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The effect of coconut palms on the pasture understoryFernando, D. N. S. January 1990 (has links)
No description available.
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New indices for the assessment of skeletal metabolism using plasma clearance of bone seeking tracersHolohan, So-Jin Park January 2000 (has links)
No description available.
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The information transmitted over a noisy nonlinear transformationOrwell, James Matthew January 2000 (has links)
No description available.
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Electron beam proximity effect correctionEa, Chee Seng January 2000 (has links)
No description available.
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High-Pressure and High-Temperature Density Measurements of n-Pentane, n-Octane, 2,2,4-Trimethylpentane, Cyclooctane, n-Decane, and TolueneWu, Yue 19 October 2010 (has links)
Information on the density of hydrocarbons at high pressures and temperatures is of great importance in many fields, such as the study of ultra-deep reservoirs up to ~240 MPa and 250°C. However, density data at such high pressures and temperatures are often not available in the literature. In this study, experimental densities are reported for n-pentane, n-octane, 2,2,4-trimethylpentane, cyclooctane, n-decane, and toluene to ~280 MPa and ~250°C. These experimental densities are in good agreement with available literature data, although the literature data for many of these fluids do not extend to the pressures and temperatures utilized in this study.
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A Comparison of Body Composition between Eumenorrheic and Amenorrheic Adolescent Cross-Country RunnersBonis, Marc 22 May 2006 (has links)
The purpose of the study was to examine the relationship and comparisons of athletic amenorrhea and bone mineral density in adolescent, cross-country runners. Subjects: Twenty-eight female adolescent cross-country runners (Mean Age + SD = 15.0 + 1.3 years); consisting of seventeen eumenorrheics & eleven amenorrheics. Design: The design consisted of a sixmonth longitudinal design in which the subjects were measured before and after cross-country season for height, weight, and lean tissue (LT), body fat (BF), bone mineral content (BMC), and bone mineral density (BMD) using whole-body scan densitiometry with a Lunar Dual-energy X-ray Absorptiometer (DXA). Run performance, weekly training volumes, menstrual dysfunction, menarchal age, nutritional information, and stress fractures were reported by the subjects. Statistical analyses consisted of Pearson product-moment and partial correlations to examine the associations of the variables, paired t-tests to measure seasonal body composition changes, multivariate analysis (MANOVA & MANCOVA) to investigate the subgroup differences of variables, and simple linear regression to determine the best body composition predictor variable for BMD. Results: The eumenorrheic subgroup's BMD was significantly greater than the amenorrheic subgroup's BMD (F(1, 54) = 16.22, p<.05, partial h² =.231). The eumenorrheic subgroup's bodyweight (F(1, 54) = 7.65, p<.05, partial h² =.124), BF (F(1, 54) = 8.56, p<.05, partial h² =.137), and BMC (F(1, 54) = 8.52, p<.05, partial h² =.136) were significantly greater than the amenorrheic subgroup. There was also a significant seasonal increase in BMD (t(27) = -4.01, p <.05) for the overall group. Bodyweight was the body composition component that best predicted BMD (F(1, 26) = 46.434, p<.05, R² =.641). There were no significant subgroup differences with respect to run performance, stress fractures, and nutritional supplementation. Conclusions: Athletic amenorrhea was highly associated with lower levels of BMD in adolescent, cross-country runners. Athletic amenorrhea was also highly associated with lower levels of bodyweight, BF, and BMC in adolescent cross-country runners. Finally, cross-country running was highly associated with increased BMD in adolescent athletes. Implications: The long-term implication of the study is that subjects with lower levels of BMD may be at a greater risk of osteoporosis. Recommendations: Educate and instruct runners to utilize proper training methods so the healthful benefits of crosscountry running, as well as improved performance, are obtained.
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Determination of Noncovalent Intermolecular Interaction Energy from Electron DensitiesMa, Yuguang 21 May 2004 (has links)
Noncovalent intermolecular interactions, widely found in molecular clusters and bio-molecules, play a key role in many important processes, such as phase changes, folding of proteins and molecular recognition. However, accurate calculation of interaction energies is a very difficult task because the interactions are normally very weak. Rigorous expressions for the electrostatic and polarization interaction energies between two molecules A and B, in term of the electronic densities, have been programmed: (see formula in document). Z is atomic charge, ρ0 is the electron density of the isolated molecule and Δρind is the electron density change of the molecule caused by polarization. With some approximations, procedures for electrostatic and polarization energy calculations were developed that involve numerical integration. Electrostatic and polarization energies for several bimolecular systems, some of which are hydrogen bonded, were calculated and the results were compared to other theoretical and experimental data.
