GC/MS法分析油松节挥发油化学成分

用气相色谱-质谱法对山东昆嵛山产油松节挥发油进行化学成分的分析。采用水蒸气蒸馏法从油松节中提取挥发油。采用不同类型的毛细管柱进行分析，找出最佳分析条件，用归一化法测定其含量，并用气相色谱-质谱法对化学成分进行鉴定。共鉴定了48个成分，占挥发油总成分的84％以上。结果表明，此方法稳定可靠，重现性好，适用于中药挥发油的化学成分分析。     

马山前胡挥发油化学成分研究

本文用毛细管气相色谱、气相色谱／质谱／计算、气相色谱／红外光谱等现代仪器分析技术，对马山前胡挥发油的化学成分进行了分析研究，从毛细管色谱分离出８０多个峰，确认了其中３７种成分，占色谱总馏出峰面积的９７％以上，该挥发油的主要化学成分为蒎烯。     

GC-MS法分析康定鼠尾草花挥发油中的化学成分

用水蒸气蒸馏法从康定鼠尾草花中提取挥发油,并用气相色谱/质谱联用技术(GC-MS)对挥发油的化学成分进行分离鉴定,用气相色谱峰面积归一化法确定各组分的相对含量,结果从康定鼠尾草花挥发油中鉴定出89种化合物,占总挥发油量的95%以上,其中主要成分是二苯胺(21.528%)、芳樟醇(9.873%)、2-丙酮基-3-蒈烯(7.533%)、1,3,3-三甲基-2-丁酮-环己二烯(5.088%)。本文通过对康定鼠尾草花挥发油化学成分的研究,为鼠尾草资源的进一步开发利用提供实验依据。     

白千层挥发油化学成分分析

用毛细管气相色谱、气相色谱－ 质谱－ 计算机分析技术, 对植物白千层枝叶挥发油化学成分进行了分析研究, 从这种植物挥发油中分离出８０ 个以上的组分, 确认了其中的３５ 种成分, 所鉴定的组分占挥发油色谱总峰面积的９０ ％ 以上。     

GC／MS法测定木香挥发油化学成分

用气相色谱-质谱法对木香挥发油进行化学成分的分析。采用水蒸气馏法从木香中提取挥发油。试用不同类型的毛细管柱进行分析,找出最佳分析条件,用归一化法测定其含量,并用气相色谱-质谱法对化学成分进行鉴定。共鉴定了38个成分,占挥发油总成分的86%以上。方法稳定可靠。重现性好,适用于中药挥发油的化学成分分析。     

苦丁茶冬青挥发油成分的GC-MS分析

采用乙醚超声萃取-水蒸气蒸馏方法提取苦丁茶冬青的挥发油，用气相色谱-质谱联用分析，鉴定了挥发油中的57个成分，其中主要成分是醇、醛、酮、醚、脂肪酸、脂肪酸酯及含氧萜类等化合物。     

GC/MS法研究苦黄注射液中挥发油成分

利用气相色谱-质谱联用装置分析了苦黄注射液中挥发油的化学成分及相对含量。共鉴定了55个化合物，其中以单萜和倍半萜为主，占已鉴定的挥发油种类的56．36％和3．63％，为挥发油的主要成分。     

沙枣花挥发油化学成分的研究

本文用自制的水蒸汽蒸馏－溶剂萃取装置从沙枣花鲜花中提取挥发油，测得其含量为0.1%,用毛细管气相色谱-质谱法对挥发油的化学成分进行了研究,色谱分离出85个组分,质谱鉴定了其中47个组分,主要组分为反式肉桂酸乙酯,占总色谱峰面积的78.88%,IR和NMR为主要成分的鉴定提供了佐证。     

不同产地莪术挥发油的有效成分

用HP6890/5973气相色谱-质谱联用仪分析了四川、福建、浙江产的莪术挥发油的有效成分，结果表明不同产地莪术挥发油的成分差异较大，提示在选择莪术油为原粒制备制剂时要规定产地。     

