368 research outputs found
Visual memory for random block patterns defined by luminance and color contrast
We studied the ability of human subjects to memorize the visual information in computer-generated random block patterns defined either by luminance contrast, by color contrast, or by both. Memory performance declines rapidly with increasing inter-stimulus interval, showing a half-life of approximately 3 s. We further show that memory performance declines with eccentricity approximately as a Gaussian function of position. Memory decay functions did not depend on whether the patterns were defined by luminance or color contrast. Changing both luminance and color components of block patterns in conjunction did not improve performance suggesting a single memory mechanism is used to store luminance and color derived pattern information. Our results further suggest that color identity (hue, saturation) and pattern information extracted from color- or luminance-contrast are stored independently of each other
A second-order orientation-contrast stimulus for population-receptive-field-based retinotopic mapping
Visual field or retinotopic mapping is one of the most frequently used
paradigms in fMRI. It uses activity evoked by position-varying high luminance
contrast visual patterns presented throughout the visual field for determining
the spatial organization of cortical visual areas. While the advantage of using
high luminance contrast is that it tends to drive a wide range of neural
populations - thus resulting in high signal-to-noise BOLD responses - this may
also be a limitation, especially for approaches that attempt to squeeze more
information out of the BOLD response, such as population receptive field (pRF)
mapping. In that case, more selective stimulation of a subset of neurons -
despite reduced signals - could result in better characterization of pRF
properties. Here, we used a second-order stimulus based on local differences in
orientation texture - to which we refer as orientation contrast - to perform
retinotopic mapping. Participants in our experiment viewed arrays of Gabor
patches composed of a foreground (a bar) and a background. These could only be
distinguished on the basis of a difference in patch orientation. In our
analyses, we compare the pRF properties obtained using this new orientation
contrast-based retinotopy (OCR) to those obtained using classic luminance
contrast-based retinotopy (LCR). Specifically, in higher order cortical visual
areas such as LO, our novel approach resulted in non-trivial reductions in
estimated population receptive field size of around 30%. We discuss how OCR -
by limiting receptive field scatter and reducing BOLD displacement - may result
in more accurate pRF localization as well. We conclude that using our approach,
it is possible to selectively target particular neuronal populations, opening
the way to use pRF modeling to dissect the response properties of more
clearly-defined neuronal populations in different visual areas.Comment: Yildirim, F., et al., A second-order orientation-contrast stimulus
for population-receptive-field-based retinotopic mapping, NeuroImage (2017
Preview of partial stimulus information in search prioritizes features and conjunctions, not locations
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216040.pdf (publisher's version ) (Open Access)Visual search often requires combining information on distinct visual features such as color and orientation, but how the visual system does this is not fully understood. To better understand this, we showed observers a brief preview of part of a search stimulus - either its color or orientation - before they performed a conjunction search task. Our experimental questions were (1) whether observers would use such previews to prioritize either potential target locations or features, and (2) which neural mechanisms might underlie the observed effects. In two experiments, participants searched for a prespecified target in a display consisting of bar elements, each combining one of two possible colors and one of two possible orientations. Participants responded by making an eye movement to the selected bar. In our first experiment, we found that a preview consisting of colored bars with identical orientation improved saccadic target selection performance, while a preview of oriented gray bars substantially decreased performance. In a follow-up experiment, we found that previews consisting of discs of the same color as the bars (and thus without orientation information) hardly affected performance. Thus, performance improved only when the preview combined color and (noninformative) orientation information. Previews apparently result in a prioritization of features and conjunctions rather than of spatial locations (in the latter case, all previews should have had similar effects). Our results thus also indicate that search for, and prioritization of, combinations involve conjunctively tuned neural mechanisms. These probably reside at the level of the primary visual cortex.13 p
An Explanation for the Role of the Amygdala in Aesthetic Judgments
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168787.pdf (publisher's version ) (Open Access)It has been proposed that the top-down guidance of feature-based attention is the basis for the involvement of the amygdala in various tasks requiring emotional decision-making (Jacobs, Renken, Aleman & Cornelissen, 2012). Aesthetic judgements are correlated with particular visual features and can be considered emotional in nature (Jacobs et al., 2016). Moreover, we have previously shown that various aesthetic judgements result in observers preferentially attending to different visual features (Jacobs et al., 2010). Here, we argue that - together - this explains why the amygdalae become active during aesthetic judgements of visual materials. We discuss potential implications and predictions of this theory that can be tested experimentally.7 p
Predictive masking of an artificial scotoma is associated with a system-wide reconfiguration of neural populations in the human visual cortex
