Biology:Connectomics
Connectomics is the production and study of connectomes: comprehensive maps of connections within an organism's nervous system. More generally, it can be thought of as the study of neuronal wiring diagrams with a focus on how structural connectivity, individual synapses, cellular morphology, and cellular ultrastructure contribute to the make up of a network. The nervous system is a network made of billions of connections and these connections are responsible for our thoughts, emotions, actions, memories, function and dysfunction. Therefore, the study of connectomics aims to advance our understanding of mental health and cognition by understanding how cells in the nervous system are connected and communicate. Because these structures are extremely complex, methods within this field use a high-throughput application of functional and structural neural imaging, most commonly magnetic resonance imaging (MRI), electron microscopy, and histological techniques in order to increase the speed, efficiency, and resolution of these nervous system maps. To date, tens of large scale datasets have been collected spanning the nervous system including the various areas of cortex, cerebellum,[1][2] the retina,[3] the peripheral nervous system[4] and neuromuscular junctions.[5]
Generally speaking, there are two types of connectomes; macroscale and microscale. Macroscale connectomics refers to using functional and structural MRI data to map out large fiber tracts and functional gray matter areas within the brain in terms of blood flow (functional) and water diffusivity (structural). Microscale connectomics is the mapping of small organisms' complete connectome using microscopy and histology. That is, all connections that exist in their central nervous system.
Methods
Macroscale Connectomics
Macroscale connectomes are commonly collected using diffusion-weighted magnetic resonance imaging (dMRI or DW-MRI) and functional magnetic resonance imaging (fMRI). dMRI datasets can span the entire brain, imaging white matter between the cortex and subcortex, providing information about the diffusion of water molecules in brain tissue, and allowing researchers to infer the orientation and integrity of white matter pathways.[6] dMRI can be used in conjunction with tractography where it enables the reconstruction of white matter tracts in the brain.[6] It does so by measuring the diffusion of water molecules in multiple directions, as dMRI can estimate the local fiber orientations and generate a model of the brain's fiber pathways.[6] Meanwhile, tractography algorithms trace the likely trajectories of these pathways, providing a representation of the brain's anatomical connectivity.[6] Metrics such as fractional anisotropy (FA), mean diffusivity (MD), or connectivity strength can be computed from dMRI data to assess the microstructural properties of white matter and quantify the strength of (long-range) connections between brain regions.[7]
In contrast to dMRI, fMRI datasets measure cerebral blood flow in the brain, as a marker of neuronal activation. One of the benefits of MRI is it offers in vivo information about the connectivity between different brain areas. fMRI measures the blood oxygenation level-dependent (BOLD) signal, which reflects changes in cerebral blood flow and oxygenation associated with neural activity, as regulated by the neurovascular unit.[8] Resting-state functional connectivity (RSFC) analysis is a common method to measure connectomes using fMRI that involves acquiring fMRI data while the subject is at rest and not performing any specific tasks or stimuli.[9] RSFC examines the temporal correlation of the BOLD signals between different brain regions (after accounting for the confounding effect of other regions), providing insights into functional connectivity.[8]
Neuromodulation allows clinicians to utilize stimulatory techniques to treat neurological and psychiatric disorders, such as major depressive disorder (MDD), Alzheimer's, and schizophrenia while providing insights into the connectome.[10] Specifically, Transcranial magnetic stimulation (TMS) is a non-invasive neuromodulation technique that applies strong magnetic pulses between scalp electrodes which target specific brain regions with electrical currents.[11] This can temporarily disrupt or enhance the activity of specific brain areas and observe changes in connectivity.[11] Transcranial direct current stimulation (tDCS) is another non-invasive neuromodulation technique that applies a constant but relatively weak electrical current for a few minutes, modulating neuronal excitability.[12] It allows researchers to investigate the causal relationship between targeted brain regions and changes in connectivity.[12] tDCS increases the functional connectivity within the brain, with a bias towards specific networks (e.g., cortical processing), and may even cause structural changes to take place in the white matter via myelination and in the gray matter via synaptic plasticity.[12] Another imaging technique is deep brain stimulation (DBS), an invasive neuromodulation technique that involves surgically implanting electrodes into specific brain regions in order to apply localized, high-frequency electrical impulses.[13] This technique modulates brain networks and is often used to alleviate motor symptoms from disorders like Parkinson's, essential tremor, and dystonia.[14] The functional and structural connectivity between electrodes can be used to predict patient outcomes and estimate optimal connectivity profiles.[13]
Electrophysiological Methods
Electrophysiological methods measure the difference in signals from different parts of the brain to estimate the connectivity between them, a process that requires a low signal-to-noise ratio to maintain the accuracy of the measurements and sufficient spatial resolution to support the connectivity between specific regions of the brain.[15] These methods offer insights into real-time neural dynamics and functional connectivity between brain regions. Electroencephalography (EEG) measures the differences in the electrical potential generated by oscillating currents at the surface of the scalp, due to the non-invasive, external placement of the electrodes.[16] Meanwhile, magnetoencephalography (MEG) relies on the magnetic fields generated by the electrical activity of the brain to collect information.[16]
Macroscale connectomics has furthered our understanding of various brain networks including visual,[17][18] brainstem,[19][20] and language networks,[21][22] among others.
