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Dive into the research topics where Antal Berényi is active.

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Featured researches published by Antal Berényi.


Nature Neuroscience | 2012

A toolbox of Cre-dependent optogenetic transgenic mice for light-induced activation and silencing

Linda Madisen; Tianyi Mao; Henner Koch; Jia Min Zhuo; Antal Berényi; Shigeyoshi Fujisawa; Yun Wei A Hsu; Alfredo J. Garcia; Xuan Gu; Sébastien Zanella; Jolene Kidney; Hong Gu; Yimei Mao; Bryan M. Hooks; Edward S. Boyden; György Buzsáki; Jan-Marino Ramirez; Allan R. Jones; Karel Svoboda; Xue Han; Eric E. Turner; Hongkui Zeng

Cell type–specific expression of optogenetic molecules allows temporally precise manipulation of targeted neuronal activity. Here we present a toolbox of four knock-in mouse lines engineered for strong, Cre-dependent expression of channelrhodopsins ChR2-tdTomato and ChR2-EYFP, halorhodopsin eNpHR3.0 and archaerhodopsin Arch-ER2. All four transgenes mediated Cre-dependent, robust activation or silencing of cortical pyramidal neurons in vitro and in vivo upon light stimulation, with ChR2-EYFP and Arch-ER2 demonstrating light sensitivity approaching that of in utero or virally transduced neurons. We further show specific photoactivation of parvalbumin-positive interneurons in behaving ChR2-EYFP reporter mice. The robust, consistent and inducible nature of our ChR2 mice represents a significant advance over previous lines, and the Arch-ER2 and eNpHR3.0 mice are to our knowledge the first demonstration of successful conditional transgenic optogenetic silencing. When combined with the hundreds of available Cre driver lines, this optimized toolbox of reporter mice will enable widespread investigations of neural circuit function with unprecedented reliability and accuracy.


Science | 2012

Closed-Loop Control of Epilepsy by Transcranial Electrical Stimulation

Antal Berényi; Mariano Belluscio; Dun Mao; György Buzsáki

Current on Demand Deep brain electrical stimulation can be a successful therapy in Parkinsons disease, in depression, and in several other psychiatric diseases, especially in drug-resistant cases. Unfortunately, chronic, continuous stimulation is associated with multiple side effects. This could be alleviated by delivering the electrical perturbation only when it is necessary, using closed-loop stimulation. Such an approach is essential for epilepsy, where seizures occur very rarely but with serious consequences. In a rat model for epilepsy, Berényi et al. (p. 735) prevented seizures by transcranial electrical stimulation using a closed-loop system. Transcranial electrical stimulation was highly effective and reduced seizure duration, on average, by 60 %. In a rodent model of petit mal epilepsy, the onset of a seizure triggers an electrical pulse that cuts short the seizure. Many neurological and psychiatric diseases are associated with clinically detectable, altered brain dynamics. The aberrant brain activity, in principle, can be restored through electrical stimulation. In epilepsies, abnormal patterns emerge intermittently, and therefore, a closed-loop feedback brain control that leaves other aspects of brain functions unaffected is desirable. Here, we demonstrate that seizure-triggered, feedback transcranial electrical stimulation (TES) can dramatically reduce spike-and-wave episodes in a rodent model of generalized epilepsy. Closed-loop TES can be an effective clinical tool to reduce pathological brain patterns in drug-resistant patients.


Journal of Neurophysiology | 2014

Large-scale, high-density (up to 512 channels) recording of local circuits in behaving animals

Antal Berényi; Zoltán Somogyvári; A. Nagy; Lisa Roux; John Long; Shigeyoshi Fujisawa; Eran Stark; Anthony Leonardo; Tim Harris; György Buzsáki

Monitoring representative fractions of neurons from multiple brain circuits in behaving animals is necessary for understanding neuronal computation. Here, we describe a system that allows high-channel-count recordings from a small volume of neuronal tissue using a lightweight signal multiplexing headstage that permits free behavior of small rodents. The system integrates multishank, high-density recording silicon probes, ultraflexible interconnects, and a miniaturized microdrive. These improvements allowed for simultaneous recordings of local field potentials and unit activity from hundreds of sites without confining free movements of the animal. The advantages of large-scale recordings are illustrated by determining the electroanatomic boundaries of layers and regions in the hippocampus and neocortex and constructing a circuit diagram of functional connections among neurons in real anatomic space. These methods will allow the investigation of circuit operations and behavior-dependent interregional interactions for testing hypotheses of neural networks and brain function.


Neuron | 2014

Theta phase segregation of input-specific gamma patterns in entorhinal-hippocampal networks.

