing luminance contrast or both kinds of contrast. Although we found that grasps of isoluminant stimuli had a slightly steeper slope relating the maximum grip aperture to disc size, all other measures of grip quality were unaffected. Overall, our results do not support the view that isoluminance of stimulus and background impedes the planning of a grasping movement
Genetic and behavioral determinants of hippocampal volume recovery during abstinence from alcohol
Alcohol-dependent individuals (ALC) have smaller hippocampi and poorer neurocognition than healthy controls. Results from studies on the association between alcohol consumption and hippocampal volume have been mixed, suggesting that comorbid or premorbid factors (i.e., those present prior to the initiation of alcohol dependence) determine hippocampal volume in ALC. We aimed to characterize the effects of select comorbid (i.e., cigarette smoking) and premorbid factors (brain-derived neurotrophic factor [BDNF] genotype [Val66Met rs6265]) on hippocampal volume in an ALC cohort followed longitudinally into extended abstinence. One hundred twenty-one adult ALC in treatment (76 smokers, 45 non-smokers) and 35 non-smoking light-drinking controls underwent quantitative magnetic resonance imaging, BDNF genotyping, and neurocognitive assessments. Representative subgroups were studied at 1 week, 1 month, and at an average of 7 months of abstinence. ALC had smaller hippocampi than healthy controls at all time points. Hippocampal volume at 1 month of abstinence correlated with lower visuospatial function. Smoking status did not influence hippocampal volume or hippocampal volume recovery during abstinence. However, only BDNF Val homozygotes tended to have hippocampal volume increases over 7 months of abstinence, and Val homozygotes had significantly larger hippocampi than Met carriers at 7 months of abstinence. These findings suggest that BDNF genotype, but not smoking status or measures of drinking severity, regulate functionally relevant hippocampal volume recovery in abstinent ALC. Future studies aimed at exploring genetic determinants of brain morphometry in ALC may need to evaluate individuals during extended abstinence after the acute environmental effects of chronic alcohol consumption have waned
ENIGMA-anxiety working group : Rationale for and organization of large-scale neuroimaging studies of anxiety disorders
Altres ajuts: Anxiety Disorders Research Network European College of Neuropsychopharmacology; Claude Leon Postdoctoral Fellowship; Deutsche Forschungsgemeinschaft (DFG, German Research Foundation, 44541416-TRR58); EU7th Frame Work Marie Curie Actions International Staff Exchange Scheme grant 'European and South African Research Network in Anxiety Disorders' (EUSARNAD); Geestkracht programme of the Netherlands Organization for Health Research and Development (ZonMw, 10-000-1002); Intramural Research Training Award (IRTA) program within the National Institute of Mental Health under the Intramural Research Program (NIMH-IRP, MH002781); National Institute of Mental Health under the Intramural Research Program (NIMH-IRP, ZIA-MH-002782); SA Medical Research Council; U.S. National Institutes of Health grants (P01 AG026572, P01 AG055367, P41 EB015922, R01 AG060610, R56 AG058854, RF1 AG051710, U54 EB020403).Anxiety disorders are highly prevalent and disabling but seem particularly tractable to investigation with translational neuroscience methodologies. Neuroimaging has informed our understanding of the neurobiology of anxiety disorders, but research has been limited by small sample sizes and low statistical power, as well as heterogenous imaging methodology. The ENIGMA-Anxiety Working Group has brought together researchers from around the world, in a harmonized and coordinated effort to address these challenges and generate more robust and reproducible findings. This paper elaborates on the concepts and methods informing the work of the working group to date, and describes the initial approach of the four subgroups studying generalized anxiety disorder, panic disorder, social anxiety disorder, and specific phobia. At present, the ENIGMA-Anxiety database contains information about more than 100 unique samples, from 16 countries and 59 institutes. Future directions include examining additional imaging modalities, integrating imaging and genetic data, and collaborating with other ENIGMA working groups. The ENIGMA consortium creates synergy at the intersection of global mental health and clinical neuroscience, and the ENIGMA-Anxiety Working Group extends the promise of this approach to neuroimaging research on anxiety disorders
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