Your search keyword '"Parvocellular"' showing total 359 results

151. The Development and Aging of the Magnocellular and Parvocellular Visual Pathways as Indicated by VEP Recordings between 5 and 84 Years of Age

Author

Szabolcs Kéri, György Benedek, Gyongyi Horvath, Gábor Braunitzer, and Márta Janáky

Subjects

0301 basic medicine, genetic structures, Cognitive Neuroscience, media_common.quotation_subject, parvocellular, Stimulation, Visual evoked potentials, Visual system, Article, Developmental psychology, 03 medical and health sciences, 0302 clinical medicine, Parvocellular cell, Healthy volunteers, Contrast (vision), pattern-reversal VEP, development, aging, magnocellular, media_common, Cell Biology, Sensory Systems, Ophthalmology, 030104 developmental biology, Pattern reversal, Checkerboard pattern, Psychology, Neuroscience, 030217 neurology & neurosurgery, Optometry

Abstract

It is well known that pattern reversal visual evoked potentials (VEPs) are age-sensitive. Through the use of this technique, it is possible to assess both of the major visual pathways (i.e., the magnocellular and parvocellular ones) in terms of function and development. What developmental path these pathways follow, and if they develop/age in parallel across the human lifespan is a matter of ongoing debate, yet, only a few VEP studies have dealt with this issue. This cross-sectional study examined a sample of 115 healthy volunteers aged 5 to 84 years. Beyond the standard checkerboard pattern reversal stimulation at 97% contrast, we recorded pattern-reversal VEPs at 6% contrast to selectively stimulate the M pathway and isoluminant red and green checkerboard stimulation was also used to selectively stimulate the P pathway. Our results do not support the developmental advantage of any of the pathways. The development of both pathways appear to take a remarkably long time (well into the 30s), and the signs of aging become marked over 50 years of age, especially in the case of the magnocellular pathway.

Published

2016

152. The Pattern of Retinal Ganglion Cell Loss in OPA1-Related Autosomal Dominant Optic Atrophy Inferred From Temporal, Spatial, and Chromatic Sensitivity Losses

Author

University of Helsinki, Department of Ophthalmology and Otorhinolaryngology, Majander, Anna, Joao, Catarina, Rider, Andrew T., Henning, G. Bruce, Votruba, Marcela, Moore, Anthony T., Yu-Wai-Man, Patrick, Stockman, Andrew, University of Helsinki, Department of Ophthalmology and Otorhinolaryngology, Majander, Anna, Joao, Catarina, Rider, Andrew T., Henning, G. Bruce, Votruba, Marcela, Moore, Anthony T., Yu-Wai-Man, Patrick, and Stockman, Andrew

Abstract

PURPOSE. Progressive retinal ganglion cell (RGC) loss is the pathological hallmark of autosomal dominant optic atrophy (DOA) caused by pathogenic OPA1 mutations. The aim of this study was to conduct an in-depth psychophysical study of the visual losses in DOA and to infer any selective vulnerability of visual pathways subserved by different RGC subtypes. METHODS. We recruited 25 patients carrying pathogenic OPA1 mutations and age-matched healthy individuals. Spatial contrast sensitivity functions (SCSFs) and chromatic contrast sensitivity were quantified, the latter using the Cambridge Colour Test. In 11 patients, long (L) and short (S) wavelength-sensitive cone temporal acuities were measured as a function of target illuminance, and L-cone temporal contrast sensitivity (TCSF) as a function of temporal frequency. RESULTS. Spatial contrast sensitivity functions were abnormal, with the loss of sensitivity increasing with spatial frequency. Further, the highest L-cone temporal acuity fell on average by 10 Hz and the TCSFs by 0.66 log(10) unit. Chromatic thresholds along the protan, deutan, and tritan axes were 8, 9, and 14 times higher than normal, respectively, with losses increasing with age and S-cone temporal acuity showing the most significant age-related decline. CONCLUSIONS. Losses of midget parvocellular, parasol magnocellular, and bistratified koniocellular RGCs could account for the losses of high spatial frequency sensitivity and protan and deutan sensitivities, high temporal frequency sensitivity, and S-cone temporal and tritan sensitivities, respectively. The S-cone-related losses showed a significant deterioration with increasing patient age and could therefore prove useful biomarkers of disease progression in DOA.

Published

2017

153. Testing the generality of the zoom-lens model: Evidence for visual-pathway specific effects of attended-region size on perception

Author

Goodhew, Stephanie Catherine, Lawrence, Rebecca, Edwards, Mark, Goodhew, Stephanie Catherine, Lawrence, Rebecca, and Edwards, Mark

Abstract

There are volumes of information available to process in visual scenes. Visual spatial attention is a critically important selection mechanism that prevents these volumes from overwhelming our visual system's limited-capacity processing resources. We were interested in understanding the effect of the size of the attended area on visual perception. The prevailing model of attended-region size across cognition, perception, and neuroscience is the zoom-lens model. This model stipulates that the magnitude of perceptual processing enhancement is inversely related to the size of the attended region, such that a narrow attended-region facilitates greater perceptual enhancement than a wider region. Yet visual processing is subserved by two major visual pathways (magnocellular and parvocellular) that operate with a degree of independence in early visual processing and encode contrasting visual information. Historically, testing of the zoom-lens has used measures of spatial acuity ideally suited to parvocellular processing. This, therefore, raises questions about the generality of the zoom-lens model to different aspects of visual perception. We found that while a narrow attended-region facilitated spatial acuity and the perception of high spatial frequency targets, it had no impact on either temporal acuity or the perception of low spatial frequency targets. This pattern also held up when targets were not presented centrally. This supports the notion that visual attended-region size has dissociable effects on magnocellular versus parvocellular mediated visual processing.

Published

2017

154. Scotopic Vision Is Selectively Processed in Thick-Type Columns in Human Extrastriate Cortex.

Author

Tootell RBH and Nasr S

Subjects

Adult, Color Vision physiology, Female, Humans, Male, Retinal Rod Photoreceptor Cells physiology, Visual Cortex diagnostic imaging, Visual Pathways diagnostic imaging, Young Adult, Magnetic Resonance Imaging methods, Night Vision physiology, Photic Stimulation methods, Visual Cortex physiology, Visual Pathways physiology

Abstract

In humans, visual stimuli can be perceived across an enormous range of light levels. Evidence suggests that different neural mechanisms process different subdivisions of this range. For instance, in the retina, stimuli presented at very low (scotopic) light levels activate rod photoreceptors, whereas cone photoreceptors are activated relatively more at higher (photopic) light levels. Similarly, different retinal ganglion cells are activated by scotopic versus photopic stimuli. However, in the brain, it remains unknown whether scotopic versus photopic information is: 1) processed in distinct channels, or 2) neurally merged. Using high-resolution functional magnetic resonance imaging at 7 T, we confirmed the first hypothesis. We first localized thick versus thin-type columns within areas V2, V3, and V4, based on photopic selectivity to motion versus color, respectively. Next, we found that scotopic stimuli selectively activated thick- (compared to thin-) type columns in V2 and V3 (in measurements of both overlap and amplitude) and V4 (based on overlap). Finally, we found stronger resting-state functional connections between scotopically dominated area MT with thick- (compared to thin-) type columns in areas V2, V3, and V4. We conclude that scotopic stimuli are processed in partially segregated parallel streams, emphasizing magnocellular influence, from retina through middle stages of visual cortex., (© The Author(s) 2020. Published by Oxford University Press.)

Published

2021

155. Binocular treatment in adult amblyopia is based on parvocellular or magnocellular pathway.

Author

Shuai L, Leilei Z, Wen W, Shu W, Gangsheng L, Yinglong L, Guoke Y, Xinrong C, Hong L, and Rongfeng L

Subjects

Adult, Amblyopia physiopathology, Anisometropia physiopathology, Contrast Sensitivity physiology, Depth Perception physiology, Female, Humans, Male, Strabismus physiopathology, Visual Acuity physiology, Young Adult, Amblyopia therapy, Anisometropia therapy, Discrimination Learning physiology, Strabismus therapy, Vision, Binocular physiology, Visual Perception physiology

Abstract

Introduction: Amblyopia is speculated to be an untreatable disease in the patient, who is beyond the critical period of vision; however, currently, it is treatable in adults., Purpose: This study aimed to elucidate whether the treatment is useful in both anisometropic amblyopia and strabismic amblyopia. In addition, the differences were detected between anisometropic amblyopia and strabismic amblyopia after the same perceptual treatment and whether the suppression in anisometropic amblyopia or strabismic amblyopia could be decreased before and after the treatment., Methods: A binocular perceptual learning was applied for the treatment, the suppression was measured, and the patients were followed up for 2 months after training. Anisometropic amblyopia and strabismic amblyopia groups were subjected to the assessment of stereo, visual acuity, contrast sensitivity, and suppression before and after the training., Results: After 6 weeks of "Diploma Gabor Orientation Coherence" training, in the anisometropic amblyopia group, the outcomes of visual acuity (t = 3.114, p = 0.026) and contrast sensitivity (t = 7.786, p = 0.001) were increased significantly. While in the strabismic amblyopia group, the outcomes of stereo (t = 2.987, p = 0.040) and contrast sensitivity (t = 3.638, p = 0.022) were increased significantly., Conclusion: After Diploma Gabor Orientation Coherence training in the same frequency and in the same duration, the anisometropic amblyopia group got an improvement in visual acuity, but the strabismic amblyopia group got an improvement in stereo. As there are evidences to show that anisometropic amblyopia and strabismic amblyopia were injured in different pathways, we think the diverse results might come from the different pathway injury in anisometropic amblyopia and strabismic amblyopia.