中国菖蒲属植物根茎挥发油成分分析及其资源的合理利用

 〕用毛细管气相色谱和色谱-质谱技术第一次系统地分析了国产菖蒲属植物根茎挥发油的化学成分，并根据其化学成分探讨了我国菖蒲药材资源的合理利用问题。     

螯形主体分子的设计、包结性能及其在细辛挥发油 有效成分选择分离中的应用

设计了两种新的具有螯形骨架的主体分子反式-1,2-二苯基-1,2-苊二醇(1)和顺式-1,2-二(1'-萘基)-1,2-苊二醇(2),主体(1),(2)可与许多有机小分子化合物形成配位包合物。用IR和粉末XRD表征了主体分子(1)和(2)的包结物,用^1NMR测定了包结物的主客体分子摩尔比：(1)·DMF(1:2),(1)·DMSO(1:2),(1)·THF(1:2),(1)·二氧六环(1:1),(1)·吡啶(1:1),(2)·DMF(1:1)和(2)·DMSO(1:1)。单晶X射线衍射分析了包结物的晶体结构,(1)·DMF：空间群Pnaa,a=0.9377(1)nm,b=1.4351(1)nm,c=4.0463(3)nm;(1)·DMSO：空间群Pbcn,a=1.6278(1)nm,b=1.0751(1)nm,c=1.4980(1)nm;(2)·DMF：P2~1/n,a=0.9796(1)nm,b=1.2377(1)nm,c=2.2344(3)nm,β=93.02(1)°;游离主体(1)：空间群P1,a=1.0461(1)nm,b=1.1213(1)nm,c=1.5496(1)nm,α=81.74(1)°,β=75.71(1)°,γ=89.00(1)°;分析了主体分子的刚性和柔韧性对包结性能的影响。并研究了主体分子(1)选择分离细辛挥发油,将顺甲基异丁香酚从挥发油中分离出来。     

三氯苯的标准生成焓和异构化焓

报导了用精密转动弹量热计测定诸三氯苯燃烧热的实验结果,并计算出这些化合物在液态(或固态)和气态下的标准生成焓.同时还计算出它们的异构化焓和原子化热,并与一般公认为比较精确的热化学键能模式的计算值进行比较和讨论.     

Purification of Complex of SAV1 with PP1A

SAV1 is a core component involved in the Hippo pathway which can control the organ size via regulating cell proliferation and apoptosis simultaneously. We explored the regulatory mechanism of SAV1. We established the HEK293T cell pool, the cells in which can stably express SAV1 by retroviruses infection and found that SAV1 stable cells reduced the movement of themselves and resulted in multicellular aggregation. We purified SAV1 interacting protein complex using streptavidin resin and subsequently analyzed the digested peptides by high performance liquid chromatography(HPLC)-MS/MS. Results show that about 150 proteins were identified in the complex of SAV1 with protein. TUBA1A, OTUD4, and ATD were identified as proteins interacting with SAV1. Importantly, PP1A, serine/threonine protein phosphatase PP1-alpha 1 catalytic subunit, was also in the top 10 list. The interaction between PP1A and SAV1 was detected by both co-immunoprecipitation(CO-IP) and immunostaining. Our results indicate that PP1A might be the phosphatase of SAV1 and may take part in the regulation of the Hippo pathway.     

Cycloaddition of benzoheteroazepine III Reaction of 2,3-dihydro-1H-15benzodiazepines with dichlorocarbene and stereo-structures of products

Reaction of 2, 3-dihydro-1H-1. 5-benzodiazepines with dichlorocarbene generated in situ using benzyltriethylammonium chloride (TEBA) as a phase transfer catalyst in chloroform-aqueous sodium hydroxide mixture gave mainly 1,2-cycloadducts, cis and trans-1a, 3-disubstituted-1, 1-dichloro-1a, 2,3,4-tetrahydro-1H-azirino[1,2-a][1,5]benzodiazepines (2.3), and formylated 1,2-cycloadducts, trans-1a,3-disubstituted-1, 1-dichloro-4-formyl-1a, 2, 3, 4–1 H-azirino[1, 2-a][1, 5]benzodiacepines (4). The stereo-structures of cycloadducts and the mechanism are also discussed.     