A second method for the computing of intermolecular interaction energies has also been developed. It involves a “supermolecule” calculation for the entire system, followed by a partitioning of the overall electric density into the two interacting components and then application of eq. (1) to find the interaction energy. In this approach, according to Feynman’s explanation to intermolecular interactions, all contributions are treated in a unified manner. The advantages of this method are that it avoids treating the supersystem and subsystems separately and no basis set superposition error (BSSE) correction is needed. Interaction energies for several
hydrogen-bonded systems are calculated by this method. Compared with the result from experiment and high level ab initio calculation, the results are quite reliable.
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OxLDL induziert über die Regulation der p27Kip1 Expression die Proliferation in HUVEC: Rolle von RhoA / Oxidized LDL induced Proliferation in HUVEC via Regulation of p27Kip1 Expression: Role of RhoAGegenheimer, Katrin January 2008 (has links) (PDF)
Zellproliferation stellt einen integralen Bestandteil der Plaqueentstehung und somit der Atherosklerose dar. Zahlreiche Studien belegen, daß oxidativ verändertes LDL eine Schlüsselrolle in diesem Pathomechanismus spielt. Neben einer Reihe von proatherogenen Eigenschaften, vermag oxLDL die Zellzyklusregulation insbesondere über den Zyklinkinaseinhibitors p27kip1 zu beeinflussen. Als wichtigen Regulator der Zellproliferation wurde die kleine GTPase RhoA identifiziert. Vor diesem Hintergrund sollte in der vorliegenden Arbeit die oxLDL induzierte Expressionsminderung des Zyklinkinaseinhibitors p27kip1 sowie Zellproliferation über eine Aktivierung des RhoA/Rho-Kinase Signalwegs untersucht werden. Die Aktivierung von RhoA in HUVEC durch oxLDL sollte mittels immunhistochemischem Nachweisverfahren sichtbar gemacht werden. Weiterhin war interessant welche Rolle RhoA in der Signaltransduktion von oxLDL-Wirkungen spielt. Aus diesem Grund und um die Wirkung von RhoA analysieren zu können verwendeten wir die inaktive RhoA N19-Mutante und untersuchten sowohl die Auswirkung der RhoA-Hemmung auf die oxLDL induzierte Zellproliferation als auch auf die oxLDL induzierte p27kip1 Suppression. Zusätzlich sollten die Auswirkungen der Hemmung des nachgeschalteten Effektorproteins von RhoA nämlich Rho-Kinase mittels Y27632 auf die oxLDL-vermittelte Zellproliferation dargestellt werden. Es konnte gezeigt werden, daß oxLDL RhoA zu stimulieren vermag, indem die Translokation von RhoA aus dem Zytosol in die Plasmamembran, als Marker für die Aktivierung von RhoA nach oxLDL Stimulation sichtbar gemacht werden konnte. Die deutlichste Translokation von RhoA wurde nach 5 minütiger oxLDL Inkubation nachgewiesen. Die Hemmung der RhoA Aktivierung durch Transfektion einer dominant negativen RhoA N19 Mutante verdeutlichte, daß sowohl die oxLDL induzierte p27Kip1 Suppression in HUVEC als auch die oxLDL induzierte Proliferation auf die oxLDL vermittelte RhoA Aktivierung angewiesen sind. In Endothelzellen, welche nur mit dem Leervektor pcDNA3 transfiziert waren (Kontrolle), bestätigte sich nach einer vierstündigen oxLDL Inkubation wie in den früheren Untersuchungen eine signifikante Expressionsverminderung von p27Kip1 um ca. 66%. Im Gegensatz dazu konnte in Zellen, die mit der dominant-negativen RhoA N19 Mutante transfiziert waren keine p27Kip1 Suppression festgestellt werden. Ebenso zeigte sich in MTT-Assays bei Zellen mit der inaktiven RhoA N19 Mutante eine nahezu vollständig fehlende Proliferationsantwort. Im Anschluß daran, wurde in weiteren MTT-Assays die oxLDL induzierte Proliferation unter der Verwendung des Rho-Kinase Inhibitors Y27632 untersucht und eine signifikant reduzierte Proliferationsrate von 166 + 19 % im Vergleich zu Kontrollzellen 200 + 12 % nachgewiesen. Dieses Ergebnis könnte dadurch erklärt werden, daß neben dem nachgeschaltetem Effektorprotein Rho-Kinase, die Phosphatidylinositol 3-Kinase (PI3K) in der RhoA vermittelten p27Kip1 Suppression und Zellzyklusprogression eine zusätzliche Rolle zu spielen scheint. Zusammenfassend läßt sich sagen, daß sowohl die oxLDL induzierte Expressionsverminderung von p27Kip1 in HUVEC und somit die Zellprogression als auch die oxLDL induzierte Endothelproliferation auf die oxLDL vermittelte RhoA Aktivierung angewiesen ist. Diese Ergebnisse aus der