Published

2020

156. Metabotropic glutamate receptor 5 shows different patterns of localization within the parallel visual pathways in macaque and squirrel monkeys

Author

Julia A. Mavity-Hudson, Ashley Wenger, Vivien A. Casagrande, and Yuri Shostak

Subjects

koniocellular, parvocellular, Biology, Visual system, Lateral geniculate nucleus, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, immunocytochemistry, Postsynaptic potential, Eye and Brain, mental disorders, Neuropil, medicine, visual cortex, 030304 developmental biology, Original Research, 0303 health sciences, magnocellular, electron microscopy, Metabotropic glutamate receptor 5, Glutamate receptor, Sensory Systems, Ophthalmology, Koniocellular cell, Metabotropic receptor, medicine.anatomical_structure, nervous system, Neuroscience, 030217 neurology & neurosurgery

Abstract

Yuri Shostak,1,5Ashley Wenger,4 Julia Mavity-Hudson,1 Vivien A Casagrande1–3 1Department of Cell and Developmental Biology, 2Department of Psychology, 3Department of Ophthalmology and Visual Sciences, 4Undergraduate Neuroscience Program, Vanderbilt University, Nashville, TN, USA; 5Foreign Trade Unitary Enterprise, Minsk, Belarus Abstract: Glutamate is used as an excitatory neurotransmitter by the koniocellular (K), magnocellular (M), and parvocellular (P) pathways to transfer signals from the primate lateral geniculate nucleus (LGN) to primary visual cortex (V1). Glutamate acts through both fast ionotropic receptors, which appear to carry the main sensory message, and slower, modulatory metabotropic receptors (mGluRs). In this study, we asked whether mGluR5 relates in distinct ways to the K, M, and P LGN axons in V1. To answer this question, we used light microscopic immunocytochemistry and preembedding electron microscopic immunogold labeling to determine the localization of mGluR5 within the layers of V1 in relation to the K, M, and P pathways in macaque and squirrel monkeys. These pathways were labeled separately via wheat germ agglutinin–horseradish peroxidase (WGA–HRP) injections targeting the LGN layers. mGluR5 is of interest because it: 1) has been shown to be expressed in the thalamic input layers; 2) appears to be responsible for some types of oscillatory firing, which could be important in the binding of visual features; and 3) has been associated with a number of sensory-motor gating-related pathologies, including schizophrenia and autism. Our results demonstrated the presence of mGluR5 in the neuropil of all V1 layers. This protein was lowest in IVCa (M input) and the infragranular layers. In layer IVC, mGluR5 also was found postsynaptic to about 30% of labeled axons, but the distribution was uneven, such that postsynaptic mGluR5 label tended to occur opposite smaller (presumed P), and not larger (presumed M) axon terminals. Only in the K pathway in layer IIIB, however, was mGluR5 always found in the axon terminals themselves. The presence of mGluR5 in K axons and not in M and P axons, and the presence of mGluR5 postsynaptic mainly to smaller P and not larger M axons suggest that the response to the release of glutamate is modulated in distinct ways within and between the parallel visual pathways of primates. Keywords: electron microscopy, immunocytochemistry, koniocellular, magnocellular, parvocellular, visual cortex

Published

2015

157. Selective spatial enhancement: Attentional spotlight size impacts spatial but not temporal perception

Author

Goodhew, Stephanie Catherine, Shen, Elizabeth, Edwards, Mark, Goodhew, Stephanie Catherine, Shen, Elizabeth, and Edwards, Mark

Abstract

An important but often neglected aspect of attention is how changes in the attentional spotlight size impact perception. The zoom-lens model predicts that a small ("focal") attentional spotlight enhances all aspects of perception relative to a larger ("diffuse" spotlight). However, based on the physiological properties of the two major classes of visual cells (magnocellular and parvocellular neurons) we predicted trade-offs in spatial and temporal acuity as a function of spotlight size. Contrary to both of these accounts, however, across two experiments we found that attentional spotlight size affected spatial acuity, such that spatial acuity was enhanced for a focal relative to a diffuse spotlight, whereas the same modulations in spotlight size had no impact on temporal acuity. This likely reflects the function of attention: to induce the high spatial resolution of the fovea in periphery, where spatial resolution is poor but temporal resolution is good. It is adaptive, therefore, for the attentional spotlight to enhance spatial acuity, whereas enhancing temporal acuity does not confer the same benefit.

Published

2016

158. Parvocellular and Magnocellular Contributions to the Initial Generators of the Visual Evoked Potential: High-Density Electrical Mapping of the “C1” Component

Author

Foxe, John J., Strugstad, E. Cathrine, Sehatpour, Pejman, Molholm, Sophie, Pasieka, Wren, Schroeder, Charles E., and McCourt, Mark E.

Published

2008

159. Processing of natural temporal stimuli by macaque retinal ganglion cells

Subjects

magnocellular, macaque, parvocellular, COLOR-VISION, PRIMARY VISUAL-CORTEX, LIGHT ADAPTATION, retinal ganglion cells, GAIN-CONTROL, NEURAL CODE, CHROMATIC MODULATION, INFORMATION-THEORY, natural stimuli, LATERAL GENICULATE-NUCLEUS, SENSITIVITY, information theory, RESPONSES

Abstract

This study quantifies the performance of primate retinal ganglion cells in response to natural stimuli. Stimuli were confined to the temporal and chromatic domains and were derived from two contrasting environments, one typically northern European and the other a flower show. The performance of the cells was evaluated by investigating variability of cell responses to repeated stimulus presentations and by comparing measured to model responses. Both analyses yielded a quantity called the coherence rate (in bits per second), which is related to the information rate. Magnocellular (MC) cells yielded coherence rates of up to 100 bits/sec, rates of parvocellular (PC) cells were much lower, and short wavelength (S)-cone-driven ganglion cells yielded intermediate rates. The modeling approach showed that for MC cells, coherence rates were generated almost exclusively by the luminance content of the stimulus. Coherence rates of PC cells were also dominated by achromatic content. This is a consequence of the stimulus structure; luminance varied much more in the natural environment than chromaticity. Only approximately one-sixth of the coherence rate of the PC cells derived from chromatic content, and it was dominated by frequencies below 10 Hz. S-cone-driven ganglion cells also yielded coherence rates dominated by low frequencies. Below 2–3 Hz, PC cell signals contained more power than those of MC cells. Response variation between individual ganglion cells of a particular class was analyzed by constructing generic cells, the properties of which may be relevant for performance higher in the visual system. The approach used here helps define retinal modules useful for studies of higher visual processing of natural stimuli.

Published

2002

160. Functional mapping of the magnocellular and parvocellular subdivisions of human LGN

Author

Michael A. Silver, Essa Yacoub, Rachel N. Denison, An T. Vu, and David A. Feinberg

Subjects

Adult, Male, Parvocellular, Visual perception, genetic structures, 7T, Photic Stimulation, 1.1 Normal biological development and functioning, Cognitive Neuroscience, Stimulus (physiology), Lateral geniculate nucleus, computer.software_genre, Brain mapping, Medical and Health Sciences, Article, Contrast Sensitivity, Clinical Research, Underpinning research, Parvocellular cell, Voxel, Parallel processing, Humans, Eye Disease and Disorders of Vision, Spatial organization, Brain Mapping, Neurology & Neurosurgery, Magnocellular, fMRI, Psychology and Cognitive Sciences, Neurosciences, Geniculate Bodies, Magnetic Resonance Imaging, Neurology, nervous system, Space Perception, Visual Perception, Female, sense organs, Psychology, Neuroscience, computer, psychological phenomena and processes

Abstract

The magnocellular (M) and parvocellular (P) subdivisions of primate LGN are known to process complementary types of visual stimulus information, but a method for noninvasively defining these subdivisions in humans has proven elusive. As a result, the functional roles of these subdivisions in humans have not been investigated physiologically. To functionally map the M and P subdivisions of human LGN, we used high-resolution fMRI at high field (7. T and 3. T) together with a combination of spatial, temporal, luminance, and chromatic stimulus manipulations. We found that stimulus factors that differentially drive magnocellular and parvocellular neurons in primate LGN also elicit differential BOLD fMRI responses in human LGN and that these responses exhibit a spatial organization consistent with the known anatomical organization of the M and P subdivisions. In test-retest studies, the relative responses of individual voxels to M-type and P-type stimuli were reliable across scanning sessions on separate days and across sessions at different field strengths. The ability to functionally identify magnocellular and parvocellular regions of human LGN with fMRI opens possibilities for investigating the functions of these subdivisions in human visual perception, in patient populations with suspected abnormalities in one of these subdivisions, and in visual cortical processing streams arising from parallel thalamocortical pathways. © 2014 Elsevier Inc.

Published

2014

161. Peripheral global neglect in high vs. low autistic tendency

Author

David P. Crewther and D.P. Crewther

Subjects

Autism-spectrum quotient, medicine.medical_specialty, Visual perception, genetic structures, media_common.quotation_subject, lcsh:BF1-990, Illusion, global percept, parvocellular, autism, Audiology, behavioral disciplines and activities, Foveal, Parvocellular cell, medicine, Contrast (vision), Psychology, Original Research Article, General Psychology, media_common, magnocellular, autistic tendency, diamond illusion, Visual field, lcsh:Psychology, local percept, Percept, AQ, Neuroscience

Abstract

In addition to its core social deficits, autism is characterized by altered visual perception, with a preference for local percept in those high in autistic tendency. Here, the balance of global vs. local percepts for the perceptually rivalrous diamond illusion was assessed between groups scoring high and low on the Autism Spectrum Quotient (AQ). The global percept of a diamond shape oscillating horizontally behind three occluders can as easily be interpreted as the local percept of four line elements, each moving vertically. Increasing the luminance contrast of the occluders with respect to background resulted in an increase of initial global percept in both groups, with no difference in sensitivity between groups. Presenting the target further into the periphery resulted in a marked increase in the percentage of global perception with visual field eccentricity. However, while the performance for centrally presented diamond targets was not different between AQ groups, the peripheral global performance of the High AQ group was significantly reduced compared with the Low AQ group. On the basis of other imaging studies, this peripheral but not foveal global perceptual neglect may indicate an abnormal interaction between striate cortex and the Lateral Occipital Complex (LOC), or to differences in the deployment of attention between the two groups.

