1,541 research outputs found
Complex Grey Matter Structure Segmentation in Brains via Deep Learning: Example of the Claustrum
Segmentationand parcellation of the brain has been widely performed on brain
MRI using atlas-based methods. However, segmentation of the claustrum, a thin
and sheet-like structure between insular cortex and putamen has not been
amenable to automatized segmentation, thus limiting its investigation in larger
imaging cohorts. Recently, deep-learning based approaches have been introduced
for automated segmentation of brain structures, yielding great potential to
overcome preexisting limitations. In the following, we present a multi-view
deep-learning based approach to segment the claustrum in T1-weighted MRI scans.
We trained and evaluated the proposed method on 181 manual bilateral claustrum
annotations by an expert neuroradiologist serving as reference standard.
Cross-validation experiments yielded median volumetric similarity, robust
Hausdor? distance and Dice score of 93.3%, 1.41mm and 71.8% respectively which
represents equal or superior segmentation performance compared to human
intra-rater reliability. Leave-one-scanner-out evaluation showed good
transfer-ability of the algorithm to images from unseen scanners, however at
slightly inferior performance. Furthermore, we found that AI-based claustrum
segmentation benefits from multi-view information and requires sample sizes of
around 75 MRI scans in the training set. In conclusion, the developed algorithm
has large potential in independent study cohorts and to facilitate MRI-based
research of the human claustrum through automated segmentation. The software
and models of our method are made publicly available.Comment: submitted to a journa
The structure of a resuscitation-promoting factor domain from Mycobacterium tuberculosis shows homology to lysozymes
Resuscitation-promoting factor (RPF) proteins reactivate stationary-phase cultures of (G+C)-rich Gram-positive bacteria including the causative agent of tuberculosis, Mycobacterium tuberculosis. We report the solution structure of the RPF domain from M. tuberculosis Rv1009 (RpfB) solved by heteronuclear multidimensional NMR. Structural homology with various glycoside hydrolases suggested that RpfB cleaved oligosaccharides. Biochemical studies indicate that a conserved active site glutamate is important for resuscitation activity. These data, as well as the presence of a clear binding pocket for a large molecule, indicate that oligosaccharide cleavage is probably the signal for revival from dormancy
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Simple method for sub-diffraction resolution imaging of cellular structures on standard confocal microscopes by three-photon absorption of quantum dots
This study describes a simple technique that improves a recently developed 3D sub-diffraction imaging method based on three-photon absorption of commercially available quantum dots. The method combines imaging of biological samples via tri-exciton generation in quantum dots with deconvolution and spectral multiplexing, resulting in a novel approach for multi-color imaging of even thick biological samples at a 1.4 to 1.9-fold better spatial resolution. This approach is realized on a conventional confocal microscope equipped with standard continuous-wave lasers. We demonstrate the potential of multi-color tri-exciton imaging of quantum dots combined with deconvolution on viral vesicles in lentivirally transduced cells as well as intermediate filaments in three-dimensional clusters of mouse-derived neural stem cells (neurospheres) and dense microtubuli arrays in myotubes formed by stacks of differentiated C2C12 myoblasts
Ergodic Jacobi matrices and conformal maps
We study structural properties of the Lyapunov exponent and the
density of states for ergodic (or just invariant) Jacobi matrices in a
general framework. In this analysis, a central role is played by the function
as a conformal map between certain domains. This idea goes
back to Marchenko and Ostrovskii, who used this device in their analysis of the
periodic problem
The effect of intervertebral cartilage on neutral posture and range of motion in the necks of sauropod dinosaurs
The necks of sauropod dinosaurs were a key factor in their evolution. The habitual posture and range of motion of these necks has been controversial, and computer-aided studies have argued for an obligatory sub-horizontal pose. However, such studies are compromised by their failure to take into account the important role of intervertebral cartilage. This cartilage takes very different forms in different animals. Mammals and crocodilians have intervertebral discs, while birds have synovial joints in their necks. The form and thickness of cartilage varies significantly even among closely related taxa. We cannot yet tell whether the neck joints of sauropods more closely resembled those of birds or mammals. Inspection of CT scans showed cartilage:bone ratios of 4.5% for Sauroposeidon and about 20% and 15% for two juvenile Apatosaurus individuals. In extant animals, this ratio varied from 2.59% for the rhea to 24% for a juvenile giraffe. It is not yet possible to disentangle ontogenetic and taxonomic signals, but mammal cartilage is generally three times as thick as that of birds. Our most detailed work, on a turkey, yielded a cartilage:bone ratio of 4.56%. Articular cartilage also added 11% to the length of the turkey's zygapophyseal facets. Simple image manipulation suggests that incorporating 4.56% of neck cartilage into an intervertebral joint of a turkey raises neutral posture by 15°. If this were also true of sauropods, the true neutral pose of the neck would be much higher than has been depicted. An additional 11% of zygapophyseal facet length translates to 11% more range of motion at each joint. More precise quantitative results must await detailed modelling. In summary, including cartilage in our models of sauropod necks shows that they were longer, more elevated and more flexible than previously recognised
