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Content available Exploring the Influence of NC on the Crystallization of HTPE
100%
Ren Z. , Li X. , Liu M. , Zhang X. , Xie L.
Central European Journal of Energetic Materials
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2023
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tom Vol. 20, no. 3
318--339
EN
A series of polymer blends of nitrocellulose (NC) and hydroxy terminated polyether (HTPE) in different proportions were prepared by a solution mixing method. The diffraction peak positions and peak intensities of the blends were analyzed by X-ray diffraction. The relative crystallinity of HTPE in the blends was analyzed by differential scanning calorimetry. The crystal morphology of the NC/HTPE blends was observed with a polarizing microscope. The results demonstrated that there is a certain degree of crystallinity in pure HTPE, while the crystallinity of NC/HTPE blends was gradually decreased as NC was added. In addition, when the mass fraction of NC in the blends was more than 40%, the crystallinity of the blends was hardly observed by these characterization methods, which demonstrated that the crystallinity of HTPE could be easily inhibited by NC.
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Content available remote Development of a rapid LC-MS/MS assay to determine letrozole in human plasma and its application in a pharmacokinetic study after oral administration
72%
Li P. , Zhang X. , Wang S. , Wang J. , Liu Z. , Wang C. , Tong W. , Liu L.
Acta Chromatographica
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2022
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tom Vol. 34, no. 2
179--184
EN
Letrozole is one of the third generation aromatase inhibitors. It is suitable for the treatment of postmenopausal patients with advanced breast cancer and early treatment of breast cancer. It is necessary to develop a rapid, reliable, selective and sensitive LC–MS/MS assay to determine letrozole in human plasma to evaluate the clinical efficacy and adverse reactions with clinical pharmacokinetic and therapeutic drug monitoring. Separation was carried out on a Kromasil-C18 column using acetonitrile-water (55: 45, v/v) as mobile phase. Detection was carried out by multiple reaction monitoring on a 3200Qtrap mass spectrometry. The method needed one-step protein precipitation procedure only, and the cycle time was 2.5 min allowing 500–550 samples per day. It was linear within 0.30–50.00 ng/mL for plasma with the limit of detection (LOD) of 0.030 ng/mL. The intra- and inter-day RSD were 5.51–8.63%, 2.28–9.95% and the RE was 0.18–1.65%. The recovery rates of letrozole and internal standard for plasma were 89.30–98.55%. Letrozole was stable under all the conditions in the study. The method was sensitive enough to quantitate letrozole over a period of 288 h after giving a single oral dose of 2.5 mg–24 Chinese healthy volunteers. The absorption of letrozole was rapid with small individual difference, the tissue distribution of letrozole was more than that in blood, and the clearance was slow. Letrozole was similar to three-compartment model in vivo. Due to metabolism and excretion, the AUCs of letrozole varied greatly among individuals.
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