Добірка наукової літератури з теми "Graph theory, mouse, neuroscience, connectomics"

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Статті в журналах з теми "Graph theory, mouse, neuroscience, connectomics"

1

Rodríguez-Méndez, Diego Alonzo, Daniel San-Juan, Mark Hallett, Chris G. Antonopoulos, Erick López-Reynoso, and Ricardo Lara-Ramírez. "A new model for freedom of movement using connectomic analysis." PeerJ 10 (August 11, 2022): e13602. http://dx.doi.org/10.7717/peerj.13602.

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Анотація:
The problem of whether we can execute free acts or not is central in philosophical thought, and it has been studied by numerous scholars throughout the centuries. Recently, neurosciences have entered this topic contributing new data and insights into the neuroanatomical basis of cognitive processes. With the advent of connectomics, a more refined landscape of brain connectivity can be analysed at an unprecedented level of detail. Here, we identify the connectivity network involved in the movement process from a connectomics point of view, from its motivation through its execution until the sense of agency develops. We constructed a “volitional network” using data derived from the Brainnetome Atlas database considering areas involved in volitional processes as known in the literature. We divided this process into eight processes and used Graph Theory to measure several structural properties of the network. Our results show that the volitional network is small-world and that it contains four communities. Nodes of the right hemisphere are contained in three of these communities whereas nodes of the left hemisphere only in two. Centrality measures indicate the nucleus accumbens is one of the most connected nodes in the network. Extensive connectivity is observed in all processes except in Decision (to move) and modulation of Agency, which might correlate with a mismatch mechanism for perception of Agency.
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2

Bassett, Danielle S., and Edward T. Bullmore. "Small-World Brain Networks Revisited." Neuroscientist 23, no. 5 (September 21, 2016): 499–516. http://dx.doi.org/10.1177/1073858416667720.

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It is nearly 20 years since the concept of a small-world network was first quantitatively defined, by a combination of high clustering and short path length; and about 10 years since this metric of complex network topology began to be widely applied to analysis of neuroimaging and other neuroscience data as part of the rapid growth of the new field of connectomics. Here, we review briefly the foundational concepts of graph theoretical estimation and generation of small-world networks. We take stock of some of the key developments in the field in the past decade and we consider in some detail the implications of recent studies using high-resolution tract-tracing methods to map the anatomical networks of the macaque and the mouse. In doing so, we draw attention to the important methodological distinction between topological analysis of binary or unweighted graphs, which have provided a popular but simple approach to brain network analysis in the past, and the topology of weighted graphs, which retain more biologically relevant information and are more appropriate to the increasingly sophisticated data on brain connectivity emerging from contemporary tract-tracing and other imaging studies. We conclude by highlighting some possible future trends in the further development of weighted small-worldness as part of a deeper and broader understanding of the topology and the functional value of the strong and weak links between areas of mammalian cortex.
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3

Biswas, Rahul, and Eli Shlizerman. "Statistical perspective on functional and causal neural connectomics: The Time-Aware PC algorithm." PLOS Computational Biology 18, no. 11 (November 14, 2022): e1010653. http://dx.doi.org/10.1371/journal.pcbi.1010653.

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The representation of the flow of information between neurons in the brain based on their activity is termed the causal functional connectome. Such representation incorporates the dynamic nature of neuronal activity and causal interactions between them. In contrast to connectome, the causal functional connectome is not directly observed and needs to be inferred from neural time series. A popular statistical framework for inferring causal connectivity from observations is the directed probabilistic graphical modeling. Its common formulation is not suitable for neural time series since it was developed for variables with independent and identically distributed static samples. In this work, we propose to model and estimate the causal functional connectivity from neural time series using a novel approach that adapts directed probabilistic graphical modeling to the time series scenario. In particular, we develop the Time-Aware PC (TPC) algorithm for estimating the causal functional connectivity, which adapts the PC algorithm—a state-of-the-art method for statistical causal inference. We show that the model outcome of TPC has the properties of reflecting causality of neural interactions such as being non-parametric, exhibits the directed Markov property in a time-series setting, and is predictive of the consequence of counterfactual interventions on the time series. We demonstrate the utility of the methodology to obtain the causal functional connectome for several datasets including simulations, benchmark datasets, and recent multi-array electro-physiological recordings from the mouse visual cortex.
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4

Kerstjens, Stan, Gabriela Michel, and Rodney J. Douglas. "Constructive connectomics: How neuronal axons get from here to there using gene-expression maps derived from their family trees." PLOS Computational Biology 18, no. 8 (August 25, 2022): e1010382. http://dx.doi.org/10.1371/journal.pcbi.1010382.

