Touch
touch
sensorimotor control, mouvement, touch, EEG
Traditionally, touch is associated with exteroception and is rarely considered a relevant sensory cue for controlling movements in space, unlike vision. We developed a technique to isolate and measure tactile involvement in controlling sliding finger movements over a surface. Young adults traced a 2D shape with their index finger under direct or mirror-reversed visual feedback to create a conflict between visual and somatosensory inputs. In this context, increased reliance on somatosensory input compromises movement accuracy. Based on the hypothesis that tactile cues contribute to guiding hand movements when in contact with a surface, we predicted poorer performance when the participants traced with their bare finger compared to when their tactile sensation was dampened by a smooth, rigid finger splint. The results supported this prediction. EEG source analyses revealed smaller current in the source-localized somatosensory cortex during sensory conflict when the finger directly touched the surface. This finding supports the hypothesis that, in response to mirror-reversed visual feedback, the central nervous system selectively gated task-irrelevant somatosensory inputs, thereby mitigating, though not entirely resolving, the visuo-somatosensory conflict. Together, our results emphasize touch’s involvement in movement control over a surface, challenging the notion that vision predominantly governs goal-directed hand or finger movements.
SISSA cognitive neuroscience PhD
Up to 2 PhD positions in Cognitive Neuroscience are available at SISSA, Trieste, starting October 2024. SISSA is an elite postgraduate research institution for Maths, Physics and Neuroscience, located in Trieste, Italy. SISSA operates in English, and its faculty and student community is diverse and strongly international. The Cognitive Neuroscience group (https://phdcns.sissa.it/) hosts 6 research labs that study the neuronal bases of time and magnitude processing, visual perception, motivation and intelligence, language, tactile perception and learning, and neural computation. Our research is highly interdisciplinary; our approaches include behavioural, psychophysics, and neurophysiological experiments with humans and animals, as well as computational, statistical and mathematical models. Students from a broad range of backgrounds (physics, maths, medicine, psychology, biology) are encouraged to apply. The selection procedure is now open. The application deadline is 27 August 2024. Please apply here (https://www.sissa.it/bandi/ammissione-ai-corsi-di-philosophiae-doctor-posizioni-cofinanziate-dal-fondo-sociale-europeo), and see the admission procedure page (https://phdcns.sissa.it/admission-procedure) for more information. Note that the positions available for the Fall admission round are those funded by the "Fondo Sociale Europeo Plus", accessible through the first link above. Please contact the PhD Coordinator Mathew Diamond (diamond@sissa.it) and/or your prospective supervisor for more information and informal inquiries.
Touch in romantic relationships
Responsive behavior is crucial to relationship quality and well-being across a variety of interpersonal domains. In this talk I will share research from studies in which we investigate how responsiveness is conveyed nonverbally in the context of male friendships and in heterosexual romantic relationships, largely focusing on affectionate touch as a nonverbal signal of understanding, validation, and care
New mechanically-gated ion channels and tethers for touch
How the brain uses experience to construct its multisensory capabilities
This talk will not be recorded
A sense without sensors: how non-temporal stimulus features influence the perception and the neural representation of time
Any sensory experience of the world, from the touch of a caress to the smile on our friend’s face, is embedded in time and it is often associated with the perception of the flow of it. The perception of time is therefore a peculiar sensory experience built without dedicated sensors. How the perception of time and the content of a sensory experience interact to give rise to this unique percept is unclear. A few empirical evidences show the existence of this interaction, for example the speed of a moving object or the number of items displayed on a computer screen can bias the perceived duration of those objects. However, to what extent the coding of time is embedded within the coding of the stimulus itself, is sustained by the activity of the same or distinct neural populations and subserved by similar or distinct neural mechanisms is far from clear. Addressing these puzzles represents a way to gain insight on the mechanism(s) through which the brain represents the passage of time. In my talk I will present behavioral and neuroimaging studies to show how concurrent changes of visual stimulus duration, speed, visual contrast and numerosity, shape and modulate brain’s and pupil’s responses and, in case of numerosity and time, influence the topographic organization of these features along the cortical visual hierarchy.