Synthesis of derivatives of 1-phenylhydropyrimidines

The synthesis has been effected, via the corresponding N-phenyl-ß-aminopropionic acids, of 1-(o-methoxyphenyl)-, 1-(o-ethoxyphenyl)-, and 1-(o-tolyl)dihydrouracils and also of 1-(o-methoxyphenyl)-, 1-(o-ethoxyphenyl)-, and 1-(o-tolyl)-2-thiodihydrouracils. The dihydrouracits and thiodihydrouracils obtained have been reduced with LiAlH₄ to the corresponding 2-oxohexahydro-, and 2-thioxohexahydropyrimidines. By the action of bromine and the subsequent splitting out of HBr, the dihydrouracils have been converted into 1-(o-methoxyphenyl)-, 1-(o-ethoxyphenyl)-, and 1-(o-tolyl)uracils.     

Laser spectroscopic studies of several Rydberg states of MgO

We report extensive spectroscopic measurements of rovibronic transitions from the MgO X 1Sigma+ ground state to the high-energy E 1Sigma+, F 1Pi1, and G 1Pi1 Rydberg states. Perturbations in the E 1Sigma+ and G 1Pi1 states were observed. The Rydberg molecular orbital character of the three states is examined, given ab initio calculations by Thummel et al. [Chem. Phys. 129, 417 (1989)]. It is concluded that the E 1Sigma+ and G 1Pi1 states consist primarily of the MgO+ X 2Pi ionic core, surrounded by 3ppi and 3psigma Rydberg electron clouds, respectively, and that the F 1Pi1 state consists primarily of the MgO+ A 2Sigma+ ionic core surrounded by a 3ppi Rydberg electron cloud. Spectroscopic characterizations of some unassigned vibrational levels of analogous MgO 3Pi2 states in this energy region are also reported.     

α-羟基二茂铁类衍生物的合成及其晶体结构

通过甲酰基二茂铁与苯乙酮，硝基甲烷及丙酮的缩合反应，我们制得了其缩合产物-α-羟基-β-羰基化合物。并对甲酰基二茂铁与苯乙酮的缩合产物进行了X射线单晶结构分析。结果表明：该晶体属于单斜晶系，空间群为P 2~1/n，a=0.6022(1)，b=2.735(1)，c=0.9416(1)nm，β=99.02(1)°，V=1.532(1)(nm)^3，Mr=334.20，Z=4，Dx=1.45g/cm^3，μ=9.68cm^-^1，F(000)=696。     

Kinetic investigations of the process of encapsulation of small hydrocarbons into a cavitand-porphyrin

Exchange of guest molecules into capsule shaped host molecules is the most fundamental process in host-guest chemistry. Several examples of quantitative measurements of guest exchange rates have been reported. However, there have been no reports on the activation energies of these processes. A molecule known as cavitand-porphyrin (H2CP) has been reported to have a flexible host structure capable of facilitating moderate guest exchange rates suitable for kinetic measurements of the guest exchange process with 1H NMR. In this article, various kinetic and thermodynamic parameters related to the process of encapsulation of small hydrocarbons into H2CP in CDCl3 solution were determined by 2D exchange spectroscopy (EXSY): association and dissociation rate constants (k(ass) = 320 M-1 s-1, k(diss) = 1.4 s-1 for methane at 25 degrees C), the corresponding activation energies (E(a,ass) = 27 kJ.mol-1, E(a,diss) = 58 kJ.mol-1), and thermodynamic parameters for each process (DeltaG++(ass) = 59 kJ.mol-1, DeltaG++(diss) = 72 kJ.mol-1, DeltaH++(ass) = 25 kJ.mol-1, DeltaH++(diss) = 55 kJ.mol-1, DeltaS++(ass) = -113 J.K-1.mol-1, and DeltaH++(diss) = 58 J.K-1.mol-1 for methane). The thermodynamic parameters (DeltaG degrees = -13 kJ.mol-1, DeltaH degrees = -31 kJ.mol-1, DeltaS degrees = -60 J.K-1.mol-1 for methane) for this encapsulation equilibrium determined by EXSY were comparable to those for methane determined by 1D 1H NMR titration (DeltaG degrees = -11 kJ.mol-1, DeltaH degrees = -33 kJ.mol-1, DeltaS degrees = -75 J.K-1.mol-1 for methane). In addition, the structure of the methane encapsulation process was revealed by ab initio MO calculations. The activation energies for methane association/dissociation were estimated from MP2 calculations (E(a,ass) = 58.3 kJ.mol-1, E(a,diss) = 89.1 kJ.mol-1, and DeltaH degrees = -30.8 kJ.mol-1). These values are in accord with the experimentally determined values. The observed guest exchange rates and energies are compared with the corresponding values of various reported capsule-shaped hosts.     

