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De Koninck, Yves

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De Koninck

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Yves

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Université Laval. Département de psychiatrie et de neurosciences

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ncf10336471

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A 0.13- μm CMOS SoC for simultaneous multichannel optogenetics and neural recording

2018-09-02, Gagnon-Turcotte, Gabriel, Noormohammadi Khiarak, Mehdi, Ethier, Christian, De Koninck, Yves, Gosselin, Benoit

This paper presents a 0.13-μm CMOS system-onchip (SoC) for simultaneous multichannel optogenetics and multichannel neural recording in freely moving laboratory animals. This fully integrated system provides 10 multimodal recording channels with analog-to-digital conversion and a four- channel LED driver circuit for optogenetic stimulation. The bio-amplifier design includes a programmable bandwidth (BW) (0.5 Hz–7 kHz) to collect either the action potentials (APs) and/or the local field potentials (LFPs) and has a noise efficiency factor (NEF) of 2.30 for an input-referred noise of 3.2 μVrms within a BW of 10–7 kHz. The low-power delta–sigma () MASH 1-1-1 analog-to-digital converter (ADC) is designed to work at low oversampling ratios (OSRs) (≤50) and has an effective number of bits (ENOB) of 9.75 bits at an OSR of 25 (BW of 10 kHz). The utilization of a ADC is the key to address the flexibility needed to address different noise versus power consumption tradeoff of various experimental settings. It leverages a new technique that reduces its size by subtracting the output of each branch in the digital domain, instead of in the analog domain as done conventionally. The ADC is followed by an on-chip fourthorder cascaded integrator-comb (CIC4) decimation filter (DF). A whole recording channel, including the bio-amplifier, the MASH 1-1-1, and the DF consumes 11.2 μW. Optical stimulation is performed with an LED driver using a regulated cascode current source with feedback that can accommodate a wide range of LED parameters and battery voltages. The SoC is validated in vivo within a wireless experimental platform in both the ventral posteromedial nucleus (VPM) and cerebral motor cortex brain regions of a virally mediated Channelrhodopsin-2. (ChR2) rat.

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A wireless electro-optic platform for multimodal electrophysiology and optogenetics in freely moving rodents

2021-08-16, Bilodeau, Guillaume, Gagnon-Turcotte, Gabriel, L. Gagnon, Léonard, Keramidis, Iason, De Koninck, Yves, Ethier, Christian, Gosselin, Benoit, Timofeev, Igor

This paper presents the design and the utilization of a wireless electro-optic platform to perform simultaneous multimodal electrophysiological recordings and optogenetic stimulation in freely moving rodents. The developed system can capture neural action potentials (AP), local field potentials (LFP) and electromyography (EMG) signals with up to 32 channels in parallel while providing four optical stimulation channels. The platform is using commercial off-the-shelf components (COTS) and a low-power digital field-programmable gate array (FPGA), to perform digital signal processing to digitally separate in real time the AP, LFP and EMG while performing signal detection and compression for mitigating wireless bandwidth and power consumption limitations. The different signal modalities collected on the 32 channels are time-multiplexed into a single data stream to decrease power consumption and optimize resource utilization. The data reduction strategy is based on signal processing and real-time data compression. Digital filtering, signal detection, and wavelet data compression are used inside the platform to separate the different electrophysiological signal modalities, namely the local field potentials (1–500 Hz), EMG (30–500 Hz), and the action potentials (300–5,000 Hz) and perform data reduction before transmitting the data. The platform achieves a measured data reduction ratio of 7.77 (for a firing rate of 50 AP/second) and weights 4.7 g with a 100-mAh battery, an on/off switch and a protective plastic enclosure. To validate the performance of the platform, we measured distinct electrophysiology signals and performed optogenetics stimulation in vivo in freely moving rondents. We recorded AP and LFP signals with the platform using a 16-microelectrode array implanted in the primary motor cortex of a Long Evans rat, both in anesthetized and freely moving conditions. EMG responses to optogenetic Channelrhodopsin-2 induced activation of motor cortex via optical fiber were also recorded in freely moving rodents.