Development of an open-source femtosecond fiber laser system for multiphoton microscopy
This talk will present a low-cost protocol for fabricating an easily constructed femtosecond (fs) fiber laser system suitable for routine multiphoton microscopy (1060–1080 nm, 1 W average power, 70 fs pulse duration, 30–70 MHz repetition rate). Concepts well-known in the laser physics community essential to proper laser operation, but generally obscure to biophysicists and biomedical engineers, will be clarified. The parts list (~$13K US dollars), the equipment list (~$40K+), and the intellectual investment needed to build the laser will be described. A goal of the presentation will be to engage with the audience to discuss trade-offs associated with a custom-built fs fiber laser versus purchasing a commercial system. I will also touch on my research group’s plans to further develop this custom laser system for multiplexed cancer imaging as well as recent developments in the field that promise even higher performance fs fiber lasers for approximately the same cost and ease of construction.
Learning to see stuff
Humans are very good at visually recognizing materials and inferring their properties. Without touching surfaces, we can usually tell what they would feel like, and we enjoy vivid visual intuitions about how they typically behave. This is impressive because the retinal image that the visual system receives as input is the result of complex interactions between many physical processes. Somehow the brain has to disentangle these different factors. I will present some recent work in which we show that an unsupervised neural network trained on images of surfaces spontaneously learns to disentangle reflectance, lighting and shape. However, the disentanglement is not perfect, and we find that as a result the network not only predicts the broad successes of human gloss perception, but also the specific pattern of errors that humans exhibit on an image-by-image basis. I will argue this has important implications for thinking about appearance and vision more broadly.
A possible role of the posterior alpha as a railroad switcher between dorsal and ventral pathways
Suppose you are on your favorite touchscreen device consciously and deliberately deciding emails to read or delete. In other words, you are consciously and intentionally looking, tapping, and swiping. Now suppose that you are doing this while neuroscientists are recording your brain activity. Eventually, the neuroscientists are familiar enough with your brain activity and behavior that they run an experiment with subliminal cues which reveals that your looking, tapping, and swiping seem to be determined by a random switch in your brain. You are not aware of it, or its impact on your decisions or movements. Would these predictions undermine your sense of free will? Some have argued that it should. Although this inference from unreflective and/or random intention mechanisms to free will skepticism, may seem intuitive at first, there are already objections to it. So, even if this thought experiment is plausible, it may not actually undermine our sense of free will.
Diurnal rhythms of the eye
Do all components of the living human eye have a measurable diurnal rhythm? In this talk I will discuss methodologies and results of studies on adolescents and young adults. I will also touch upon the associations between diurnal rhythms of the eye and behavioral activities.
Multisensory interactions in temporal frequency processing
Object recognition by touch and other senses
Neural signature for accumulated evidence underlying temporal decisions
Cognitive models of timing often include a pacemaker analogue whose ticks are accumulated to form an internal representation of time, and a threshold that determines when a target duration has elapsed. However, clear EEG manifestations of these abstract components have not yet been identified. We measured the EEG of subjects while they performed a temporal bisection task in which they were requested to categorize visual stimuli as short or long in duration. We report an ERP component whose amplitude depends monotonically on the stimulus duration. The relation of the ERP amplitude and stimulus duration can be captured by a simple model, adapted from a known drift-diffusion model for time perception. It includes a noisy accumulator that starts with the stimulus onset and a threshold. If the threshold is reached during stimulus presentation, the stimulus is categorized as "long", otherwise the stimulus is categorized as "short". At the stimulus offset, a response proportional to the distance to the threshold is emitted. This simple model has two parameters that fit both the behavior and ERP amplitudes recorded in the task. Two subsequent experiments replicate and extend this finding to another modality (touch) as well as to different time ranges (subsecond and suprasecond), establishing the described ERP component as a useful handle on the cognitive processes involved in temporal decisions.
Context matters: vision and touch in action
Mechanistic insights from a mouse model of HCN1 developmental epileptic encephalopathy
Pathogenic variants in HCN1 are associated with severe developmental and epileptic encephalopathies (DEE). We have engineered the Hcn1 M294L heterozygous knock-in (Hcn1M294L) mouse which is a homolog of the de novo HCN1 M305L recurrent pathogenic variant. The mouse recapitulates the phenotypic features of patients including having spontaneous seizures and a learning deficit. In this talk I will present experimental work that probes the molecular and cellular mechanisms underlying hyper-excitability in the mouse model. This will include testing the efficacy of currently available antiepileptic drugs and a novel precision medicine approach. I will also briefly touch on how disease biology can give insights into the biophysical properties of HCN channels.