Microscopic observation of magnon bound states and their dynamics
More than eighty years ago, H. Bethe pointed out the existence of bound
states of elementary spin waves in one-dimensional quantum magnets. To date,
identifying signatures of such magnon bound states has remained a subject of
intense theoretical research while their detection has proved challenging for
experiments. Ultracold atoms offer an ideal setting to reveal such bound states
by tracking the spin dynamics after a local quantum quench with single-spin and
single-site resolution. Here we report on the direct observation of two-magnon
bound states using in-situ correlation measurements in a one-dimensional
Heisenberg spin chain realized with ultracold bosonic atoms in an optical
lattice. We observe the quantum walk of free and bound magnon states through
time-resolved measurements of the two spin impurities. The increased effective
mass of the compound magnon state results in slower spin dynamics as compared
to single magnon excitations. In our measurements, we also determine the decay
time of bound magnons, which is most likely limited by scattering on thermal
fluctuations in the system. Our results open a new pathway for studying
fundamental properties of quantum magnets and, more generally, properties of
interacting impurities in quantum many-body systems.Comment: 8 pages, 7 figure
Gene set of nuclear-encoded mitochondrial regulators is enriched for common inherited variation in obesity
There are hints of an altered mitochondrial function in obesity. Nuclear-encoded genes are relevant for mitochondrial function (3 gene sets of known relevant pathways: (1) 16 nuclear regulators of mitochondrial genes, (2) 91 genes for oxidative phosphorylation and (3) 966 nuclear-encoded mitochondrial genes). Gene set enrichment analysis (GSEA) showed no association with type 2 diabetes mellitus in these gene sets. Here we performed a GSEA for the same gene sets for obesity. Genome wide association study (GWAS) data from a case-control approach on 453 extremely obese children and adolescents and 435 lean adult controls were used for GSEA. For independent confirmation, we analyzed 705 obesity GWAS trios (extremely obese child and both biological parents) and a population-based GWAS sample (KORA F4, n = 1,743). A meta-analysis was performed on all three samples. In each sample, the distribution of significance levels between the respective gene set and those of all genes was compared using the leading-edge-fraction-comparison test (cut-offs between the 50(th) and 95(th) percentile of the set of all gene-wise corrected p-values) as implemented in the MAGENTA software. In the case-control sample, significant enrichment of associations with obesity was observed above the 50(th) percentile for the set of the 16 nuclear regulators of mitochondrial genes (p(GSEA,50) = 0.0103). This finding was not confirmed in the trios (p(GSEA,50) = 0.5991), but in KORA (p(GSEA,50) = 0.0398). The meta-analysis again indicated a trend for enrichment (p(MAGENTA,50) = 0.1052, p(MAGENTA,75) = 0.0251). The GSEA revealed that weak association signals for obesity might be enriched in the gene set of 16 nuclear regulators of mitochondrial genes
Susceptibility to tuberculosis is associated with variants in the ASAP1 gene encoding a regulator of dendritic cell migration
Human genetic factors predispose to tuberculosis (TB). We studied 7.6 million genetic variants in 5,530 people with pulmonary TB and in 5,607 healthy controls. In the combined analysis of these subjects and the follow-up cohort (15,087 TB patients and controls altogether), we found an association between TB and variants located in introns of the ASAP1 gene on chromosome 8q24 (P = 2.6 × 10−11 for rs4733781; P = 1.0 × 10−10 for rs10956514). Dendritic cells (DCs) showed high ASAP1 expression that was reduced after Mycobacterium tuberculosis infection, and rs10956514 was associated with the level of reduction of ASAP1 expression. The ASAP1 protein is involved in actin and membrane remodeling and has been associated with podosomes. The ASAP1-depleted DCs showed impaired matrix degradation and migration. Therefore, genetically determined excessive reduction of ASAP1 expression in M. tuberculosis–infected DCs may lead to their impaired migration, suggesting a potential mechanism of predisposition to TB
Protein trafficking through the endosomal system prepares intracellular parasites for a home invasion
Toxoplasma (toxoplasmosis) and Plasmodium (malaria) use unique secretory organelles for migration, cell invasion, manipulation of host cell functions, and cell egress. In particular, the apical secretory micronemes and rhoptries of apicomplexan parasites are essential for successful host infection. New findings reveal that the contents of these organelles, which are transported through the endoplasmic reticulum (ER) and Golgi, also require the parasite endosome-like system to access their respective organelles. In this review, we discuss recent findings that demonstrate that these parasites reduced their endosomal system and modified classical regulators of this pathway for the biogenesis of apical organelles
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