Dustin J. Hayden scite author profile

Stimulus-selective response plasticity (SRP) is a robust and lasting modification of primary visual cortex (V1) that occurs in response to exposure to novel visual stimuli. It is readily observed as a pronounced increase in the magnitude of visual evoked potentials (VEPs) recorded in response to phase-reversing grating stimuli in neocortical layer 4. The expression of SRP at the individual neuron level is equally robust, but the qualities vary depending on the neuronal type and how activity is measured. This form of plasticity is highly selective for stimulus features such as stimulus orientation, spatial frequency, and contrast. Several key insights into the significance and underlying mechanisms of SRP have recently been made. First, it occurs concomitantly and shares core mechanisms with behavioral habituation, indicating that SRP reflects the formation of long-term familiarity that can support recognition of innocuous stimuli. Second, SRP does not manifest within a recording session but only emerges after an off-line period of several hours that includes sleep. Third, SRP requires not only canonical molecular mechanisms of Hebbian synaptic plasticity within V1, but also the opposing engagement of two key subclasses of cortical inhibitory neuron: the parvalbumin- and somatostatin-expressing GABAergic interneurons. Fourth, pronounced shifts in the power of cortical oscillations from high frequency (gamma) to low frequency (alpha/beta) oscillations provide respective readouts of the engagement of these inhibitory neuronal subtypes following familiarization. In this article we will discuss the implications of these findings and the outstanding questions that remain to gain a deeper understanding of this striking form of experience-dependent plasticity.

show abstract

Normal sleep bouts are not essential for C. elegans survival and FoxO is important for compensatory changes in sleep

Bennett

Khoruzhik

Hayden

et al. 2018

BMC Neurosci

View full text Add to dashboard Cite

BackgroundSleep deprivation impairs learning, causes stress, and can lead to death. Notch and JNK-1 pathways impact C. elegans sleep in complex ways; these have been hypothesized to involve compensatory sleep. C. elegans DAF-16, a FoxO transcription factor, is required for homeostatic response to decreased sleep and DAF-16 loss decreases survival after sleep bout deprivation. Here, we investigate connections between these pathways and the requirement for sleep after mechanical stress.ResultsReduced function of Notch ligand LAG-2 or JNK-1 kinase resulted in increased time in sleep bouts during development. These animals were inappropriately easy to arouse using sensory stimulation, but only during sleep bouts. This constellation of defects suggested that poor quality sleep bouts in these animals might activate homeostatic mechanisms, driving compensatory increased sleep bouts. Testing this hypothesis, we found that DAF-16 FoxO function was required for increased sleep bouts in animals with defective lag-2 and jnk-1, as loss of daf-16 reduced sleep bouts back to normal levels. However, loss of daf-16 did not suppress arousal thresholds defects. Where DAF-16 function was required differed; in lag-2 and jnk-1 animals, daf-16 function was required in neurons or muscles, respectively, suggesting that disparate tissues can drive a coordinated response to sleep need. Sleep deprivation due to mechanical stimulation can cause death in many species, including C. elegans, suggesting that sleep is essential. We found that loss of sleep bouts in C. elegans due to genetic manipulation did not impact their survival, even in animals lacking DAF-16 function. However, we found that sleep bout deprivation was often fatal when combined with the concurrent stress of mechanical stimulation.ConclusionsTogether, these results in C. elegans confirm that Notch and JNK-1 signaling are required to achieve normal sleep depth, suggest that DAF-16 is required for increased sleep bouts when signaling decreases, and that failure to enter sleep bouts is not sufficient to cause death in C. elegans, unless paired with concurrent mechanical stress. These results suggest that mechanical stress may directly contribute to death observed in previous studies of sleep deprivation and/or that sleep bouts have a uniquely restorative role in C. elegans sleep.Electronic supplementary materialThe online version of this article (10.1186/s12868-018-0408-1) contains supplementary material, which is available to authorized users.

show abstract

Visual recognition is heralded by shifts in local field potential oscillations and inhibitory networks in primary visual cortex

Hayden

Montgomery

Cooke

et al. 2020

Preprint

View full text Add to dashboard Cite

Filtering out familiar, irrelevant stimuli eases the computational burden on the cerebral cortex. Inhibition is a candidate mechanism in this filtration process. Oscillations in the cortical local field potential (LFP) serve as markers of the engagement of different inhibitory neurons. In awake mice, we find pronounced changes in LFP oscillatory activity present in layer 4 of primary visual cortex (V1) with progressive stimulus familiarity. Over days of repeated stimulus presentation, low frequency (alpha/beta ∼15 Hz peak) power increases while high frequency (gamma ∼65 Hz peak) power decreases. This high frequency activity re-emerges when a novel stimulus is shown. Thus, high frequency power is a marker of novelty while low frequency power signifies familiarity. Two-photon imaging of neuronal activity reveals that parvalbumin-expressing inhibitory neurons disengage with familiar stimuli and reactivate to novelty, consistent with their known role in gamma oscillations, whereas somatostatin-expressing inhibitory neurons show opposing activity patterns, indicating a contribution to the emergence of lower frequency oscillations. We also reveal that stimulus familiarity and novelty have differential effects on oscillations and cell activity over a shorter timescale of seconds. Taken together with previous findings, we propose a model in which two interneuron circuits compete to drive familiarity or novelty encoding.

show abstract

scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.

Contact Info

customersupport@researchsolutions.com

10624 S. Eastern Ave., Ste. A-614

Henderson, NV 89052, USA

This site is protected by reCAPTCHA and the Google Privacy Policy and Terms of Service apply.

Blog Terms and Conditions API Terms Privacy Policy Contact Cookie Preferences Do Not Sell or Share My Personal Information

Made with 💙 for researchers

Part of the Research Solutions Family.

Dustin J. Hayden

Visual Recognition Is Heralded by Shifts in Local Field Potential Oscillations and Inhibitory Networks in Primary Visual Cortex

Stimulus-Selective Response Plasticity in Primary Visual Cortex: Progress and Puzzles

Normal sleep bouts are not essential for C. elegans survival and FoxO is important for compensatory changes in sleep

Visual recognition is heralded by shifts in local field potential oscillations and inhibitory networks in primary visual cortex

Contact Info

Product

Resources

About