960 resultados para binary descriptor


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Mode of access: Internet.

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"Supported in part...under Grant No. US NSF GJ812 and Grant No. US NSF GJ813."

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Bibliography: p. 26.

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"UILU-ENG 84 1703"--Cover.

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"Supported by Contract AT (11-1)-1018 with the U.S. Atomic Engery Commission."

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Thesis (M.S.)--University of Illinois at Urbana-Champaign.

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Includes bibliographical references (leaves 132-134).

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Includes bibliographical references.

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"Materials Laboratory, Contract No. AF33(616)-5771, Project No. 7021."

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"Prepared under the sponsorship of Rome Air Development Center, Air Research and Development Command, United States Air Force, Griffiss Air Force Base, New York, Advanced Development Laboratory. Contract no. AF 30 (602)-1702, project no. 4519, task no. 45232."

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"Materials Central, Contract no. 33(616)-5995. Project no. 7351.

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Adsorption of p-cresol, nitrobenzene and p-nitrophenol on treated and untreated carbons is investigated systematically. The effects of carbon surface chemistry and solution pH are studied and discussed. All adsorption experiments were carried out in pH-controlled solutions to examine the adsorption properties of the adsorption systems where the solutes are in molecular as well as ionic forms. Using the homogeneous Langmuir equation, the single solute parameters are determined. These parameters are then used to predict the binary solute adsorption isotherms and gain further insights into the adsorption process. (C) 2002 Elsevier Science Ltd. All rights reserved.

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The prevalence of obesity in the western world is dramatically rising, with many of these individuals requiring therapeutic intervention for a variety of disease states. Despite the growing prevalence of obesity there is a paucity of information describing how doses should be adjusted, or indeed whether they need to be adjusted, in the clinical setting. This review is aimed at identifying which descriptors of body size provide the most information about the relationship between dose and concentration in the obese. The size descriptors, weight, lean body weight, ideal body weight, body surface area, body mass index, fat-free mass, percent ideal body weight, adjusted body weight and predicted normal body weight were considered as potential size descriptors. We conducted an extensive review of the literature to identify studies that have assessed the quantitative relationship between the parameters clearance (CL) and volume of distribution (V) and these descriptors of body size. Surprisingly few studies have addressed the relationship between obesity and CL or V in a quantitative manner. Despite the lack of studies there were consistent findings: (i) most studies found total body weight to be the best descriptor of V. A further analysis of the studies that have addressed V found that total body weight or another descriptor that incorporated fat mass was the preferred descriptor for drugs that have high lipophilicity; (ii) in contrast, CL was best described by lean body mass and no apparent relationship between lipophilicity or clearance mechanism and preference for body size descriptor was found. In conclusion, no single descriptor described the influence of body size on both CL and V equally well. For drugs that are dosed chronically, and therefore CL is of primary concern, dosing for obese patients should not be based on their total weight. If a weight-based dose individualization is required then we would suggest that chronic drug dosing in the obese subject should be based on lean body weight, at least until a more robust size descriptor becomes available.