共查询到20条相似文献,搜索用时 93 毫秒
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以手性高效液相色谱分析法为检测手段,研究了AOT-水-正庚烷微乳液反应介质中,脂肪酶催化消旋布洛芬的不对称酯合成反应。结果表明,在此反应介质中,消旋布洛芬与正辛醇能顺利地进行酯合成反应,转化率达0.3613,产物为光学纯度很高的S-构型布洛芬辛酯,其对映体过量值为0.9732。微乳液中的含水量叫。值(水与表面活性剂的摩尔数比)及AOT浓度主要影响酯合成反应转化率,对产物对映体过量值没有太大的影响;不同链长的脂肪醇不仅影响酯合成反应速率及其对应的最佳ω0值,还影响产物的对映体过量值。 相似文献
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本文对固相肽合成中得到普遍应用的四种接肽方法的活化方式、反应途径、优点与不足及近年来的进展情况作了较为详细的介绍相综述。 相似文献
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利用标记药物布洛芬及保泰松研究萘啶酸与血清白蛋白的结合作用 总被引:2,自引:0,他引:2
血清白蛋白与萘啶酸的结合,可以猝灭萘啶酸-铽螯合体系的特征荧光,保泰松(Phenylbutazone)及布洛芬(Ibuprofen)等药物在白蛋白的特定结合位置与其具有较强的结合作用,因此,可用作白蛋白分子结合位置的标记物。本文以保泰松或布洛芬作标记物,探讨了牛血清白蛋白及人血清白蛋白对萘啶酸-铽螯合体系特征荧光的不同影响方式,并根据蛋白结合位上药物的置换作用确定了萘啶酸在牛血清白蛋白分子上的结合位置。 相似文献
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纳米材料的辐射合成法制备 总被引:27,自引:0,他引:27
概述了辐射合成法制备钠米材料的基本原理及最新进展,比较了辐射合成法相对于一般纳米材料制备方法的优点,并对辐射合成方法的一步发展作了展望。 相似文献
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毛细管区带电泳法快速测定复方布洛芬片的有效成分 总被引:3,自引:0,他引:3
研究了用毛细管区带电泳法快速测定复方布洛芬片中布洛芬和伪麻黄碱含量的方法。在0.025mol/L的磷酸盐缓冲液(pH8.1)中,上述两组分可在3min内得以完全分离,用紫外检测器在210nm处检测,并以外标法定量。11次测定含有9.5mg/L盐酸伪麻黄碱和66.7mg/L布洛芬的试样溶液,相对标准偏差为2.9%(伪麻黄碱)和1.9%(布洛芬),回收率为103.1%(伪麻黄碱)和97.6%(布洛芬)。应用毛细管区带电泳法测定复方布洛芬片剂的含量,所得结果与HPLC法一致。 相似文献
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Lievano R Pérez HI Manjarrez N Solís A Solís-Oba M 《Molecules (Basel, Switzerland)》2012,17(3):3148-3154
A novel application of whole cells of Nocardia corallina B-276 for the deracemisation of ibuprofen is reported. This microorganism successfully hydrolysed ibuprofen nitrile to ibuprofen amide, and ibuprofen amide to ibuprofen, using a suspension of cells in a potassium phosphate buffer solution (0.1 M, pH = 7.0). These results can be explained by the presence of NHase and amidase enzymes, but the reactions are not enantioselective and low ee values were obtained. However, (R)-ibuprofen was isolated with > 99% ee by a deracemisation process catalysed by N. corallina B-276. This is the first report of this kind of catalysis with this microorganism. 相似文献
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M Fatnassi C Tourné-Péteilh T Mineva JM Devoisselle P Gaveau F Fayon B Alonso 《Physical chemistry chemical physics : PCCP》2012,14(35):12285-12294
Silica microspheres encapsulating ibuprofen in separated domains at the nanometre scale are formed by spray-drying and sol-gel processes. A detailed (1)H and (13)C NMR study of these microspheres shows that ibuprofen molecules are mobile and are interacting through hydrogen bonds with other ibuprofen molecules. (1)H magnetisation exchange NMR experiments were employed to characterize the size of the ibuprofen domains at the nanometre scale. These domains are solely formed by ibuprofen, and their diameters are estimated to be ~40 nm in agreement with TEM observations. The nature and formation of these particular texture and drug dispersion are discussed. 相似文献
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A capillary gas chromatographic-mass spectrometric method for the determination of ibuprofen and tetra-deuterated ibuprofen in serum is described. Ibuprofen, [ar-2H4]ibuprofen and the internal standard, [ar-2H4,3,3,3-2H3]ibuprofen, are extracted (after acidification) from serum onto a cross-linked styrene divinyl benzene resin by an automated sample processor. After elution and evaporation of the organic phase, samples are reconstituted with solvent and analyzed without derivatization by capillary gas chromatography-mass spectrometry. This methodology was used to evaluate possible kinetic isotope effects after the coadministration of an equimolar mixture of ibuprofen and the deuterium-labeled covariant in the beagle. No significant differences in absorption or elimination were observed. 相似文献
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Stephenson BC Rangel-Yagui CO Pessoa Junior A Tavares LC Beers K Blankschtein D 《Langmuir : the ACS journal of surfaces and colloids》2006,22(4):1514-1525
Surfactants can be used to increase the solubility of poorly soluble drugs in water and to increase drug bioavailability. In this article, the aqueous solubilization of the nonsteroidal, antiinflammatory drug ibuprofen is studied experimentally and theoretically in micellar solutions of anionic (sodium dodecyl sulfate, SDS), cationic (dodecyltrimethylammonium bromide, DTAB), and nonionic (dodecyl octa(ethylene oxide), C12E8) surfactants possessing the same hydrocarbon "tail" length but differing in their hydrophilic headgroups. We find that, for these three surfactants, the aqueous solubility of ibuprofen increases linearly with increasing surfactant concentration. In particular, we observed a 16-fold increase in the solubility of ibuprofen relative to that in the aqueous buffer upon the addition of 80 mM DTAB and 80 mM C12E8 but only a 5.5-fold solubility increase upon the addition of 80 mM SDS. The highest value of the molar solubilization capacity (chi) was obtained for DTAB (chi = 