vorliegenden Arbeit untermauern, daß der RhoA/Rho-Kinase Signalweg ein neuer therapeutischer bzw. medikamentöser Ansatz bei kardiovaskulären Erkrankungen sein könnte. / A typical feature of atherosclerotic plaques is increased cellular turnover, with the parallel existence of cell proliferation and cell death. Oxodized LDL plays a key role in its pathogenesis. Oxidized LDL induces proliferation in HUVEC. The influence of oxLDL on the cyclin-dependent kinase inhibitor p27Kip1, on the activity of small GTPase RhoA as a known regulator of p27Kip1, and on the resulting cell proliferation was studied. RhoA stimulation was assessed by means of its translocation from the cytosolic to the particulate fraction, an effect that is associated with RhoA activation. After oxLDL stimulation the translocation of RhoA to the cell membrane was visible after 1 min and peaked after 5 min of stimulation. We next investigated the influence of RhoA activation on oxLDL induced downregulation of p27Kip1 expression and proliferation. RhoA activity was inhibited in HUVEC by transfection with dominant inhibitory RhoA N19 mutant before stimulation with oxLDL. In cells that were transfected with dominant negative RhoA, the effect of oxLDL on p27Kip1 expression and on cellular proliferation was abolished. HUVEC that were preincubated with the Rho-kinase inhibitor Y27632 also showed a significantly decreased proliferative response to oxLDL stimulation. In summary, oxLDL induced cell-cycle progression via regulation of p27Kip1 expression, resulting in cellular proliferation, involving activation of RhoA. This results confirm, that the Rho/Rho signaling pathway could be a new target for the treatment of vascular disease.
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Bone mineral content in Hong Kong Chinese children: aged 3 to 18 years.January 1991 (has links)
Mahmood Ahmed. / Thesis (M.Phil.)--Chinese University of Hong Kong, 1991. / Includes bibliographical references. / Title / Contents --- p.i-iii / Abstract --- p.2 / Introduction --- p.5 / Definitions : --- p.7 / Chapter - --- Bone --- p.7 / Chapter - --- Bone Cells --- p.9 / Chapter - --- Types of Bone & the Mineral Contents --- p.10 / Chapter - --- Composition of Bone Mass --- p.11 / Chapter - --- Bone Mass --- p.11 / Chapter - --- Factors Affecting The Bone Mass --- p.12 / Bone Minerals --- p.13 / Non Invasive Methods of Measurement of BMC : --- p.16 / Chapter - --- Radiograph --- p.16 / Chapter - --- Quantitative Morphometric --- p.16 / Chapter - --- Radiographic Photodensitometry --- p.16 / Chapter - --- Neutron Activation --- p.17 / Chapter - --- Quantitative Computed Tomography --- p.17 / Chapter - --- Bone Absorptiometery --- p.18 / Chapter - --- Transmission of Ultrasonics --- p.18 / Chapter - --- Dual Photon Absorptiometry --- p.19 / Chapter - --- Bone Scan --- p.19 / Chapter - --- Bone - Specific Biochemical Markers --- p.20 / Chapter - --- Summary --- p.20 / Effects of Drugs on Bone Mass: --- p.22 / Chapter - --- Alcohol --- p.22 / Chapter - --- Tetracycline --- p.22 / Chapter - --- Corticosteroid --- p.23 / Chapter - --- Antacids --- p.23 / Chapter - --- Estrogen --- p.24 / Chapter - --- Vitamins --- p.24 / Causes of Osteopenia in Children --- p.25 / Physical Activity and BMC --- p.28 / Bone Mineral Content - Reviews : --- p.30 / Chapter - --- In Neonates --- p.30 / Chapter - --- Normative Surveys in Children --- p.32 / Chapter - --- Skeletal Abnormalities --- p.35 / HK Chinese Children: / Chapter - --- A General View --- p.37 / Objectives of Study --- p.40 / Chapter - --- Determination of Normal Range --- p.40 / Chapter - --- Determination of Peak Bone Mass --- p.41 / Measurement of BMC : --- p.43 / Chapter - --- Material --- p.43 / Methods and Subjects --- p.46 / Chapter - --- Location of Scanning Site --- p.46 / Chapter - --- Recruitment of Subjects --- p.47 / Chapter - --- Statistical Analysis --- p.48 / Reproducibility of Measurement: --- p.56 / Chapter - --- The Means --- p.56 / Chapter - --- The Correlations --- p.57 / Results --- p.58 / Chapter - --- 6 months to 3 years --- p.58 / Chapter - --- 3 to 7 years --- p.60 / Chapter - --- 7 to 18 years --- p.61 / Chapter - --- 3 to 18 years --- p.62 / Chapter - --- Dual Energy X-Ray Absorptiometry versus Single Photon Absorptiometry --- p.66 / Graphs & Charts / Chapter - --- Age Distribution --- p.50 / Chapter - --- Dominance Distribution --- p.51 / Chapter - --- BMC from 0.6 to 