Preparing molecularly imprinted nanoparticles of saponins via cooperative imprinting strategy

Saponin is an important class of natural products with various pharmacological activities. The selective separation of saponins is an essential step before further analysis. Molecular imprinting has been an effective strategy for preparing antibody mimics. However, a facile and efficient imprinting strategy for saponins is still lacking owing to their amphiphilic nature. Herein, we have prepared the saponins imprinted nanoparticles via cooperative imprinting strategy. This new strategy relies on the combination of various non‐covalent interactions (hydrophobic and hydrogen bonding) and covalent boronate affinity interactions. The obtained imprinted nanoparticles could rebind specific saponins from complex matrices with good selectivity, superb tolerance to interference, and fast binding equilibrium. This method was verified to be versatile and facile. Thus, this strategy could greatly facilitate the preparation of imprinted nanoparticles for the specific recognition of saponins.     

Strategy for the chiral separation of non-acidic pharmaceuticals using capillary electrochromatography

In completion of an earlier defined generic chiral screening approach, a generic separation strategy for basic, bifunctional, and neutral compounds was proposed and evaluated. This strategy adds to a previously defined strategy for acidic compounds. The screening experiment of the actual strategy used a mobile phase of 5 mM phosphate buffer pH 11.5/ACN (30/70 v/v), a temperature of 25 degrees C, and a voltage of 15 kV. The selected chiral stationary phases were Chiralpak AD-RH, Chiralcel OD-RH, Chiralcel OJ-RH, and Chiralpak AS-RH, all based on polysaccharide selectors. It was seen that 31 out of 48 test compounds were partially or baseline-resolved under screening conditions. After execution of the optimization steps of the strategy, this number increased to 41, with a total of 21 baseline-separated compounds. Combined with the results obtained from the acidic test set examined in the earlier defined strategy, of all tested compounds 82.5% showed enantioselectivity and 49.2% could be baseline-separated.     

Structural Transformation: Assembly of an Otherwise Inaccessible DNA Nanocage

A strategy of structural transformation for the assembly of DNA nanocages that can not be assembled directly is described. In this strategy, a precursor DNA nanocage is assembled first and then is isothermally transformed into a desired, complicated nanocage. A dramatic, conformational change accompanies the transformation. This strategy has been proven to be successful by native polyacrylamide gel electrophoresis (PAGE) and cryogenic electron microscopy (cryoEM) imaging. We expect that the strategy of structural transformation will be useful for the assembly of many otherwise inaccessible DNA nanostructures and help to increase the structural complexity of DNA nanocages.     

A quick and effective multivariate statistical strategy for imaging mass spectrometry

A new multivariate statistical strategy for analyzing large datasets that are produced by imaging mass spectrometry（IMS） techniques is reported.The strategy divides the whole datacube of the sample into several subsets and analyses them one by one to obtain the results.Instead of analyzing the whole datacube at one time,the strategy makes the analysis easier and decreases the computation time greatly.In this report,the IMS data are produced by the air flow-assisted ionization IMS（AFAI-IMS）.The strategy can be used in combination with most multivariate statistical analysis methods.In this paper,the strategy was combined with the principal component analysis（PCA） and partial least square analysis（PLS）.It was proven to be effective by analyzing the handwriting sample.By using the strategy,the m/z corresponding to the specific lipids in rat brain tissue were distinguished successfully.Moreover the analysis time grew linearly instead of exponentially as the size of sample increased.The strategy developed in this study has enormous potential for searching for the mjz of potential biomarkers quickly and effectively.     

Copper(II)-catalyzed-α-C(sp3)-H activation of cyclic amines: A simple and efficient strategy for the synthesis of fused pyrazole derivatives

In this paper, we have described a simple and efficient strategy for the synthesis of fused pyrazole derivatives. The key steps of our strategy involves hydroamination, copper-catalyzed cross dehydrogenative coupling (CDC) followed by aromatization (aerial oxidation) in one-pot. Our strategy offers a valuable alternative to known methods for synthesis of fused pyrazole derivatives. Overall, we have synthesized 13 diverse fused pyrazole derivatives in moderate to excellent yields.     