Published

2014

162. Pulse and steady-pedestal contrast discrimination: effect of spatial parameters

Author

Joel Pokorny, Vincent C. W. Sun, and Vivianne C. Smith

Subjects

Adult, Male, Parvocellular, Psychometrics, Stimulus (physiology), Summation, Contrast Sensitivity, Discrimination, Psychological, Psychophysics, Humans, Visual Pathways, Power function, Lighting, Contrast discrimination, Two-alternative forced choice, Magnocellular, Spatial summation, Mathematical analysis, Observer (special relativity), Sensory Systems, Square degree, Ophthalmology, Female, Asymptote, Psychology, Neuroscience

Abstract

The goal of this study was to establish the spatial summation properties associated with inferred PC- and MC-pathway mediated psychophysical contrast discrimination. Previous work has established two paradigms that reveal characteristic signatures of these pathways. In the pulse paradigm, a four-square array was pulsed briefly, on a constant background. In the steady-pedestal paradigm, the stimulus array was presented continuously as a steady-pedestal within a constant surround. In both paradigms, one square differed from the others, giving the observer a forced choice spatial discrimination task. Area summation functions derived for the pulse paradigm decreased with area, with a slope of −0.25 on a log–log axis. Area summation functions derived for the steady-pedestal paradigm decreased as a power function of area, approaching an asymptote above one square degree. The latter are consistent with the classical data of threshold spatial summation.

Published

2001

163. Chromatic and luminance contributions to a hyperacuity task

Author

Barry B. Lee and Lukas Rüttiger

Subjects

Male, Retinal Ganglion Cells, Parvocellular, Color vision, Visual Acuity, Color Vision Defects, Luminance, Contrast Sensitivity, Optics, Parvocellular cell, Psychophysics, Animals, Humans, Chromatic scale, Hyperacuity, business.industry, Magnocellular, Ganglion cells, Figure–ground, Sensory Systems, Ophthalmology, Differential threshold, Sensory Thresholds, Macaca, business, Psychology, Color Perception, Photic Stimulation

Abstract

Displacement thresholds with incremental chromatic and luminance edges were measured on different backgrounds. Above 3% luminance contrast, thresholds were always similar. At luminance contrasts below 3%, luminance edges could not be detected, but chromatic edges were still visible. At these low contrasts displacement thresholds for chromatic edges increased to a high level. We interpret these data in terms of multiple mechanisms; above 3% contrast a luminance mechanism determines thresholds, but when, at lower contrasts, chromatic mechanisms support detection, they also support the spatial task. Physiological data were consistent with the different mechanisms originating at the retinal ganglion cell level.

Published

2000

164. Fine Structure of Parvocellular Receptive Fields in the Primate Fovea Revealed by Laser Interferometry

Author

Martin J.M. Lankheet, Peter Lennie, Matthew J. McMahon, and David R. Williams

Subjects

Parvocellular, Retinal circuitry, Fovea Centralis, Light, genetic structures, media_common.quotation_subject, Spatial vision, Models, Neurological, Normal Distribution, Visual Acuity, Acuity, Lateral geniculate nucleus, Optics, Parvocellular cell, medicine, Animals, Fiber Optic Technology, Contrast (vision), ARTICLE, media_common, Physics, Communication, Retina, Fourier Analysis, business.industry, Lasers, General Neuroscience, Ganglion cells, Neural Inhibition, LGN, Interferometry, medicine.anatomical_structure, Receptive field, Retinal Cone Photoreceptor Cells, Macaca, sense organs, Spatial frequency, Visual Fields, Visual angle, business

Abstract

Optical blurring in the eye prevents conventional physiological techniques from revealing the fine structure of the small parvocellular receptive fields in the primate foveain vivo. We explored the organization of receptive fields in macaque parvocellular lateral geniculate nucleus cells by using sinusoidal interference fringes formed directly on the retina to measure spatial frequency tuning at different orientations. Most parvocellular cells in and near the fovea respond reliably to spatial frequencies up to and beyond 100 cycles/° of visual angle, implying center input arising mainly from a single cone. Temporal frequency and contrast response characteristics were also measured at spatial frequencies up to 130 cycles/°. We compared our spatial frequency data with the frequency responses of model receptive fields that estimate the number, configuration, and weights of cones that feed the center and surround. On the basis of these comparisons, we infer possible underlying circuits. Most cells had irregular spatial frequency–response curves that imply center input from more than one cone. The measured responses are consistent with a single cone center together with weak input from nearby cones. By exposing a fine structure that cannot be discerned by conventional techniques, interferometry allows functional measurements of the early neural mechanisms in spatial vision.

Published

2000

165. Contributions of parvocellular and magnocellular pathways to visual perception near the hands are not fixed, but can be dynamically altered

Author

Goodhew, Stephanie Catherine, Clarke, Ruby, Goodhew, Stephanie Catherine, and Clarke, Ruby

Abstract

Visual perception is altered near the hands, and several mechanisms have been proposed to account for this, including differences in attention and a bias toward magnocellular-preferential processing. Here we directly pitted these theories against one another in a visual search task consisting of either magnocellular- or parvocellular-preferred stimuli. Surprisingly, we found that when a large number of items are in the display, there is a parvocellular processing bias in near-hand space. Considered in the context of existing results, this indicates that hand proximity does not entail an inflexible bias toward magnocellular processing, but instead that the attentional demands of the task can dynamically alter the balance between magnocellular and parvocellular processing that accompanies hand proximity.

Published

2015

166. Altered visual perception near the hands: a critical review of attentional and neurophysiological models

Author

Goodhew, Stephanie Catherine, Edwards, Mark, Ferber, Susanne, Pratt, Jay, Goodhew, Stephanie Catherine, Edwards, Mark, Ferber, Susanne, and Pratt, Jay

Abstract

Visual perception changes as a function of hand proximity. While various theoretical accounts have been offered for this alteration (attentional prioritisation, bimodal cell involvement, detailed evaluation, and magnocellular neuron input enhancement), the current literature lacks consensus on these mechanisms. The purpose of this review, therefore, is to critically review the existing body of literature in light of these distinct theoretical accounts. We find that a growing number of results support the magnocellular (M-cell) enhancement account, and are difficult to reconcile with general attention-based explanations. Despite this key theoretical development in the field, there has been some ambiguity with interpretations offered in recent papers, for example, equating the existing attentional and M-cell based explanations, when in fact they make contrasting predictions. We therefore highlight the differential predictions arising from the distinct theoretical accounts. Importantly, however, we also offer novel perspectives that synthesises the role of attention and neurophysiological mechanisms in understanding altered visual perception near the hands. We envisage that this theoretical development will ensure that the field can progress from documenting behavioural differences, to a consensus on the underlying visual and neurophysiological mechanisms.

Published

2015

167. Developmental dyslexia: A deficit in magnocellular-parvocellular co-activation, not simply in pure magnocellular activation.

Author

Contemori G, Battaglini L, Barollo M, Ciavarelli A, and Casco C

Subjects

Adolescent, Child, Child, Preschool, Female, Humans, Male, Contrast Sensitivity physiology, Dyslexia physiopathology, Visual Pathways physiology, Visual Perception physiology

Abstract

The magnocellular deficit theory of dyslexia suggests a selective impairment in contrast detection of stimuli involving pure magnocellular response (e.g. Gabor patches of 0.5 c/deg, 30 Hz, low contrast). An alternative hypothesis is that, dyslexia may be associated with a reduction of typical facilitation that normal readers present for stimuli relying on low-level magno-parvo co-activation, relative to stimuli eliciting pure magno activation. According to this hypothesis, any advantage in contrast sensitivity, produced by either decreasing stimuli temporal frequency (from 30 to 10 Hz, Experiment 1) or using static stimuli of increasing spatial frequency (from 0.5 to 4 c/deg, Experiment 2), would be ascribed to the coexisting responses of the magnocellular and parvocellular systems. In the control group, this advantage in contrast sensitivity was found for a 0.5 c/deg Gabor (either static or flickering at 10 Hz) and for a static Gabor of 4 c/deg. In contrast to magnocellular deficit theory predictions, dyslexic individuals showed no deficit in the unmixed magnocellular response. However, they showed no advantage when the relative weight between magnocellular and parvocellular inputs was thrown off balance in favor of the latter. These results suggest that in order to interpret low-level visual deficits in dyslexia, it is worth considering that fast, feedforward low-frequency representations of spatial structures may result from the coexisting responses of two systems. Our results suggest that in dyslexia, the relative contribution of these two systems in visual processing is perturbed, and that this may have detrimental consequences in word processing, both within the parafovea and the fovea during fixation., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

168. The koniocellular whiteboard.

Author

Martin PR and Solomon SG

Subjects

Animals, Humans, Visual Cortex physiology, Visual Pathways physiology, Teaching Materials, Visual Cortex cytology, Visual Fields physiology, Visual Pathways cytology

Abstract

In 1994 Vivien Casagrande published a review paper in which she summarized evidence for a koniocellular pathway to visual cortex. Here we try to explain how that review moved the field forward, and summarize some key unanswered questions about koniocellular pathways., (© 2018 Wiley Periodicals, Inc.)