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Sensory afferents use different coding strategies for heat and cold

2018-05-15, Bélanger, Erik, De Koninck, Yves, Côté, Sylvain L., Wang, Feng, Côté, Daniel, Prescott, Steven A., Desrosiers, Patrick

Primary afferents transduce environmental stimuli into electrical activity that is transmitted centrally to be decoded into corresponding sensations. However, it remains unknown how afferent populations encode different somatosensory inputs. To address this, we performed two-photon Ca2+ imaging from thousands of dorsal root ganglion (DRG) neurons in anesthetized mice while applying mechanical and thermal stimuli to hind paws. We found that approximately half of all neurons are polymodal and that heat and cold are encoded very differently. As temperature increases, more heating-sensitive neurons are activated, and most individual neurons respond more strongly, consistent with graded coding at population and single-neuron levels, respectively. In contrast, most cooling-sensitive neurons respond in an ungraded fashion, inconsistent with graded coding and suggesting combinatorial coding, based on which neurons are co-activated. Although individual neurons may respond to multiple stimuli, our results show that different stimuli activate distinct combinations of diversely tuned neurons, enabling rich population-level coding.

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Striatal neurons expressing D1 and D2 receptors are morphologically distinct and differently affected by dopamine denervation in mice

2017-01-27, Gagnon, Dave, De Koninck, Yves, Beaulieu, Jean Martin, Sánchez, Maria Gabriela, Parent, Martin, Petryszyn, Sarah, Parent, André, Bories, Cyril

The loss of nigrostriatal dopamine neurons in Parkinson’s disease induces a reduction in the number of dendritic spines on medium spiny neurons (MSNs) of the striatum expressing D1 or D2 dopamine receptor. Consequences on MSNs expressing both receptors (D1/D2 MSNs) are currently unknown. We looked for changes induced by dopamine denervation in the density, regional distribution and morphological features of D1/D2 MSNs, by comparing 6-OHDA-lesioned double BAC transgenic mice (Drd1a-tdTomato/Drd2-EGFP) to sham-lesioned animals. D1/D2 MSNs are uniformly distributed throughout the dorsal striatum (1.9% of MSNs). In contrast, they are heterogeneously distributed and more numerous in the ventral striatum (14.6% in the shell and 7.3% in the core). Compared to D1 and D2 MSNs, D1/D2 MSNs are endowed with a smaller cell body and a less profusely arborized dendritic tree with less dendritic spines. The dendritic spine density of D1/D2 MSNs, but also of D1 and D2 MSNs, is significantly reduced in 6-OHDA-lesioned mice. In contrast to D1 and D2 MSNs, the extent of dendritic arborization of D1/D2 MSNs appears unaltered in 6-OHDA-lesioned mice. Our data indicate that D1/D2 MSNs in the mouse striatum form a distinct neuronal population that is affected differently by dopamine deafferentation that characterizes Parkinson’s disease.

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A wireless electro-optic headstage with a 0.13-μm CMOS customintegrated DWT neural signal decoder for closed-loop optogenetics

2019-07-23, Gagnon-Turcotte, Gabriel, Keramidis, Iason, Ethier, Christian, De Koninck, Yves, Gosselin, Benoit

We present awireless electro-optic headstage that uses a 0.13-μm CMOS custom integrated circuit (IC) implementing a digital neural decoder (ND-IC) for enabling real-time closed-loop (CL) optogenetics. The ND-IC processes the neural activity data using three digital cores: 1) the detector core detects and extracts the action potential (AP) of individual neurons by using an adaptive threshold; 2) the data compression core compresses the detected AP by using an efficient Symmlet-2 discrete wavelet transform (DWT) processor for decreasing the amount of data to be transmitted by the low-power wireless link; and 3) the classification core sorts the compressed AP into separated clusters on the fly according to their wave shapes. The ND-IC encompasses several innovations: 1) the compression core decreases the complexity from O(n2) to O(n· log(n)) compared to the previous solutions, while using two times less memory, thanks to the use of a new coefficient sorting tree; and 2) the AP classification core reuses both the compressed DWT coefficients to perform implicit dimensionality reduction, which allows for performing intensive signal processing on-chip, while increasing power and hardware efficiency. This core also reuses the signal standard deviation already computed by theAPdetector core as threshold for performing automatic AP sorting. The headstage also introduces innovations by enabling a new wireless CL scheme between the neural data acquisition module and the optical stimulator. Our CL scheme uses the AP sorting and timing information produced by the ND-IC for detecting complex firing patternswithin the brain. The headstage is also smaller (1.13 cm3), lighter (3.0 g with a 40mAhbattery) and less invasive than the previous solutions, while providing a measured autonomy of 2h40, with the ND-IC. The whole system and the ND-IC are first validated in vivo in the LD thalamus of a Long-Evans rat, and then in freely-moving CL experiments involving a mouse virally expressing ChR2-mCherry in inhibitory neurons of the prelimbic cortex, and the results show that our system works well within an in vivo experimental setting with a freely moving mouse.