A Self-Supporting Strategy for Gas-Phase and Slurry-Phase Ethylene Polymerization using Late-Transition-Metal Catalysts

The polyolefin industry is dominated by gas-phase and slurry-phase polymerization using heterogeneous catalysts. In contrast, academic research is focused on homogeneous systems, especially for late-transition-metal catalysts. The heterogenization of homogeneous catalysts is a general strategy to provide catalyst solutions for existing industrial polyolefin synthesis. Herein, we report an alternative, potentially general strategy for using homogeneous late-transition-metal catalysts in gas-phase and slurry-phase polymerization. In this self-supporting strategy, catalysts with moderate chain-walking capabilities produced porous polymer supports during gas-phase ethylene polymerization. Chain walking, in which the metal center can move up and down the polymer chain during polymerization, ensures that the metal center can travel along the polymer chain to find suitable sites for ethylene enchainment. This strategy enables simple heterogenization of catalysts on solid supports for slurry-phase polymerization. Most importantly, various branched ultra-high-molecular-weight polyethylenes can be prepared under various polymerization conditions with proper catalyst selection.     

直接甲醇燃料电池甲醇传质过程分析及浓度控制策略

甲醇溶液浓度对于直接甲醇燃料电池(DMFC)的性能具有重要影响。 本文旨在建立一种能在电源系统中有效控制甲醇浓度的策略。 通过构建电池内甲醇物料守恒和热守恒方程,确定了基于电量和温度这两个参数的甲醇浓度控制策略。 通过测试温度-浓度关系验证了控制策略的可行性。 结果表明,采用该策略,DMFC电源系统稳定运行超过420 min;合适的甲醇浓度范围为0.70~0.87 mol/L。 该策略完成了甲醇浓度控制的目标,并将在电源系统中发挥重要作用。     

生物质能源的开发与利用

本文概述了生物质能源的特征以及发展生物质能源的意义,综述了国内外生物质能源开发与利用的现状,简介了中国石油天然气股份有限公司生物质能源的发展思路、部署及工作进展。中国石油天然气股份有限公司生物质能源发展策略重点放在发展生物柴油和燃料乙醇。本文结合公司生物质能源长期发展战略以及实际工作开展情况分别从生物柴油、燃料乙醇两个方面详细探讨了所面临的生物质能源化工关键技术的需求,并提出相关发展建议。     

INHIBIT‐Inspired Two‐Output DNA Logic Gates Based on Surface‐Enhanced Raman Scattering

Herein, we presented a novel logic gate based on an INHIBITION gate that performs parallel readouts. Logic gates performing INHIBITION and YES/OR were constructed using surface‐enhanced Raman scattering as optical outputs for the first time. The strategy allowed for simultaneous reading of outputs in one tube. The applicability of this strategy has been successfully exemplified in the construction of half‐adder using the two‐output logic gates as reporting gates. This reporting strategy provides additional design flexibility for dynamic DNA devices.     

A two-component small molecule system for activity-based detection and signal amplification: application to the visual detection of threshold levels of Pd(II)

A detection and signal amplification strategy aimed toward threshold diagnostic assays for use in resource-limited settings is described. The strategy employs two small molecule reagents that work in tandem. One reagent detects a specific analyte, while the second amplifies a colorimetric readout autocatalytically. The strategy is demonstrated using palladium(II) as a model analyte.     