Microscale Connectomics
On the other hand, microscale connectomes focus on resolving individual cell-to-cell connectivity within much smaller volumes of nervous system tissue. These datasets are commonly collected using electron microscopy (EM) and offer single synapse resolution. The first microscale connectome encompassing an entire nervous system was produced for the nematode C. elegans in 1986.[23] This was done by manually annotating printouts of the EM scans.[23] Advances in EM acquisition, image alignment and segmentation, and manipulation of large datasets have since allowed for larger volumes to be imaged and segmented more easily. EM has been used to produce connectomes from a variety of nervous system samples, including publicly available datasets that encompass the entire brain[24] and ventral nerve cord[25][26] of adult Drosophila melanogaster, the full central nervous system (connected brain and ventral nerve cord) of larval Drosophila melanogaster,[27] and volumes from mouse[28] and human cortex.[29][30] The National Institutes of Health (NIH) has now invested in creating an EM connectome of an entire mouse brain.[31]
Electron microscopy is the imaging technique that provides the highest spatial resolution, which is crucial for being able to recover presynaptic and postsynaptic sites as well as fine morphological details. However, other imaging modalities are approaching the nanometer-scale resolution necessary for microscale connectomics. X-ray nanotomography using a synchotron source can now reach <100 nm resolution, and can theoretically continue to improve.[32] Unlike EM, this technique does not require the tissue being imaged to be stained with heavy metals or to be physically sectioned.[32] Conventional light microscopy is constrained by light diffraction. Researchers have recently used stimulated emission depletion (STED) microscopy, a super-resolution light microscopy technique, to image the extracellular space of a sample from mouse hippocampus, allowing for reconstruction of all neurites within this volume.[33] They then re-imaged the same tissue for fluorescently-tagged synaptic markers to find synaptic connectivity in the sample.[33] However, this approach was limited to ~130 nm resolution, and was therefore not able resolve thin axons.[33]
Tools
One of the main tools used for connectomics research at the macroscale level is MRI.[34] When used together, a resting-state fMRI and a dMRI dataset provide a comprehensive view of how regions of the brain are structurally connected, and how closely they are communicating.[35][36]
The main tool for connectomics research at the microscale level is chemical brain preservation followed by 3D electron microscopy,[37] used for neural circuit reconstruction. Correlative microscopy, which combines fluorescence with 3D electron microscopy, results in more interpretable data as is it able to automatically detect specific neuron types and can trace them in their entirety using fluorescent markers.[38]
To see one of the first micro-connectomes at full-resolution, visit the Open Connectome Project, which is hosting several connectome datasets, including the 12TB dataset from Bock et al. (2011).
Model systems
Aside from the human brain, some of the model systems used for connectomics research are the mouse,[39] the fruit fly,[40][41] the nematode C. elegans,[42][43] and the barn owl.[44]
Caenorhabditis Elegans
The Caenorhabditis Elegans roundworm is a highly researched organism in the field of connectomics, of which a full connectome has been mapped using various imaging techniques, mainly serial-electron microscopy;[45] This process involved studying the aging process of the C. elegans brain by comparing varying worms from birth to adulthood.[46] Researchers found the biggest change with age is the wiring circuits, and that connectivity between and within brain regions increases with age.[46] Regardless of the massive achievement of mapping the full C. Elegans connectome, more information is yet to be discovered about this brain network; The researchers noted that this can be done using comparative connectomics, comparing and contrasting different species' brain networks to pinpoint relations in behavior.[46]
The C. elegans has a simple nervous system, and data collection is more attainable. A study created a code that searches the connections within the C. elegans mapped connectome, as this data is already readily available. The findings were able to collect information about sensory neurons, interneurons, neck motor neurons, behavior, environmental influences, and more in deep detail.[47] Overall, the experiment investigates the connection between neuroanatomy and behavior given that there is a lot of available information about the worm already discovered.[47]
To provide context, the C. elegans roundworm has 302 neurons and 5000 synaptic connections, while the human brain has 100 billion neurons and more than 100 trillion chemical synapses.[48] The human connectome has yet to be fully mapped with a limiting factor being the sheer amount of data collection that this will require in addition to the complexity in comparing individual connectomes given the great degree of variation in human neural circuits.[49]
The drosophila connectome is mostly complete, allowing a visual representation of the anatomical structure and an easier way for researchers to study drosophila neural circuits. Already, this has allowed researchers to identify differences in compartments and their electrophysiology characteristics.[50]
Mouse
An online database known as MouseLight displays over 1000 neurons mapped in the mouse brain based on a collective database of sub-micron resolution images of these brains. This platform illustrates the thalamus, hippocampus, cerebral cortex, and hypothalamus based on single-cell projections.[51] Imaging technology to produce this mouse brain does not allow an in-depth look at synapses but can show axonal arborizations which contain many synapses.[52] A limiting factor to studying mouse connectomes, much like with humans, is the complexity of labeling all the cell types of the mouse brain; This is a process that would require the reconstruction of 100,000+ neurons and the imaging technology is advanced enough to do so.[52]
Mice models in the lab have provided insight into genetic brain disorders, one study manipulated mice with a deletion of 22q11.2 (chromosome 22, a likely known genetic risk factor that leads to schizophrenia).[53] The findings of this study showed that this impaired neural activity in mice's working memory is similar to what it does in humans.[53]
Leading Connectomics Labs
The Lichtman Lab of Harvard University is a leading force in the field of connectomics, investigating how synaptic connectivity and competition change with age using advanced imaging techniques on model organisms such as mice, zebrafish, and C. elegans.[54] This lab is led by neuroscientist, Harvard professor, and renowned researcher, Jeff Lichtman. The Lichtman Lab research had major impacts on the field of connectomics from their development of Brainbrow, which also had a spinoff expansion into Zebrabow technology from their work with zebrafish.[55] This is an in vivo imaging technique that uses multicolor cell labeling that allows researchers to distinguish by cell type and pathway using different Cre lines.[52]
