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Concentration invariant odor coding [PrePrint]

Wilson, Christopher D; Serrano, Gabriela O; Koulakov, Alexei A; Rinberg, Dmitry
Humans can identify visual objects independently of view angle and lighting, words independently of volume and pitch, and smells independently of concentration. The computational principles underlying invariant object recognition remain mostly unknown. Here we propose that, in olfaction, a small and relatively stable set made of the earliest activated receptors forms a code for concentration invariant odor identity. One prediction of this "primacy coding" scheme is that decisions based on odor identity can be made solely using early odor-evoked neural activity. Using an optogenetic masking paradigm, we define the sensory integration time necessary for odor identification and demonstrate that animals can use information occurring <100 ms after inhalation onset to identify odors. Using multi-electrode array recordings of odor responses in the olfactory bulb, we find that concentration invariant units respond earliest and at latencies that are within this behaviorally-defined time window. We propose a computational model demonstrating how such a code can be read by neural circuits of the olfactory system
ORIGINAL:0012315
ISSN: 2692-8205
CID: 2773682

Concentration invariant odor identity coding [Meeting Abstract]

Rinberg, Dmitry
ISI:000386126000038
ISSN: 1464-3553
CID: 2773672

Genetic dissection of amine sensitivity in mice [Meeting Abstract]

Dewan, A; Cichy, A; Zhang, J; Rinberg, D; Bozza, T
A fundamental question in olfaction is how individual olfactory receptors contribute to odor perception. The Trace Amine- Associated Receptors (TAARs) are a small set of evolutionarily conserved main olfactory receptors that respond preferentially to amines and that contribute significantly to amine perception. We are using a combination of gene targeting, electrophysiology, in vivo imaging, and behavior to dissect the contribution of individual TAARs to amine sensitivity. Odorant detection thresholds were measured in mice lacking specific TAAR genes using a go-no go behavioral assay. Genetic deletion of all olfactory TAARs causes a 10-fold decrease in sensitivity to isopentylamine and a 50-fold decrease in sensitivity to phenylethylamine. This indicates that TAARs play a significant role in determining behavioral sensitivity to amines. Our electrophysiological and in vivo imaging experiments indicate that the TAARs are broadly tuned to amines. Phenylethylamine preferentially activates TAAR4, and isopentylamine activates both TAAR4 and TAAR3, with TAAR3 being slightly more sensitive. Genetic deletion of TAAR4 by itself elicits a 10-fold decrease in sensitivity to phenylethylamine, indicating that TAAR4 is the most sensitive receptor for this odorant. Behavioral threshold for isopenylamine is not affected by TAAR4 deletion, indicating that isopentylamine sensitivity may be set by TAAR3, or may be set by either TAAR3 or TAAR4. Our results indicate that single olfactory receptors can contribute significantly to odor detection, and that the TAARs are most likely the most sensitive amine receptors. More generally, our approach allows us to characterize for the first time in mammals how chemical detection at the molecular level relates to olfactory performance at the behavioral level
EMBASE:72061537
ISSN: 0379-864x
CID: 1841062

Novel Behavioral Paradigm Reveals Lower Temporal Limits on Mouse Olfactory Decisions

Resulaj, Arbora; Rinberg, Dmitry
Temporal limits on perceptual decisions set strict boundaries on the possible underlying neural computations. How odor information is encoded in the olfactory system is still poorly understood. Here, we sought to define the limit on the speed of olfactory processing. To achieve this, we trained mice to discriminate different odor concentrations in a novel behavioral setup with precise odor delivery synchronized to the sniffing cycle. Mice reported their choice by moving a horizontal treadmill with their front limbs. We found that mice reported discriminations of 75% accuracy in 70-90 ms after odor inhalation. For a low concentration and nontrigeminal odorant, this time was 90-140 ms, showing that mice process odor information rapidly even in the absence of trigeminal stimulation. These response times establish, after accounting for odor transduction and motor delays, that olfactory processing can take tens of milliseconds. This study puts a strong limit on the underlying neural computations and suggests that the action potentials forming the neural basis for these decisions are fired in a few tens of milliseconds. SIGNIFICANCE STATEMENT: Understanding how sensory information is processed requires different approaches that span multiple levels of investigation from genes to neurons to behavior. Limits on behavioral performance constrain the possible neural mechanisms responsible for specific computations. Using a novel behavioral paradigm, we established that mice can make decisions about odor intensity surprisingly fast. After accounting for sensory and motor delays, the limit on some olfactory neural computations can be as low as a few tens of milliseconds, which suggests that only the first action potentials across a population of neurons contribute to these computations.
PMCID:4540801
PMID: 26290243
ISSN: 1529-2401
CID: 1732362

Neural Coding of Perceived Odor Intensity(1,2,3)

Sirotin, Yevgeniy B; Shusterman, Roman; Rinberg, Dmitry
Stimulus intensity is a fundamental perceptual feature in all sensory systems. In olfaction, perceived odor intensity depends on at least two variables: odor concentration; and duration of the odor exposure or adaptation. To examine how neural activity at early stages of the olfactory system represents features relevant to intensity perception, we studied the responses of mitral/tufted cells (MTCs) while manipulating odor concentration and exposure duration. Temporal profiles of MTC responses to odors changed both as a function of concentration and with adaptation. However, despite the complexity of these responses, adaptation and concentration dependencies behaved similarly. These similarities were visualized by principal component analysis of average population responses and were quantified by discriminant analysis in a trial-by-trial manner. The qualitative functional dependencies of neuronal responses paralleled psychophysics results in humans. We suggest that temporal patterns of MTC responses in the olfactory bulb contribute to an internal perceptual variable: odor intensity.
PMCID:4672005
PMID: 26665162
ISSN: 2373-2822
CID: 1877852