Published

2019

169. Magnocellular and parvocellular pathway contributions to facial threat cue processing.

Author

Cushing CA, Im HY, Adams RB Jr, Ward N, and Kveraga K

Subjects

Adult, Cues, Facial Expression, Fear psychology, Female, Humans, Male, Visual Perception physiology, Amygdala physiology, Emotions physiology, Fear physiology, Fixation, Ocular physiology

Abstract

Human faces evolved to signal emotions, with their meaning contextualized by eye gaze. For instance, a fearful expression paired with averted gaze clearly signals both presence of threat and its probable location. Conversely, direct gaze paired with facial fear leaves the source of the fear-evoking threat ambiguous. Given that visual perception occurs in parallel streams with different processing emphases, our goal was to test a recently developed hypothesis that clear and ambiguous threat cues would differentially engage the magnocellular (M) and parvocellular (P) pathways, respectively. We employed two-tone face images to characterize the neurodynamics evoked by stimuli that were biased toward M or P pathways. Human observers (N = 57) had to identify the expression of fearful or neutral faces with direct or averted gaze while their magnetoencephalogram was recorded. Phase locking between the amygdaloid complex, orbitofrontal cortex (OFC) and fusiform gyrus increased early (0-300 ms) for M-biased clear threat cues (averted-gaze fear) in the β-band (13-30 Hz) while P-biased ambiguous threat cues (direct-gaze fear) evoked increased θ (4-8 Hz) phase locking in connections with OFC of the right hemisphere. We show that M and P pathways are relatively more sensitive toward clear and ambiguous threat processing, respectively, and characterize the neurodynamics underlying emotional face processing in the M and P pathways., (© The Author(s) 2019. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2019

170. Red Affects Reaction Times and Hit Rates in a 2AFC Classification Task

Author

Garofalo, Gioacchino, Ferrari, Vera, and Bruno, Nicola

Subjects

reaction time, magnocellular, Gabor patches, red backgrounds, parvocellular

Abstract

We measured reaction times and hit rates in a 2AFC orientation discrimination task. Gabor patches at different spatial frequencies and two levels of contrast (0.15 and 0.6) were presented surrounded by red, blue, or grey isoluminant backgrounds.. Results revealed lower accuracy and slower reaction times when the gabors were surrounded by red in comparison to blue or grey backgrounds. We interpret these results as evidence that i) exposure to long-wavelength light interferes with both magnocellular and parvocellular processing; but ii) long-wavelength light causes greater relative inhibition of magnocellular processing. These findings are relevant to the interpretation of studies that use red backgrounds to selectively isolate magnocellular contributions, and may have implications for the interpretation of studies of the effect of red contexts on diverse perceptual and cognitive tasks.

Published

2014

171. Rod inputs to macaque ganglion cells

Author

Jan Kremers, Vivianne C. Smith, Joel Pokorny, and Barry B. Lee

Subjects

Parvocellular, Retinal Ganglion Cells, genetic structures, Macaque, Luminance, Rods, Rod, chemistry.chemical_compound, Parvocellular cell, Retinal Rod Photoreceptor Cells, biology.animal, medicine, Animals, Visual Pathways, Rod-Cone Interaction, Retina, biology, Magnocellular, Ganglion cells, Retinal, Sensory Systems, Ganglion, Macaca fascicularis, Ophthalmology, medicine.anatomical_structure, chemistry, Cones, Biophysics, Retinal Cone Photoreceptor Cells, sense organs, Neuroscience, Photic Stimulation

Abstract

The strength of rod inputs to ganglion cells was assessed in the macaque retina at retinal positions within 3–15 deg eccentricity. The experimental paradigm used temporally modulated heterochromatic lights whose relative phase was varied. This paradigm provided a sensitive test to detect rod input. In parvocellular (PC) pathway cells, the gain of the cone-driven signal decreased with decrease in luminance. At 2 td a weak rod response, of a few impulses per second for 100% rod modulation, was revealed in about 60% of cells. For blue-on cells, the cone-driven response also decreased with retinal illuminance, but no rod response could be found. In magnocellular (MC) pathway cells, rod input was much more apparent. Responses became rod dominated at and below 20 td; we cannot exclude rod intrusion at higher retinal illuminances. Responsivity was maintained even at low retinal illuminances. Temporal-frequency dependent rod-cone interactions were observed in MC-pathway cells. Rod responses were of longer latency than cone responses, but there was no evidence of any difference in rod latency between parvocellular and magnocellular pathways.

Published

1997

172. Early Impairment of Foveal Magno- and Parvo-cellular Pathways in Juxta Chiasmal Tumours

Author

N. J. Gutowski, Mark O. Scase, and J. R. Heron

Subjects

Adenoma, Adult, Male, Retinal Ganglion Cells, Fovea Centralis, vision, medicine.medical_specialty, Visual acuity, genetic structures, Visual impairment, parvocellular, visual impairment, Visual Physiology, Visual system, chiasm dysfunction, Contrast Sensitivity, Craniopharyngioma, Optics, Parvocellular cell, Foveal, Ophthalmology, Psychophysics, medicine, Humans, Pituitary Neoplasms, Visual Pathways, Evoked potential, Aged, magnocellular, business.industry, Middle Aged, eye diseases, Sensory Systems, pituitary tumours, Pattern Recognition, Visual, Optic Chiasm, Sensory Thresholds, Optic chiasma, Evoked Potentials, Visual, Female, Visual Fields, medicine.symptom, business, Psychology, Color Perception, fovea

Abstract

Foveal pathway visual function was assessed in 11 patients having tumours extending into the suprasellar region but without evidence of visual impairment as assessed by visual acuity and Bjerrum screen campimetry. Psychophysical and routine visual evoked potential (VEP) measurements were obtained from the eye ipsilateral to the maximal suprasellar extension. The sensitivity of luminance and chromatic pathways was assessed psychophysically by measuring increment thresholds for white and red flashes of light presented on a white adapting field. Temporal sensitivity was assessed psychophysically by measuring threshold modulation sensitivity for sinusoidally modulating stimuli (de Lange attenuation characteristic). The patient group showed approximately equal significant psychophysical losses in chromatic, luminance and temporal sensitivities relative to normal controls. Midline VEP P100 latencies of the patient group did not significantly differ from those of the normal control group. It is concluded that tumours extending into the suprasellar region can cause foveal pathway dysfunction affecting both magno- and parvo-cellular pathways, even in the presence of normal visual acuity and fields suggesting a more widespread and insidious abnormality of the visual pathways in this condition than previously thought.

Published

1997

173. Schizophrenia spectrum participants have reduced visual contrast sensitivity to chromatic (red/green) and luminance (light/dark) stimuli: new insights into information processing, visual channel function and antipsychotic effects

Author

Karen R. Dobkins, Kathleen M. Shafer, Kristin S. Cadenhead, and Jessica E. McGovern

Subjects

Parvocellular, Psychosis, medicine.medical_specialty, medicine.medical_treatment, lcsh:BF1-990, parvocellular, Audiology, Developmental psychology, Parvocellular cell, visual contrast sensitivity, medicine, Psychology, Chromatic scale, Motion perception, Original Research Article, Antipsychotic, General Psychology, Backward masking, magnocellular, Magnocellular, medicine.disease, Schizotypal personality disorder, schizophrenia, lcsh:Psychology, Schizophrenia, schizotypal, Cognitive Sciences

Abstract

Background: Individuals with schizophrenia spectrum diagnoses have deficient visual information processing as assessed by a variety of paradigms including visual backward masking, motion perception and visual contrast sensitivity (VCS). In the present study, the VCS paradigm was used to investigate potential differences in magnocellular (M) vs. parvocellular (P) channel function that might account for the observed information processing deficits of schizophrenia spectrum patients. Specifically, VCS for near threshold luminance (black/white) stimuli is known to be governed primarily by theM channel, while VCS for near threshold chromatic (red/green) stimuli is governed by the P channel. Methods: VCS for luminance and chromatic stimuli (counterphase-reversing sinusoidal gratings, 1.22 c/degree, 8.3 Hz) was assessed in 53 patients with schizophrenia (including 5 offantipsychotic medication), 22 individuals diagnosed with schizotypal personality disorder and 53 healthy comparison subjects. Results: Schizophrenia spectrum groups demonstrated reduced VCS in both conditions relative to normals, and there was no significant group by condition interaction effect. Post-hoc analyses suggest that it was the patients with schizophrenia on antipsychotic medication as well as SPD participants who accounted for the deficits in the luminance condition. Conclusions: These results demonstrate visual information processing deficits in schizophrenia spectrum populations but do not support the notion of selective abnormalities in the function of subcortical channels as suggested by previous studies. Further work is needed in a longitudinal design to further assess VCS as a vulnerability marker for psychosis as well as the effect of antipsychotic agents on performance in schizophrenia spectrum populations. © 2013 Cadenhead, Dobkins, McGovern and Shafer.

Published

2013

174. Contrast dependence of motion-onset and pattern-reversal evoked potentials

Author

Henk Spekreijse, Miroslav Kuba, Colin Blakemore, and Zuzana Kubová

Subjects

Parvocellular, Adult, Time Factors, genetic structures, Motion Perception, Fixation, Ocular, Visual evoked potentials, Stimulus (physiology), Contrast Sensitivity, Nuclear magnetic resonance, Optics, Parvocellular cell, Humans, Motion onset, Visual Cortex, High contrast, business.industry, Chemistry, musculoskeletal, neural, and ocular physiology, Magnocellular, Contrast, Sensory Systems, Ophthalmology, Electrophysiology, Pattern reversal, Pattern Recognition, Visual, Motion pathway, Negative peak, Evoked Potentials, Visual, business, Human

Abstract

This study deals with the effect of stimulus contrast, between 1.3% and 96%, on the visual evoked potentials (VEPs) for onset of motion and for pattern reversal of checkerboard stimuli. The VEPs for pattern reversal and for the onset of motion both contain an initial positive peak (P1; peak latency about 120 msec) followed by a later negative peak (N2; peak latency 160–200 msec). However the P1 peak dominates the pattern-reversal VEP when recorded from the midline occipital lead, where it is maximal, while the N2 peak is larger in the motion-onset VEP, especially when recorded from unipolar lateral occipital leads. Whereas the amplitude of the P1 peak in both the pattern-reversal VEP and the motion-onset VEP decreases with decreasing contrast (becoming undetectable at a contrast of about 2% for the motion-onset VEP), the amplitude of the N2 peak in both types of VEP does not vary significantly with contrast, above a contrast of 1.3%. The increase in peak latency with decreasing contrast is also more pronounced for the positive than the negative peaks of both types of VEP. Taking into account the high contrast sensitivity of the magnocellular system (thought to be involved in the processing of motion) compared with the parvocellular system (probably more concerned with the processing of form), our findings suggest that for both motion-onset and pattern-reversal VEPs the negative peak is attributable to the motion-processing magnocellular pathway and the positive peak to the form-processing parvocellular system.

