聚酰胺-胺(PAMAM)树状大分子对甲氨蝶呤的包合及缓释研究

以甲氨蝶呤(MTX)为模型药物,研究了G5.0PAMAM树状大分子对其包合和释放,并用13^CNMR对PAMAM-MTX包合物进行了表征.UV-Vis研究结果表明,1个G5.0PAMAM树状大分子能包合27个MTX分子,体外释放研究表明,在37℃,pH=7.4的10mmol/LTris-HCl缓冲溶液中G5.0PAMAM树状大分子对MTX具有明显的缓释作用.     

Radiosynthesis and evaluation of novel [99mTc(I)]+ and [99mTc(I)(CO)3]+ complexes with a 4-nitroimidazole isocyanide for imaging tumor hypoxia

[^99mTc(I)]⁺ and [^99mTc(I)(CO)₃]⁺ complexes with isocyanide exhibit high stability, which makes them suitable platforms to develop novel ^99mTc radiopharmaceuticals. To develop novel ^99mTc radiotracers for imaging hypoxia, in this study, a novel L ligand (4-nitroimidazole isocyanide derivative) was synthesized and labelled using [^99mTc(I)]⁺ core and [^99mTc(I)(CO)₃]⁺ core to produce [^99mTc(L)₆]⁺ and [^99mTc(CO)₃(L)₃]⁺ with high yields. To verify the structure of the ^99mTc complexes, corresponding rhenium analogues were synthesized and characterized. Both of the ^99mTc complexes were stable and hydrophilic. in vitro cellular uptake results showed they could exhibit good hypoxic selectivity. The evaluation of biodistribution in mice bearing S180 tumors indicated both of them could accumulate in tumor. Between them, [^99mTc(L)₆]⁺ exhibited higher tumor uptake and tumor/non-target ratio than [^99mTc(CO)₃(L)₃]⁺. Further, single photon emission computed tomography (SPECT) imaging studies of [^99mTc(L)₆]⁺ indicated an obvious accumulation in tumor and the value of the region-of-interest (ROI) ratio of the uptake for the tumor site to the corresponding non-tumor region was 5.64 ± 0.52. The above results suggested [^99mTc(L)₆]⁺ would be a potential tracer for imaging tumor hypoxia.     

Synthesis and biological evaluation of 99mTc tricarbonyl complex of O,O′‐diethylethylenediamine‐N,N′‐di‐3‐propanoate as potential tumour diagnostic agent

The extensive development of radiopharmaceuticals towards early tumour detection and treatment has increased the demand for new ligands with higher tumour selectivity. Research has been done on the potential of the novel O,O′‐diethylethylenediamine‐N,N′‐di‐3‐propanoate ( L ) ligand as a radionuclide vehicle for tumour targeting. Under alkaline conditions, L hydrolyses and produces half ester ligand ( L' ) and diacid ligand ( L'' ), with characteristic donor atom array N,N,O. Ligand L was successfully labelled with ^99mTc at pH = 9 by coordination with the octahedral fac‐[^99mTc(CO)₃(H₂O)₃]⁺ intermediate, forming the main radioproduct fac‐[^99mTcL′(CO)₃] (Tc1). The ^99mTc complex showed a low lipophilic character (log P = 0.48) and low binding affinity to human serum albumin (2.51 ± 0.48%). In vitro stability studies in saline and human plasma, as well as challenge studies with cysteine and histidine, revealed high stability of the complex during 24 h. Biodistribution studies of Tc1 in female C57BL/6 mice bearing B16/F1 melanoma metastases showed significant tumour uptake: 9.81 ± 1.19%ID g^?1 in the liver, 5.87 ± 0.54%ID g^?1 in the lungs and 3.17 ± 0.33%ID g^?1 in the ovary at 30 min post‐injection. Favourable physicochemical properties, satisfactory in vitro/in vivo stability and biodistribution profile in the experimental metastatic melanoma model indicate the possible application of the radiolabelled ligand in tumour diagnosis. Copyright © 2015 John Wiley & Sons, Ltd.     

Comparative Study of a Series of 99mTc(CO)3 Mannosylated Dextran Derivatives for Sentinel Lymph Node Detection

Sentinel lymph node detection (SLND) is rapidly entering common practice in the management of patients with tumors. The introduction of mannose molecules to ^99mTc-labeled dextrans, so far, showed that the sentinel node could trap these agents due to their recognition by the mannose receptors of lymph node macrophages. The current study aimed to synthesize, characterize, and biologically evaluate a series of mannosylated dextran derivatives labeled with ^99mTc for potential use in SLND. The compounds were designed to have a dextran with a molecular weight of 10–500 kDa as a backbone, S-derivatized cysteines, efficient SNO chelators, and mannose moieties for binding to mannose receptors. They were successfully synthesized, thoroughly characterized using NMR techniques, and labeled with the fac-[^99mTc(CO)₃]⁺ synthon. Labeling with high yields and radiochemical purities was achieved with all derivatives. In vivo biodistribution and imaging studies demonstrated high uptake in the first lymph node and low uptakes in the following node and confirmed the ability to visualize the SLN. Among the compounds studied, ^99mTc-D75CM demonstrated the most attractive biological features, and in combination with the high radiochemical yield and stability of the compound, its further evaluation as a new radiopharmaceutical for sentinel lymph node detection was justified.     