Synthesis and conjugation of oligosaccharide analogues of fragments of the immunoreactive glycan part of the circulating anodic antigen of the parasite Schistosoma mansoni

The gut-associated circulating anodic antigen (CAA) is one of the major excretory antigens produced by the parasite Schistosoma mansoni. The immunoreactive part of CAA is a threonine-linked polysaccharide composed of long stretches of the unique repeating disaccharide-->6)-[beta-D-GlcpA-(1-->3)]-beta-D-GalpNAc-(1-->. Previously, using surface plasmon resonance and ELISA techniques, it has been shown that some anti-CAA IgM monoclonal antibodies (MAbs) also recognize members of a series of bovine serum albumin (BSA)-coupled synthetic di- to penta-saccharide fragments of the CAA glycan. To generate information on the molecular level about the glycan specificity of the relevant IgM MAbs, two series of oligosaccharides related to the CAA disaccharide epitope were synthesized, and coupled to BSA. The first three analogues, beta-D-GlcpA-(1-->3)-[small beta]-D-GlcpNAc-(1-->O), beta-D-GlcpNAc-(1-->6)-[beta-D-GlcpA-(1-->3)]-beta-D-GlcpNAc-(1-->O), and beta-D-GlcpA-(1-->3)-beta-D-GlcpNAc-(1-->6)-[beta-D-GlcpA-(1-->3)]-beta-D-GlcpNAc-(1-->O), wherein the native beta-D-GalpNAc moiety was replaced by beta-D-GlcpNAc, were synthesized to investigate the specificity of the selected MAbs to the carbohydrate backbone of CAA. The second series of analogues, beta-D-Glcp6S-(1-->3)-beta-D-GalpNAc-(1-->O), beta-D-GalpNAc-(1-->6)-[beta-D-Glcp6S-(1-->3)]-beta-D-GalpNAc-(1-->O), and beta-D-Glcp6S-(1-->3)-beta-D-GalpNAc-(1-->6)-[beta-D-Glcp6S-(1-->3)]-beta-D-GalpNAc-(1-->O), wherein the native beta-D-GlcpA moiety was replaced by beta-D-Glcp6S, was synthesized to evaluate the importance of the type/nature of the charge of CAA for the MAb recognition.     

联萘衍生物的磺化反应研究

研究了1-和2-苯基萘, 1, 1'-和2, 2'-联萘, 2, 2-二羟基-, 2, 2'-二甲氧基和-2, 2'-甲基磺酰氧基-1, 1'-联萘等七种萘衍生物和三氧化硫的磺化反应。1-苯基萘和1, 1'-联萘的磺化先发生在4位上, 第二取代位置为6和7位。2-苯基萘和2, 2'-联萘均首先得到8位磺酸取代物, 进一步磺化得到8, 4'-和8, 8'-二磺酸取代物。2, 2'-二甲氧基-1, 1'-联萘以13:87的比例得到3位和6位磺酸取代物。2, 2'-二甲磺酰氧基-1, 1'-联萘以58:42的比例得到5位和6位磺酸取代物。2, 2'-二羟基-1, 1'-联萘的等摩尔磺化得到比例为35:65的5位和6位磺酸取代物, 和大于6摩尔的SO~3反应则以62:38的比例得到5位和6位磺酸取代物。