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During brain development, billions of axons must navigate over multiple spatial scales to reach specific neuronal targets, and so build the processing circuits that generate the intelligent behavior of animals. However, the limited information capacity of the zygotic genome puts a strong constraint on how, and which, axonal routes can be encoded. We propose and validate a mechanism of development that can provide an efficient encoding of this global wiring task. The key principle, confirmed through simulation, is that basic constraints on mitoses of neural stem cells—that mitotic daughters have similar gene expression to their parent and do not stray far from one another—induce a global hierarchical map of nested regions, each marked by the expression profile of its common progenitor population. Thus, a traversal of the lineal hierarchy generates a systematic sequence of expression profiles that traces a staged route, which growth cones can follow to their remote targets. We have analyzed gene expression data of developing and adult mouse brains published by the Allen Institute for Brain Science, and found them consistent with our simulations: gene expression indeed partitions the brain into a global spatial hierarchy of nested contiguous regions that is stable at least from embryonic day 11.5 to postnatal day 56. We use this experimental data to demonstrate that our axonal guidance algorithm is able to robustly extend arbors over long distances to specific targets, and that these connections result in a qualitatively plausible connectome. We conclude that, paradoxically, cell division may be the key to uniting the neurons of the brain.
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5

Li, Zhuliu, Tianci Song, Jeongsik Yong, and Rui Kuang. "Imputation of spatially-resolved transcriptomes by graph-regularized tensor completion." PLOS Computational Biology 17, no. 4 (April 7, 2021): e1008218. http://dx.doi.org/10.1371/journal.pcbi.1008218.

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High-throughput spatial-transcriptomics RNA sequencing (sptRNA-seq) based on in-situ capturing technologies has recently been developed to spatially resolve transcriptome-wide mRNA expressions mapped to the captured locations in a tissue sample. Due to the low RNA capture efficiency by in-situ capturing and the complication of tissue section preparation, sptRNA-seq data often only provides an incomplete profiling of the gene expressions over the spatial regions of the tissue. In this paper, we introduce a graph-regularized tensor completion model for imputing the missing mRNA expressions in sptRNA-seq data, namely FIST, Fast Imputation of Spatially-resolved transcriptomes by graph-regularized Tensor completion. We first model sptRNA-seq data as a 3-way sparse tensor in genes (p-mode) and the (x,y) spatial coordinates (x-mode andy-mode) of the observed gene expressions, and then consider the imputation of the unobserved entries or fibers as a tensor completion problem in Canonical Polyadic Decomposition (CPD) form. To improve the imputation of highly sparse sptRNA-seq data, we also introduce a protein-protein interaction network to add prior knowledge of gene functions, and a spatial graph to capture the the spatial relations among the capture spots. The tensor completion model is then regularized by a Cartesian product graph of protein-protein interaction network and the spatial graph to capture the high-order relations in the tensor. In the experiments, FIST was tested on ten 10x Genomics Visium spatial transcriptomic datasets of different tissue sections with cross-validation among the known entries in the imputation. FIST significantly outperformed the state-of-the-art methods for single-cell RNAseq data imputation. We also demonstrate that both the spatial graph and PPI network play an important role in improving the imputation. In a case study, we further analyzed the gene clusters obtained from the imputed gene expressions to show that the imputations by FIST indeed capture the spatial characteristics in the gene expressions and reveal functions that are highly relevant to three different kinds of tissues in mouse kidney.
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Rosenthal, Sara Brin, Hao Wang, Da Shi, Cin Liu, Ruben Abagyan, Linda K. McEvoy, and Chi-Hua Chen. "Mapping the gene network landscape of Alzheimer’s disease through integrating genomics and transcriptomics." PLOS Computational Biology 18, no. 2 (February 25, 2022): e1009903. http://dx.doi.org/10.1371/journal.pcbi.1009903.

