Characterization of linear epitope of the beta(2)-microglobulin via combination of MALDI-TOF-MS with immunoaffinity

Matrix-assisted laser desorption ionization time-of-flight mass spectrometry(MALDI-TOF-MS), in combination with immunoaffinity provided a powerful tool for determining epitope (antigenic determinant) in protein. The linear epitope of the beta(2)-microglobulin was characterized in the paper. The method as follows: at first beta(2)-microglobulin was digested by a proteolytic enzyme to produce an appropriate set of peptide fragments, then peptide fragments containing the linear epitope were selected and separated from the pool of peptide fragments by immunoprecipitation with the monoclonal antibody. The agarose beads were collected carefully after the reaction. Unbound peptides would be washed away, while the peptides containing the epitope would remain bound to the immobilized antibody after. the beads were washed several times with appropriate buffer. At last the masses of the bound peptides were identified directly by MALDI-TOF MS. Using Endoproteinase Glu-C Endoproteinase Lys-C and Trypsin in the experiment, the linear epitope of beta(2)-microglobulin was located within peptide fragment 59-69, that is, DWSFYLLYYTE.

Two-Dimensional Kinetics Of Beta(2)-Integrin And Icam-1 Bindings Between Neutrophils And Melanoma Cells In A Shear Flow

Cell adhesion, mediated by specific receptor-ligand interactions, plays an important role in biological processes such as tumor metastasis and inflammatory cascade. For example, interactions between beta(2)-integrin ( lymphocyte function-associated antigen-1 and/or Mac-1) on polymorphonuclear neutrophils (PMNs) and ICAM-1 on melanoma cells initiate the bindings of melanoma cells to PMNs within the tumor microenvironment in blood flow, which in turn activate PMN-melanoma cell aggregation in a near-wall region of the vascular endothelium, therefore enhancing subsequent extravasation of melanoma cells in the microcirculations. Kinetics of integrin-ligand bindings in a shear flow is the determinant of such a process, which has not been well understood. In the present study, interactions of PMNs with WM9 melanoma cells were investigated to quantify the kinetics of beta(2)-integrin and ICAM-1 bindings using a cone-plate viscometer that generates a linear shear flow combined with a two-color flow cytometry technique. Aggregation fractions exhibited a transition phase where it first increased before 60 s and then decreased with shear durations. Melanoma-PMN aggregation was also found to be inversely correlated with the shear rate. A previously developed probabilistic model was modified to predict the time dependence of aggregation fractions at different shear rates and medium viscosities. Kinetic parameters of beta(2)-integrin and ICAM-1 bindings were obtained by individual or global fittings, which were comparable to respectively published values. These findings provide new quantitative understanding of the biophysical basis of leukocyte-tumor cell interactions mediated by specific receptor-ligand interactions under shear flow conditions.

Heterodimerization of integrin Mac-1 subunits studied by single-molecule imaging

Heterodimerization of integrin Mac-1 (alpha(M) beta(2)) Subunits plays important role on regulating leukocytes adhesion to extracellular matrix or endothelial cells. Here, using total internal reflection microscopy, we investigated the heterodimerization of integrin Mac-1 subunits at the single-molecule level in live cells. Individual alpha(M) subunit fused to the enhanced yellow fluorescent protein (eYFP) was imaged at the basal plasma membrane of live Chinese hamster ovary (CHO) cells. Through analysis of mean square displacement (MSD), diffusion coefficient, the size of restricted domain and fraction of molecules undergoing restricted diffusion, we found that as compared with the diffusion in the absence of beta(2) subunit, the diffusion of single-molecule of alpha(M)-YFP was suppressed significantly in the presence of beta(2) subunit. Thus, based on the oligomerization-induced trapping model, we suggested that in the presence of beta(2) subunit, the am subunit may form heterodimer with it. (C) 2008 Elsevier Inc. All rights reserved.

Detection of constitutive heterodimerization of the integrin Mac-1 subunits by fluorescence resonance energy transfer in living cells

Macrophage differentiation antigen associated with complement three receptor function (Mac-1) belongs to beta(2) subfamily of integrins that mediate important cell-cell and cell-extracellular matrix interactions. Biochemical studies have indicated that Mac-1 is a constitutive heterodimer in vitro. Here, we detected the heterodimerization of Mac-1 subunits in living cells by means of two fluorescence resonance energy transfer (FRET) techniques (fluorescence microscopy and fluorescence spectroscopy) and our results demonstrated that there is constitutive heterodimerization of the Mac-1 subunits and this constitutive heterodimerization of the Mac-1 subunits is cell-type independent. Through FRET imaging, we found that heterodimers of Mac-1 mainly localized in plasma membrane, perinuclear, and Golgi area in living cells. Furthermore, through analysis of the estimated physical distances between cyan fluorescent protein (CFP) and yellow fluorescent protein (YFP) fused to Mac-1 subunits, we suggested that the conformation of Mac-1 subunits is not affected by the fusion of CFP or YFP and inferred that Mac-1 subunits take different conformation when expressed in Chinese hamster ovary (CHO) and human embryonic kidney (HEK) 293T cells, respectively. (c) 2006 Elsevier Inc. All rights reserved.