Dark matter of the bulb [Comment]

Devore, Sasha; Rinberg, Dmitry
PMID: 24671062
ISSN: 1097-6256
CID: 953042

Comparing thoracic and intra-nasal pressure transients to monitor active odor sampling during odor-guided decision making in the mouse

Reisert, Johannes; Golden, Glen J; Matsumura, Koichi; Smear, Matt; Rinberg, Dmitry; Gelperin, Alan
BACKGROUND: Recording of physiological parameters in behaving mice has seen an immense increase over recent years driven by, for example, increased miniaturization of recording devices. One parameter particularly important for odorant-driven behaviors is the breathing frequency, since the latter dictates the rate of odorant delivery to the nasal cavity and the olfactory receptor neurons located therein. NEW METHOD: Typically, breathing patterns are monitored by either measuring the breathing-induced temperature or pressure changes in the nasal cavity. Both require the implantation of a nasal cannula and tethering of the mouse to either a cable or tubing. To avoid these limitations we used an implanted pressure sensor which reads the thoracic pressure and transmits the data telemetrically, thus making it suitable for experiments which require a freely moving animal. RESULTS: Mice performed a Go/NoGo odorant-driven behavioral task with the implanted pressure sensor, which proved to work reliably to allow recording of breathing signals over several weeks from a given animal. COMPARISON TO EXISTING METHOD(S): We simultaneously recorded the thoracic and nasal pressure changes and found that measuring the thoracic pressure change yielded similar results compared to measurements of nasal pressure changes. CONCLUSION: Telemetrically recorded breathing signals are a feasible method to monitor odorant-guided behavioral changes in breathing rates. Its advantages are most significant when recording from a freely moving animal over several weeks. The advantages and disadvantages of different methods to record breathing patterns are discussed.
PMCID:3858470
PMID: 24056232
ISSN: 0165-0270
CID: 781212

A network that performs brute-force conversion of a temporal sequence to a spatial pattern: relevance to odor recognition

Sanders, Honi; Kolterman, Brian E; Shusterman, Roman; Rinberg, Dmitry; Koulakov, Alexei; Lisman, John
A classic problem in neuroscience is how temporal sequences (TSs) can be recognized. This problem is exemplified in the olfactory system, where an odor is defined by the TS of olfactory bulb (OB) output that occurs during a sniff. This sequence is discrete because the output is subdivided by gamma frequency oscillations. Here we propose a new class of "brute-force" solutions to recognition of discrete sequences. We demonstrate a network architecture in which there are a small number of modules, each of which provides a persistent snapshot of what occurs in a different gamma cycle. The collection of these snapshots forms a spatial pattern (SP) that can be recognized by standard attractor-based network mechanisms. We will discuss the implications of this strategy for recognizing odor-specific sequences generated by the OB.
PMCID:4166365
PMID: 25278870
ISSN: 1662-5188
CID: 1298972

Multiple perceptible signals from a single olfactory glomerulus

Smear, Matthew; Resulaj, Admir; Zhang, Jingji; Bozza, Thomas; Rinberg, Dmitry
Glomeruli are functional units in the olfactory system. The mouse olfactory bulb contains roughly 2,000 glomeruli, each receiving inputs from olfactory sensory neurons (OSNs) that express a specific odorant receptor gene. Odors typically activate many glomeruli in complex combinatorial patterns and it is unknown which features of neuronal activity in individual glomeruli contribute to odor perception. To address this, we used optogenetics to selectively activate single, genetically identified glomeruli in behaving mice. We found that mice could perceive the stimulation of a single glomerulus. Single-glomerulus stimulation was also detected on an intense odor background. In addition, different input intensities and the timing of input relative to sniffing were discriminated through one glomerulus. Our data suggest that each glomerulus can transmit odor information using identity, intensity and temporal coding cues. These multiple modes of information transmission may enable the olfactory system to efficiently identify and localize odor sources.
PMID: 24056698
ISSN: 1097-6256
CID: 612992

Non-redundant coding of aversive odours in the main olfactory pathway

Dewan, Adam; Pacifico, Rodrigo; Zhan, Ross; Rinberg, Dmitry; Bozza, Thomas
Many species are critically dependent on olfaction for survival. In the main olfactory system of mammals, odours are detected by sensory neurons that express a large repertoire of canonical odorant receptors and a much smaller repertoire of trace amine-associated receptors (TAARs). Odours are encoded in a combinatorial fashion across glomeruli in the main olfactory bulb, with each glomerulus corresponding to a specific receptor. The degree to which individual receptor genes contribute to odour perception is unclear. Here we show that genetic deletion of the olfactory Taar gene family, or even a single Taar gene (Taar4), eliminates the aversion that mice display to low concentrations of volatile amines and to the odour of predator urine. Our findings identify a role for the TAARs in olfaction, namely, in the high-sensitivity detection of innately aversive odours. In addition, our data reveal that aversive amines are represented in a non-redundant fashion, and that individual main olfactory receptor genes can contribute substantially to odour perception.
PMCID:3663888
PMID: 23624375
ISSN: 0028-0836
CID: 366492