Another notable lab is the Lee Lab of Harvard Medical School which aims to look at how neural networks are organized by function based on the observed activity of these circuits in model organisms, a field known as "functional connectomics".[56]
Applications
By comparing diseased and healthy connectomes, we can gain insight into certain psychopathologies, such as neuropathic pain, and potential therapies for them. Generally, the field of neuroscience would benefit from standardization and raw data. For example, connectome maps can be used to inform computational models of whole-brain dynamics.[57][self-published source?] Current neural networks mostly rely on probabilistic representations of connectivity patterns.[58] Connectivity matrices (checkerboard diagrams of connectomics) have been used in stroke recovery to evaluate the response to treatment via Transcranial Magnetic Stimulation.[59] Similarly, connectograms (circular diagrams of connectomics) have been used in traumatic brain injury cases to document the extent of damage to neural networks.[60][61]
Looking into these methods of research, they can reveal information about different mental illnesses and brain disorders. The tracking of brain networks in alignment with diseases and illnesses would be enhanced by these advanced technologies that can produce complex images of neural networks.[62] With this in mind, diseases can not only be tracked, but predicted based on behavior of previous cases, a process that would take an extensive period of time to collect and record.[62] Specifically, studies on different brain disorders such as schizophrenia and bipolar disorder with a focus on the connectomics involved reveal information. Both of these disorders have a similar genetic origin,[62][63] and research found that those with higher polygenic scores for schizophrenia and bipolar disorder have lower amounts of connectivity shown through neuroimaging.[64] This method of research tackles real-world applications of connectomics, combining methods of imaging with genetics to dig deeper into the origins and outcomes of genetically related disorders.[62] Another study supports the finding that there is relation between connectivity and likelihood of disease, as researchers found those diagnosed with schizophrenia have less structurally complete brain networks.[65] The main drawback in this area of connectomics is not being able to achieve images of whole-brain networks, therefore it is hard to make complete and accurate assumptions about cause and effect of diseases' neural pathways.[65] Connectomics has been used to study patients with strokes using MRI imaging, however because such little research is done in this specific area, conclusions cannot be drawn regarding the relation between strokes and connectivity.[66] The research did find results that highlight an association between poor connectivity in the language system and poor motor coordination, however the results were not substantial enough to make a bold claim.[66] For behavioral disorders, it can be difficult to diagnose and treat because most situations revolve on a symptoms-based approach. However, this can be difficult because many disorders have overlapping symptoms. Connectomics has been used to find neuromarkers associated with social anxiety disorder (SAD) at a high precision rate in improving related symptoms.[67] This is an expanding field and there is room for greater application to mental health disorders and brain malfunction, in which current research is building on neural networks and the psychopathology involved.[68]
The human connectome can be viewed as a graph, and the rich tools, definitions and algorithms of the Graph theory can be applied to these graphs. Comparing the connectomes (or braingraphs) of healthy women and men, Szalkai et al.[69][70] have shown that in several deep graph-theoretical parameters, the structural connectome of women is significantly better connected than that of men. For example, women's connectome has more edges, higher minimum bipartition width, larger eigengap, greater minimum vertex cover than that of men. The minimum bipartition width (or, in other words, the minimum balanced cut) is a well-known measure of quality of computer multistage interconnection networks, it describes the possible bottlenecks in network communication: The higher this value is, the better is the network. The larger eigengap shows that the female connectome is better expander graph than the connectome of males. The better expanding property, the higher minimum bipartition width and the greater minimum vertex cover show deep advantages in network connectivity in the case of female braingraph.
Local measures of difference between populations of those graph have been also introduced (e.g. to compare case versus control groups).[71] Those can be found by using either an adjusted t-test,[72] or a sparsity model,[71] with the aim of finding statistically significant connections which are different among those groups.
Human connectomes have an individual variability, which can be measured with the cumulative distribution function, as it was shown in.[73] By analyzing the individual variability of the human connectomes in distinct cerebral areas, it was found that the frontal and the limbic lobes are more conservative, and the edges in the temporal and occipital lobes are more diverse. A "hybrid" conservative/diverse distribution was detected in the paracentral lobule and the fusiform gyrus. Smaller cortical areas were also evaluated: precentral gyri were found to be more conservative, and the postcentral and the superior temporal gyri to be very diverse.
Comparison to genomics
The recent advancements in the field of connectomics have sparked conversation around its relation to the field of genomics. Recently, scientists in the field have highlighted the parallels between this project and large-scale genomics initiatives.[74] Additionally, they have referenced the need for integration with other scientific disciplines, particularly genetics. While genomics focuses on the genetic blueprint of an organism, connectomics provides insights into the structural and functional connectivity of the brain. By integrating these two fields, researchers can explore how genetic variations and gene expression patterns influence the wiring and organization of neural circuits.[75] This interdisciplinary approach helps uncover the relationship between genes, neural connectivity, and brain function. Additionally, connectomics can benefit from genomics by leveraging genetic tools and techniques to manipulate specific genes or neuronal populations to study their impact on neural circuitry and behavior.[74] Understanding the genetic basis of neural connectivity can enhance our understanding of brain development, neural plasticity, and the mechanisms underlying various neurological disorders.
