12 research outputs found
The Spatial and Temporal Structure of Neural Activity across the Fly Brain
What are the spatial and temporal scales of brainwide neuronal activity? We used swept, confocally-aligned planar excitation (SCAPE) microscopy to image all cells in a large volume of the brain of adult Drosophila with high spatiotemporal resolution while flies engaged in a variety of spontaneous behaviors. This revealed neural representations of behavior on multiple spatial and temporal scales. The activity of most neurons correlated (or anticorrelated) with running and flailing over timescales that ranged from seconds to a minute. Grooming elicited a weaker global response. Significant residual activity not directly correlated with behavior was high dimensional and reflected the activity of small clusters of spatially organized neurons that may correspond to genetically defined cell types. These clusters participate in the global dynamics, indicating that neural activity reflects a combination of local and broadly distributed components. This suggests that microcircuits with highly specified functions are provided with knowledge of the larger context in which they operate
optogenetic control of Drosophila using a red-shifted channelrhodopsin reveals experience-dependent influences on courtship
Articles nAture methods | ADVANCE ONLINE PUBLICATION | optogenetics allows the manipulation of neural activity in freely moving animals with millisecond precision, but its application in Drosophila melanogaster has been limited. here we show that a recently described red activatable channelrhodopsin (reachr) permits control of complex behavior in freely moving adult flies, at wavelengths that are not thought to interfere with normal visual function. this tool affords the opportunity to control neural activity over a broad dynamic range of stimulation intensities. using time-resolved activation, we show that the neural control of male courtship song can be separated into (i) probabilistic, persistent and (ii) deterministic, command-like components. the former, but not the latter, neurons are subject to functional modulation by social experience, which supports the idea that they constitute a locus of state-dependent influence. this separation is not evident using thermogenetic tools, a result underscoring the importance of temporally precise control of neuronal activation in the functional dissection of neural circuits in Drosophila. D. melanogaster is one of the most powerful model organisms available for the genetic dissection of neural circuit function 1,2 . Likewise, the use of light-sensitive microbial opsins, such as channelrhodopsin, has revolutionized the functional dissection of neural circuits in behaving animals In the absence of facile optogenetic manipulation, dTRPA1, a thermosensitive cation channel, has been the preferred metho
Optogenetic control of Drosophila using a red-shifted channelrhodopsin reveals experience-dependent influences on courtship
Optogenetics allows the manipulation of neural activity in freely moving animals with millisecond precision, but its application in Drosophila melanogaster has been limited. Here we show that a recently described red activatable channelrhodopsin (ReaChR) permits control of complex behavior in freely moving adult flies, at wavelengths that are not thought to interfere with normal visual function. This tool affords the opportunity to control neural activity over a broad dynamic range of stimulation intensities. Using time-resolved activation, we show that the neural control of male courtship song can be separated into (i) probabilistic, persistent and (ii) deterministic, command-like components. The former, but not the latter, neurons are subject to functional modulation by social experience, which supports the idea that they constitute a locus of state-dependent influence. This separation is not evident using thermogenetic tools, a result underscoring the importance of temporally precise control of neuronal activation in the functional dissection of neural circuits in Drosophila
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Characterization of global brain state dynamics in Drosophila melanogaster
Internal states, such as arousal and hunger, elevate the probability of a set of behaviors and persist on longer timescales than the behaviors that they predict. These states are triggered by sensors (e.g. neurotransmitters, biogenic amines) within the animal that detect internal homeostatic conditions and external factors. However, the sustained nature of internal states and the diversity of behaviors associated with a singular state suggest that state is represented not only by hormonal and modulatory signals but also by the coordinated activity of neurons within the central brain. Additionally, recent evidence suggests that internal states are represented throughout cortex in rodents and in many neuropil regions in Drosophila. In this thesis, I suggest how persistent states are represented globally in the brain by observing the activity of neurons, at the single-neuron level, distributed throughout the brain of Drosophila melanogaster and determining on what timescales their neural activity predicts behavior.
To do this, we first establish a strategy to rapidly capture brain-wide activity of an awake, freely behaving Drosophila adult. We employ Swept Confocally Aligned Planar Excitation (SCAPE) microscopy, which has been shown to be an effective tool for volumetric imaging in a wide range of living samples, including zebrafish and Drosophila larvae. SCAPE's volumetric imaging speeds exceed those of point-scanning methods ten- to hundred-fold, and offers additional advantages, such as reduced phototoxicity and high signal-to-noise. The optical geometry of SCAPE consists of a single objective located directly above the sample. Therefore, this single stationary objective lens allows for imaging of intact, behaving animals like adult flies. Here, we characterize the spatial resolution of the system with respect to in vivo imaging of neurons in the adult fly brain. We show that we can achieve single-cell resolution, even in closely-spaced or dense neuronal populations. Additionally, we show that high-speed imaging of calcium activity throughout the whole brain can be performed at 20 fly brain volumes per second. These rates allow us to monitor neural dynamics occurring on the time scale of hundreds of milliseconds, which lets us capture the dynamics of popular calcium indicators like GCaMP. Moreover, we have demonstrated the feasibility of this approach to optically record odor responses of individual neurons in the olfactory circuit, while the animal freely behaves on a spherical treadmill.