Published

1995

175. Functional mapping of the magnocellular and parvocellular subdivisions of human LGN.

Author

Denison, Rachel N, Denison, Rachel N, Vu, An T, Yacoub, Essa, Feinberg, David A, Silver, Michael A, Denison, Rachel N, Denison, Rachel N, Vu, An T, Yacoub, Essa, Feinberg, David A, and Silver, Michael A

Abstract

The magnocellular (M) and parvocellular (P) subdivisions of primate LGN are known to process complementary types of visual stimulus information, but a method for noninvasively defining these subdivisions in humans has proven elusive. As a result, the functional roles of these subdivisions in humans have not been investigated physiologically. To functionally map the M and P subdivisions of human LGN, we used high-resolution fMRI at high field (7 T and 3 T) together with a combination of spatial, temporal, luminance, and chromatic stimulus manipulations. We found that stimulus factors that differentially drive magnocellular and parvocellular neurons in primate LGN also elicit differential BOLD fMRI responses in human LGN and that these responses exhibit a spatial organization consistent with the known anatomical organization of the M and P subdivisions. In test-retest studies, the relative responses of individual voxels to M-type and P-type stimuli were reliable across scanning sessions on separate days and across sessions at different field strengths. The ability to functionally identify magnocellular and parvocellular regions of human LGN with fMRI opens possibilities for investigating the functions of these subdivisions in human visual perception, in patient populations with suspected abnormalities in one of these subdivisions, and in visual cortical processing streams arising from parallel thalamocortical pathways.

Published

2014

176. Développement des voies visuelles primaires au cours de la première année de vie chez le bébé prématuré et le béné né à terme : une étude en électrophysiologie à haute densité

Author

Tremblay, Emmanuel, Lepore, Franco, and McKerral, Michelle

Subjects

Parvocellular, Enfant, Brain topography, Vision, Magnocellulaire, Magnocellular, Topographie, Contraste, Contrast, Brain development, Aires extrastriées, Potentiel évoqué, Fréquences spatiales, Visual maturation, Visual evoked potentials, Spatial frequency, Parvocellulaire, Infants, Développement

Abstract

Thèse numérisée par la Division de la gestion de documents et des archives de l'Université de Montréal.

Published

2009

177. Schizophrenia spectrum participants have reduced visual contrast sensitivity to chromatic (red/green) and luminance (light/dark) stimuli: new insights into information processing, visual channel function, and antipsychotic effects.

Author

Cadenhead, Kristin S, Cadenhead, Kristin S, Dobkins, Karen, McGovern, Jessica, Shafer, Kathleen, Cadenhead, Kristin S, Cadenhead, Kristin S, Dobkins, Karen, McGovern, Jessica, and Shafer, Kathleen

Abstract

BackgroundIndividuals with schizophrenia spectrum diagnoses have deficient visual information processing as assessed by a variety of paradigms including visual backward masking, motion perception and visual contrast sensitivity (VCS). In the present study, the VCS paradigm was used to investigate potential differences in magnocellular (M) vs. parvocellular (P) channel function that might account for the observed information processing deficits of schizophrenia spectrum patients. Specifically, VCS for near threshold luminance (black/white) stimuli is known to be governed primarily by the M channel, while VCS for near threshold chromatic (red/green) stimuli is governed by the P channel.MethodsVCS for luminance and chromatic stimuli (counterphase-reversing sinusoidal gratings, 1.22 c/degree, 8.3 Hz) was assessed in 53 patients with schizophrenia (including 5 off antipsychotic medication), 22 individuals diagnosed with schizotypal personality disorder and 53 healthy comparison subjects.ResultsSchizophrenia spectrum groups demonstrated reduced VCS in both conditions relative to normals, and there was no significant group by condition interaction effect. Post-hoc analyses suggest that it was the patients with schizophrenia on antipsychotic medication as well as SPD participants who accounted for the deficits in the luminance condition.ConclusionsThese results demonstrate visual information processing deficits in schizophrenia spectrum populations but do not support the notion of selective abnormalities in the function of subcortical channels as suggested by previous studies. Further work is needed in a longitudinal design to further assess VCS as a vulnerability marker for psychosis as well as the effect of antipsychotic agents on performance in schizophrenia spectrum populations.

Published

2013

178. Biased Oxytocinergic Modulation of Midbrain Dopamine Systems.

Author

Xiao, Lei, Priest, Michael F., Nasenbeny, Jordan, Lu, Ting, and Kozorovitskiy, Yevgenia

Subjects

*DOPAMINE, *OXYTOCIN, *ELECTROPHYSIOLOGY, *G proteins, *G protein coupled receptors

Abstract

Summary The release of dopamine (DA) regulates rewarding behavior and motor actions through striatum-targeting efferents from ventral tegmental area (VTA) and substantia nigra pars compacta (SNc). Here, we map and functionally characterize axonal projections from oxytocin neurons in the hypothalamic paraventricular nucleus to midbrain DA regions. Electrophysiological recordings of DA neurons reveal that both the application of oxytocin and optogenetic stimulation of oxytocinergic terminals suffice to increase DA neuron activity in the VTA but downregulate it in SNc. This biased modulation is mediated by oxytocin and vasopressin G-protein-coupled receptors. Oxytocin release directly activates DA neurons and indirectly inhibits them through local GABA neurons, but the relative magnitudes of the two mechanisms differ in VTA and SNc. Oxytocin-modulated DA neurons give rise to canonical striatal projections. Since hypothalamic oxytocinergic projections also target the striatum, oxytocin is poised to bias the balance of DA tone through multiple sites in vertebrate reward circuits. [ABSTRACT FROM AUTHOR]

Published

2017

179. Psychophysical assessment of magno- and parvocellular function in schizophrenia

Author

Kenneth Knoblauch, Maria Giovanna Ducato, Frédéric Devinck, Sandrine Delord, Pierre Thomas, Delphine Pins, Muriel Boucart, Equipe de Psychologie Cognitive, Université Bordeaux Segalen - Bordeaux 2-EA3662, Neurosciences fonctionnelles et pathologies (NFP), Université de Picardie Jules Verne (UPJV)-CHU Amiens-Picardie-Université de Lille, Droit et Santé-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Centre National de la Recherche Scientifique (CNRS), Section of Neurobiology, Physiology and Behavior, Department of Ophthalmology, University of California [Davis] (UC Davis), University of California-University of California, Cerveau et vision, Institut National de la Recherche Agronomique (INRA)-Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-IFR19-Institut National de la Santé et de la Recherche Médicale (INSERM), Knoblauch, Kenneth, and University of California (UC)-University of California (UC)

Subjects

Male, Light, genetic structures, Physiology, Motion Perception, Luminance, 0302 clinical medicine, Discrimination, Psychological, Psychophysics, MESH: Discrimination (Psychology), MESH: Contrast Sensitivity, MESH: Middle Aged, Middle Aged, Sensory Systems, MESH: Photic Stimulation, Pattern Recognition, Visual, MESH: Motion Perception, [SDV.MHEP.OS] Life Sciences [q-bio]/Human health and pathology/Sensory Organs, Female, Schizophrenic Psychology, [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Psychology, Cognitive psychology, MESH: Schizophrenic Psychology, Adult, Parvocellular, MESH: Space Per, Adolescent, MESH: Pattern Recognition, Visual, Stimulus (physiology), MESH: Psychophysics, Contrast Sensitivity, 03 medical and health sciences, Judgment, Parvocellular cell, Humans, Visual Pathways, [SDV.NEU] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], [SDV.MHEP.OS]Life Sciences [q-bio]/Human health and pathology/Sensory Organs, MESH: Adolescent, MESH: Judgment, MESH: Humans, Magnocellular, MESH: Adult, MESH: Schizophrenia, MESH: Light, MESH: Male, 030227 psychiatry, nervous system, Space Perception, Schizophrenia, sense organs, Neuroscience, MESH: Female, 030217 neurology & neurosurgery, Photic Stimulation

Abstract

Recently developed psychophysical techniques permit the biasing of the processing of the stimulus by early visual channels so that responses reflect characteristics of either magno- or parvocellular pathways (Pokorny & Smith, 1997). We used such techniques to test psychophysically whether the global magnocellular dysfunction reported in schizophrenia also affects early processes. Seven schizophrenic patients and 19 normal controls participated. The task was a four-alternative forced-choice luminance discrimination, using a 2 × 2 configuration of four 1-deg squares. Target luminance threshold was determined in three conditions: the stimulus, including the target, was pulsed for 17 ms (pulse paradigm); the target was presented on a steady background of four squares (steady paradigm), or the target was presented alone (no background paradigm). We replicated previous results demonstrating magnocellular and parvocellular signatures in control participants. No evidence for an early magnocellular deficit could be detected as the thresholds of all schizophrenic observers were higher both in the steady paradigm (presumed magnocellular mediation) and in the pulse paradigm (presumed parvocellular mediation). Magnocellular dysfunction, if present in schizophrenia, must concern more integrated processes, possibly at levels at which parvocellular and magnocellular paths interact.

Published

2006

180. Development of neuroendocrine neurons in the mammalian hypothalamus.

Author

Alvarez-Bolado G

Subjects

Animals, Cell Movement, Gene Regulatory Networks, Hypothalamus cytology, Mammals metabolism, Neurons cytology, Neurosecretory Systems cytology

Abstract

The neuroendocrine system consists of a heterogeneous collection of (mostly) neuropeptidergic neurons found in four hypothalamic nuclei and sharing the ability to secrete neurohormones (all of them neuropeptides except dopamine) into the bloodstream. There are, however, abundant hypothalamic non-neuroendocrine neuropeptidergic neurons developing in parallel with the neuroendocrine system, so that both cannot be entirely disentangled. This heterogeneity results from the workings of a network of transcription factors many of which are already known. Olig2 and Fezf2 expressed in the progenitors, acting through mantle-expressed Otp and Sim1, Sim2 and Pou3f2 (Brn2), regulate production of magnocellular and anterior parvocellular neurons. Nkx2-1, Rax, Ascl1, Neurog3 and Dbx1 expressed in the progenitors, acting through mantle-expressed Isl1, Dlx1, Gsx1, Bsx, Hmx2/3, Ikzf1, Nr5a2 (LH-1) and Nr5a1 (SF-1) are responsible for tuberal parvocellular (arcuate nucleus) and other neuropeptidergic neurons. The existence of multiple progenitor domains whose progeny undergoes intricate tangential migrations as one source of complexity in the neuropeptidergic hypothalamus is the focus of much attention. How neurosecretory cells target axons to the medial eminence and posterior hypophysis is gradually becoming clear and exciting progress has been made on the mechanisms underlying neurovascular interface formation. While rat neuroanatomy and targeted mutations in mice have yielded fundamental knowledge about the neuroendocrine system in mammals, experiments on chick and zebrafish are providing key information about cellular and molecular mechanisms. Looking forward, data from every source will be necessary to unravel the ways in which the environment affects neuroendocrine development with consequences for adult health and disease.