The human genome project initially faced many of the above criticisms, but was nevertheless completed ahead of schedule and has led to many advances in genetics. Some have argued that analogies can be made between genomics and connectomics, and therefore we should be at least slightly more optimistic about the prospects in connectomics.[76] Others have criticized attempts towards a microscale connectome, arguing that we don't have enough knowledge about where to look for insights, or that it cannot be completed within a realistic time frame.[77]
Human Connectome Project
The Human Connectome Project (HCP)[78] is an initiative launched in 2009 by the National Institutes of Health (NIH) to map the neural pathways that underlie human brain function.[79] The goal was to obtain and distribute information regarding the structural and functional connections within the human brain, improving imaging and analysis methods to enhance resolution and practicality in the realm of connectomics.[79] By understanding the wiring patterns within and across individuals, researchers hope to unravel the electrical signals that give rise to our thoughts, emotions, and behaviors. Additional programs within the Connectome Initiative, such as the Lifespan Connectome and Disease Connectome, focus on mapping brain connections across different age groups and studying connectome variations in individuals with specific clinical diagnoses.[79] The Connectome Coordination Facility serves as a centralized repository for HCP data and provides support to researchers.[79] The success of this project has opened the door to understanding how connectomics might be influential in other areas of neuroscience. The potential of a "Connectome II" project has been referenced recently, which would focus on developing a scanner designed for high-throughput studies involving multiple subjects.[80] The project would aim to utilize recent advancements in visualization technologies towards a higher spatial resolution in imaging structural connectivity.[80] Advancements in this area might also involve incorporating wearable mobile technology to acquire various types of behavioral data, complementing the neuroimaging information gathered by the scanner.[80]
Eyewire game
Eyewire is an online game developed by American scientist Sebastian Seung of Princeton University. It uses social computing to help map the connectome of the brain. It has attracted over 130,000 players from over 100 countries.
Business Development
Omniscient Neurotechnology, a startup out of Australia co-founded by Michael Sughrue and Stephane Doyen, is currently the primary business endeavor incorporating connectomics into their development of neuronal brain maps. These maps provide a comprehensive understanding of neural connections and cell-to-cell communication, which were previously inaccessible through MRI and CT scans.[81] This technology is targeted at surgeons and researchers who might utilize the maps to identify abnormal neural connections and misfiring neurons to make more precise decisions regarding surgeries and therapies.[82] The technology behind the brain maps was developed using machine learning algorithms applied to MRI scans, and it has been likened to "Google Maps for the brain".[81] They have launched two products, "Quicktome'' and “Infinitome”. Quicktome is a digital brain mapping platform intended to provide neurosurgeons with insights into a patient's brain networks before performing brain surgery, ultimately working to streamline the process of neurosurgical planning and provide greater insights for patient care.[82] The platform uses data from a single non-invasive MRI scan, which is processed automatically and delivered through an intuitive web-based app.[82] The platform allows visualization of critical brain networks and helps neurosurgeons make more informed decisions, reduce surgical uncertainty, and have better patient conversations about surgical outcomes.[82] In 2021, Quicktome received regulatory clearance from the FDA, Health Canada, and the Therapeutic Goods Administration of Australia.[83] The company's other product, "Infinitome", defines a neuroscience research platform that allows for revolutionary data and image analysis of the brain using computational neuroscience6. It is a cloud-based platform that complies with HIPAA regulations, and it can generate network maps of the human brain from original MRI data.[83] By utilizing machine learning to automate the extraction of insights from brain data specific to individual patients, Infinitome is intended to accelerate the research and clinical trial processes related to complex diseases. Ultimately, Omniscient Neurotechnology is aimed at improving the diagnosis and treatment processes of brain-related disorders. Recently, Omniscient Neurotechnology raised $30 million in a Series B funding round, helping to support further research and technological development.[83]
Public Datasets
Websites to explore publicly available connectomics datasets:
Macroscale Connectomics (Healthy Young Adult Datasets)
- Human Connectome Project Young Adult
- Amsterdam Open MRI Collection
- Harvard Brain Genomic Superstruct Project
For a more comprehensive list of open macroscale datasets, check out this article
Microscale Connectomics
- Whole C. elegans connectome
- NeuPRINT Fly Hemibrain
- Flywire (whole fly brain)
- MICrONS Explorer (mouse cortical data)
- H01 Browser Release (human cortical data)
See also
- Dynamic Functional Connectivity
- List of Functional Connectivity Software
- Human Connectome Project
- Budapest Reference Connectome
- https://eyewire.org/explore
References
- ↑ "New insights into cortico-basal-cerebellar connectome: clinical and physiological considerations". Brain 143 (2): 396–406. February 2020. doi:10.1093/brain/awz310. PMID 31628799.
- ↑ Nguyen TM, Thomas LA, Rhoades JL, Ricchi I, Yuan XC, Sheridan A, et al. (2021-11-30). "Structured connectivity in the cerebellum enables noise-resilient pattern separation". pp. 2021.11.29.470455. bioRxiv 10.1101/2021.11.29.470455v1.
- ↑ "Connectomic reconstruction of the inner plexiform layer in the mouse retina". Nature 500 (7461): 168–174. August 2013. doi:10.1038/nature12346. PMID 23925239. Bibcode: 2013Natur.500..168H.
- ↑ "Reconstruction of motor control circuits in adult Drosophila using automated transmission electron microscopy". Cell 184 (3): 759–774.e18. February 2021. doi:10.1016/j.cell.2020.12.013. PMID 33400916.
- ↑ "Muscle networks: Connectivity analysis of EMG activity during postural control". Scientific Reports 5: 17830. December 2015. doi:10.1038/srep17830. PMID 26634293. Bibcode: 2015NatSR...517830B.
- ↑ 6.0 6.1 6.2 6.3 Sotiropoulous, Statmotios; Zalesky, Andrew (June 27, 2017). "Building connectomes using diffusion MRI: why, how and but". NMR in Biomedicine 32 (4): e3752. doi:10.1002/nbm.3752. PMID 28654718.
- ↑ Figure 7. Strong long-range connections can delocalize a subset of eigenvectors.. doi:10.7554/elife.01239.010.