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Integration of multi-omics data with molecular interaction networks enables elucidation of the pathophysiology of Alzheimer’s disease (AD). Using the latest genome-wide association studies (GWAS) including proxy cases and the STRING interactome, we identified an AD network of 142 risk genes and 646 network-proximal genes, many of which were linked to synaptic functions annotated by mouse knockout data. The proximal genes were confirmed to be enriched in a replication GWAS of autopsy-documented cases. By integrating the AD gene network with transcriptomic data of AD and healthy temporal cortices, we identified 17 gene clusters of pathways, such as up-regulated complement activation and lipid metabolism, down-regulated cholinergic activity, and dysregulated RNA metabolism and proteostasis. The relationships among these pathways were further organized by a hierarchy of the AD network pinpointing major parent nodes in graph structure including endocytosis and immune reaction. Control analyses were performed using transcriptomics from cerebellum and a brain-specific interactome. Further integration with cell-specific RNA sequencing data demonstrated genes in our clusters of immunoregulation and complement activation were highly expressed in microglia.
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7

Matelsky, Jordan K., Elizabeth P. Reilly, Erik C. Johnson, Jennifer Stiso, Danielle S. Bassett, Brock A. Wester, and William Gray-Roncal. "DotMotif: an open-source tool for connectome subgraph isomorphism search and graph queries." Scientific Reports 11, no. 1 (June 22, 2021). http://dx.doi.org/10.1038/s41598-021-91025-5.

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AbstractRecent advances in neuroscience have enabled the exploration of brain structure at the level of individual synaptic connections. These connectomics datasets continue to grow in size and complexity; methods to search for and identify interesting graph patterns offer a promising approach to quickly reduce data dimensionality and enable discovery. These graphs are often too large to be analyzed manually, presenting significant barriers to searching for structure and testing hypotheses. We combine graph database and analysis libraries with an easy-to-use neuroscience grammar suitable for rapidly constructing queries and searching for subgraphs and patterns of interest. Our approach abstracts many of the computer science and graph theory challenges associated with nanoscale brain network analysis and allows scientists to quickly conduct research at scale. We demonstrate the utility of these tools by searching for motifs on simulated data and real public connectomics datasets, and we share simple and complex structures relevant to the neuroscience community. We contextualize our findings and provide case studies and software to motivate future neuroscience exploration.
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8

Hanalioglu, Sahin, Siyar Bahadir, Ilkay Isikay, Pinar Celtikci, Emrah Celtikci, Fang-Cheng Yeh, Kader Karli Oguz, and Taghi Khaniyev. "Group-Level Ranking-Based Hubness Analysis of Human Brain Connectome Reveals Significant Interhemispheric Asymmetry and Intraparcel Heterogeneities." Frontiers in Neuroscience 15 (December 21, 2021). http://dx.doi.org/10.3389/fnins.2021.782995.

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Objective: Graph theory applications are commonly used in connectomics research to better understand connectivity architecture and characterize its role in cognition, behavior and disease conditions. One of the numerous open questions in the field is how to represent inter-individual differences with graph theoretical methods to make inferences for the population. Here, we proposed and tested a simple intuitive method that is based on finding the correlation between the rank-ordering of nodes within each connectome with respect to a given metric to quantify the differences/similarities between different connectomes.Methods: We used the diffusion imaging data of the entire HCP-1065 dataset of the Human Connectome Project (HCP) (n = 1,065 subjects). A customized cortical subparcellation of HCP-MMP atlas (360 parcels) (yielding a total of 1,598 ROIs) was used to generate connectivity matrices. Six graph measures including degree, strength, coreness, betweenness, closeness, and an overall “hubness” measure combining all five were studied. Group-level ranking-based aggregation method (“measure-then-aggregate”) was used to investigate network properties on population level.Results: Measure-then-aggregate technique was shown to represent population better than commonly used aggregate-then-measure technique (overall rs: 0.7 vs 0.5). Hubness measure was shown to highly correlate with all five graph measures (rs: 0.88–0.99). Minimum sample size required for optimal representation of population was found to be 50 to 100 subjects. Network analysis revealed a widely distributed set of cortical hubs on both hemispheres. Although highly-connected hub clusters had similar distribution between two hemispheres, average ranking values of homologous parcels of two hemispheres were significantly different in 71% of all cortical parcels on group-level.Conclusion: In this study, we provided experimental evidence for the robustness, limits and applicability of a novel group-level ranking-based hubness analysis technique. Graph-based analysis of large HCP dataset using this new technique revealed striking hemispheric asymmetry and intraparcel heterogeneities in the structural connectivity of the human brain.
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9

Markett, Sebastian, Christian Montag, and Martin Reuter. "Network Neuroscience and Personality." Personality Neuroscience 1 (2018). http://dx.doi.org/10.1017/pen.2018.12.