Published

2019

181. Differential magnocellular versus parvocellular pathway contributions to the combinatorial processing of facial threat.

Author

Adams RB Jr, Im HY, Cushing C, Boshyan J, Ward N, Albohn DN, and Kveraga K

Subjects

Adult, Amygdala physiology, Cues, Female, Humans, Magnetic Resonance Imaging, Male, Nerve Net physiology, Photic Stimulation methods, Brain physiology, Facial Expression, Fear psychology

Abstract

Recently, speed of presentation of facially expressive stimuli was found to influence the processing of compound threat cues (e.g., anger/fear/gaze). For instance, greater amygdala responses were found to clear (e.g., direct gaze anger/averted gaze fear) versus ambiguous (averted gaze anger/direct gaze fear) combinations of threat cues when rapidly presented (33 and 300ms), but greater to ambiguous versus clear threat cues when presented for more sustained durations (1, 1.5, and 2s). A working hypothesis was put forth (Adams et al., 2012) that these effects were due to differential magnocellular versus parvocellular pathways contributions to the rapid versus sustained processing of threat, respectively. To test this possibility directly here, we restricted visual stream processing in the fMRI environment using facially expressive stimuli specifically designed to bias visual input exclusively to the magnocellular versus parvocellular pathways. We found that for magnocellular-biased stimuli, activations were predominantly greater to clear versus ambiguous threat-gaze pairs (on par with that previously found for rapid presentations of threat cues), whereas activations to ambiguous versus clear threat-gaze pairs were greater for parvocellular-biased stimuli (on par with that previously found for sustained presentations). We couch these findings in an adaptive dual process account of threat perception and highlight implications for other dual process models within psychology., (© 2019 Elsevier B.V. All rights reserved.)

Published

2019

182. Low spatial frequency contrast sensitivity deficits in migraine are not visual pathway selective

Author

McKendrick, Allison, Sampson, Geoff, McKendrick, Allison, and Sampson, Geoff

Published

2009

183. Independent patterns of damage within magno-, parvo- and koniocellular pathways in Parkinson's disease

Author

Cristina Januário, Vasco Forjaz, Frederico S. Regateiro, Maria Fátima Silva, António Freire, Pedro Faria, and Miguel Castelo-Branco

Subjects

Parvocellular, Male, Aging, Fovea Centralis, Parkinson's disease, genetic structures, media_common.quotation_subject, Population, Koniocellular, Vision Disorders, Frequency-doubling illusion, Visual system, Retina, Contrast Sensitivity, Parvocellular cell, Sensory threshold, Neural Pathways, medicine, Psychophysics, Contrast (vision), Humans, Contrast sensitivity, education, media_common, education.field_of_study, Magnocellular, Parkinson Disease, Middle Aged, medicine.disease, Illusions, Koniocellular cell, Sensory Thresholds, Parkinson’s disease, Visual Perception, Female, Neurology (clinical), Psychology, Neuroscience, Color Perception, Photic Stimulation

Abstract

Sensory deficits have been documented in Parkinson's disease, in particular within the visual domain. However, ageing factors related to the brain and to neural and non-neural ocular structures could explain some of the previously reported results, in particular the claimed impairment within the koniocellular pathway. This study addressed visual impairment attributable to the magno- (luminance), parvo- (red-green) and koniocellular (blue-yellow) pathways in a population of Parkinson's disease patients. To avoid potentially confounding factors, all subjects underwent a full neurophthalmological assessment which led to exclusion of subjects with increased intraocular pressure, diabetes even in the absence of retinopathy, and ocular abnormalities (from a total of 72 patients' eyes, 12 were excluded). Both parvo- and koniocellular pathways were studied by means of contrast sensitivity (CS) measurements along protan, tritan and deutan axes and also by fitting chromatic discrimination ellipses using eight measured contrast axes. Magnocellular function was assessed, using stimuli that induce a frequency doubling illusion, in 17 locations in the fovea and periphery. Achromatic (luminance modulation) thresholds were significantly higher in Parkinson's disease both in foveal and peripheral locations. A significant impairment was observed along protan and deutan axes, but only marginally along the tritan axis. These results were corroborated by a significant elongation of chromatic discrimination ellipses in our Parkinson's disease group. Correlation analysis showed that achromatic and chromatic CS measures were independent, which implies that multiple visual pathways are affected independently in Parkinson's disease. Magnocellular impairment was significantly correlated with age and disease stage, in contrast to the measured chromatic deficits. We conclude that in Parkinson's disease, independent damage occurs in the early magno- and parvocellular pathways. Furthermore, traditional koniocellular probing strategies in Parkinson's disease may be confounded by ageing factors, which may reconcile the previously reported controversial findings concerning chromatic impairment in Parkinson's disease.

Published

2005

184. The spatial structure of cone-opponent receptive fields in macaque retina.

Author

Lee BB, Cooper B, and Cao D

Subjects

Animals, Color Perception physiology, Macaca fascicularis, Photic Stimulation, Retinal Cone Photoreceptor Cells physiology, Retinal Ganglion Cells physiology, Visual Fields physiology

Abstract

The receptive field structure of long (L) to middle (M) wavelength (L/M) cone-opponent ganglion cells of the parafoveal macaque retina was investigated using drifting gratings. Gratings were luminance, chromatic or selective for the L- or M-cones. Based on these spatial tuning curves, receptive field profiles for the individual cones were derived. Receptive field profiles were coarse compared to single cones, and often could not be described by a simple Gaussian, having shallower flanks. There was a continuum of spatial properties, which blurred any systematic distinction between Type I and Type II receptive fields. Opponent center-surround organization within a single cone was rare. Usually, responses to all four grating types could be described based on the cone receptive field profiles. An exception was a few cells that showed irregularities of amplitude and phase at high spatial frequencies for one or other of the cone isolating conditions. The data are related to standard models of M/L opponent receptive fields and implications for central processing are considered., (Copyright © 2017. Published by Elsevier Ltd.)

Published

2018

185. Extrafoveally applied flashing light affects contrast thresholds of achromatic and S-cone isolating, but not L-M cone modulated stimuli.

Author

Őze A, Puszta A, Buzás P, Kóbor P, Braunitzer G, and Nagy A

Subjects

Adult, Female, Humans, Male, Photic Stimulation, Visual Pathways physiology, Young Adult, Color Perception physiology, Contrast Sensitivity physiology, Retinal Cone Photoreceptor Cells physiology, Sensory Thresholds physiology

Abstract

Flashing light stimulation is often used to investigate the visual system. However, the magnitude of the effect of this stimulus on the various subcortical pathways is not well investigated. The signals of conscious vision are conveyed by the magnocellular, parvocellular and koniocellular pathways. Parvocellular and koniocellular pathways (or more precisely, the L-M opponent and S-cone isolating channels) can be accessed by isoluminant red-green (L-M) and S-cone isolating stimuli, respectively. The main goal of the present study was to explore how costimulation with strong white extrafoveal light flashes alters the perception of stimuli specific to these pathways. Eleven healthy volunteers with negative neurological and ophthalmological history were enrolled for the study. Isoluminance of L-M and S-cone isolating sine-wave gratings was set individually, using the minimum motion procedure. The contrast thresholds for these stimuli as well as for achromatic gratings were determined by an adaptive staircase procedure where subjects had to indicate the orientation (horizontal, oblique or vertical) of the gratings. Thresholds were then determined again while a strong white peripheral light flash was presented 50 ms before each trial. Peripheral light flashes significantly (p < 0.05) increased the contrast thresholds of the achromatic and S-cone isolating stimuli. The threshold elevation was especially marked in case of the achromatic stimuli. However, the contrast threshold for the L-M stimuli was not significantly influenced by the light flashes. We conclude that extrafoveally applied light flashes influence predominantly the perception of achromatic stimuli., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

186. The Importance of Spatial Visual Scene Parameters in Predicting Optimal Cone Sensitivities in Routinely Trichromatic Frugivorous Old-World Primates.

Author

Matthews T, Osorio D, Cavallaro A, and Chittka L

Abstract

Computational models that predict the spectral sensitivities of primate cone photoreceptors have focussed only on the spectral, not spatial, dimensions. On the ecologically valid task of foraging for fruit, such models predict the M-cone ("green") peak spectral sensitivity 10-20 nm further from the L-cone ("red") sensitivity peak than it is in nature and assume their separation is limited by other visual constraints, such as the requirement of high-acuity spatial vision for closer M and L peak sensitivities. We explore the possibility that a spatio-chromatic analysis can better predict cone spectral tuning without appealing to other visual constraints. We build a computational model of the primate retina and simulate chromatic gratings of varying spatial frequencies using measured spectra. We then implement the case study of foveal processing in routinely trichromatic primates for the task of discriminating fruit and leaf spectra. We perform an exhaustive search for the configurations of M and L cone spectral sensitivities that optimally distinguish the colour patterns within these spectral images. Under such conditions, the model suggests that: (1) a long-wavelength limit is required to constrain the L cone spectral sensitivity to its natural position; (2) the optimal M cone peak spectral sensitivity occurs at ~525 nm, close to the observed position in nature (~535 nm); (3) spatial frequency has a small effect upon the spectral tuning of the cones; (4) a selective pressure toward less correlated M and L spectral sensitivities is provided by the need to reduce noise caused by the luminance variation that occurs in natural scenes.