- ↑ 8.0 8.1 Deligianni, Fani; Centeno, Maria; Carmichael, David W.; Clayden, Jonathan D. (2014). "Relating resting-state fMRI and EEG whole-brain connectomes across frequency bands". Frontiers in Neuroscience 8: 258. doi:10.3389/fnins.2014.00258. ISSN 1662-453X. PMID 25221467.
- ↑ Zhu, Feiyin; Tang, Liying (July 5, 2019). "Resting-state functional magnetic resonance imaging (fMRI) and functional connectivity density mapping in patients with corneal ulcer". Neuropsychiatric Disease and Treatment 15: 1833–1844. doi:10.2147/NDT.S210658. PMID 31308676.
- ↑ Horn, Andreas; Fox, Michael D. (2020-11-01). "Opportunities of connectomic neuromodulation" (in en). NeuroImage 221: 117180. doi:10.1016/j.neuroimage.2020.117180. ISSN 1053-8119. PMID 32702488.
- ↑ 11.0 11.1 Xia, Mingrui; He, Yong (2022-10-01). "Connectome-guided transcranial magnetic stimulation treatment in depression" (in en). European Child & Adolescent Psychiatry 31 (10): 1481–1483. doi:10.1007/s00787-022-02089-1. ISSN 1435-165X. PMID 36151354.
- ↑ 12.0 12.1 12.2 Kunze, Tim; Hunold, Alexander; Haueisen, Jens; Jirsa, Viktor; Spiegler, Andreas (2016-10-15). "Transcranial direct current stimulation changes resting state functional connectivity: A large-scale brain network modeling study" (in en). NeuroImage. Transcranial electric stimulation (tES) and Neuroimaging 140: 174–187. doi:10.1016/j.neuroimage.2016.02.015. ISSN 1053-8119. PMID 26883068. https://www.sciencedirect.com/science/article/pii/S1053811916001221.
- ↑ 13.0 13.1 Wang, Qiang; Akram, Harith; Muthuraman, Muthuraman; Gonzalez-Escamilla, Gabriel; Sheth, Sameer A.; Oxenford, Simón; Yeh, Fang-Cheng; Groppa, Sergiu et al. (2021-01-01). "Normative vs. patient-specific brain connectivity in deep brain stimulation" (in en). NeuroImage 224: 117307. doi:10.1016/j.neuroimage.2020.117307. ISSN 1053-8119. PMID 32861787.
- ↑ Benabid, Alim Louis (2003-12-01). "Deep brain stimulation for Parkinson's disease" (in en). Current Opinion in Neurobiology 13 (6): 696–706. doi:10.1016/j.conb.2003.11.001. ISSN 0959-4388. PMID 14662371. https://www.sciencedirect.com/science/article/pii/S0959438803001739.
- ↑ Sadaghiani, Sepideh; Brookes, Matthew J; Baillet, Sylvain (2022-02-15). "Connectomics of human electrophysiology" (in en). NeuroImage 247: 118788. doi:10.1016/j.neuroimage.2021.118788. ISSN 1053-8119. PMID 34906715.
- ↑ 16.0 16.1 Sadaghiani, Sepideh; Brookes, Matthew J.; Baillet, Sylvain (2022-02-15). "Connectomics of human electrophysiology" (in en). NeuroImage 247: 118788. doi:10.1016/j.neuroimage.2021.118788. ISSN 1053-8119. PMID 34906715.
- ↑ "Automated retinofugal visual pathway reconstruction with multi-shell HARDI and FOD-based analysis". NeuroImage 125: 767–779. January 2016. doi:10.1016/j.neuroimage.2015.11.005. PMID 26551261.
- ↑ "Defining Meyer's loop-temporal lobe resections, visual field deficits and diffusion tensor tractography". Brain 132 (Pt 6): 1656–1668. June 2009. doi:10.1093/brain/awp114. PMID 19460796.
- ↑ The Human Central Nervous System. 2008. doi:10.1007/978-3-540-34686-9. ISBN 978-3-540-34684-5.
- ↑ "Organization of Brainstem Nuclei". The Human Nervous System. Elsevier. 2012. pp. 260–327. doi:10.1016/b978-0-12-374236-0.10008-2. ISBN 9780123742360. https://ro.uow.edu.au/cgi/viewcontent.cgi?article=4108&context=hbspapers.
- ↑ "DTI tractography of the human brain's language pathways". Cerebral Cortex 18 (11): 2471–2482. November 2008. doi:10.1093/cercor/bhn011. PMID 18281301.
- ↑ "Perisylvian language networks of the human brain". Annals of Neurology 57 (1): 8–16. January 2005. doi:10.1002/ana.20319. PMID 15597383.
- ↑ 23.0 23.1 White, J. G.; Southgate, E.; Thomson, J. N.; Brenner, S. (1986-11-12). "The structure of the nervous system of the nematode Caenorhabditis elegans" (in en). Philosophical Transactions of the Royal Society of London. B, Biological Sciences 314 (1165): 1–340. doi:10.1098/rstb.1986.0056. ISSN 0080-4622. Bibcode: 1986RSPTB.314....1W. https://royalsocietypublishing.org/doi/10.1098/rstb.1986.0056.
- ↑ Dorkenwald, Sven; Matsliah, Arie; Sterling, Amy R; Schlegel, Philipp; Yu, Szi-chieh; McKellar, Claire E.; Lin, Albert; Costa, Marta et al. (2023-06-30) (in en). Neuronal wiring diagram of an adult brain (Report). Neuroscience. doi:10.1101/2023.06.27.546656. PMID 37425937.