Effect of antibody immobilization strategies on the analytical performance of a surface plasmon resonance-based immunoassay

Antibody immobilization strategies (random, covalent, orientated and combinations of each) were examined to determine their performance in a surface plasmon resonance-based immunoassay using human fetuin A (HFA) as the model antigen system. The random antibody immobilization strategy selected was based on passive adsorption of anti-HFA antibody on 3-aminopropyltriethoxysilane (APTES)-functionalized gold (Au) chips. The covalent strategy employed covalent crosslinking of anti-HFA antibody on APTES-functionalized chips using 1-ethyl-3-[3-dimethylaminopropyl]carbodiimide (EDC) and sulfo-N-hydroxysuccinimide (SNHS). The orientation strategy used passive adsorption of protein A (PrA) on Au chips, with subsequent binding of the anti-HFA antibody in an orientated fashion via its fragment crystallisable (Fc) region. In the covalent-orientated strategy, PrA was first bound covalently, to the surface, which in turn, then binds the anti-HFA antibody in an orientated manner. Finally, in the most widely used strategy, covalent binding of anti-HFA antibody to carboxymethyldextran (CM5-dextran) was employed. This immobilization strategy gave the highest anti-HFA antibody immobilization density, whereas the highest HFA response was obtained with the covalent-orientated immobilization strategy. Therefore, the covalent-orientated strategy was the best for SPR-based HFA immunoassay and can detect 0.6-20.0 ng/mL of HFA in less than 10 min.     

A new strategy for the synthesis of benzylic sulfonamides: palladium-catalyzed arylation and sulfonamide metathesis

An efficient two-step strategy has been developed to access diversely functionalized benzylic sulfonamides. Execution of this strategy required the development of two reaction methods: the palladium-catalyzed cross-coupling of aryl halides with CH-acidic methanesulfonamides and a metathesis reaction between the resulting alpha-arylated sulfonamides and diverse amines. The broad scope of the cross-coupling process combined with a versatile sulfonamide metathesis constitutes an efficient strategy for the synthesis of various benzylic sulfonamides.     

Cross metathesis functionalization of polyolefins

A cross metathesis strategy is reported for the post-polymerization functionalization of the pendant vinyl groups present in a range of polyolefin architectures. This represents a general strategy for the synthesis of tailored random and block copolymers as well as homopolymers.     

Frame‐Guided Assembly of Amphiphiles

Frame‐guided assembly, a recently discovered strategy for amphiphilic assembly, is discussed as a strategy for constructing vesicle assemblies with programmed geometries and dimensions under identical surrounding conditions. The strategy is inspired by the cytoskeletal‐membrane protein–lipid bilayer structure and shows great potential in the understanding and controlling of the amphiphilic assembly process. Both the principles and basic requirements are discussed, along with recently reported examples. The prospects and potential investigations of frame‐guided assembly are also proposed.     

催化不对称反应新进展—不对称活化

介绍了催化不对称催化反应中的一个新概念一不对称活化(asymmetric activation)及其研究的最新进展。运用不对称活化策略,一个光学活性的或者甚至外消旋的催化剂可以被另一种手性活化剂(chiral activator)选择性地活化,从而催化反应生成非外消旋产物。该方法较不对称去活化(asymmetric deactivation)方法的优点是被活化的催化剂能够产生较使用光学纯催化剂更高对映体过量的产物。     

基于TMT10-plex等量标记结合SMOAC富集磷酸肽的定量磷酸化蛋白质组性能评价

探索并建立了一种快速、 简便且高通量定量磷酸化蛋白质组的策略, 即采用连续互补的磷酸化富集方法SMOAC(Sequential enrichment of metal oxide affinity chromatography)结合TMT(Tandem mass tag)标记技术定量磷酸化蛋白质组学. 以3例经紫草素处理的及3例正常的人肝癌 HepG2 细胞为实验材料, 经Trypsin酶解后的肽段用TMT10-plex试剂进行等量标记, 标记肽段先经TiO₂富集, 收集包含磷酸化肽段的洗脱液, 接着用次氮基三醋酸铁(Fe-NTA)对TiO₂的流穿液和清洗液进行二次富集, 再次收集包含磷酸化肽段的洗脱液. 整个实验流程做2组, 对其中一组的2次洗脱液分别分析, 另一组的2次洗脱液合并分析. 在SMOAC的2次洗脱液合并分析中鉴定到4263个磷酸化蛋白上超过13000条磷酸化肽, 富集特异性>97%, 其中被定量的磷酸化蛋白为3848个, 占总鉴定量的90%以上. 研究结果表明, SMOAC 能够有效提高磷酸化肽段的鉴定效率, 且能与TMT等量标记试剂结合, 实现对少量蛋白样品的磷酸化蛋白定量分析.     