Published

2018

187. Tracking changes in spatial frequency sensitivity during natural image processing in school age: an event-related potential study.

Author

Rokszin AA, Győri-Dani D, Bácsi J, Nyúl LG, and Csifcsák G

Subjects

Adolescent, Age Factors, Child, Female, Humans, Male, Oculomotor Nuclear Complex physiology, Reaction Time physiology, Child Development physiology, Evoked Potentials, Visual physiology, Pattern Recognition, Visual physiology, Photic Stimulation methods, Space Perception physiology

Abstract

Several studies have shown that behavioral and electrophysiological correlates of processing visual images containing low or high spatial frequency (LSF or HSF) information undergo development after early childhood. However, the maturation of spatial frequency sensitivity during school age has been investigated using abstract stimuli only. The aim of the current study was to assess how LSF and HSF features affect the processing of everyday photographs at the behavioral and electrophysiological levels in children aged 7-15 years and adults. We presented grayscale images containing either animals or vehicles and their luminance-matched modified versions filtered at low or high spatial frequencies. Modulations of classification accuracy, reaction time, and visual event-related potentials (posterior P1 and N1 components) were compared across five developmental groups and three image types. We found disproportionately worse response accuracies for LSF stimuli relative to HSF images in children aged 7 or 8 years, an effect that was accompanied by smaller LSF-evoked P1 amplitudes during this age period. At 7 or 8 years of age, P1 and N1 amplitudes were modulated by HSF and LSF stimuli (P1: HSF > LSF; N1: LSF > HSF), with a gradual shift toward the opposite pattern (P1: LSF > HSF; N1: HSF > LSF) with increasing age. Our results indicate that early cortical processing of both spatial frequency ranges undergo substantial development during school age, with a relative delay of LSF analysis, and underline the utility of our paradigm in tracking the maturation of LSF versus HSF sensitivity in this age group., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2018

188. Characteristics of contrast processing deficits in X-linked retinoschisis

Author

Gerald A. Fishman, Claire S. Barnes, and Kenneth R. Alexander

Subjects

Adult, Male, medicine.medical_specialty, Fovea Centralis, Visual acuity, genetic structures, Retinoschisis, Eye disease, parvocellular, Visual Acuity, 050105 experimental psychology, Contrast Sensitivity, 03 medical and health sciences, 0302 clinical medicine, Optics, Discrimination, Psychological, Optical coherence tomography, Parvocellular cell, Ophthalmology, medicine, Electroretinography, Psychophysics, Humans, 0501 psychology and cognitive sciences, 10. No inequality, Retina, magnocellular, medicine.diagnostic_test, business.industry, 05 social sciences, Macular degeneration, Middle Aged, medicine.disease, Sensory Systems, medicine.anatomical_structure, Case-Control Studies, Sensory Thresholds, 030221 ophthalmology & optometry, Female, sense organs, retinal disease, medicine.symptom, business, Tomography, Optical Coherence, Retinopathy

Abstract

Contrast sensitivity and contrast discrimination were evaluated in six males with X-linked retinoschisis (XLRS), a form of early-onset macular degeneration, using testing paradigms designed to favor either the magnocellular (MC) or parvocellular (PC) pathway. Compared to a group of age-similar control observers, the patients with XLRS showed a pronounced loss of contrast sensitivity at high spatial frequencies, consistent with their reduced visual acuities. At low spatial frequencies, the patients’ deficits were greater under conditions favoring the MC pathway, for both contrast sensitivity and contrast discrimination. The pattern of contrast sensitivity loss shown by the patients with XLRS could be simulated in control observers by testing at a parafoveal locus, although by optical coherence tomography, none of the patients with XLRS had eccentric fixation. The pattern of findings indicates that the foveas of patients with XLRS functionally resemble the normal parafoveal retina.

Published

2004

189. Interactions between luminance and colour channels in visual search and their relationship to parallel neural channels in vision

Author

Li, Josephine, Sampson, Geoff, Vidyasagar, Trichur, Li, Josephine, Sampson, Geoff, and Vidyasagar, Trichur

Published

2007

190. The spatiotemporal precision of ganglion cell signals: a comparison of physiological and psychophysical performance with moving gratings

Author

Barry B. Lee, Hao Sun, and Lukas Rüttiger

Subjects

Parvocellular, Retinal Ganglion Cells, genetic structures, Spatiotemporal, Motion Perception, Visual Acuity, law.invention, law, Parvocellular cell, Sensory threshold, medicine, Psychophysics, Animals, Humans, Motion perception, Physics, Retina, Fourier Analysis, Noise (signal processing), Vernier scale, Magnocellular, Contrast, Sensory Systems, Ophthalmology, Macaca fascicularis, medicine.anatomical_structure, Sensory Thresholds, Space Perception, Spatial frequency, Neuroscience, Photic Stimulation, Vernier

Abstract

Comparison of the spatiotemporal information delivered by ganglion cells with human psychophysical performance may give insight to how retinal information is utilized by cortical mechanisms, and constrain models of spatiotemporal processing. Ganglion cells’ responses were measured with drifting gratings of various spatial and temporal frequencies and contrasts. The spatiotemporal precision of cell responses was estimated in terms of a noise measure and phase variation, and compared to human vernier performance. Noise and phase variation of magnocellular (MC) cells was least at low temporal frequencies, despite their transient responses. The patterns of spatiotemporal precision of MC cells resembled the patterns of human vernier thresholds while those of parvocellular cells did not, implying use of MC cells’ signals in these tasks. The analysis further implied that cortical mechanisms must perform a sophisticated spatiotemporal analysis over local ganglion cell arrays.

Published

2003

191. The chromatic input to global motion perception

Author

Marco Bertamini, Sophie Wuerger, and Alexa I. Ruppertsberg

Subjects

Parvocellular, Light, Color vision, Physiology, Color, Cone-opponent mechanisms, Isoluminance, Koniocellular, Motion, Random-dot kinematogram, Sensory Systems, Motion Perception, Luminance, Motion (physics), Contrast Sensitivity, Psychophysics, Humans, Computer vision, Motion perception, Chromatic scale, Communication, business.industry, Koniocellular cell, Sensory Thresholds, Human visual system model, Retinal Cone Photoreceptor Cells, Visual Perception, Artificial intelligence, business, Psychology, Artifacts, Color Perception, Photic Stimulation

Abstract

For over 30 years there has been a controversy over whether color-defined motion can be perceived by the human visual system. Some results suggest that there is no chromatic motion mechanism at all, whereas others do find evidence for a purely chromatic motion mechanism. Here we examine the chromatic input to global motion processing for a range of color directions in the photopic luminance range. We measure contrast thresholds for global motion identification and simple detection using sparse random-dot kinematograms. The results show a discrepancy between the two chromatic axes: whereas it is possible for observers to perform the global motion task for stimuli modulated along the red–green axis, we could not assess the contrast threshold required for stimuli modulated along the yellowish-violet axis. The contrast required for detection for both axes, however, are well below the contrasts required for global motion identification. We conclude that there is a significant red–green input to global motion processing providing further evidence for the involvement of the parvocellular pathway. The lack of S-cone input to global motion processing suggests that the koniocellular pathway mediates the detection but not the processing of complex motion for our parameter range.

Published

2003

192. Spatial and temporal chromatic contrast: Effects on chromatic discrimination for stimuli varying in L- and M-cone excitation

Author

Zele, Andrew, Smith, Vivianne, Pokorny, Joel, Zele, Andrew, Smith, Vivianne, and Pokorny, Joel

Abstract

Discrimination for equiluminant chromatic stimuli that vary in L- and M-cone excitation depends on the chromaticity difference between the test field and the surrounding area. The current study investigated the effect of the proximity in space and time of a surround to the test field on chromatic contrast discrimination. The experimental paradigm isolated spatial, temporal, and spatial-and-temporal chromatic contrast effects on discrimination. Chromatic contrast discrimination thresholds were assessed by a four-alternative spatial forced-choice procedure. Stimuli were either metameric to the equal energy spectrum, or varied in L-cone activation along a line of constant S-cone activation. A model based on primate parvocellular pathway physiology described the data. Spatial and temporal contrast produced equivalent reductions in chromatic discriminability as the chromatic difference between the test and surround increased. For all test chromaticities, discrimination was best in the absence of chromatic contrast. Chromatic contrast discrimination is determined by either the spatial or temporal contrast component of the signal.

Published

2006

193. Modulation sensitivity of ganglion cells in peripheral retina of macaque

Author

Lukas Rüttiger, Paul R. Martin, Barry B. Lee, Samuel G. Solomon, and Andrew White

Subjects

Parvocellular, Retinal Ganglion Cells, Time Factors, genetic structures, media_common.quotation_subject, Flicker fusion threshold, Biology, Temporal, Macaque, Contrast Sensitivity, Flicker Fusion, 03 medical and health sciences, 0302 clinical medicine, Parvocellular cell, biology.animal, medicine, Psychophysics, Contrast (vision), Animals, 030304 developmental biology, media_common, 0303 health sciences, Retina, Flicker, Magnocellular, Contrast, Sensory Systems, eye diseases, Peripheral, Ganglion, Ophthalmology, medicine.anatomical_structure, Sensory Thresholds, Macaca, sense organs, Neuroscience, 030217 neurology & neurosurgery, Photic Stimulation

Abstract

There is ample psychophysical evidence that flicker is more salient in the peripheral than the central visual field, but the physiological basis of this eccentricity-dependant change is unclear. Here, we compared responsivity to temporal modulation of ganglion cells in central and peripheral primate retina. Above 30 Hz modulation frequency, both magnocellular (MC) and parvocellular (PC) pathway cells are more responsive in peripheral retina. This suggests that an increase in high-frequency temporal responsiveness arises in outer retina before the MC and PC pathways diverge. In both central and peripheral retina, the critical fusion frequency of MC cells is higher than that of PC cells. This result is consistent with other evidence that psychophysical flicker sensitivity is mediated by the MC pathway.