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AbstractPersonality and individual differences originate from the brain. Despite major advances in the affective and cognitive neurosciences, however, it is still not well understood how personality and single personality traits are represented within the brain. Most research on brain-personality correlates has focused either on morphological aspects of the brain such as increases or decreases in local gray matter volume, or has investigated how personality traits can account for individual differences in activation differences in various tasks. Here, we propose that personality neuroscience can be advanced by adding a network perspective on brain structure and function, an endeavor that we label personality network neuroscience.With the rise of resting-state functional magnetic resonance imaging (MRI), the establishment of connectomics as a theoretical framework for structural and functional connectivity modeling, and recent advancements in the application of mathematical graph theory to brain connectivity data, several new tools and techniques are readily available to be applied in personality neuroscience. The present contribution introduces these concepts, reviews recent progress in their application to the study of individual differences, and explores their potential to advance our understanding of the neural implementation of personality.Trait theorists have long argued that personality traits are biophysical entities that are not mere abstractions of and metaphors for human behavior. Traits are thought to actually exist in the brain, presumably in the form of conceptual nervous systems. A conceptual nervous system refers to the attempt to describe parts of the central nervous system in functional terms with relevance to psychology and behavior. We contend that personality network neuroscience can characterize these conceptual nervous systems on a functional and anatomical level and has the potential do link dispositional neural correlates to actual behavior.
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10

Carrasco, Andres, Dorothy E. Oorschot, Paolo Barzaghi, and Jeffery R. Wickens. "Three-Dimensional Spatial Analyses of Cholinergic Neuronal Distributions Across The Mouse Septum, Nucleus Basalis, Globus Pallidus, Nucleus Accumbens, and Caudate-Putamen." Neuroinformatics, July 6, 2022. http://dx.doi.org/10.1007/s12021-022-09588-1.

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AbstractNeuronal networks are regulated by three-dimensional spatial and structural properties. Despite robust evidence of functional implications in the modulation of cognition, little is known about the three-dimensional internal organization of cholinergic networks in the forebrain. Cholinergic networks in the forebrain primarily occur in subcortical nuclei, specifically the septum, nucleus basalis, globus pallidus, nucleus accumbens, and the caudate-putamen. Therefore, the present investigation analyzed the three-dimensional spatial organization of 14,000 cholinergic neurons that expressed choline acetyltransferase (ChAT) in these subcortical nuclei of the mouse forebrain. Point process theory and graph signal processing techniques identified three topological principles of organization. First, cholinergic interneuronal distance is not uniform across brain regions. Specifically, in the septum, globus pallidus, nucleus accumbens, and the caudate-putamen, the cholinergic neurons were clustered compared with a uniform random distribution. In contrast, in the nucleus basalis, the cholinergic neurons had a spatial distribution of greater regularity than a uniform random distribution. Second, a quarter of the caudate-putamen is composed of axonal bundles, yet the spatial distribution of cholinergic neurons remained clustered when axonal bundles were accounted for. However, comparison with an inhomogeneous Poisson distribution showed that the nucleus basalis and caudate-putamen findings could be explained by density gradients in those structures. Third, the number of cholinergic neurons varies as a function of the volume of a specific brain region but cell body volume is constant across regions. The results of the present investigation provide topographic descriptions of cholinergic somata distribution and axonal conduits, and demonstrate spatial differences in cognitive control networks. The study provides a comprehensive digital database of the total population of ChAT-positive neurons in the reported structures, with the x,y,z coordinates of each neuron at micrometer resolution. This information is important for future digital cellular atlases and computational models of the forebrain cholinergic system enabling models based on actual spatial geometry.
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Дисертації з теми "Graph theory, mouse, neuroscience, connectomics"

1

Coletta, Ludovico. "Mapping the mouse connectome with voxel resolution." Doctoral thesis, Università degli studi di Trento, 2022. http://hdl.handle.net/11572/335245.