The visual brain has the remarkable capacity to complete our percept of the world even when the information extracted from the visual scene is incomplete. This ability to predict missing information based on information from spatially adjacent regions is an intriguing attribute of healthy vision. Yet, it gains particular significance when it masks the perceptual consequences of a retinal lesion, leaving patients unaware of their partial loss of vision and ultimately delaying diagnosis and treatment. At present, our understanding of the neural basis of this masking process is limited which hinders both quantitative modelling as well as translational application. To overcome this, we asked the participants to view visual stimuli with and without superimposed artificial scotoma (AS). We used fMRI to record the associated cortical activity and applied model-based analyses to track changes in cortical population receptive fields and connectivity in response to the introduction of the AS. We found that throughout the visual field and cortical hierarchy, pRFs shifted their preferred position towards the AS border. Moreover, extrastriate areas biased their sampling of V1 towards sections outside the AS projection zone, thereby effectively masking the AS with signals from spared portions of the visual field. We speculate that the signals that drive these system-wide population modifications originate in extrastriate visual areas and, through feedback, also reconfigure the neural populations in the earlier visual areas
Studying Cortical Plasticity in Ophthalmic and Neurological Disorders:From Stimulus-Driven to Cortical Circuitry Modeling Approaches
Unsolved questions in computational visual neuroscience research are whether and how neurons and their connecting cortical networks can adapt when normal vision is compromised by a neurodevelopmental disorder or damage to the visual system. This question on neuroplasticity is particularly relevant in the context of rehabilitation therapies that attempt to overcome limitations or damage, through either perceptual training or retinal and cortical implants. Studies on cortical neuroplasticity have generally made the assumption that neuronal population properties and the resulting visual field maps are stable in healthy observers. Consequently, differences in the estimates of these properties between patients and healthy observers have been taken as a straightforward indication for neuroplasticity. However, recent studies imply that the modeled neuronal properties and the cortical visual maps vary substantially within healthy participants, e.g., in response to specific stimuli or under the influence of cognitive factors such as attention. Although notable advances have been made to improve the reliability of stimulus-driven approaches, the reliance on the visual input remains a challenge for the interpretability of the obtained results. Therefore, we argue that there is an important role in the study of cortical neuroplasticity for approaches that assess intracortical signal processing and circuitry models that can link visual cortex anatomy, function, and dynamics
Progression of Visual Pathway Degeneration in Primary Open-Angle Glaucoma:A Longitudinal Study
Background: Primary open-angle glaucoma (POAG) patients exhibit widespread white matter (WM) degeneration throughout their visual pathways. Whether this degeneration starts at the pre- or post-geniculate pathways remains unclear. In this longitudinal study, we assess the progression of WM degeneration exhibited by the pre-geniculate optic tracts (OTs) and the post-geniculate optic radiations (ORs) of POAG patients over time, aiming to determine the source and pattern of spread of this degeneration. Methods: Diffusion-weighted MRI scans were acquired for 12 POAG patients and 14 controls at two time-points 5.4 +/- 2.1 years apart. Fiber density (FD), an estimate of WM axonal density, was computed for the OTs and ORs of all participants in an unbiased longitudinal population template space. First, FD was compared between POAG patients and the controls at time-point 1 (TP1) and time-point 2 (TP2) independently. Secondly, repeated measures analysis was performed for FD change in POAG patients between the two time-points. Finally, we compared the rate of FD change over time between the two groups. Results: Compared to the controls, POAG patients exhibited significantly lower FD in the left OT at TP1 and in both OTs and the left OR at TP2. POAG patients showed a significant loss of FD between the time-points in the right OT and both ORs, while the left OR showed a significantly higher rate of FD loss in POAG patients compared to the controls. Conclusions: We find longitudinal progression of neurodegenerative WM changes in both the pre- and post-geniculate visual pathways of POAG patients. The pattern of changes suggests that glaucomatous WM degeneration starts at the pre-geniculate pathways and then spreads to the post-geniculate pathways. Furthermore, we find evidence that the trans-synaptic spread of glaucomatous degeneration to the post-geniculate pathways is a prolonged process which continues in the absence of detectable pre-geniculate degenerative progression. This suggests the presence of a time window for salvaging intact post-geniculate pathways, which could prove to be a viable therapeutic target in the future
Investigating changes in axonal density and morphology of glaucomatous optic nerves using fixel-based analysis
PURPOSE: To characterize neurodegeneration of glaucomatous optic nerves (ONs) in terms of changes in axonal density and morphology using fixel-based analysis (FBA), a novel framework for analyzing diffusion-weighted MRI (DWI). Furthermore, we aimed to explore the potential of FBA measures as biomarkers of glaucomatous ON degeneration. METHODS: DWI scans were obtained from 15 glaucoma patients and 15 controls. ONs were tracked and segmented into their three anatomical segments; intraorbital (IO), intracanalicular (ICAN) and intracranial (ICRAN). For each segment, FBA measures were computed, which included fiber density (FD; a measure of axonal density), fiber-bundle cross-section (FC; an estimate of morphological changes), and fiber density and cross-section (FDC). Peripapillary retinal nerve fiber layer (pRNFL) thickness and visual field mean deviation (VFMD) were assessed for glaucoma patients. ANCOVA was used to compare FBA values between the two groups, and Spearman's correlation analysis was used to test the correlation between FBA measures and pRNFL thickness and VFMD. RESULTS: All glaucomatous ON segments showed a significant loss of FD and FDC compared to the controls, while a loss of FC was found in the IO and ICRAN segments only. FD and FDC values of the IO and ICAN segments of glaucomatous ONs showed significant correlations with pRNFL thickness and VFMD. CONCLUSIONS: Glaucomatous ONs exhibit lower FD and FC compared to controls, indicating axonal loss and gross atrophy. The correlation between FBA measures of glaucomatous ONs and established clinical tests of glaucoma demonstrates the potential of FBA measures as biomarkers of glaucomatous ON degeneration
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