Published

2002

194. Neuropeptide expression in rat paraventricular hypothalamic neurons that project to the spinal cord

Author

Hallbeck, Martin, Larhammar, Dan, Blomqvist, Anders, Hallbeck, Martin, Larhammar, Dan, and Blomqvist, Anders

Abstract

The paraventricular hypothalamic nucleus (PVH) exerts many of its regulatory functions through projections to spinal cord neurons that control autonomic and sensory functions. By using in situ hybridization histochemistry in combination with retrograde tract tracing, we analyzed the peptide expression among neurons in the rat PVH that send axons to the spinal cord. Projection neurons were labeled by immunohistochemical detection of retrogradely transported cholera toxin subunit B, and radiolabeled long riboprobes were used to identify neurons containing dynorphin, enkephalin, or oxytocin mRNA. Of the spinally projecting neurons in the PVH, approximately 40% expressed dynorphin mRNA, 40% expressed oxytocin mRNA, and 20% expressed enkephalin mRNA. Taken together with our previous findings on the distribution of vasopressin-expressing neurons in the PVH (Hallbeck and Blomqvist [1999] J. Comp. Neurol. 411:201–211), the results demonstrated that the different PVH subdivisions display distinct peptide expression patterns among the spinal cord–projecting neurons. Thus, the lateral parvocellular subdivision contained large numbers of spinal cord–projecting neurons that express any of the four investigated peptides, whereas the ventral part of the medial parvocellular subdivision displayed a strong preponderance for dynorphin- and vasopressin-expressing cells. The dorsal parvocellular subdivision almost exclusively contained dynorphin- and oxytocin-expressing spinal cord–projecting neurons. This parcellation of the peptide-expressing neurons suggested a functional diversity among the spinal cord–projecting subdivisions of the PVH that provide an anatomic basis for its various and distinct influences on autonomic and sensory processing at the spinal level.

Published

2001

195. Dynorphin mRNA-expressing neurons in the rat paraventricular hypothalamic nucleus project to the spinal cord

Author

Hallbeck, Martin and Hallbeck, Martin

Abstract

The opioid peptide dynorphin is important for the regulation of neuronal activity in the spinal cord. Because dynorphin is produced by neurons throughout the neuraxis, there are many putative sources for spinal dynorphin fibers, in addition to those originating from spinal cord neurons. Using a sensitive double-labeling technique combining in situ hybridization and tract tracing, the present study demonstrates that the paraventricular hypothalamic nucleus (PVH) of adult naı̈ve male Sprague–Dawley rats contains large numbers of dynorphin mRNA-producing cells with projections to the spinal cord. Thus, more than 40% of the spinally projecting neurons in PVH were found to express dynorphin mRNA. This novel finding suggests that the PVH is a major source of spinal dynorphin that may be of importance for the processing of pain and visceral information.

Published

2000

196. On using Vernier acuity to assess magnocellular sensitivity

Author

Skottun, Bernt C. and Skoyles, John R.

Subjects

*VISUAL acuity, *CELLULAR signal transduction, *SCHIZOPHRENIA, *AMBLYOPIA, *VISION disorders, *SENSITIVITY analysis

Abstract

Abstract: A recent study [Keri, S., & Benedek, G. (2009). Visual pathway deficit in female fragile × premutation carriers: A potential endophenotype. Brain and Cognition, 69, 291–295] has found Vernier acuity deficiencies together with contrast sensitivity defects consistent with a magnocellular deficit in female fragile × premutation carriers. This may appear to support the notion that Vernier acuity may serve as a test of magnocellular sensitivity. However, Vernier acuity deficiencies have been reported in other conditions (e.g., schizophrenia, amblyopia and cortical visual impairment) where there is little evidence for magnocellular deficits. The observation that Vernier acuity deficiencies can occur without magnocellular deficits indicates that Vernier acuity is not a reliable test of magnocellular sensitivity. [Copyright &y& Elsevier]

Published

2010

197. Interaction of Top-Down and Bottom-Up Search with Magnocellular- and Parvocellular-Mediated Stimuli

Author

Garrett, James Samuel

Subjects

Psychology, visual search, top-down, bottom-up, spatial frequency, magnocellular, parvocellular

Abstract

The current study simultaneously examined the potentiality of a magnocellular attentional advantage and the competition between top-down and bottom-up processing on attention during visual search as measured by covert and overt visual attention. Specifically, the study tested two opposing views of the competition between top-down and bottom-up processing. The contingent involuntary orienting hypothesis (Folk, Remington, & Johnston, 1992), states that goal directed search is not affected by target-irrelevant stimuli. In contrast, the distractor interference paradigm (Theeuwes, 1994), states that goal directed search can be affected by target-irrelevant stimuli if more salient than the rest of the search array. The study utilized a search array of contrast-equated orientation and spatial frequency modulated Gabor patches to preferentially activate the magnocellular and parvocellular visual streams in order to test for a magnocellular attentional advantage. Participants were asked to find a singleton target Gabor patch amongst a field of distractor Gabor patches. The results were mixed. Top-down search for a spatial frequency singleton provided support for the distractor interference paradigm while top-down search for an orientation singleton provided support for the contingent involuntary orientating hypothesis. These mixed results suggest top-down versus bottom-up search is more complicated than these two theories suggest. By demonstrating the effect of a target-irrelevant distractor on response time and accuracy, I provide that a bottom-up attentional priority exists when performing a top-down search for an orientation singleton, but not for a spatial frequency singleton. Additionally, the current study could find no evidence for a magnocellular attentional advantage.

Published

2016

198. Separate magnocellular and parvocellular contributions from temporal analysis of the multifocal VEP

Author

David P. Crewther, Alexander Klistorner, and Sheila G. Crewther

Subjects

Parvocellular, Adult, Retinal Ganglion Cells, genetic structures, Light, Adaptation (eye), Contrast Sensitivity, Optics, Parvocellular cell, Psychophysics, medicine, Humans, Latency (engineering), Evoked potential, Visual Cortex, business.industry, Magnocellular, Geniculate Bodies, Temporal analysis, Sensory Systems, Electrophysiology, Ophthalmology, Visual cortex, medicine.anatomical_structure, Magnocellular cell, Evoked Potentials, Visual, VEP, business, Psychology, Neuroscience

Abstract

Temporal analysis of the multifocal cortical visual evoked potential (VEP) was studied using pseudo-random (m-sequence) achromatic stimulation. The effects of variation of luminance contrast on the first-order response were complex. At low to mid contrasts (

Published

1997

199. Selective temporal interactions between processing streams with differential sensitivity for colour and luminance contrast

Author

Ute Leonards and Wolf Singer

Subjects

Parvocellular, Adult, Visual perception, Time Factors, genetic structures, Adolescent, Color vision, media_common.quotation_subject, pathways, Magnocellular pathways, Luminance, behavioral disciplines and activities, Colour-sensitive channels, Contrast Sensitivity, Optics, Parvocellular cell, Neural Pathways, medicine, Contrast (vision), Humans, Computer vision, Sensitivity (control systems), Lighting, media_common, Visual Cortex, business.industry, Middle Aged, Sensory Systems, Luminance-sensitive channels, Ophthalmology, Visual cortex, medicine.anatomical_structure, Spectrophotometry, Double flash, Temporal interactions, Artificial intelligence, Psychology, business, psychological phenomena and processes, Color Perception

Abstract

Temporal interactions between spatially separated visual stimuli were investigated in human observers. Subjects had to judge whether briefly presented targets consisted of a single or a double flash. Simultaneous presentation of unattended single or double flash distractors impaired performance if target and distractor followed different time courses, confirming previous findings. This interference occurred only when targets had high luminance contrast or were isoluminant and when distractors had high or low luminance contrast, but not when targets had low luminance contrast or when distractors were isoluminant. Low luminance contrast distractors strongly influenced high luminance contrast targets but not vice versa. These results suggest that (i) information about the precise temporal structure of stimuli is conveyed preferentially by the luminance-sensitive magnocellular system; and (ii) that this information influences judgements on the temporal patterning of signals transmitted by the colour-sensitive parvocellular system. © 1997 Elsevier Science Ltd. All rights reserved.

Published

1997

200. Spinal cord-projecting vasopressinergic neurons in the rat paraventricular hypothalamus

Author

Hallbeck, Martin, Blomqvist, Anders, Hallbeck, Martin, and Blomqvist, Anders

Abstract

The paraventricular hypothalamic nucleus (PVH) is a key structure for the maintenance of homeostasis. Homeostatic regulation includes modulation of signaling in the spinal cord. This may be exerted by neurons in the PVH with spinal projections. However, the PVH is not a homogeneous structure, but consists of anatomically and functionally distinct subdivisions. In this study, we have analyzed the distribution of spinal cord-projecting PVH neurons that express vasopressin, an important neuropeptide in autonomic regulation. Vasopressinergic neurons were identified with a radiolabeled riboprobe complementary to vasopressin mRNA combined with immunohistochemical labeling of retrogradely transported cholera toxin subunit b in spinally projecting neurons. More than 40% of the spinally projecting neurons in the PVH of naive Sprague-Dawley rats were found to express vasopressin mRNA. The lateral parvocellular subdivision and the ventral part of the medial parvocellular subdivision contained the densest distribution of spinal cord-projecting vasopressin mRNA-expressing neurons. The magnocellular subdivisions displayed large numbers of vasopressin mRNA-expressing neurons, but very few of those projected to the spinal cord. The dorsal parvocellular subdivision contained a large number of spinally projecting neurons, but very few of those expressed vasopressin mRNA. These findings show that the PVH gives rise to a major vasopressinergic projection to the spinal cord and that the spinal cord-projecting vasopressinergic neurons are parceled into anatomically distinct cell groups. This provides an anatomical basis for a selective activation of functionally different groups in the PVH as part of a behaviorally adaptive response, including modulation of autonomic activity and pain processing at the spinal level.

Published

1999