1,224 research outputs found

    Platelet-Derived Growth Factor Receptor Ī² Is Critical for Zebrafish Intersegmental Vessel Formation

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    Background: Platelet-derived growth factor receptor Ī² (PDGFRĪ²) is a tyrosine kinase receptor known to affect vascular development. The zebrafish is an excellent model to study specific regulators of vascular development, yet the role of PDGF signaling has not been determined in early zebrafish embryos. Furthermore, vascular mural cells, in which PDGFRĪ² functions cell autonomously in other systems, have not been identified in zebrafish embryos younger than 72 hours post fertilization. Methodology/Principal Findings: In order to investigate the role of PDGFRĪ² in zebrafish vascular development, we cloned the highly conserved zebrafish homolog of PDGFRĪ². We found that pdgfrĪ² is expressed in the hypochord, a developmental structure that is immediately dorsal to the dorsal aorta and potentially regulates blood vessel development in the zebrafish. Using a PDGFR tyrosine kinase inhibitor, a morpholino oligonucleotide specific to PDGFRĪ², and a dominant negative PDGFRĪ² transgenic line, we found that PDGFRĪ² is necessary for angiogenesis of the intersegmental vessels. Significance/Conclusion: Our data provide the first evidence that PDGFRĪ² signaling is required for zebrafish angiogenesis. We propose a novel mechanism for zebrafish PDGFRĪ² signaling that regulates vascular angiogenesis in the absence of mural cells

    Possible retardation effects of quark confinement on the meson spectrum

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    The reduced Bethe-Salpeter equation with scalar confinement and vector gluon exchange is applied to quark-antiquark bound states. The so called intrinsic flaw of Salpeter equation with static scalar confinement is investigated. The notorious problem of narrow level spacings is found to be remedied by taking into consideration the retardation effect of scalar confinement. Good fit for the mass spectrum of both heavy and light quarkomium states is then obtained.Comment: 14 pages in LaTex for

    WormBase: a multi-species resource for nematode biology and genomics

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    WormBase (http://www.wormbase.org/) is the central data repository for information about Caenorhabditis elegans and related nematodes. As a model organism database, WormBase extends beyond the genomic sequence, integrating experimental results with extensively annotated views of the genome. The WormBase Consortium continues to expand the biological scope and utility of WormBase with the inclusion of large-scale genomic analyses, through active data and literature curation, through new analysis and visualization tools, and through refinement of the user interface. Over the past year, the nearly complete genomic sequence and comparative analyses of the closely related species Caenorhabditis briggsae have been integrated into WormBase, including gene predictions, ortholog assignments and a new synteny viewer to display the relationships between the two species. Extensive site-wide refinement of the user interface now provides quick access to the most frequently accessed resources and a consistent browsing experience across the site. Unified single-page views now provide complete summaries of commonly accessed entries like genes. These advances continue to increase the utility of WormBase for C.elegans researchers, as well as for those researchers exploring problems in functional and comparative genomics in the context of a powerful genetic system

    OSM-11 Facilitates LIN-12 Notch Signaling during Caenorhabditis elegans Vulval Development

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    Notch signaling is critical for cell fate decisions during development. Caenorhabditis elegans and vertebrate Notch ligands are more diverse than classical Drosophila Notch ligands, suggesting possible functional complexities. Here, we describe a developmental role in Notch signaling for OSM-11, which has been previously implicated in defecation and osmotic resistance in C. elegans. We find that complete loss of OSM-11 causes defects in vulval precursor cell (VPC) fate specification during vulval development consistent with decreased Notch signaling. OSM-11 is a secreted, diffusible protein that, like previously described C. elegans Delta, Serrate, and LAG-2 (DSL) ligands, can interact with the lineage defective-12 (LIN-12) Notch receptor extracellular domain. Additionally, OSM-11 and similar C. elegans proteins share a common motif with Notch ligands from other species in a sequence defined here as the Delta and OSM-11 (DOS) motif. osm-11 loss-of-function defects in vulval development are exacerbated by loss of other DOS-motif genes or by loss of the Notch ligand DSL-1, suggesting that DOS-motif and DSL proteins act together to activate Notch signaling in vivo. The mammalian DOS-motif protein Deltalike1 (DLK1) can substitute for OSM-11 in C. elegans development, suggesting that DOS-motif function is conserved across species. We hypothesize that C. elegans OSM-11 and homologous proteins act as coactivators for Notch receptors, allowing precise regulation of Notch receptor signaling in developmental programs in both vertebrates and invertebrates

    The lncRNA landscape of breast cancer reveals a role for DSCAM-AS1 in breast cancer progression.

