1,061 research outputs found
The role of environmental feedback in a brain state switch from passive to active sensing
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The cortical states of wakefulness
Cortical neurons process information on a background of spontaneous, ongoing activity with distinct spatiotemporal profiles defining different cortical states. During wakefulness, cortical states alter constantly in relation to behavioral context, attentional level or general motor activity. In this review article, we will discuss our current understanding of cortical states in awake rodents, how they are controlled, their impact on sensory processing, and highlight areas for future research. A common observation in awake rodents is the rapid change in spontaneous cortical activity from high-amplitude, low-frequency (LF) fluctuations, when animals are quiet, to faster and smaller fluctuations when animals are active. This transition is typically thought of as a change in global brain state but recent work has shown variation in cortical states across regions, indicating the presence of a fine spatial scale control system. In sensory areas, the cortical state change is mediated by at least two convergent inputs, one from the thalamus and the other from cholinergic inputs in the basal forebrain. Cortical states have a major impact on the balance of activity between specific subtypes of neurons, on the synchronization between nearby neurons, as well as the functional coupling between distant cortical areas. This reorganization of the activity of cortical networks strongly affects sensory processing. Thus cortical states provide a dynamic control system for the moment-by-moment regulation of cortical processing
Theory of rigid-plane phonon modes in layered crystals
The lattice dynamics of low-frequency rigid-plane modes in metallic (graphene
multilayers, GML) and in insulating (hexagonal boron-nitride multilayers, BNML)
layered crystals is investigated. The frequencies of shearing and compression
(stretching) modes depend on the layer number {\EuScript N} and are presented
in the form of fan diagrams. The results for GML and BNML are very similar. In
both cases only the interactions (van der Waals and Coulomb) between
nearest-neighbor planes are effective, while the interactions between more
distant planes are screened. A comparison with recent Raman scattering results
on low-frequency shear modes in GML [Tan {\it et al.}, arXiv:1106.1146v1
(2011)] is made. Relations with the low-lying rigid-plane phonon dispersions in
the bulk materials are established. Master curves which connect the fan diagram
frequencies for any given {\EuScript N} are derived. Static and dynamic
thermal correlation functions for rigid-layer shear and compression modes are
calculated. The results might be of use for the interpretation of friction
force experiments on multilayer crystals
Modifications of Gait as Predictors of Natural Osteoarthritis Progression in STR/Ort Mice
OBJECTIVE: Osteoarthritis (OA) is a common chronic disease for which disease-modifying therapies are not currently available. Studies to seek new targets for slowing the progress of OA rely on mouse models, but these do not allow for longitudinal monitoring of disease development. This study was undertaken to determine whether gait can be used to measure disease severity in the STR/Ort mouse model of spontaneous OA and whether gait changes are related to OA joint pain. METHODS: Gait was monitored using a treadmill-based video system. Correlations between OA severity and gait at 3 treadmill speeds were assessed in STR/Ort mice. Gait and pain behaviors of STR/Ort mice and control CBA mice were analyzed longitudinally, with monthly assessments. RESULTS: The best speed to identify paw area changes associated with OA severity in STR/Ort mice was found to be 17 cm · seconds(â1). Paw area was modified with age in CBA and STR/Ort mice, but this began earlier in STR/Ort mice and correlated with the onset of OA at 20 weeks of age. In addition, task noncompliance appeared at 20 weeks. Surprisingly, STR/Ort mice did not show any signs of pain with OA development, even when treated with the opioid antagonist naloxone, but did exhibit normal pain behaviors in response to complete Freund's adjuvantâinduced arthritis. CONCLUSION: The present results identify an animal model in which OA severity and OA pain can be studied in isolation from one another. The findings suggest that paw area and treadmill noncompliance may be useful tools to longitudinally monitor nonpainful OA development in STR/Ort mice. This will help in providing a noninvasive means of assessing new therapies to slow the progression of OA
Removing noise from pyrosequenced amplicons
Background
In many environmental genomics applications a homologous region of DNA from a diverse sample is first amplified by PCR and then sequenced. The next generation sequencing technology, 454 pyrosequencing, has allowed much larger read numbers from PCR amplicons than ever before. This has revolutionised the study of microbial diversity as it is now possible to sequence a substantial fraction of the 16S rRNA genes in a community. However, there is a growing realisation that because of the large read numbers and the lack of consensus sequences it is vital to distinguish noise from true sequence diversity in this data. Otherwise this leads to inflated estimates of the number of types or operational taxonomic units (OTUs) present. Three sources of error are important: sequencing error, PCR single base substitutions and PCR chimeras. We present AmpliconNoise, a development of the PyroNoise algorithm that is capable of separately removing 454 sequencing errors and PCR single base errors. We also introduce a novel chimera removal program, Perseus, that exploits the sequence abundances associated with pyrosequencing data. We use data sets where samples of known diversity have been amplified and sequenced to quantify the effect of each of the sources of error on OTU inflation and to validate these algorithms
Spectral and stratigraphic mapping of hydrated sulfate and phyllosilicate-bearing deposits in northern Sinus Meridiani, Mars
We present detailed stratigraphic and spectral analyses that focus on a region in
northern Sinus Meridiani located between 1°N to 5°N latitude and 3°W to 1°E longitude.
