Glyceryl Trinitrate: History,Mystery, and Alcohol Intolerance

Glyceryl trinitrate (GTN) is one of the earliest known treatments for angina with a fascinating history that bridges three centuries. However, despite its central role in the nitric oxide (NO) story as a NO-donating compound, establishing the precise mechanism of how GTN exerts its medicinal benefit has proven to be far more difficult. This review brings together the explosive and vasodilatory nature of this three-carbon molecule while providing an update on the likely in vivo pathways through which GTN, and the rest of the organic nitrate family, release NO, nitrite, or a combination of both, while also trying to explain nitrate tolerance. Over the last 20 years the alcohol detoxification enzyme, aldehyde dehydrogenase (ALDH), has undoubtedly emerged as the front runner to explaining GTN’s bioactivation. This is best illustrated by reduced GTN efficacy in subjects carrying the single point mutation (Glu504Lys) in ALDH, which is also responsible for alcohol intolerance, as characterized by flushing. While these findings are significant for anyone following the GTN story, they appear particularly relevant for healthcare professionals, and especially so, if administering GTN to patients as an emergency treatment. In short, although the GTN puzzle has not been fully solved, clinical study data continue to cement the importance of ALDH, as uncovered in 2002, as a key GTN activator.     

仿生信号转导体系的构建:囊泡表面磷脂信号分子诱发的乳酸脱氢酶的激活

以细胞肌醇磷脂信号转导途径为原型,在合成肽脂囊泡(人工细胞膜模型)上,利用天然磷脂为信号分子,成功地激活了处于囊泡表面的乳酸脱氢酶．为此,将1,2-二-十四烷基磷脂酰乙醇胺等天然磷脂嵌入合成肽脂N,N-二-十六烷基-N^a-6-三甲胺基己酰基-L-甘氨酰胺囊泡中,制备了稳定的混合双层膜囊泡,用透射电子显微照相、动态光散射及差示扫描量热等手段确认了混合囊泡的形态及粒径分布．以磷酸吡哆醛等维生素B6类化合物为信号分子激活剂,利用它们与天然磷脂形成复合体,进而与Cu^2 形成强的金属配合物的性质,实现了对处于囊泡表面、被Cu^2 抑制的乳酸脱氢酶的激活,构建了一个新的仿生信号转导体系．紫外一可见光谱实验证实了以上结果．此外,结果还表明囊泡表面的疏水作用和静电引力是促进天然磷脂一磷酸吡哆醛复合体形成的主要因素．囊泡表面的疏水微环境作为反应场是构建此仿生信号转导体系不可缺少的要素．     

Synthesis,characterization, and physical properties of new copolymers of poly(amino acid)–urethane—copolymers of γ‐methyl‐L‐glutamate‐N‐carboxyanhydride and urethane prepolymer

New copolymers of amino acid and urethane (PAU), in which a polyurethane segment was combined with poly(γ‐methyl‐L‐glutamate) (PMLG) of various contents, were synthesized by the copolymerization of the polyurethane prepolymer (UPP) having isocyanate groups at both terminals of the chain and γ‐methyl‐L ‐glutamate‐N‐carboxyanhydride (NCA) to improve the elastic recovery and adhesion of PMLG for application of PMLG to synthetic leather. The copolymerization of the UPP with NCA was carried out by applying the reactivity of isocyanate and the polymerization mechanism of NCA using the primary amine and tertiary amine as initiators. Infrared (IR) and ¹³C‐NMR spectra of these PAUs as well as the chemical analysis of the PAU intermediates showed that the PAUs would have a multiblock–triblock structure: namely, the PAUs consisted of the block copolymer segments of urethane and a small amount of PMLG at the center of the copolymer chain and most of the PMLG at both terminals of the copolymer chain. The elastic recovery and adhesion of these PAUs were significantly larger than those of the PMLG with the maintenance of a good sense of touch, which was a unique asset of PMLG. Furthermore, it was found that the PAUs had intermediary moisture permeability between that of PMLG and polyurethane. © 1999 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 37: 383–389, 1999     

Phase equilibrium studies on rod/solvent and rod/coil/solvent systems containing poly(α, L‐glutamate) having oligo(ethylene glycol) side chains

Phase equilibrium studies for semiconcentrated solutions of rodlike poly(γ‐benzyl L ‐glutamate) having oligo(ethylene glycol) as side chains (PBLG‐g‐OEG) have been investigated. The phase‐boundary concentrations in isotropic and anisotropic phases for N,N‐dimethylformamide (DMF) solution of PBLG‐g‐OEG with short side chains (PBLG2‐g‐380) are higher than those for solution of PBLG‐g‐OEG with long side chains (PBLG2‐g‐770). The lattice theory and the scaled particle theory for nematic solution, which don't distinguish the molecular architecture of the rodlike polymer, cannot explain this experimental result. Repulsive interaction between rodlike polymers by means of the attached side chains is proposed for the molecular orientation of PBLG‐g‐OEG in anisotropic state in order to describe the experimental result. Ternary phase diagrams of PBLG‐g‐OEG/poly(ethylene glycol) (PEG)/DMF show that the miscibility of rodlike PBLG‐g‐OEG and coiled PEG is most enhanced in the system of PBLG2‐g‐770, which has longest and largest amount of side chains. This experimental observation is explained by using the calculation based on the lattice theory and the repulsive interaction of side chains proposed above. © 2000 John Wiley & Sons, Inc. J Polym Sci B: Polym Phys 38: 1331–1340, 2000     