0.97), followed by C12E8 (chi = 0.72) and finally by SDS (chi = 0.23). A recently developed computer simulation/molecular-thermodynamic modeling approach was extended to predict theoretically the solubilization behavior of the three ibuprofen/surfactant mixtures considered. In this modeling approach, molecular-dynamics (MD) simulations were used to identify which portions of ibuprofen are exposed to water (hydrated) in a micellar environment by simulating a single ibuprofen molecule at an oil/water interface (modeling the micelle core/water interface). On the basis of this input, molecular-thermodynamic modeling was then implemented to predict (i) the micellar composition as a function of surfactant concentration, (ii) the aqueous solubility of ibuprofen as a function of surfactant concentration, and (iii) the molar solubilization capacity (chi). Our theoretical results on the solubility of ibuprofen in aqueous SDS and C12E8 surfactant solutions are in good agreement with the experimental data. The ibuprofen solubility in aqueous DTAB solutions was somewhat overpredicted because of challenges associated with accurately modeling the strong electrostatic interactions between the anionic ibuprofen and the cationic DTAB. Our results indicate that computer simulations of ibuprofen at a flat oil/water interface can be used to obtain accurate information about the hydrated and the unhydrated portions of ibuprofen in a micellar environment. This information can then be used as input to a molecular-thermodynamic model of self-assembly to successfully predict the aqueous solubilization behavior of ibuprofen in the three surfactant systems studied. 相似文献
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Dong Wang Yun Sheng Ding Jin Li Cao Yue He Sheng Feng Ye Shun Geng Min 《中国化学快报》2011,22(11):1335-1338
The NIR micro-images of ibuprofen tablets were collected in this research.Compare correlation imaging and principal component analysis(PC A) with histogram were applied to acquire the spatial distribution of ibuprofen granule.The result indicated that a similar distribution trend can be acquired by both of the two methods mentioned above;the information of PC2 results from ibuprofen mainly since the correlation coefficient between PC2 loading vector and the NIR spectrum of ibuprofen is 0.9930.The result of PCA indicated that the information of PC2 results from ibuprofen mainly for both the low and the high content of ibuprofen in the tablets.The correlation coefficient between the data of the two PC2 loading vectors of the low and the high content of ibuprofen in the tablets is 0.9998,which indicates that the result of PCA is stable and reliable. 相似文献
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The solubility of acetaminophen and ibuprofen in binary and ternary mixtures of N-methyl pyrrolidone, polyethylene glycol
600 and water at 25 °C were determined and the solubilities are mathematically represented by the Jouyban–Acree model. The
density of the solute-free solvent mixtures was measured and employed to train the Jouyban–Acree model and then the densities
of the saturated solutions were predicted. The overall mean relative deviations (OMRDs) for fitting the solubility data of
acetaminophen and ibuprofen in binary mixtures are 3.2% and 6.0%, respectively. The OMRDs for fitting the solubilities in
ternary solvent mixtures for acetaminophen and ibuprofen are 15.0% and 28.6%, respectively, and the OMRD values for predicting
all solubilities of acetaminophen and ibuprofen by a trained version of the Jouyban–Acree model are 9.4% and 17.8%, respectively.
The prediction OMRD for the density of saturated solutions is 1.9%. 相似文献
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Submicron particles with modified surface were synthesized by a simple one-pot synthesis approach and used as drug carrier for controlled release. Due to the alkalinity of MgO species on the surface, the amount of a model drug, ibuprofen, adsorbed on the modified surface was increased as compared to pure silica SBA-15 although the surface area was decreased by the surface modification. FTIR investigation indicated that the adsorption state of ibuprofen on MgO modified SBA-15 was different from that on pure silica SBA-15 and pure crystal ibuprofen. The result obtained from in vitro release test exhibited that the surface modification greatly decreased the ibuprofen release rate. In first 6 h in vitro release test, only 63% of the adsorbed ibuprofen was released from the MgO/SBA-15 (Si/Mg=20). In contrast, the release of ibuprofen was complete in 1 h from the pure silica SBA-15 under the same release conditions. The surface modified with MgO created affinity with acidic ibuprofen molecules and retarded the release rate from the mesoporous matrix. In addition, the release rate of ibuprofen could be modulated by varying the content of MgO, and was found to decrease with increasing amount of MgO on surface of SBA-15 submicron particles. 相似文献