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    Molecular classification of cancers into subtypes has resulted in an advance in our understanding of tumour biology and treatment response across multiple tumour types. However, to date, cancer profiling has largely focused on protein-coding genes, which comprise <1% of the genome. Here we leverage a compendium of 58,648 long noncoding RNAs (lncRNAs) to subtype 947 breast cancer samples. We show that lncRNA-based profiling categorizes breast tumours by their known molecular subtypes in breast cancer. We identify a cohort of breast cancer-associated and oestrogen-regulated lncRNAs, and investigate the role of the top prioritized oestrogen receptor (ER)-regulated lncRNA, DSCAM-AS1. We demonstrate that DSCAM-AS1 mediates tumour progression and tamoxifen resistance and identify hnRNPL as an interacting protein involved in the mechanism of DSCAM-AS1 action. By highlighting the role of DSCAM-AS1 in breast cancer biology and treatment resistance, this study provides insight into the potential clinical implications of lncRNAs in breast cancer

    QCD predictions for annihilation decays of P-wave quarkonia to next-to-leading order in Ī±s\alpha_s

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    The decay rates of P-wave heavy quarkonia to light hadrons are presented to leading order in v2v^2 and next-to-leading order in Ī±s\alpha_s. They include contributions from both the color-singlet component and the color-octet component of quarkonia. Applying these results to charmonium and using measured decay rates for the Ļ‡c1\chi_{c1} and Ļ‡c2\chi_{c2} by E760, we determine the two nonperturbative decay matrix elements, and then predict the hadronic decay rates of Ļ‡c0\chi_{c0} and hch_c, and the electromagnetic decay rates of Ļ‡c0\chi_{c0} and Ļ‡c2\chi_{c2}. The obtained decay rates of Ļ‡c0ā†’LH\chi_{c0}\to LH and Ļ‡c0ā†’Ī³Ī³\chi_{c0}\to\gamma\gamma are in agreement with the Crystal Ball result, and also with the new measurement by BES. However, the results for Ī“(Ļ‡c0ā†’LH)\Gamma(\chi_{c0}\to LH) are dependent on the choice of renormalization scale.Comment: 10 pages Latex(5 figures included). We have corrected a numerical error in Eq.(5) and Eq.(11

    Large Possible retardation effects of quark confinement on the meson spectrum II

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    We present the results of a study of heavy-light-quark bound states in the context of the reduced Bethe-Salpeter equation with relativistic vector and scalar interactions. We find that satisfactory fits may also be obtained when the retarded effect of the quark-antiquark interaction is concerned.Comment: 11 pages, RevTex, to appear in PR

    A population of luminous accreting black holes with hidden mergers

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    Major galaxy mergers are thought to play an important part in fuelling the growth of supermassive black holes. However, observational support for this hypothesis is mixed, with some studies showing a correlation between merging galaxies and luminous quasars and others showing no such association. Recent observations have shown that a black hole is likely to become heavily obscured behind merger-driven gas and dust, even in the early stages of the merger, when the galaxies are well separated (5 to 40 kiloparsecs). Merger simulations further suggest that such obscuration and black-hole accretion peaks in the final merger stage, when the two galactic nuclei are closely separated (less than 3 kiloparsecs). Resolving this final stage requires a combination of high-spatial-resolution infrared imaging and high-sensitivity hard-X-ray observations to detect highly obscured sources. However, large numbers of obscured luminous accreting supermassive black holes have been recently detected nearby (distances below 250 megaparsecs) in X-ray observations. Here we report high-resolution infrared observations of hard-X-ray-selected black holes and the discovery of obscured nuclear mergers, the parent populations of supermassive-black-hole mergers. We find that obscured luminous black holes (bolometric luminosity higher than 2x10^44 ergs per second) show a significant (P<0.001) excess of late-stage nuclear mergers (17.6 per cent) compared to a sample of inactive galaxies with matching stellar masses and star formation rates (1.1 per cent), in agreement with theoretical predictions. Using hydrodynamic simulations, we confirm that the excess of nuclear mergers is indeed strongest for gas-rich major-merger hosts of obscured luminous black holes in this final stage.Comment: To appear in the 8 November 2018 issue of Nature. This is the authors' version of the wor
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