Multiphoton imaging with next-generation indicators
Two-photon (2P) in vivo functional imaging of genetically encoded fluorescent Ca2+indicators (GECIs) for neuronal activity has become a broadly applied standard tool in modern neuroscience, because it allows simultaneous imaging of the activity of many neurons at high spatial resolution within living animals. Unfortunately, the most commonly used light-sources – tunable femtosecond pulsed ti:sapphire lasers – can be prohibitively expensive for many labs and fall short of delivering sufficient powers for some new ultra-fast 2P microscopy modalities. Inexpensive homebuilt or industrial light sources such as Ytterbium fiber lasers (YbFLs) show great promise to overcome these limitations as they are becoming widely available at costs orders of magnitude lower and power outputs of up to many times higher than conventional ti:sapphire lasers. However, these lasers are typically bound to emitting a single wavelength (i.e., not tunable) centered around 1020-1060 nm, which fails to efficiently excite state of the art green GECIs such as jGCaMP7 or 8. To this end, we designed and characterized spectral variants (yellow CaMP = YCaMP) of the ultrasensitive genetically encoded calcium indicator jGCaMP7, that allows for efficient 2P-excitation at wavelengths above 1010nm. In this talk I will give a brief overview over some of the reasons why using a fiber laser for 2P excitation might be right for you. I will talk about the development of jYCaMP and some exciting new experimental avenues that it has opened while touching on the prospect that shifting biosensors yellow could have for the 2P imaging community. Please join me for an interesting and fun discussion on whether “yellow is the new green” after the talk!
The Many (Cortical) Layers of Touch
Applications of Multisensory Facilitation of Learning
In this talk I’ll discuss translation of findings of multisensory facilitation of learning to cognitive training. I’ll first review some early findings of multisensory facilitation of learning and then discuss how we have been translating these basic science approaches into gamified training interventions to improve cognitive functions. I’ll touch on approaches to training vision, hearing and working memory that we are developing at the UCR Brain Game Center for Mental Fitness and Well-being. I look forward to discussing both the basic science but also the complexities of how to translate approaches from basic science into the more complex frameworks often used in interventions.
Under Pressure: the role of PIEZO ion channels in interoception
PIEZO ion channels detect force in cellular membranes. They are expressed in a wide variety of mammalian tissues, including the vasculature, lymphatic system, and the nervous system. We have found that PIEZO2 in sensory neurons is required for the mechanical senses of touch and proprioception, but our understanding of internal organ sensing, interoception, is far behind. I will describe our findings on the role of PIEZO ion channels in the lesser-known interoceptive senses in multiple organ systems.
Sensory and metasensory responses during sequence learning in the mouse somatosensory cortex
Sequential temporal ordering and patterning are key features of natural signals, used by the brain to decode stimuli and perceive them as sensory objects. Touch is one sensory modality where temporal patterning carries key information, and the rodent whisker system is a prominent model for understanding neuronal coding and plasticity underlying touch sensation. Neurons in this system are precise encoders of fluctuations in whisker dynamics down to a timescale of milliseconds, but it is not clear whether they can refine their encoding abilities as a result of learning patterned stimuli. For example, can they enhance temporal integration to become better at distinguishing sequences? To explore how cortical coding plasticity underpins sequence discrimination, we developed a task in which mice distinguished between tactile ‘word’ sequences constructed from distinct vibrations delivered to the whiskers, assembled in different orders. Animals licked to report the presence of the target sequence. Optogenetic inactivation showed that the somatosensory cortex was necessary for sequence discrimination. Two-photon imaging in layer 2/3 of the primary somatosensory “barrel” cortex (S1bf) revealed that, in well-trained animals, neurons had heterogeneous selectivity to multiple task variables including not just sensory input but also the animal’s action decision and the trial outcome (presence or absence of the predicted reward). Many neurons were activated preceding goal-directed licking, thus reflecting the animal’s learnt action in response to the target sequence; these neurons were found as soon as mice learned to associate the rewarded sequence with licking. In contrast, learning evoked smaller changes in sensory response tuning: neurons responding to stimulus features were already found in naïve mice, and training did not generate neurons with enhanced temporal integration or categorical responses. Therefore, in S1bf sequence learning results in neurons whose activity reflects the learnt association between target sequence and licking, rather than a refined representation of sensory features. Taken together with results from other laboratories, our findings suggest that neurons in sensory cortex are involved in task-specific processing and that an animal does not sense the world independently of what it needs to feel in order to guide behaviour.