Detection of constitutive homomeric associations of the integrins Mac-1 subunits by fluorescence resonance energy transfer in living cells

Integrins alpha(M)beta(2) plays important role on leukocytes, such as adhesion, migration, phagocytosis, and apoptosis. It was hypothesized that homomeric associations of integrin subunits provide a driving force for integrins activation, and simultaneously inducing the formation of integrins clusters. However, experimental reports on homomeric associations between integrin subunits are still controversial. Here, we proved the homomeric associations of the isolated Mac-1 subunits in living cells using three-channel fluorescence resonance energy transfer (FRET) microscopy and FRET spectra methods. We found that the extent of homomeric associations between beta(2) subunits is higher than alpha(M) subunits. Furthermore, FRET imaging indicated that the extent of homomeric associations of the Mac-1 subunits is higher along the plasma membrane than in the cytoplasm. Finally, we suggested that homomeric associations of the transmernbrane domains or/and cytoplasmic domains may provide the driving force for the formation of constitutive homomeric associations between alpha(M) or beta(2) subunits. (c) 2006 Elsevier Inc. All rights reserved.

Stejnulxin, a novel snake C-type lectin-like protein from Trimeresurus stejnegeri venom is a potent platelet agonist acting specifically via GPVl

Stejnulxin, a novel snake C-type lectin-like protein with potent platelet activating activity, was purified and characterized from Trimeresurus stejnegeri venom. Under non-reducing conditions, it migrated on a SDS-polyacrylamide gel with an apparent molecular mass of 120 kDa. On reduction, it separated into three polypeptide subunits with apparent molecular masses of 16 kDa (alpha), 20 kDa (beta(1)) and 22 kDa (beta(2)), respectively. The complete amino acid sequences of its subunits were deduced from cloned cDNAs. The N-terminal sequencing and cDNA cloning indicated that beta(1) and beta(2) subunits of stejnulxin have identical amino acid sequences and each contains two N-glycosylation sites. Accordingly, the molecular mass difference between 1 and 2 is caused by glycosylation heterogenity. The subunit amino acid sequences of stejnulxin are similar to those of convulxin, with sequence identities of 52.6% and 66.4% for the U. and beta, respectively. Stejnulxin induced human platelet aggregation in a dose-dependent manner. Antibodies against UNA inhibited the aggregation response to stejnulxin, indicating that activation of alpha(IIb)beta(3) and binding of fibrinogen are involved in stejnulxin-induced platelet aggregation. Antibodies against GPIbalpha or alpha(2)beta(1) as well as echicetin or rhodocetin had no significant effect on stejnulxin-induced platelet aggregation. However, platelet activation induced by stejnulxin was blocked by anti-GPVI antibodies. In addition, stejnulxin induced a tyrosine phosphorylation profile in platelets that resembled that produced by convulxin. Biotinylated stejnulxin bound specifically to platelet membrane GPVI.

Evolution of different oligorneric glycyl-tRNA synthetases

There are two oligomeric types of glycyl-tRNA synthetases (GlyRSs) in genome, the alpha(2)beta(2) tetramer and alpha(2) dimer. Here, we showed that the anticodon-binding domains (ABDs) of dimeric and tetrameric GlyRSs are non-homologous, although their catalytic central domains (CCDs) are homologous. The dimeric GlyRS_ABD is fused to the C-terminal of CCD in alpha-subunit, but the tetrameric GlyRS_ABD is to the C-terminal in beta-subunit during evolution. Generally, one species only contains one oligomeric type of GlyRS, but the both oligomeric GlyRSs with the multiple homologous domains can be observed in Magnetospirillum magnetotacticum genome, nevertheless, these homologous domains are probably from different genomes. (C) 2005 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.

顶空固相微萃取-气相色谱-质谱测定水中异味化合物

采用顶空固相微萃取-气相色谱/质谱联用测定了水中常见的3种异味化合物,即2-甲基异茨醇、土腥素和β-柠檬醛。研究并讨论了纤维头的类型、盐的种类和浓度、温度、萃取时间、搅拌和解吸时间等因素对异味化合物萃取量的影响。结果表明:在水样中加入30%(W/V)的NaCl溶液,采用65μmPDMS/DVB纤维头,在搅拌的条件下,于60℃顶空萃取40min为异味化合物固相微萃取的最佳条件。在优化的条件下,使异味化合物吸附于纤维涂层后,将其在250℃高温下解吸,再用GC-MS分析。土腥素、β-柠檬醛、2-甲基异茨醇的检出