- ↑ Phelps, Jasper S.; Hildebrand, David Grant Colburn; Graham, Brett J.; Kuan, Aaron T.; Thomas, Logan A.; Nguyen, Tri M.; Buhmann, Julia; Azevedo, Anthony W. et al. (February 2021). "Reconstruction of motor control circuits in adult Drosophila using automated transmission electron microscopy". Cell 184 (3): 759–774.e18. doi:10.1016/j.cell.2020.12.013. ISSN 0092-8674. PMID 33400916. PMC 8312698. https://doi.org/10.1016/j.cell.2020.12.013.
- ↑ Takemura, Shin-ya; Hayworth, Kenneth J; Huang, Gary B; Januszewski, Michal; Lu, Zhiyuan; Marin, Elizabeth C; Preibisch, Stephan; Xu, C Shan et al. (2023-06-06) (in en). A Connectome of the Male Drosophila Ventral Nerve Cord (Report). Neuroscience. doi:10.1101/2023.06.05.543757. http://biorxiv.org/lookup/doi/10.1101/2023.06.05.543757.
- ↑ Winding, Michael; Pedigo, Benjamin D.; Barnes, Christopher L.; Patsolic, Heather G.; Park, Youngser; Kazimiers, Tom; Fushiki, Akira; Andrade, Ingrid V. et al. (2023-03-10). "The connectome of an insect brain" (in en). Science 379 (6636): eadd9330. doi:10.1126/science.add9330. ISSN 0036-8075. PMID 36893230.
- ↑ The MICrONS Consortium; Bae, J. Alexander; Baptiste, Mahaly; Bishop, Caitlyn A.; Bodor, Agnes L.; Brittain, Derrick; Buchanan, JoAnn; Bumbarger, Daniel J. et al. (2021-07-29) (in en). Functional connectomics spanning multiple areas of mouse visual cortex (Report). Neuroscience. doi:10.1101/2021.07.28.454025. http://biorxiv.org/lookup/doi/10.1101/2021.07.28.454025.
- ↑ Shapson-Coe, Alexander; Januszewski, Michał; Berger, Daniel R.; Pope, Art; Wu, Yuelong; Blakely, Tim; Schalek, Richard L.; Li, Peter H. et al. (2021-05-30) (in en). A connectomic study of a petascale fragment of human cerebral cortex (Report). Neuroscience. doi:10.1101/2021.05.29.446289. http://biorxiv.org/lookup/doi/10.1101/2021.05.29.446289.
- ↑ Loomba, Sahil; Straehle, Jakob; Gangadharan, Vijayan; Heike, Natalie; Khalifa, Abdelrahman; Motta, Alessandro; Ju, Niansheng; Sievers, Meike et al. (2022-07-08). "Connectomic comparison of mouse and human cortex" (in en). Science 377 (6602). doi:10.1126/science.abo0924. ISSN 0036-8075.
- ↑ "BRAIN CONNECTS: A Center for High-throughput Integrative Mouse Connectomics". https://reporter.nih.gov/search/OZaPZ82vPUynldKK6St1Pg/project-details/10665380.
- ↑ 32.0 32.1 Kuan, Aaron T.; Phelps, Jasper S.; Thomas, Logan A.; Nguyen, Tri M.; Han, Julie; Chen, Chiao-Lin; Azevedo, Anthony W.; Tuthill, John C. et al. (December 2020). "Dense neuronal reconstruction through X-ray holographic nano-tomography" (in en). Nature Neuroscience 23 (12): 1637–1643. doi:10.1038/s41593-020-0704-9. ISSN 1097-6256. PMID 32929244.
- ↑ 33.0 33.1 33.2 Velicky, Philipp; Miguel, Eder; Michalska, Julia M.; Lyudchik, Julia; Wei, Donglai; Lin, Zudi; Watson, Jake F.; Troidl, Jakob et al. (August 2023). "Dense 4D nanoscale reconstruction of living brain tissue" (in en). Nature Methods 20 (8): 1256–1265. doi:10.1038/s41592-023-01936-6. ISSN 1548-7091. PMID 37429995.
- ↑ "Diffusion spectrum magnetic resonance imaging (DSI) tractography of crossing fibers". NeuroImage 41 (4): 1267–1277. July 2008. doi:10.1016/j.neuroimage.2008.03.036. PMID 18495497.
- ↑ "Greater than the sum of its parts: a review of studies combining structural connectivity and resting-state functional connectivity". Brain Structure & Function 213 (6): 525–533. October 2009. doi:10.1007/s00429-009-0208-6. PMID 19565262.
- ↑ "Predicting human resting-state functional connectivity from structural connectivity". Proceedings of the National Academy of Sciences of the United States of America 106 (6): 2035–2040. February 2009. doi:10.1073/pnas.0811168106. PMID 19188601. Bibcode: 2009PNAS..106.2035H.
- ↑ "Exploring the retinal connectome". Molecular Vision 17: 355–379. February 2011. PMID 21311605.
- ↑ BV, DELMIC. "Neuroscience: Synaptic connectivity in the songbird brain - Application Note | DELMIC" (in en). http://request.delmic.com/neuroscience.
- ↑ "Network anatomy and in vivo physiology of visual cortical neurons". Nature 471 (7337): 177–182. March 2011. doi:10.1038/nature09802. PMID 21390124. Bibcode: 2011Natur.471..177B.
- ↑ "Semi-automated reconstruction of neural circuits using electron microscopy". Current Opinion in Neurobiology 20 (5): 667–675. October 2010. doi:10.1016/j.conb.2010.08.002. PMID 20833533.
- ↑ "A Complete Electron Microscopy Volume of the Brain of Adult Drosophila melanogaster". Cell 174 (3): 730–743.e22. July 2018. doi:10.1016/j.cell.2018.06.019. PMID 30033368.