Novel mechanisms of neurogenesis and neural repair
In order to re-install neurogenesis after loss of neurons upon injury or neurodegeneration, we need to understand the basic principles of neurogenesis. I will first discuss about our discovery of a novel centrosome protein (Camargo et al., 2019) and discuss unpublished work about the great diversity of interphase centrosome proteomes and their relevance for neurodevelopmental disorders. I would then present work on a master regulator of neural stem cell amplification and brain folding (Stahl et al., 2013; Esgleas et al., 2020) to proceed presenting data on utilizing some of these factors for turning astrocytes into neurons. I will present data on the critical role of mitochondria in this conversion process (Gascon et al., 2016, Russo et al., 2020) and how it regulates the speed of conversion also showing unpublished data. If time permits I may touch on recent progress in in vivo reprogramming (Mattugini et al., 2019). Taken together, these data highlight the surprising specificity and importance of organelle diversity from centrosome, nucleolus and mitochondria as key regulators in development and reprogramming.
Mapping early brain network changes in neurodegenerative and cerebrovascular disorders: a longitudinal perspective
The spatial patterning of each neurodegenerative disease relates closely to a distinct structural and functional network in the human brain. This talk will mainly describe how brain network-sensitive neuroimaging methods such as resting-state fMRI and diffusion MRI can shed light on brain network dysfunctions associated with pathology and cognitive decline from preclinical to clinical dementia. I will first present our findings from two independent datasets on how amyloid and cerebrovascular pathology influence brain functional networks cross-sectionally and longitudinally in individuals with mild cognitive impairment and dementia. Evidence on longitudinal functional network organizational changes in healthy older adults and the influence of APOE genotype will be presented. In the second part, I will describe our work on how different pathology influences brain structural network and white matter microstructure. I will also touch on some new data on how brain network integrity contributes to behavior and disease progression using multivariate or machine learning approaches. These findings underscore the importance of studying selective brain network vulnerability instead of individual region and longitudinal design. Further developed with machine learning approaches, multimodal network-specific imaging signatures will help reveal disease mechanisms and facilitate early detection, prognosis and treatment search of neuropsychiatric disorders.
Novel Tools for Spatial and Temporal Genomics
The precise spatial localization of molecular signals within tissues richly informs the mechanisms of tissue formation and function. Here, we’ll introduce Slide-seq, a technology which enables transcriptome-wide measurements with near-single cell spatial resolution. We’ll describe recent experimental and computational advances to enable Slide-seq in biological contexts in biological contexts where high detection sensitivity is important. More broadly, we’ll discuss the promise and challenges of spatial transcriptomics for tissue genomics. Lastly, we’ll touch upon novel molecular recording technologies, which allows recording of the absolute time dynamics of gene expression in live systems into DNA sequences.
The oxytocin system in the embodied brain: Social touch and communicative behaviours
Parallel ascending spinal pathways for affective touch and pain
Each day we experience myriad somatosensory stimuli: hugs from loved ones, warm showers, a mosquito bite, and sore muscles after a workout. These tactile, thermal, itch, and nociceptive signals are detected by peripheral sensory neuron terminals distributed throughout our body, propagated into the spinal cord, and then transmitted to the brain through ascending spinal pathways. Primary sensory neurons that detect a wide range of somatosensory stimuli have been identified and characterized. In contrast, very little is known about how peripheral signals are integrated and processed within the spinal cord and conveyed to the brain to generate somatosensory perception and behavioral responses. We tackled this question by developing new mouse genetic tools to define projection neuron (PN) subsets of the anterolateral pathway, a major ascending spinal cord pathway, and combining these new tools with advanced anatomical, physiological, and behavioral approaches. We found that Gpr83+ PNs, a newly identified subset of spinal cord output neurons, and Tacr1+ PNs are largely non-overlapping populations that innervate distinct sets of subnuclei within the lateral parabrachial nucleus (PBNL) of the pons in a zonally segregated manner. In addition, Gpr83+ PNs are highly sensitive to cutaneous mechanical stimuli, receive strong synaptic inputs from primary mechanosensory neurons, and convey tactile information bilaterally to the PBNL in a non-topographically organized manner. Remarkably, Gpr83+ mechanosensory limb of the anterolateral pathway controls behaviors associated with different hedonic values (appetitive or aversive) in a scalable manner. This is the first study to identify a dedicated spinal cord output pathway that conveys affective touch signals to the brain and to define parallel ascending circuit modules that cooperate to convey tactile, thermal and noxious cutaneous signals from the spinal cord to the brain. This study has also revealed exciting new therapeutic opportunities for developing treatments for neurological disorders associated with pain and affective touch.