Several stratigraphically distinct units are defined and mapped using morphologic
expression, spectral properties, and superposition relationships. Previously unreported
exposures of hydrated sulfates and Fe/Mg smectites are identified using MRO CRISM and
MEX OMEGA nearâinfrared (1.0 to 2.5 ”m) spectral reflectance observations. Layered
deposits with monohydrated and polyhydrated sulfate spectral signatures that occur in
association with a northeastâsouthwest trending valley are reexamined using highresolution
CRISM, HiRISE, and CTX images. Layers that are spectrally dominated by
monohydrated and polyhydrated sulfates are intercalated. The observed compositional
layering implies that multiple wetting events, brine recharge, or fluctuations in evaporation
rate occurred. We infer that these hydrated sulfateâbearing layers were unconformably
deposited following the extensive erosion of preexisting layered sedimentary rocks and
may postdate the formation of the sulfateâ and hematiteâbearing unit analyzed by the MER
Opportunity rover. Therefore, at least two episodes of deposition separated by an
unconformity occurred. Fe/Mg phyllosilicates are detected in units that predate the sulfateand
hematiteâbearing unit. The presence of Fe/Mg smectite in older units indicates that the
relatively low pH formation conditions inferred for the younger sulfateâ and hematitebearing
unit are not representative of the aqueous geochemical environment that prevailed
during the formation and alteration of earlier materials. Sedimentary deposits indicative of
a complex aqueous history that evolved over time are preserved in Sinus Meridiani, Mars
Detection of arcs in Saturn's F ring during the 1995 Sun ring-plane crossing
Observations of the November 1995 Sun crossing of the Saturn's ring-plane
made with the 3.6m CFH telescope, using the UHAO adaptive optics system, are
presented here. We report the detection of four arcs located in the vicinity of
the F ring. They can be seen one day later in HST images. The combination of
both data sets gives accurate determinations of their orbits. Semi-major axes
range from 140020 km to 140080 km, with a mean of 140060 +- 60 km. This is
about 150 km smaller than previous estimates of the F ring radius from Voyager
1 and 2 data, but close to the orbit of another arc observed at the same epoch
in HST images.Comment: 8 pages, 3 figures, 1 table, To appear in A&A, for comments :
[email protected]
Nanoscale regulation of L-type calcium channels differentiates between ischemic and dilated cardiomyopathies.
Background Subcellular localization and function of L-type calcium channels (LTCCs) play an important role in regulating contraction of cardiomyocytes. Understanding how this is affected by the disruption of transverse tubules during heart failure could lead to new insights into the disease. Methods Cardiomyocytes were isolated from healthy donor hearts, as well as from patients with cardiomyopathies and with left ventricular assist devices. Scanning ion conductance and confocal microscopy was used to study membrane structures in the cells. Super-resolution scanning patch-clamp was used to examine LTCC function in different microdomains. Computational modeling predicted the impact of these changes to arrhythmogenesis at the whole-heart level. Findings We showed that loss of structural organization in failing myocytes leads to re-distribution of functional LTCCs from the T-tubules to the sarcolemma. In ischemic cardiomyopathy, the increased LTCC open probability in the T-tubules depends on the phosphorylation by protein kinase A, whereas in dilated cardiomyopathy, the increased LTCC opening probability in the sarcolemma results from enhanced phosphorylation by calcium-calmodulin kinase II. LVAD implantation corrected LTCCs pathophysiological activity, although it did not improve their distribution. Using computational modeling in a 3D anatomically-realistic human ventricular model, we showed how LTCC location and activity can trigger heart rhythm disorders of different severity. Interpretation Our findings demonstrate that LTCC redistribution and function differentiate between disease aetiologies. The subcellular changes observed in specific microdomains could be the consequence of the action of distinct protein kinases. Funding This work was supported by NIH grant (ROI-HL 126802 to NT-JG) and British Heart Foundation (grant RG/17/13/33173 to JG, project grant PG/16/17/32069 to RAC). Funders had no role in study design, data collection, data analysis, interpretation, writing of the repor
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