Erik W. Schomburg; Antonio Fernández-Ruiz; Kenji Mizuseki; Antal Berényi; Costas A. Anastassiou; Christof Koch; György Buzsáki

Precisely how rhythms support neuronal communication remains obscure. We investigated interregional coordination of gamma oscillations using high-density electrophysiological recordings in the rat hippocampus and entorhinal cortex. We found that 30-80 Hz gamma dominated CA1 local field potentials (LFPs) on the descending phase of CA1 theta waves during navigation, with 60-120 Hz gamma at the theta peak. These signals corresponded to CA3 and entorhinal input, respectively. Above 50 Hz, interregional phase-synchronization of principal cell spikes occurred mostly for LFPs in the axonal target domain. CA1 pyramidal cells were phase-locked mainly to fast gamma (>100 Hz) LFP patterns restricted to CA1, which were strongest at the theta trough. While theta phase coordination of spiking across entorhinal-hippocampal regions depended on memory demands, LFP gamma patterns below 100 Hz in the hippocampus were consistently layer specific and largely reflected afferent activity. Gamma synchronization as a mechanism for interregional communication thus rapidly loses efficacy at higher frequencies.


Neuron | 2012

Traveling Theta Waves along the Entire Septotemporal Axis of the Hippocampus

Jagdish Patel; Shigeyoshi Fujisawa; Antal Berényi; Sébastien Royer; Gyoergy Buzsaki

A topographical relationship exists between the hippocampus-entorhinal cortex and the neocortex. However, it is not known how these anatomical connections are utilized during information exchange and behavior. We recorded theta oscillations along the entire extent of the septotemporal axis of the hippocampal CA1 pyramidal layer. While the frequency of theta oscillation remained same along the entire long axis, the amplitude and coherence between recording sites decreased from dorsal to ventral hippocampus (VH). Theta phase shifted monotonically with distance along the longitudinal axis, reaching ∼180° between the septal and temporal poles. The majority of concurrently recorded units were phase-locked to the local field theta at all dorsoventral segments. The power of VH theta had only a weak correlation with locomotion velocity, and its amplitude varied largely independently from theta in the dorsal part. Thus, theta oscillations can temporally combine or segregate neocortical representations along the septotemporal axis of the hippocampus.


Proceedings of the National Academy of Sciences of the United States of America | 2014

Optogenetic activation of septal cholinergic neurons suppresses sharp wave ripples and enhances theta oscillations in the hippocampus

Marie Vandecasteele; Viktor Varga; Antal Berényi; Edit Papp; Péter Barthó; Laurent Venance; Tamás F. Freund; György Buzsáki

Significance Theta oscillations are a prominent rhythm of the brain occurring during active behavior and rapid eye movement sleep and thought to provide the temporal frame for the encoding of information. Acetylcholine modulation is a major player in hippocampal theta rhythm, as demonstrated by lesion and pharmacological manipulations of cholinergic receptors, yet the link between the activity of septal cholinergic neurons and the theta rhythm is not fully understood. We used specific optogenetic stimulation of the septo-hippocampal cholinergic neurons in the anesthetized and behaving mouse to decipher the effects of cholinergic stimulation on hippocampal network activity and show that in addition to promoting theta oscillations it suppresses sharp wave ripples and peri-theta band activity. Theta oscillations in the limbic system depend on the integrity of the medial septum. The different populations of medial septal neurons (cholinergic and GABAergic) are assumed to affect different aspects of theta oscillations. Using optogenetic stimulation of cholinergic neurons in ChAT-Cre mice, we investigated their effects on hippocampal local field potentials in both anesthetized and behaving mice. Cholinergic stimulation completely blocked sharp wave ripples and strongly suppressed the power of both slow oscillations (0.5–2 Hz in anesthetized, 0.5–4 Hz in behaving animals) and supratheta (6–10 Hz in anesthetized, 10–25 Hz in behaving animals) bands. The same stimulation robustly increased both the power and coherence of theta oscillations (2–6 Hz) in urethane-anesthetized mice. In behaving mice, cholinergic stimulation was less effective in the theta (4–10 Hz) band yet it also increased the ratio of theta/slow oscillation and theta coherence. The effects on gamma oscillations largely mirrored those of theta. These findings show that medial septal cholinergic activation can both enhance theta rhythm and suppress peri-theta frequency bands, allowing theta oscillations to dominate.


Neuron | 2015

Tools for probing local circuits: high-density silicon probes combined with optogenetics.

György Buzsáki; Eran Stark; Antal Berényi; Dion Khodagholy; Daryl R. Kipke; Euisik Yoon; Kensall D. Wise

To understand how function arises from the interactions between neurons, it is necessary to use methods that allow the monitoring of brain activity at the single-neuron, single-spike level and the targeted manipulation of the diverse neuron types selectively in a closed-loop manner. Large-scale recordings of neuronal spiking combined with optogenetic perturbation of identified individual neurons has emerged as a suitable method for such tasks in behaving animals. To fully exploit the potential power of these methods, multiple steps of technical innovation are needed. We highlight the current state-of-the-art in electrophysiological recording methods, combined with optogenetics, and discuss directions for progress. In addition, we point to areas where rapid development is in progress and discuss topics where near-term improvements are possible and needed.


