97 research outputs found

    Rapid Formation of Molecular Clouds and Stars in the Solar Neighborhood

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    Observations of both star-forming regions and young, gas-free stellar associations indicate that most nearby molecular clouds form stars only over a short time span before dispersal; large-scale flows in the diffuse interstellar medium have the potential for forming clouds sufficiently rapidly, and for producing stellar populations with ages much less than the lateral crossing times of their host molecular clouds. We identify four important factors for understanding rapid star formation and short cloud lifetimes. First, much of the accumulation and dispersal of clouds near the solar circle might occur in the atomic phase; only the high-density portion of a cloud's lifecycle is spent in the molecular phase, thus helping to limit molecular cloud ``lifetimes''. Second, once a cloud achieves a high enough column density to form \h2 and CO, gravitational forces become larger than typical interstellar pressure forces; thus star formation can follow rapidly upon molecular gas formation and turbulent dissipation in limited areas of each cloud complex. Third, typical magnetic fields are not strong enough to prevent rapid cloud formation and gravitational collapse. Fourth, rapid dispersal of gas by newly-formed stars, and reduction of shielding by a small expansion of the cloud after the first events of star formation, might limit the length of the star formation epoch and the lifetime of a cloud in its molecular state. This picture emphasizes the importance of large-scale boundary conditions for understanding molecular cloud formation, and implies that star formation is a highly dynamic, rather than quasi-static, process.Comment: 41 pages, 10 figures, accepted by Ap

    Activation of Human T-Helper/Inducer Cell, T-Cytotoxic Cell, B-Cell, and Natural Killer (NK)-Cells and induction of Natural Killer Cell Activity against K562 Chronic Myeloid Leukemia Cells with Modified Citrus Pectin

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    <p>Abstract</p> <p>Background</p> <p>Modified citrus pectin (MCP) is known for its anti-cancer effects and its ability to be absorbed and circulated in the human body. In this report we tested the ability of MCP to induce the activation of human blood lymphocyte subsets like T, B and NK-cells.</p> <p>Methods</p> <p>MCP treated human blood samples were incubated with specific antibody combinations and analyzed in a flow cytometer using a 3-color protocol. To test functionality of the activated NK-cells, isolated normal lymphocytes were treated with increasing concentrations of MCP. Log-phase PKH26-labeled K562 leukemic cells were added to the lymphocytes and incubated for 4 h. The mixture was stained with FITC-labeled active form of caspase 3 antibody and analyzed by a 2-color flow cytometry protocol. The percentage of K562 cells positive for PKH26 and FITC were calculated as the dead cells induced by NK-cells. Monosaccharide analysis of the MCP was performed by high-performance anion-exchange chromatography with pulse amperometric detection (HPAEC-PAD).</p> <p>Results</p> <p>MCP activated T-cytotoxic cells and B-cell in a dose-dependent manner, and induced significant dose-dependent activation of NK-cells. MCP-activated NK-cells demonstrated functionality in inducing cancer cell death. MCP consisted of oligogalacturonic acids with some containing 4,5-unsaturated non-reducing ends.</p> <p>Conclusions</p> <p>MCP has immunostimulatory properties in human blood samples, including the activation of functional NK cells against K562 leukemic cells in culture. Unsaturated oligogalacturonic acids appear to be the immunostimulatory carbohydrates in MCP.</p

    Detection of all four dengue serotypes in Aedes aegypti female mosquitoes collected in a rural area in Colombia

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    The Aedes aegypti vector for dengue virus (DENV) has been reported in urban and periurban areas. The information about DENV circulation in mosquitoes in Colombian rural areas is limited, so we aimed to evaluate the presence of DENV in Ae. aegypti females caught in rural locations of two Colombian municipalities, Anapoima and La Mesa. Mosquitoes from 497 rural households in 44 different rural settlements were collected. Pools of about 20 Ae. aegypti females were processed for DENV serotype detection. DENV in mosquitoes was detected in 74% of the analysed settlements with a pool positivity rate of 62%. The estimated individual mosquito infection rate was 4.12% and the minimum infection rate was 33.3/1,000 mosquitoes. All four serotypes were detected; the most frequent being DENV-2 (50%) and DENV-1 (35%). Two-three serotypes were detected simultaneously in separate pools. This is the first report on the co-occurrence of natural DENV infection of mosquitoes in Colombian rural areas. The findings are important for understanding dengue transmission and planning control strategies. A potential latent virus reservoir in rural areas could spill over to urban areas during population movements. Detecting DENV in wild-caught adult mosquitoes should be included in the development of dengue epidemic forecasting models
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