2.9 years --- p.59 / Chapter - --- BMC Male & Female Difference --- p.63 / Chapter - --- BMC Dominance Difference --- p.64 / Chapter - --- BMC Predicted & Measured Value --- p.65 / Chapter - --- BMD by SPA vs DEXA --- p.67 / Discussions --- p.68 / Chapter - --- BMC & Total Body Calcium --- p.68 / Chapter - --- Age --- p.70 / Chapter - --- Handedness --- p.71 / Chapter - --- Bone Width --- p.72 / Chapter - --- Weight --- p.73 / Chapter - --- Sex --- p.73 / Chapter - --- Height --- p.74 / Chapter - --- "Nutritional Status, Calc. Intak" --- p.74 / Comparison --- p.75 / Chapter - --- BMC in Pathological Conditions --- p.75 / Chapter - --- Comparison with other series --- p.76 / Conclusion --- p.82 / Diagram --- p.45 / Chapter - --- Schematic Diagram of Equipment --- p.45 / Picture --- p.52 / Chapter - --- Single Photon Absorptiometry --- p.52 / Chapter - --- Dual Energy X-Ray Absorptiometry --- p.53 / Chapter - --- Single Photon Absorptiometry (Neonates) --- p.54 / Chapter - --- Photon Absorption Technique --- p.55 / Table --- p.78 / Chapter - --- Table I (Average yearly BMC & BMD) --- p.78 / Chapter - --- Table II(Average yearly Change in BMC) --- p.79 / Chapter - --- TableIII(BMC from 3 to 18 years) --- p.80 / Chapter - --- Table IV (Regression Analysis) --- p.81 / Appendix --- p.83 / Acknowledgements --- p.95 / References --- p.96-99
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Characteristics associated with bone mineral density screening in a sample of adults with intellectual disabilitiesDreyfus, Deborah Elizabeth January 2012 (has links)
Thesis (M.S.)--Boston University / PLEASE NOTE: Boston University Libraries did not receive an Authorization To Manage form for this thesis or dissertation. It is therefore not openly accessible, though it may be available by request. If you are the author or principal advisor of this work and would like to request open access for it, please contact us at open-help@bu.edu. Thank you. / Adults with Intellectual Disability (ID) are at an elevated risk of osteoporosis based on lower peak bone mass and medical characteristics. However, there is little data as to how the medical characteristics affect screening or at what ages people are being screened. Methods: A secondary cross-sectional data analysis of was conducted of 4777 adults witl1 Intellectual Disability to determine characteristics associated with an elevated risk for osteoporosis and receipt of bone density screening. Hypotheses were that increasing age, use of antiseizure medication, living in a 24 hour residential setting, and receiving a flu vaccine increased the likelihood of screening. Bivariate analyses were initially performed, tl1en data were stratified by gender and logistic regressions were performed. Findings: 22.2% of the sample in this study received bone density screening. Bivariate odds ratios identified each of the hypothesized variables as significantly associated with receiving screening. Additionally, many of the covariates analyzed identified significant associations with receiving screening.Data were then stratified by gender and evaluated in a logistic regression. In men, increasing age, tl1e use of antiepileptic medication (adjusted odds ratio (OR) 1.5; 95% confidence interval (CI) 1.2-2.0), and receiving the flu vaccine (adjusted OR 1.5; 95% CI 1.2-2.0) were associated witl1 an increased likelihood of screening, controlling for confounding. Living in a 24 hour residential setting was not significantly associated with screening (adjusted OR 1.2; 95% CI 0.91-1.6). In women, increasing age, the use of antiepileptic medication (adjusted OR 1.5; 95% CI 1.2-1.9), receiving the flu vaccine (adjusted OR 1.4; 95% CI 1.1-1.8), and living in a 24 hour residential setting (adjusted OR 1.4; 95% CI 1.1 -1.8) were all significantly associated with receiving screening. A history of Down syndrome, noted to increase risk of osteoporosis, was associated with a decreased likehl1ood of screening (adjusted OR 0.67; 95% CI 0.4 7-0. 94) in women, although it was not a significant association in men. Conclusions: While most variables related to osteoporosis are associated with an increased likelihood of screening, screening rates among in adults witl1 ID were low. Additionally, men and women have differences in variables related to screening. Better education and improved awareness may increase rates. / 2031-01-02
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