1,074 research outputs found
Design of foot-launched powered hang glider (FLPHG)
PrĂĄce se zabĂ˝vĂĄ pĹedpisy pro stavbu a provoz pomocnĂŠ pohonnĂŠ jednotky. StanovenĂm rychlostnĂch polĂĄr vybranĂ˝ch kluzĂĄkĹŻ. VĂ˝poÄtem vĂ˝konĹŻ nutnĂ˝ch pro pohon tÄchto kluzĂĄkĹŻ pomocĂ pomocnĂŠ pohonnĂŠ jednotky a vĂ˝bÄrem vhodnĂ˝ch motorĹŻ.This thesis deals with regulations for constuction and service of foot- launched powered hang glider. It was determined speed polar. Calculate necessary thrust and power. Then was choosen adequate engine
Pediatric Patients with Intravascular Devices: Polymicrobial Bloodstream Infections and Risk Factors
A retrospective study was conducted, including 61 patients with long-term intravascular devices (IVDs) admitted to the Childrens Hospital Los Angeles with diverse underlying diseases, different types of catheters, and culture-proven catheter-related bloodstream infections (BSIs). Within these patients, 125 catheter-related BSIs occurred, and the incidence of monomicrobial and polymicrobial BSIs was evaluated. Risk factors for polymicrobial BSIs were determined. Forty-two BSIs contained more than one pathogen. These polymicrobial BSIs were observed more often in younger patients (<4.1 years versus âĽ4.1 years) and less in patients using venous implanted ports. No other associations were found between the occurrences of polymicrobial BSIs and underlying diseases, other types of catheters, host defense status, parenteral nutrition, recurrences, or catheter removal. Patients with long-term IVDs at a younger age have a higher risk of developing a polymicrobial BSI. Future prospective studies should address the issue of polymicrobial infection in IVDs in more detail
The predictive capacity of uterine artery Doppler for preterm birthâA cohort study
Funding Information NHMRC Practitioner Fellowship. Grant Number: GNT1082548Peer reviewedPublisher PD
Prenatal diagnosis of a trisomy 7/trisomy 13 mosaicism
Double aneuploidy mosaicism of two different aneuploidy cell lines is rare. We describe for the first time a double trisomy mosaicism, involving chromosomes 7 and 13 in a fetus presenting with multiple congenital anomalies. No evidence for chimerism was found by DNA genotyping. The origin of both trisomies are consistent with isodisomy of maternal origin. Therefore, it is most likely that the double trisomy mosaicism arose from two independent events very early in embryonic development. The trisomy 7 and 13 cells were shown to be of maternal origin
Actinobaculum schaalii, a Common Uropathogen in Elderly Patients, Denmark
This organism is identified more often by PCR than by cultivation
Modulation of cytokine release and neutrophil function by granulocyte colony-stimulating factor during endotoxemia in humans
In this double-blind, cross-over, placebo-controlled, randomized study, two groups of eight healthy male volunteers were challenged with endotoxin (4 ng/kg) on two occasions, once in conjunction with placebo and once with granulocyte colony-stimulating factor (G-CSF; 5 microg/kg). In group 1, G-CSF was administered intravenously 2 hours before endotoxin challenge; in group 2, G-CSF was administered subcutaneously 24 hours before endotoxin challenge. In group 1, G-CSF significantly enhanced the release of tumor necrosis factor (TNF), interleukin-6 (IL-6), IL-8, IL-1 receptor antagonist (IL-1ra), and soluble TNF receptors. In group 2, G-CSF significantly reduced IL-8 concentrations and modestly attenuated TNF and IL-6 levels. In this group, IL-1ra and soluble TNF receptors were enhanced by G-CSF pretreatment and lipopolysaccharide (LPS)-induced soluble TNF receptor release was further augmented, whereas LPS-induced IL-1ra concentrations remained unaltered. Both pretreatments with G-CSF increased LPS-induced peripheral neutrophilia; the expression of CD11b, CD18, and CD67; and the release of elastase and lactoferrin. Both pretreatments also down-regulated neutrophil L-selectin expression and prevented the endotoxin-induced pulmonary neutrophil accumulation during the first 2 hours after endotoxin challenge. These data indicate that two different pretreatments with G-CSF result in differential effects on LPS-induced cytokine release but similar effects on LPS-induced neutrophil activation and changes in expression of cell surface molecules. Finally, regardless of the effects of G-CSF on LPS-induced cytokine release, G-CSF blocks LPS-induced pulmonary granulocyte accumulatio
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