Photolithographic synthesis of cyclic peptide arrays using a differential deprotection strategy

We report here a strategy for the photolithographic synthesis of diverse, spatially addressable arrays of cyclic peptides which employs a differential deprotection strategy for the combinatorial addition of side chains to a pre-fabricated cyclic core.     

Reversed-phase depletion coupled with hydrophilic affinity enrichment for the selective isolation of N-linked glycopeptides by using Click OEG-CD matrix

Selective enrichment of glycopeptides is of great importance for protein glycosylation analysis using mass spectrometry since the signals of glycopeptides could be severely suppressed by the coexisting non-glycosylated peptides in the protein digest. In the present work, a strategy for N-linked glycopeptide enrichment through reversed-phase depletion coupled with hydrophilic affinity enrichment by applying the customized matrix named Click OEG-CD is developed. Compared with single hydrophilic interaction liquid chromatography (HILIC) mode, the strategy exhibited remarkably higher selectivity for N-linked glycopeptides. As many as 22, 18, and eight glycopeptides were detected in the glycopeptide fraction enriched with the strategy from the digests of human immunoglobulin G, horseradish peroxidase and bovine ribonuclease B, respectively. In addition, the strategy also showed high glycosylation microheterogeneity coverage for the enrichment of human α₁-acid glycoprotein glycopeptides. More than 170 glycopeptides covering all the glycosylation sites were detected in the enriched fraction. The revered-phase liquid chromatography depletion coupled with HILIC enrichment strategy by using Click OEG-CD matrix is expected to show more potential in further applications in glycosylation analysis.     

Maintenance of a calibration model for near infrared spectrometry by a combined principal component analysis-partial least squares approach

A novel strategy for building and maintaining calibration models has been developed for use when the future boundaries of the sample set are unknown or likely to change. Such a strategy could have an impact on the economics and time required to obtain and maintain a calibration model for routine analysis. The strategy is based on both principal component analysis (PCA) and partial least squares (PLS) multivariate techniques. The principal action of the strategy is to define how “similar” a new sample is to the samples currently defining the calibration dataset. This step is performed by residuals analysis, following PCA. If the new sample is considered to have a spectrum “similar” to previously available spectra, then the model is assumed able to predict the analyte concentration. Conversely, if the new sample is considered “dissimilar”, then there is new information in this sample, which is unknown to the calibration model and the new sample is added automatically to the calibration set in order to improve the model. The strategy has been applied to a real industrial dataset provided by BP Amoco Chemicals. The data consists of spectra of 102 sequential samples of a raw material. The strategy produced an accurate calibration model for both target components starting with only the first four samples, and required a further 17 reference measurements to maintain the model for the whole sampling sequence, which was over a 1-year period.     

Implementation of a rapid and automated high performance liquid chromatography method development strategy for pharmaceutical drug candidates

A comprehensive, fully automated strategy is demonstrated for HPLC-UV chromatographic method development using ChromSword optimization software. The strategy involves: (1) the automated screening of various column and mobile phase combinations, (2) rational selection of the best starting conditions; and (3) subsequent automated method development to generate optimized separation methods. Pharmaceutical compounds were applied to solve problematic drug impurity separations. ChromSword software automates the screening, optimization, and documentation steps thus reducing the method development time. The strategy was compared to a manual method development approach showing the automated method strategy affords better selectivity in a shorter time.