- ↑ "Wiring optimization can relate neuronal structure and function". Proceedings of the National Academy of Sciences of the United States of America 103 (12): 4723–4728. March 2006. doi:10.1073/pnas.0506806103. PMID 16537428. Bibcode: 2006PNAS..103.4723C.
- ↑ "Structure of deviations from optimality in biological systems". Proceedings of the National Academy of Sciences of the United States of America 106 (48): 20544–20549. December 2009. doi:10.1073/pnas.0905336106. PMID 19918070. Bibcode: 2009PNAS..10620544P.
- ↑ "Auditory processing, plasticity, and learning in the barn owl". ILAR Journal 51 (4): 338–352. 2010. doi:10.1093/ilar.51.4.338. PMID 21131711.
- ↑ "WormWiring". https://www.wormwiring.org/.
- ↑ 46.0 46.1 46.2 "Connectomes across development reveal principles of brain maturation". Nature 596 (7871): 257–261. August 2021. doi:10.1038/s41586-021-03778-8. PMID 34349261. Bibcode: 2021Natur.596..257W.
- ↑ 47.0 47.1 "Connecting a connectome to behavior: an ensemble of neuroanatomical models of C. elegans klinotaxis". PLOS Computational Biology 9 (2): e1002890. 2013-02-07. doi:10.1371/journal.pcbi.1002890. PMID 23408877. Bibcode: 2013PLSCB...9E2890I.
- ↑ "Overview" (in en). https://medicine.yale.edu/lab/colon_ramos/overview/.
- ↑ "What is Connectomics?" (in en). 2019-04-11. https://www.news-medical.net/life-sciences/What-is-Connectomics.aspx.
- ↑ Marder, Eve; Eisen, Michael B; Pipkin, Jason et al., eds (September 2020). "A connectome and analysis of the adult Drosophila central brain". eLife 9: e57443. doi:10.7554/eLife.57443. PMID 32880371.
- ↑ "MouseLight". http://www.mouselight.janelia.org/.
- ↑ 52.0 52.1 52.2 "Reconstruction of 1,000 Projection Neurons Reveals New Cell Types and Organization of Long-Range Connectivity in the Mouse Brain". Cell 179 (1): 268–281.e13. September 2019. doi:10.1016/j.cell.2019.07.042. PMID 31495573.
- ↑ 53.0 53.1 "Impaired hippocampal-prefrontal synchrony in a genetic mouse model of schizophrenia". Nature 464 (7289): 763–767. April 2010. doi:10.1038/nature08855. PMID 20360742. Bibcode: 2010Natur.464..763S.
- ↑ "Research" (in en). https://lichtmanlab.fas.harvard.edu/research.
- ↑ "Zebrabow: multispectral cell labeling for cell tracing and lineage analysis in zebrafish". Development 140 (13): 2835–2846. July 2013. doi:10.1242/dev.094631. PMID 23757414.
- ↑ "Research" (in en-US). https://www.lee.hms.harvard.edu/research.
- ↑ http://www.scholarpedia.org/article/Connectome[unreliable medical source?][yes|permanent dead link|dead link}}]
- ↑ Friston, Karl J., ed (August 2009). "Towards reproducible descriptions of neuronal network models". PLOS Computational Biology 5 (8): e1000456. doi:10.1371/journal.pcbi.1000456. PMID 19662159. Bibcode: 2009PLSCB...5E0456N.
- ↑ "Changes in the Brain Connectome Following Repetitive Transcranial Magnetic Stimulation for Stroke Rehabilitation". Cureus 13 (10): e19105. October 2021. doi:10.7759/cureus.19105. PMID 34858752.
- ↑ "Mapping connectivity damage in the case of Phineas Gage". PLOS ONE 7 (5): e37454. 2012. doi:10.1371/journal.pone.0037454. PMID 22616011. Bibcode: 2012PLoSO...737454V.
- ↑ "Patient-tailored connectomics visualization for the assessment of white matter atrophy in traumatic brain injury". Frontiers in Neurology 3: 10. 6 February 2012. doi:10.3389/fneur.2012.00010. PMID 22363313.
- ↑ 62.0 62.1 62.2 62.3 Fornito, Alex; Zalesky, Andrew; Breakspear, Michael (March 2015). "The connectomics of brain disorders" (in en). Nature Reviews Neuroscience 16 (3): 159–172. doi:10.1038/nrn3901. ISSN 1471-0048. PMID 25697159. https://www.nature.com/articles/nrn3901.
- ↑ Stahl, Eli A.; Breen, Gerome; Forstner, Andreas J.; McQuillin, Andrew; Ripke, Stephan; Trubetskoy, Vassily; Mattheisen, Manuel; Wang, Yunpeng et al. (May 2019). "Genome-wide association study identifies 30 loci associated with bipolar disorder" (in en). Nature Genetics 51 (5): 793–803. doi:10.1038/s41588-019-0397-8. ISSN 1546-1718. PMID 31043756.
- ↑ Wei, Yongbin; De Lange, Siemon C.; Savage, Jeanne E.; Tissink, Elleke; Qi, Ting; Repple, Jonathan; Gruber, Marius; Kircher, Tilo et al. (2022-11-09). "Associated Genetics and Connectomic Circuitry in Schizophrenia and Bipolar Disorder" (in en). Biological Psychiatry 94 (2): 174–183. doi:10.1016/j.biopsych.2022.11.006. ISSN 0006-3223. PMID 36803976.
- ↑ 65.0 65.1 Heuvel, Martijn P. van den; Mandl, René C. W.; Stam, Cornelis J.; Kahn, René S.; Pol, Hilleke E. Hulshoff (2010-11-24). "Aberrant Frontal and Temporal Complex Network Structure in Schizophrenia: A Graph Theoretical Analysis" (in en). Journal of Neuroscience 30 (47): 15915–15926. doi:10.1523/JNEUROSCI.2874-10.2010. ISSN 0270-6474. PMID 21106830. PMC 6633761. https://www.jneurosci.org/content/30/47/15915.