Having established a system for whole-brain imaging in Drosophila, we then use this methodology to explore the representation of two internal states: arousal, in flies freely running on a spherical treadmill, and hunger, in food-deprived flies consuming sugar. We define internal state as neural activity that predicts behavior on long timescales. To determine the timescale with which individual neurons best predict behavior, we define a regression model in which the activity of each cell is proportional to behavior filtered with unique time constant (tau_i). In freely running flies, we see that the neural activity exhibits a strikingly large dominant mode - nearly all cells across the brain are correlated with locomotion. While the median timescale is short, the distribution of timescales across all cells is broad, with some neurons correlated with locomotion on a much longer timescale, representing arousal based on our definition. In food-deprived flies fed sugar, no dominant mode exists; the neural activity tracking feeding is relatively subtle at the global scale. However, by applying the regression model to determine the timescales of individual cells, we do identify some ensembles of neurons possessing either a short timescale (tau_i 60s), putatively representing hunger. To investigate the populations that make up these different timescales, we used both genetic labeling and hierarchical clustering to determine the identity of neurons of interest. For example, in the freely running flies, we notice that cells in a dorsomedial region called the pars intercerebralis exhibit consistently large tau_i with respect to locomotion. Similarly, by genetically labeling neurons producing the hormone DH44, we see that in food-deprived flies consuming sugar, these neurons exhibit large tau_i with respect to feeding. Thus, we have identified dimensions of global dynamics, including a broadly distributed behavioral state as well as subspaces supporting putative neural correlates of the internal states of arousal and hunger. These data presented in this thesis, and the techniques we have established, have the potential to significantly impact our understanding of internal states at a global level in Drosophila melanogaster and can be extended to other organisms
Enhancing memory of television commercials through message spacing.
This is the published version. Copyright 1994 American Marketing Association.Examined the effects of message repetition, message spacing lag time, and measurement delay on memory for TV commercials among 413 older and younger adults (aged 62–83 yrs vs 20–35 yrs). Results show that in the long measurement delay condition, the recall of message contents was significantly higher with the long lag time than with the short lag time. However, in the short measurement delay condition, recall was significantly higher with the short lag time than with the long lag time. The effect of lag in forestalling memory decay appeared to be similar for both older and younger Ss. Results are interpreted based on a variation of encoding variability theory. (PsycINFO Database Record (c) 2012 APA, all rights reserved
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Optogenetic control of Drosophila using a red-shifted channelrhodopsin reveals experience-dependent influences on courtship.
Optogenetics allows the manipulation of neural activity in freely moving animals with millisecond precision, but its application in Drosophila melanogaster has been limited. Here we show that a recently described red activatable channelrhodopsin (ReaChR) permits control of complex behavior in freely moving adult flies, at wavelengths that are not thought to interfere with normal visual function. This tool affords the opportunity to control neural activity over a broad dynamic range of stimulation intensities. Using time-resolved activation, we show that the neural control of male courtship song can be separated into (i) probabilistic, persistent and (ii) deterministic, command-like components. The former, but not the latter, neurons are subject to functional modulation by social experience, which supports the idea that they constitute a locus of state-dependent influence. This separation is not evident using thermogenetic tools, a result underscoring the importance of temporally precise control of neuronal activation in the functional dissection of neural circuits in Drosophila
The spatial and temporal structure of neural activity across the fly brain
Abstract What are the spatial and temporal scales of brainwide neuronal activity? We used swept, confocally-aligned planar excitation (SCAPE) microscopy to image all cells in a large volume of the brain of adult Drosophila with high spatiotemporal resolution while flies engaged in a variety of spontaneous behaviors. This revealed neural representations of behavior on multiple spatial and temporal scales. The activity of most neurons correlated (or anticorrelated) with running and flailing over timescales that ranged from seconds to a minute. Grooming elicited a weaker global response. Significant residual activity not directly correlated with behavior was high dimensional and reflected the activity of small clusters of spatially organized neurons that may correspond to genetically defined cell types. These clusters participate in the global dynamics, indicating that neural activity reflects a combination of local and broadly distributed components. This suggests that microcircuits with highly specified functions are provided with knowledge of the larger context in which they operate