Ⅰ、KMBZ-009 改善心理应激所致认知障碍和抑郁样行为的研究 Ⅱ、银杏叶提取物及复方制剂改善老年鼠空间学习记忆的突触可塑性机理

1、KMBZ-009 改善高台应激所致认知障碍和应激相关的抑郁样行为及其相关机理 研究。 虽然适当的应激会提高动物的学习记忆功能，但过量的应激特别是无法逃避 的应激，往往导致依赖海马或前额叶的学习记忆功能受损，这与应激改变脑内应 激激素（皮质酮，皮质醇等）和神经递质的释放，影响突触传递和可塑性（包括 长时程增强和长时程抑制，LTP 和LTD）有关。一些疾病的发生、发展和恶化， 比如抑郁症（Depression）、创伤后应激障碍（PTSD），往往也和应激相关联，其 神经化学基础被证实与内分泌系统和单胺类（如五羟色，去甲肾上腺素，多巴胺） 神经递质系统的功能密切相关。遗憾的是，到目前为止还没有发现能治疗应激的 药物。本实验室过去的研究证实：KMBZ-009(申报新药时的名称为芬克罗酮，英 文名Phenchlobenpyrrone)——一种新的取代吡咯烷酮类化合物，通过调节细胞 内钙，改变脑内神经递质的释放，从而影响脑高级功能。KMBZ-009 对神经递质 释放影响是否能减轻应激导致的认知障碍及应激相关疾病的发生还没有进行研 究。本研究采用Morris 水迷宫、行为操作箱、绝望游泳、膜片钳和活体电生理 技术研究了KMBZ-009 对高台应激所致认知障碍和应激相关的抑郁样行为的影响 及其相关机理。 研究结果发现，高台应激或皮质酮注射造成大鼠空间记忆提取障碍，这与其 导致的海马CA1 区突触可塑性改变有关，而KMBZ-009 能成剂量依赖性地逆转应 激对空间记忆提取的损伤作用，这与它阻断应激或皮质酮异化的LTD 和恢复应激 或皮质酮损伤的LTP 密切相关。KMBZ-009 能部分地降低因应激而升高的血清皮 质酮含量，此外，KMBZ-009 对大鼠海马CA1 区锥体神经元的兴奋和抑制电流的 影响可能也参与了其对应激的调节作用。KMBZ-009 能显著增加海马CA1 区锥体 神经元上AMPA 受体介导的兴奋性突触后电流（EPSC）的幅度，但不影响其动力 学特性。NMDA 受体介导的EPSC 不受KMBZ-009 的影响；GABA 受体介导的抑制突 触后电流（IPSC）的幅度几乎不受KMBZ-009 的影响，而其受体动力学特性明显 被KMBZ-009 改变，表现为IPSC 恢复的时间显著延长。KMBZ-009 对CA1 区兴奋 抑制电流的调节作用，使大鼠海马细胞具有更强的维持细胞稳态的能力，从而避免应激导致神经元功能的损害。KMBZ-009 对抗应激对认知得损伤作用提示其可 能会减少动物的抑郁样行为，本实验结果发现，KMBZ-009 确实能明显减少小鼠 在强迫游泳（FST）中的不动时间，增加大鼠在72 秒低频差式强化（DRL-72s） 模型中的强化率，并降低其反应率。其机制是KMBZ-009 增加正常动物中枢神经 系统胞外NE 水平，激活alpha 和beta 肾上腺素受体，从而使得实验动物的抑郁 样行为明显减少。 2、KMBZ-009 减轻氧化应激对细胞活力、线粒体电位及海马LTP 的损伤作用。 前人的研究表明，氧自由基过多是导致老年痴呆患者和老年人神经细胞凋亡 与认知障碍的因素之一。KMBZ-009 和阿尼西坦是吡咯烷酮类化合物，研究显示 均具有促智作用。有报道指出阿尼西坦能减少神经胶质细胞在缺血缺氧时氧自由 基的生成，从而避免细胞受到氧应激损伤。本研究采用神经元原代培养和离体电 生理学方法，观察了KMBZ-009 和阿尼西坦对氧应激神经元的保护作用。结果发 现，KMBZ-009 和阿尼西坦均能保护氧应激神经元的线粒体的功能，对抗氧自由 基对神经元细胞活力的损伤，从而有效逆转了氧化应激对海马脑片CA1 区LTP 的 损伤作用。KMBZ-009 的作用效果比阿尼西坦的效果强10 倍。 3、银杏叶提取物及复方制剂改善老年大鼠空间学习记忆的突触可塑性机理。 有研究表明，银杏叶和三七叶提取物能调节神经系统的功能。本研究采用 Morris 水迷宫和活体电生理技术研究了银杏三七复方制剂及银杏叶提取物（以 标准银杏叶提取物——金纳多作为阳性对照药）改善老年大鼠空间学习记忆障碍 的突触可塑性机理研究。结果发现：老年大鼠空间学习记忆能力较差，高频诱导 不能在其海马CA1 区引发LTP，当长期服用金纳多或复方制剂一个月后，老年动 物的空间学习记忆功能得到明显改善，这可能与药物增强海马LTP 有密切关系。 复方制剂的作用效果与金纳多的效果相当。 4、悬尾应激损伤避暗作业学习行为的多巴胺D1 受体机制。 近年来的研究表明，DA 系统对应激非常敏感，应激改变PFC 内DA 的含量， 从而导致依赖于PFC 的工作记忆受损。但目前尚不知道应激对DA 系统的影响是 否涉及依赖杏仁核和海马的情绪学习记忆功能。因此，我们采用被动回避作业和 行为药理学的方法，初步探讨了此问题。结果发现：和对照组动物相比，随着悬 尾应激持续时间的增加（5min、10min、20min），动物在避暗作业作业重测试中的步入潜伏期明显缩短，当动物被悬尾应激后回到鼠笼中休息20min，其步入潜 伏期无明显变化；腹腔注射DA D1 受体拮抗剂SCH23390 呈剂量依赖性地缩短动 物的步入潜伏期，但SCH23390 腹腔注射和悬尾应激共同处理实验动物时，此种 D1 受体拮抗剂能有效逆转应激对步入潜伏期的影响；进一步的研究发现，应激 或D1 受体拮抗剂对痛觉感受的影响不是其改变动物步入潜伏期的主要因素。本 研究结果表明悬尾应激导致脑内多巴胺释放过度增加，杏仁核（可能还有海马及 相关神经回路）内的D1 受体被过度激活，从而导致小鼠在操作被动回避任务时 的记忆获得障碍。

