982 research outputs found
3C 220.3: a radio galaxy lensing a submillimeter galaxy
Herschel Space Observatory photometry and extensive multiwavelength followup
have revealed that the powerful radio galaxy 3C 220.3 at z=0.685 acts as a
gravitational lens for a background submillimeter galaxy (SMG) at z=2.221. At
an observed wavelength of 1mm, the SMG is lensed into three distinct images. In
the observed near infrared, these images are connected by an arc of 1.8" radius
forming an Einstein half-ring centered near the radio galaxy. In visible light,
only the arc is apparent. 3C 220.3 is the only known instance of strong
galaxy-scale lensing by a powerful radio galaxy not located in a galaxy cluster
and therefore it offers the potential to probe the dark matter content of the
radio galaxy host. Lens modeling rejects a single lens, but two lenses centered
on the radio galaxy host A and a companion B, separated by 1.5", provide a fit
consistent with all data and reveal faint candidates for the predicted fourth
and fifth images. The model does not require an extended common dark matter
halo, consistent with the absence of extended bright X-ray emission on our
Chandra image. The projected dark matter fractions within the Einstein radii of
A (1.02") and B (0.61") are about 0.4 +/- 0.3 and 0.55 +/- 0.3. The mass to
i-band light ratios of A and B, M/L ~ 8 +/- 4 Msun/Lsun, appear comparable to
those of radio-quiet lensing galaxies at the same redshift in the CASTLES, LSD,
and SL2S samples. The lensed SMG is extremely bright with observed f(250um) =
440mJy owing to a magnification factor mu~10. The SMG spectrum shows luminous,
narrow CIV 154.9nm emission, revealing that the SMG houses a hidden quasar in
addition to a violent starburst. Multicolor image reconstruction of the SMG
indicates a bipolar morphology of the emitted ultraviolet (UV) light suggestive
of cones through which UV light escapes a dust-enshrouded nucleus.Comment: 17 pages, 14 Figures, accepted for publication in Ap
Accelerated development of arthritis in mice lacking endothelial selectins
The selectins, along with very late antigen-4 and CD44, have been implicated in mediating leukocyte rolling interactions that lead to joint recruitment and inflammation during the pathogenesis of rheumatoid arthritis. Previously, we showed that P-selectin deficiency in mice resulted in accelerated onset of joint inflammation in the murine collagen-immunized arthritis model. Here, we report that mice deficient either in E-selectin or in E-selectin and P-selectin (E/P-selectin mutant) also exhibit accelerated development of arthritis compared with wild type mice in the CIA model, suggesting that these adhesion molecules perform overlapping functions in regulating joint disease. Analyses of cytokine and chemokine expression in joint tissue from E/P-selectin mutant mice before the onset of joint swelling revealed significantly higher joint levels of macrophage inflammatory protein-1α and IL-1β compared to wild-type mice. IL-1β remained significantly increased in E/P-selectin mutant joint tissue during the early and chronic phases of arthritis. Overall, these data illustrate the novel finding that E-selectin and P-selectin expression can significantly influence cytokine and chemokine production in joint tissue, and suggest that these adhesion molecules play important regulatory roles in the development of arthritis in E/P-selectin mutant mice
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Macrophage migration inhibitory factor: a mediator of matrix metalloproteinase-2 production in rheumatoid arthritis
Rheumatoid arthritis (RA) is a chronic inflammatory disease characterized by destruction of bone and cartilage, which is mediated, in part, by synovial fibroblasts. Matrix metalloproteinases (MMPs) are a large family of proteolytic enzymes responsible for matrix degradation. Macrophage migration inhibitory factor (MIF) is a cytokine that induces the production of a large number of proinflammatory molecules and has an important role in the pathogenesis of RA by promoting inflammation and angiogenesis. In the present study, we determined the role of MIF in RA synovial fibroblast MMP production and the underlying signaling mechanisms. We found that MIF induces RA synovial fibroblast MMP-2 expression in a time-dependent and concentration-dependent manner. To elucidate the role of MIF in MMP-2 production, we produced zymosan-induced arthritis (ZIA) in MIF gene-deficient and wild-type mice. We found that MMP-2 protein levels were significantly decreased in MIF gene-deficient compared with wild-type mice joint homogenates. The expression of MMP-2 in ZIA was evaluated by immunohistochemistry (IHC). IHC revealed that MMP-2 is highly expressed in wild-type compared with MIF gene-deficient mice ZIA joints. Interestingly, synovial lining cells, endothelial cells, and sublining nonlymphoid mononuclear cells expressed MMP-2 in the ZIA synovium. Consistent with these results, in methylated BSA (mBSA) antigen-induced arthritis (AIA), a model of RA, enhanced MMP-2 expression was also observed in wild-type compared with MIF gene-deficient mice joints. To elucidate the signaling mechanisms in MIF-induced MMP-2 upregulation, RA synovial fibroblasts were stimulated with MIF in the presence of signaling inhibitors. We found that MIF-induced RA synovial fibroblast MMP-2 upregulation required the protein kinase C (PKC), c-jun N-terminal kinase (JNK), and Src signaling pathways. We studied the expression of MMP-2 in the presence of PKC isoform-specific inhibitors and found that the PKCδ inhibitor rottlerin inhibits MIF-induced RA synovial fibroblast MMP-2 production. Consistent with these results, MIF induced phosphorylation of JNK, PKCδ, and c-jun. These results indicate a potential novel role for MIF in tissue destruction in RA
Mosaic DNA imports with interspersions of recipient sequence after natural transformation of Helicobacter pylori
Helicobacter pylori colonizes the gastric mucosa of half of the human population, causing gastritis, ulcers, and cancer. H. pylori
is naturally competent for transformation by exogenous DNA, and recombination during mixed infections of one stomach
with multiple H. pylori strains generates extensive allelic diversity. We developed an in vitro transformation protocol to study
genomic imports after natural transformation of H. pylori. The mean length of imported fragments was dependent on the
combination of donor and recipient strain and varied between 1294 bp and 3853 bp. In about 10% of recombinant clones, the