Science | 2014

Spatially Distributed Local Fields in the Hippocampus Encode Rat Position

Gautam Agarwal; Ian H. Stevenson; Antal Berényi; Kenji Mizuseki; György Buzsáki; Friedrich T. Sommer

Extracting Spatial Information The location of a rat can be deciphered from hippocampal activity by detecting the firing of individual place-selective neurons. In contrast, the local field potential (LFP), which arises from the coherent voltage fluctuations of large hippocampal cell populations, has been hard to decode. Agarwal et al. (p. 626) worked out how to recover positional information exclusively from multiple-site LFP measurements in the rat hippocampus. The information was as precise as that derived from spiking place cells. The approach might also be applicable more generally for deciphering information from coherent population activity anywhere in the brain. Electrical fields within the hippocampus can now be decoded to reveal a rat’s location. Although neuronal spikes can be readily detected from extracellular recordings, synaptic and subthreshold activity remains undifferentiated within the local field potential (LFP). In the hippocampus, neurons discharge selectively when the rat is at certain locations, while LFPs at single anatomical sites exhibit no such place-tuning. Nonetheless, because the representation of position is sparse and distributed, we hypothesized that spatial information can be recovered from multiple-site LFP recordings. Using high-density sampling of LFP and computational methods, we show that the spatiotemporal structure of the theta rhythm can encode position as robustly as neuronal spiking populations. Because our approach exploits the rhythmicity and sparse structure of neural activity, features found in many brain regions, it is useful as a general tool for discovering distributed LFP codes.


The Journal of Neuroscience | 2013

Local generation and propagation of ripples along the septotemporal axis of the hippocampus.

Jagdish Patel; Erik W. Schomburg; Antal Berényi; Shigeyoshi Fujisawa; György Buzsáki

A topographical relationship exists between the septotemporal segments of the hippocampus and their entorhinal–neocortical targets, but the physiological organization of activity along the septotemporal axis is poorly understood. We recorded sharp-wave ripple patterns in rats during sleep from the entire septotemporal axis of the CA1 pyramidal layer. Qualitatively similar ripples emerged at all levels. From the local seed, ripples traveled septally or temporally at a speed of ∼0.35 m/s, and the spatial spread depended on ripple magnitude. Ripples propagated smoothly across the septal and intermediate segments of the hippocampus, but ripples in the temporal segment often remained isolated. These findings show that ripples can combine information from the septal and intermediate hippocampus and transfer integrated signals downstream. In contrast, ripples that emerged in the temporal pole broadcast largely independent information to their cortical and subcortical targets.


Journal of Visualized Experiments | 2012

Large-scale Recording of Neurons by Movable Silicon Probes in Behaving Rodents

Marie Vandecasteele; Sébastien Royer; Mariano Belluscio; Antal Berényi; Kamran Diba; Shigeyoshi Fujisawa; Andres Grosmark; Dun Mao; Kenji Mizuseki; Jagdish Patel; Eran Stark; David Sullivan; Brendon O. Watson; György Buzsáki

A major challenge in neuroscience is linking behavior to the collective activity of neural assemblies. Understanding of input-output relationships of neurons and circuits requires methods with the spatial selectivity and temporal resolution appropriate for mechanistic analysis of neural ensembles in the behaving animal, i.e. recording of representatively large samples of isolated single neurons. Ensemble monitoring of neuronal activity has progressed remarkably in the past decade in both small and large-brained animals, including human subjects. Multiple-site recording with silicon-based devices are particularly effective because of their scalability, small volume and geometric design. Here, we describe methods for recording multiple single neurons and local field potential in behaving rodents, using commercially available micro-machined silicon probes with custom-made accessory components. There are two basic options for interfacing silicon probes to preamplifiers: printed circuit boards and flexible cables. Probe supplying companies (http://www.neuronexustech.com/; http://www.sbmicrosystems.com/; http://www.acreo.se/) usually provide the bonding service and deliver probes bonded to printed circuit boards or flexible cables. Here, we describe the implantation of a 4-shank, 32-site probe attached to flexible polyimide cable, and mounted on a movable microdrive. Each step of the probe preparation, microdrive construction and surgery is illustrated so that the end user can easily replicate the process.

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A. Nagy

University of Szeged

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Marek Wypych

Nencki Institute of Experimental Biology

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Wioletta J. Waleszczyk

Nencki Institute of Experimental Biology

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