- ↑ 66.0 66.1 Bian, Rong; Huo, Ming; Liu, Wan; Mansouri, Negar; Tanglay, Onur; Young, Isabella; Osipowicz, Karol; Hu, Xiaorong et al. (2023). "Connectomics underlying motor functional outcomes in the acute period following stroke". Frontiers in Aging Neuroscience 15. doi:10.3389/fnagi.2023.1131415. ISSN 1663-4365. PMID 36875697.
- ↑ Whitfield-Gabrieli, S.; Ghosh, S. S.; Nieto-Castanon, A.; Saygin, Z.; Doehrmann, O.; Chai, X. J.; Reynolds, G. O.; Hofmann, S. G. et al. (May 2016). "Brain connectomics predict response to treatment in social anxiety disorder" (in en). Molecular Psychiatry 21 (5): 680–685. doi:10.1038/mp.2015.109. ISSN 1476-5578. PMID 26260493.
- ↑ Menon, Vinod (2011-10-01). "Large-scale brain networks and psychopathology: a unifying triple network model" (in en). Trends in Cognitive Sciences 15 (10): 483–506. doi:10.1016/j.tics.2011.08.003. ISSN 1364-6613. PMID 21908230. https://www.sciencedirect.com/science/article/pii/S1364661311001719.
- ↑ "Graph Theoretical Analysis Reveals: Women's Brains Are Better Connected than Men's". PLOS ONE 10 (7): e0130045. 2015. doi:10.1371/journal.pone.0130045. PMID 26132764. Bibcode: 2015PLoSO..1030045S.
- ↑ "Brain size bias compensated graph-theoretical parameters are also better in women's structural connectomes". Brain Imaging and Behavior 12 (3): 663–673. June 2018. doi:10.1007/s11682-017-9720-0. PMID 28447246.
- ↑ 71.0 71.1 "MultiLink Analysis: Brain Network Comparison via Sparse Connectivity Analysis". Scientific Reports 9 (1): 65. January 2019. doi:10.1038/s41598-018-37300-4. PMID 30635604. Bibcode: 2019NatSR...9...65C.
- ↑ "Network-based statistic: identifying differences in brain networks". NeuroImage 53 (4): 1197–1207. December 2010. doi:10.1016/j.neuroimage.2010.06.041. PMID 20600983.
- ↑ "Comparative connectomics: Mapping the inter-individual variability of connections within the regions of the human brain". Neuroscience Letters 662 (1): 17–21. January 2018. doi:10.1016/j.neulet.2017.10.003. PMID 28988973.
- ↑ 74.0 74.1 "What connectomics can learn from genomics". PLOS Genetics 17 (7): e1009692. July 2021. doi:10.1371/journal.pgen.1009692. PMID 34270560.
- ↑ "Where the genome meets the connectome: Understanding how genes shape human brain connectivity". NeuroImage 244: 118570. December 2021. doi:10.1016/j.neuroimage.2021.118570. PMID 34508898.
- ↑ "Ome sweet ome: what can the genome tell us about the connectome?". Current Opinion in Neurobiology 18 (3): 346–353. June 2008. doi:10.1016/j.conb.2008.08.010. PMID 18801435.
- ↑ Vance, Ashlee (27 December 2010). "Seeking the Connectome, a Mental Map, Slice by Slice". The New York Times. https://www.nytimes.com/2010/12/28/science/28brain.html.
- ↑ "Human Connectome Project" (in en), Wikipedia, 2023-06-01, https://en.wikipedia.org/w/index.php?title=Human_Connectome_Project&oldid=1158059977, retrieved 2023-06-19
- ↑ 79.0 79.1 79.2 79.3 "Connectome Programs | Blueprint". https://neuroscienceblueprint.nih.gov/human-connectome/connectome-programs.
- ↑ 80.0 80.1 80.2 "The Human Connectome Project: A retrospective". NeuroImage 244: 118543. December 2021. doi:10.1016/j.neuroimage.2021.118543. PMID 34508893.
- ↑ 81.0 81.1 Pratap, Aayushi. "This Startup Raised $30 Million To Create Brain Maps To Aid Surgeries And Therapeutics" (in en). https://www.forbes.com/sites/aayushipratap/2021/07/19/this-startup-raised-30-million-to-create-brain-maps-to-aid-surgeries-and-therapeutics/.
- ↑ 82.0 82.1 82.2 82.3 "Brain Mapping for Neurosurgeons | Omniscient Neurotechnology" (in en). https://www.o8t.com/neurosurgeons.
- ↑ 83.0 83.1 83.2 "Omniscient Announces FDA-Clearance of New MRI-based Functional Brain Analysis Technology" (in en-US). 2023-06-02. https://finance.yahoo.com/news/omniscient-announces-fda-clearance-mri-140000493.html.
Further reading
- Friston, Karl J., ed (July 2008). "Mapping the structural core of human cerebral cortex". PLOS Biology 6 (7): e159. doi:10.1371/journal.pbio.0060159. PMID 18597554.
- "New map IDs the core of the human brain". 2008-07-02. http://www.brainmysteries.com/Research/New_map_IDs_the_core_of_the_human_brain.asp.
External links
- The NIH Blueprint for Neuroscience Research
- TED talk by Sebastian Seung: "I am my connectome".
- braingraph.org: a database of hundreds of braingraphs, computed from the data of the Human Connectome Project
Original source: https://en.wikipedia.org/wiki/Connectomics.
Read more |