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Fine-grained descriptions of brain connectivity are required to understand how neural information is processed and relayed across spatial scales. Prior investigations of the mouse brain connectome have employed discrete anatomical parcellations, limiting spatial resolution and potentially concealing network attributes critical to connectome organization. In this work, we provide a voxel-level description of the network and hierarchical structure of the directed mouse connectome, unconstrained by regional partitioning. We found that hub regions and core network components of the voxel-wise mouse connectome exhibit a rich topography encompassing key cortical and subcortical relay regions. We also typified regional substrates based on their directional topology into sink or source regions, and reported a previously unappreciated role of modulatory nuclei as critical effectors of inter-modular and network communicability. Finally, we demonstrated a close spatial correspondence between the mesoscale topography of the mouse connectome and its functional macroscale organization, showing that, like in primates and humans, the mouse cortical connectome is organized along two major topographical axes that can be linked to hierarchical patterns of laminar connectivity, and shape the topography of fMRI dynamic states, respectively. This investigation was paralleled by further studies aimed to more closely relate structural connectome features to the corresponding large scale functional networks of the mouse brain. We first focused on the mouse default mode network (DMN), describing its axonal substrates with sublaminar precision and cell-type specificity. We found that regions of the mouse DMN are predominantly located within the isocortex and exhibit preferential connectivity. Dedicated tract tracing experiments carried out by the Allen Brain Institute revealed that layer 2/3 DMN neurons projected mostly in the DMN, whereas layer 5 neurons project both in and out. Further analyses revealed the presence of separate in-DMN and out-DMN-projecting cell types with distinct genetic profiles. Lastly, we carried out a fine-grained comparison of functional topography and dynamic organization of large-scale fMRI networks in wakeful and anesthetized mice, relating the corresponding functional networks to the underlying architecture of structural connectivity. Recapitulating prior observations in conscious primates, we found that the awake mouse brain is subjected to a profound topological reconfiguration such to maximize cross-talk between cortical and subcortical neural systems, departing from the underlying structure of the axonal connectome. Taken together, these results advance our understanding of the foundational wiring principles of the mammalian connectome, and create opportunities for identifying targets of interventions to modulate brain function and its network structure in a physiologically-accessible species.
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2

(10514360), Uttara Vinay Tipnis. "Data Science Approaches on Brain Connectivity: Communication Dynamics and Fingerprint Gradients." Thesis, 2021.

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The innovations in Magnetic Resonance Imaging (MRI) in the recent decades have given rise to large open-source datasets. MRI affords researchers the ability to look at both structure and function of the human brain. This dissertation will make use of one of these large open-source datasets, the Human Connectome Project (HCP), to study the structural and functional connectivity in the brain.
Communication processes within the human brain at different cognitive states are neither well understood nor completely characterized. We assess communication processes in the human connectome using ant colony-inspired cooperative learning algorithm, starting from a source with no a priori information about the network topology, and cooperatively searching for the target through a pheromone-inspired model. This framework relies on two parameters, namely pheromone and edge perception, to define the cognizance and subsequent behaviour of the ants on the network and the communication processes happening between source and target. Simulations with different configurations allow the identification of path-ensembles that are involved in the communication between node pairs. In order to assess the different communication regimes displayed on the simulations and their associations with functional connectivity, we introduce two network measurements, effective path-length and arrival rate. These measurements are tested as individual and combined descriptors of functional connectivity during different tasks. Finally, different communication regimes are found in different specialized functional networks. This framework may be used as a test-bed for different communication regimes on top of an underlying topology.
The assessment of brain fingerprints has emerged in the recent years as an important tool to study individual differences. Studies so far have mainly focused on connectivity fingerprints between different brain scans of the same individual. We extend the concept of brain connectivity fingerprints beyond test/retest and assess fingerprint gradients in young adults by developing an extension of the differential identifiability framework. To do so, we look at the similarity between not only the multiple scans of an individual (subject fingerprint), but also between the scans of monozygotic and dizygotic twins (twin fingerprint). We have carried out this analysis on the 8 fMRI conditions present in the Human Connectome Project -- Young Adult dataset, which we processed into functional connectomes (FCs) and time series parcellated according to the Schaefer Atlas scheme, which has multiple levels of resolution. Our differential identifiability results show that the fingerprint gradients based on genetic and environmental similarities are indeed present when comparing FCs for all parcellations and fMRI conditions. Importantly, only when assessing optimally reconstructed FCs, we fully uncover fingerprints present in higher resolution atlases. We also study the effect of scanning length on subject fingerprint of resting-state FCs to analyze the effect of scanning length and parcellation. In the pursuit of open science, we have also made available the processed and parcellated FCs and time series for all conditions for ~1200 subjects part of the HCP-YA dataset to the scientific community.
Lastly, we have estimated the effect of genetics and environment on the original and optimally reconstructed FC with an ACE model.
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