Self-organisation in interneuron circuits
Inhibitory interneurons come in different classes and form intricate circuits. While our knowledge of these circuits has advanced substantially over the last decades, it is not fully understood how the structure of these circuits relates to their function. I will present some of our recent attempts to “understand” the structure of interneuron circuits by means of computational modeling. Surprisingly (at least for us), we found that prominent features of inhibitory circuitry can be accounted for by an optimisation for excitation-inhibition (E/I) balance. In particular, we find that such an optimisation generates networks that resemble mouse V1 in terms of the structure of synaptic efficacies between principal cells and parvalbumin-positive interneurons. Moreover, an optimisation for E/I balance across neuronal compartments promotes a functional diversification of interneurons into two classes that resemble parvalbumin and somatostatin-positive interneurons. Time permitting, I may briefly touch on recent work in which we link E/I balance to prediction error coding in V1.
Microneurography And Microstimulation Of Single Tactile Afferents In The Human Hand
Microneurography is a method, invented by Ake Vallbo and Karl-Erik Hagbarth in the late 1960, with which we can record the activity from single, identified nerve fibres in awake human participants. In this talk, I will then discuss the method, its advantages and limitations, and some of the key discoveries regarding coding of tactile events in the signalling from receptors in the human skin. An extension of the method is to stimulate single afferents, and record the resulting tactile sensations reported by the participants, so-called microstimulation. The first experiments were done in the 1980s, but the method has recently seen a revival, and is currently being combined with high-resolution brain imaging in the study of the relationship between tactile nerve signals, sensations, and processing of tactile information in the brain.
The geometry of cortical representations of touch in rodents
COSYNE 2022
The geometry of cortical representations of touch in rodents
COSYNE 2022
Superior colliculus supports touch-guided corrections during licking in mice
COSYNE 2023
Assessment of adverse drug effects on cognitive function in cynomolgus macaques using an automated touchscreen-based CANTAB device
FENS Forum 2024
Coding of whisker touch and movement in dysgranular somatosensory cortex
FENS Forum 2024
Communication through social touch in autism spectrum condition
FENS Forum 2024
Cortical activations associated with spatial remapping of finger touch using HR-EEG
FENS Forum 2024
Designing a transmodal technology to feel sound through touch: The multichannel vibrotactile gloves
FENS Forum 2024
The GlyT1 inhibitor bitopertin improves choice accuracy during a touchscreen-based working memory task in mice
FENS Forum 2024
Investigating the role of the subparafascicular thalamic nucleus in the processing of soft touch sensation in mice
FENS Forum 2024
Maternal versus stranger’s touch at 10 months: An fNIRS study
FENS Forum 2024
Neural response associated with the modulation of temporal summation of second pain by affective touch
FENS Forum 2024
Next-interval dynamics shape cortical processing of touch
FENS Forum 2024
A novel touch-panel-based serial reversal learning task for assessing cognitive flexibility in mice
FENS Forum 2024
TENM4 as a potential component of tethers required for touch sensation
FENS Forum 2024
Touching what you see: Multisensory location coding in mouse posterior parietal cortex
FENS Forum 2024
Unravelling the role of prefrontal α7 nicotinic acetylcholine receptors in inhibitory control in physiological and pathological contexts: A behavioral investigation using touchscreen technology
FENS Forum 2024