imported fragments of donor DNA were interrupted by short interspersed sequences of the recipient (ISR) with a mean length
of 82 bp. 18 candidate genes were inactivated in order to identify genes involved in the control of import length and
generation of ISR. Inactivation of the antimutator glycosylase MutY increased the length of imports, but did not have a
significant effect on ISR frequency. Overexpression of mutY strongly increased the frequency of ISR, indicating that MutY, while
not indispensable for ISR formation, is part of at least one ISR-generating pathway. The formation of ISR in H. pylori increases
allelic diversity, and contributes to the uniquely low linkage disequilibrium characteristic of this pathogen
Interannual variability in Transpolar Drift summer sea ice thickness and potential impact of Atlantification
Changes in Arctic sea ice thickness are the result of complex interactions of the dynamic and variable ice cover with atmosphere and ocean. Most of the sea ice exiting the Arctic Ocean does so through Fram Strait, which is why long-term measurements of ice thickness at the end of the Transpolar Drift provide insight into the integrated signals of thermodynamic and dynamic influences along the pathways of Arctic sea ice. We present an updated summer (July–August) time series of extensive ice thickness surveys carried out at the end of the Transpolar Drift between 2001 and 2020. Overall, we see a more than 20 % thinning of modal ice thickness since 2001. A comparison of this time series with first preliminary results from the international Multidisciplinary drifting Observatory for the Study of Arctic Climate (MOSAiC) shows that the modal summer thickness of the MOSAiC floe and its wider vicinity are consistent with measurements from previous years at the end of the Transpolar Drift. By combining this unique time series with the Lagrangian sea ice tracking tool, ICETrack, and a simple thermodynamic sea ice growth model, we link the observed interannual ice thickness variability north of Fram Strait to increased drift speeds along the Transpolar Drift and the consequential variations in sea ice age. We also show that the increased influence of upward-directed ocean heat flux in the eastern marginal ice zones, termed Atlantification, is not only responsible for sea ice thinning in and around the Laptev Sea but also that the induced thickness anomalies persist beyond the Russian shelves and are potentially still measurable at the end of the Transpolar Drift after more than a year. With a tendency towards an even faster Transpolar Drift, winter sea ice growth will have less time to compensate for the impact processes, such as Atlantification, have on sea ice thickness in the eastern marginal ice zone, which will increasingly be felt in other parts of the sea-ice-covered Arctic
PLANNING OF HUMAN RESOURCE COMPETENCY DEVELOPMENT IN PT.XYZ WITH TAGUCHI METHOD
The problem of human resources is still a concern within the company to remain competitive in
this globalization world. This shows that the problem of human resources greatly affect the
implementation and success of the company in achieving goals and objectives. The company
demand to obtain the development process and get quality human resources more urgent. And
the development of human resource competence is necessary. This study uses experimental
testing with several parameters of validity and reliability testing. For testing analysis using
Taguchi Method. Based on the Response Table for Signal to Noise Ratios Nominal is best
obtained taguchi test results obtained values obtained from the effect plot for means with the
approach of table of means, then the intellectual competence is needed for the improvement of
HR performance
Fusion cross section measurements of astrophysical interest for light heavy ions systems within the STELLA project
This contribution is focused on the STELLA project (STELlar LAboratory), which aims at the measurement of fusion cross sections between light heavy ions like 12C+12C, 12C+16O or 16O+16O at deep subbarrier energies. The gamma-particle coincidence technique is used in order to reduce background contributions that become dominant for measurements in the nanobarn regime. The experimental setup composed of an ultra high vacuum reaction chamber, a set of 3 silicon strip detectors, up to 36 LaBr3(Ce) scintillators from the UK FATIMA collaboration, and a fast rotating target system will be described. The 12C+12C fusion reaction has been studied from Elab = 11 to 5.6 MeV using STELLA at the Andromède facility in Orsay, France. Preliminary commissioning results are presented in this article
Syntenator: Multiple gene order alignments with a gene-specific scoring function
<p>Abstract</p> <p>Background</p> <p>Identification of homologous regions or conserved syntenies across genomes is one crucial step in comparative genomics. This task is usually performed by genome alignment softwares like WABA or blastz. In case of conserved syntenies, such regions are defined as conserved gene orders. On the gene order level, homologous regions can even be found between distantly related genomes, which do not align on the nucleotide sequence level.</p> <p>Results</p> <p>We present a novel approach to identify regions of conserved synteny across multiple genomes. Syntenator represents genomes and alignments thereof as partial order graphs (POGs). These POGs are aligned by a dynamic programming approach employing a gene-specific scoring function. The scoring function reflects the level of protein sequence similarity for each possible gene pair. Our method consistently defines larger homologous regions in pairwise gene order alignments than nucleotide-level comparisons. Our method is superior to methods that work on predefined homology gene sets (as implemented in Blockfinder). Syntenator successfully reproduces 80% of the EnsEMBL man-mouse conserved syntenic blocks. The full potential of our method becomes visible by comparing remotely related genomes and multiple genomes. Gene order alignments potentially resolve up to 75% of the EnsEMBL 1:many orthology relations and 27% of the many:many orthology relations.</p> <p>Conclusion</p> <p>We propose Syntenator as a software solution to reliably infer conserved syntenies among distantly related genomes. The software is available from <url>http://www2.tuebingen.mpg.de/abt4/plone</url>.</p
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