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A 0.13μm CMOS SoC for simultaneous multichannel optogenetics and electrophysiological brain recording

2018-03-12, Gagnon-Turcotte, Gabriel, Ethier, Christian, De Koninck, Yves, Gosselin, Benoit

Optogenetics and multi-unit electrophysiological recording are state-of-the-art approaches in neuroscience to observe neural microcircuits in vivo [1]. Thereby, brain-implantable devices incorporating optical stimulation and low-noise data acquisition means have been designed based on custom integrated circuits (IC) to study the brain of small freely behaving laboratory animals. However, no existing IC provides multichannel optogenetic photo-stimulation along with multiunit electrophysiological recording capability within the same die [2-5]. They also lack critical features: they are not multichannel and/or do not include an ADC [6], or they address only one signal modality [5-6], i.e., either local field potentials (LFP) or action potentials (AP). In this paper, we report an IC for simultaneous multichannel optogenetics and electrophysiological recording addressing both LFP and AP signals all at once. This 0.13μm CMOS chip, which includes 4/10 stimulation/recording channels, is enclosed inside a small wireless optogenetic platform, and is demonstrated with simultaneous in vivo optical stimulation and electrophysiological recordings with a virally mediated Channelrhodopsin-2 (ChR2) rat.

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A wireless headstage for combined optogenetics and multichannel electrophysiological recording

2016-06-20, Gagnon-Turcotte, Gabriel, LeChasseur, Yoan, Bories, Cyril, Messaddeq, Younès, De Koninck, Yves, Gosselin, Benoit

This paper presents a wireless headstage with realtime spike detection and data compression for combined optogenetics and multichannel electrophysiological recording. The proposed headstage, which is intended to perform both optical stimulation and electrophysiological recordings simultaneously in freely moving transgenic rodents, is entirely built with commercial off-the-shelf components, and includes 32 recording channels and 32 optical stimulation channels. It can detect, compress and transmit full action potential waveforms over 32 channels in parallel and in real time using an embedded digital signal processor based on a low-power field programmable gate array and a Microblaze microprocessor softcore. Such a processor implements a complete digital spike detector featuring a novel adaptive threshold based on a Sigma-delta control loop, and a wavelet data compression module using a new dynamic coefficient re-quantization technique achieving large compression ratios with higher signal quality. Simultaneous optical stimulation and recording have been performed in-vivo using an optrode featuring 8 microelectrodes and 1 implantable fiber coupled to a 465-nm LED, in the somatosensory cortex and the Hippocampus of a transgenic mouse expressing ChannelRhodospin (Thy1::ChR2-YFP line 4) under anesthetized conditions. Experimental results show that the proposed headstage can trigger neuron activity while collecting, detecting and compressing single cell microvolt amplitude activity from multiple channels in parallel while achieving overall compression ratios above 500. This is the first reported high-channel count wireless optogenetic device providing simultaneous optical stimulation and recording. Measured characteristics show that the proposed headstage can achieve up to 100% of true positive detection rate for signal-to-noise ratio (SNR) down to 15 dB, while achieving up to 97.28% at SNR as low as 5 dB. The implemented prototype features a lifespan of up to 105 minutes, and uses a lightweight (2.8 g) and compact (17 × 18 × 10 mm3) rigid-flex printed circuit board.