3-磷酸甘油醛脱氢酶与酵母线粒体基因组维持蛋白Mgm101的相互作用

采用酵母双杂交方法, 以Mgm101p为诱饵, 筛选酵母cDNA文库. 分离鉴定15个与Mgm101p相互作用的蛋白因子, 其中5个阳性克隆均为GPD1编码的3-磷酸甘油醛脱氢酶(GAPDH). 克隆了GPD1在 S. cerevisiae的同系物ScTDH2基因, 进行绿色荧光蛋白GFP标记、 亚细胞组分分离和蛋白质印迹分析, 结果表明, GAPDH除了在细胞质为糖酵解酶的主要作用外, 可能为多功能蛋白, 在酵母线粒体中与Mgm101p相互作用参与线粒体DNA维持的生物过程.     

Dual-Function Fibrous Co-Polypeptide Scaffolds for Neural Tissue Engineering

This paper reports dual-function (high cell attachment and cell viability) fibrous scaffolds featuring aligned fibers, displaying good biocompatibility and no cytotoxicity. These scaffolds are fabricated through the electrospinning of a co-polypeptide comprising molar equivalents of N₆-carbobenzyloxy-l -lysine and γ-benzyl-l -glutamate, with the lysine moieties enhancing cell adhesion and the neural-stimulating glutamate moieties improving cell viability. These new scaffolds allow neural cells to attach and grow effectively without any special surface treatment or coating. Pheochromocytoma (PC-12) cells grown on these scaffolds exhibit better neuronal activity and longer neurite length, relative to those grown on scaffolds prepared from their respective homo-polypeptides. When the scaffolds are partially hydrolyzed such that they present net positive charge and increased hydrophilicity, the cell viability and neurite growth both increase further. Accordingly, these novel co-polypeptide fibrous scaffolds have potential applications in neural tissue engineering.     

解木糖赖氨酸芽孢杆菌发酵和生物催化产生L-2-氨基己二酸

以解木糖赖氨酸芽孢杆菌XX-2为出发菌株，110mmol/L L-赖氨酸单盐酸盐为发酵前体，144h发酵后L-2-氨基己二酸浓度达到10.4mmol/L，产率9.5%。以解木糖赖氨酸芽孢杆菌XX-2全细胞为生物催化剂，利用共生的L-赖氨酸 6-脱氢酶和?-1-哌啶啉-6-羧酸脱氢酶催化L-赖氨酸单盐酸盐转化为L-2-氨基己二酸。最优条件为：细胞浓度45g(干重)/L，L-赖氨酸单盐酸盐浓度100mmol/L，pH7.0，温度30℃，反应时间144h。在最优条件下，从100mmol/LL-赖氨酸单盐酸盐产生90mmol/L L-2-氨基己二酸，产率90%。推测了生物催化过程中L-2-氨基己二酸产生的反应机理。     

Green synthesis of Zn nanoparticles and in situ hybridized with BSA nanoparticles for Baicalein targeted delivery mediated with glutamate receptors to U87-MG cancer cell lines

Glioblastoma multiforme (GBM) is the most aggressive malignant tumor of the brain. It has different glutamate receptor types. So, these receptors can be a suitable target for GBM treatment. The current study investigated the anticancer effects of bovine serum albumin (BSA)-Baicalein @Zn-Glu nanostructure mediated-GluRs in human glioblastoma U87 cells. BSA-Ba@Zn-Glu hybrid nanoparticles (NPs) were set and considered transporters for Baicalein (Ba) active compound delivery. BSA-Ba@Zn-Glu NPs were synthesized by a single-step reduction process. The successful production was confirmed through transmission electron microscopy (TEM), dynamic light scattering (DLS), Fourier transform infrared spectroscopy (FT-IR), and hemolysis test. The cytotoxic efficacy and apoptosis rate of the nanostructures on U87 glioblastoma cells were investigated by 3-(4,5-dimethylthialzol-a-yl)-2,5 diphenyltetrazolium bromide (MTT) and flow cytometry assays, respectively. The synthesized BSA-Ba@Zn-Glu nanostructures with a diameter of 142.40 ± 1.91 to 177.10 ± 1.87 nm and zeta potential of −10.57 ± 0.71 to −35.77 ± 0.60 mV are suitable for extravasation into tumor cells. The drug release from the BSA-Ba@Zn NPs showed controlled and pH-dependent behavior. In vitro results indicated that the BSA-Ba@Zn-Glu NPs significantly reduce cell viability and promote apoptosis of U87 cancer cells. It revealed the cytotoxic effect of the Baicalein and an increase in cellular uptake of nanoparticles by Glu receptors. Zn NPs were synthesized based on a green synthesis method. BSA NPs were used as a nano-platform for Glu conjugation and Ba drug delivery. BSA-Ba@Zn-Glu NPs induce cytotoxicity and apoptosis in human brain cancer cells (U87) in a dose-dependent manner. Finally, this nanostructure could be served in targeted drug delivery in vivo studies and applied along with other strategies such as X-ray irradiation as combinational therapies in future studies.