Scaling and the thermal conductivity of the Frenkel-Kontorova model

We have studied the dependence of the thermal conductivity kappa on the strength of the interparticle potential lambda and the strength of the external potential beta in the Frenkel-Kontorova model. We found that the functional relation can be expressed in a scaling form, kappa(proportional to) lambda 3/2/beta(2 center dot). This result is first obtained by nonequilibrium molecular dynamics. It is then confirmed by two analytical methods, the self-consistent phonon theory and the self-consistent stochastic reservoirs method. The thermal conductivity kappa is therefore a decreasing functon of beta and an increasing function of lambda.

鸡粪中活性有机酸的分离与鉴定

本文通过生物追踪实验法 ,研究了鸡粪中有机酸的生物活性成分 ,并从中筛选出了一种强活性物质 .通过红外光谱和质谱及生源关系初步确定其分子式为C36H56O18Na,名称为 3-O -D -葡萄糖 -6,1 -0 -葡萄糖酸 2 β ,2 ,2 0 -二羟基蛋甾酸钠

Studies of magnetic interactions in Mn-doped β-Ga2O3 from first-principles calculations

The magnetic behavior of Mn-doped beta-Ga2O3 is Studied from first-principles calculations within the generalized gradient approximation method. Calculations show that ferromagnetic ordering is always favorable for configurations in which two Mn ions substitute either tetrahedral or octahedral sites, and the ferromagnetic ground state is also sometimes favorable for configurations where one Mn ion substitutes a tetrahedral site and another Mn ion substitutes an octahedral site. However, the configurations of the latter case are less stable than those of the former. (c) 2008 Acta Materialia Inc. Published by Elsevier Ltd. All rights reserved.

Synthesis and biological evaluation of N-acetyl-beta-aryl-1,2-didehydroethylamines as new HIV-1 RT inhibitors in vitro

A variety of N-acetyl-o-aryl-1,2-didehydroethylamines were synthesized by direct reduction-acetylation of beta-aryl-nitroolefins and assayed as HIV-1 non-nucleoside reverse transcriptase inhibitors (NNRTIs) for the first time. Compound 7a exhibited a TI v

N,N,N ',N '-Tetramethylchloroformamidinium Chloride-Mediated Cyclizations of beta-Oxo Amides: Facile and Divergent One-Pot Synthesis of Substituted 2H-Pyrans, 4H-Pyrans and Pyridin-2(1H)-ones

An efficient and divergent one-pot synthesis of substituted 2H-pyrans, 4H-pyrans and pyridin-2(1H)-ones from beta-oxo amides based on the selection of the reaction conditions is reported. Mediated by N,N,N',N'-tetramethylchloroformamidinium chloride, beta-oxo amides underwent intermolecular cyclizations in the presence of triethylamine at room temperature to give substituted 2H-pyrans in high yields, which could be converted into substituted 4H-pyrans in the presence of sodium hydroxide in ethanol at room temperature, or into substituted pyridin-2(1H)-ones under reflux.