Synthesis, radiolabeling and biodistribution studies of [99mTc(CO)3(MN-TZ-BPA)]+ in tumor-bearing mice

This study reports the synthesis, radiolabeling and preliminary biodistribution results of [^99mTc(CO)₃(MN-TZ-BPA)]⁺ in tumor-bearing mice. The novel nitroimidazole derivative was successfully synthesized by conjugation of bis(pyridin-2-ylmethyl)amine (BPA) to 2-methyl-5-niroimidazole via “click” reaction. The ligand could be labeled by [^99mTc(CO)₃]⁺ core in high yield to get [^99mTc(CO)₃(MN-TZ-BPA)]⁺, which was very hydrophilic and was stable at room temperature. Biodistribution studies in tumor-bearing mice showed that [^99mTc(CO)₃(MN-TZ-BPA)]⁺ accumulated in the tumor with certain initial uptake while poor retention. The rapid clearance from normal organs with favorable tumor/muscle ratios warrants further research to improve tumor targeting efficacy and pharmacokinetic profile of radiolabeled nitroimidazoles by structural modification.     

负载Fe3（CO）12催化剂的制备及合成氨的催化活性

以Ｆｅ_３（ＣＯ）_（１２）为母体，以活性氧化铝或活性炭为载体制备了负载型氨合成催化剂．在固定床管式流动反应系统中测定了催化活性，并与以Ｒｕ_３（ＣＯ）_（１２）和ＲｕＣｌ_３·ｘＨ_２Ｏ为母体的负载催化剂以及低温高活性氨合成工业催化剂的活性进行了对比。结果表明：以活性炭为载体的Ｆｅ_３（ＣＯ）_（１２）催化剂在１５ＭＰａ、４００℃以上表现出很高活性，且每克纯活性组分的催化活性在某些温度下比当前活性较高的工业熔铁催化剂的活性要高得多，但低温常压下几乎无活性。负载钉催化剂在低温常压下即显活性，且以ＲｕＣｌ_３·ｘＨ_２Ｏ为母体，比以Ｒｕ_３（ＣＯ）_（１２）为母体的负载钌催化剂活性高。     

Et_3N·Mo(CO)_5催化取代2,3-二氢呋喃衍生物的合成

利用McDonald方法,制备了2-戊基-、2-(对-甲基)苯基-以及2-甲基-2-苯基-取代2,3-二氢呋喃化合物.实验表明,此种方法反应条件温和,后处理简单,适用范围广,可用以合成大量环内烯醇醚.     

Synthesis and Crystal Structure of （SiCl3）2Fe（CO）4

The compound （SiCl3）2Fe（CO）4 was synthesized and structurally characterized by X-ray single-crystal diffraction. It crystallizes in monoclinic, space group P2 1/n with α = 8.287（2）, b = 9.829（2）, c = 9.042（2） A, β = 96.19（3）°, V= 732.2（3） A^3, C4Cl6FeO4Si2, Mr = 436.77, Z = 2, Dc = 1.981 g/cm^3, F（000） = 424, μ（MoKα） = 2.282 mm^-1, the final R = 0.048 and wR = 0.164 for 1109 observed reflections （I 〉 2σ（I））. The crystal structure of （SiCl3）2Fe（CO）4 reveals that the Si（l）- Fe-Si（l）^a sequence is linear and perpendicular to the Fe（CO）4 cross-shaped plane.     

Synthesis, and Investigation of the Reactive Oxygen Species of a Novel Cyclicpeptide-2,6-dimethoxyhydroquinone-3- mercaptoacetic Acid Conjugate

In the previous paper, we had reported the synthesis of a novel series of linear peptide conjugates of the cytotoxic agent 2,6-dimethoxyhydroquinone-3-mercaptoacetic acid1 (DMQ-MA). In this paper, we choose the cyclic peptides over linear peptides as drug carriers. Our preference for this study is based on the following reason: cyclic peptides, with their N- and C- terminals blocked, are more hydrophobic and would pass through the cell membrane more readily than liner peptides2. Also cyc…     

Aggregation properties of oligo(methacrylic acid)-shelled dendrimer and its microenvironment in aqueous solutions

A third-generation poly(amido amine) dendrimer having poly(methacrylic acid) segments on the periphery (G3-PMAA) was newly synthesized. A xanthate-modified dendrimer (G3-X) was first prepared by condensation of the terminal amino groups of the poly(amido amine) dendrimer with an activated-ester xanthate. G3-PMAA was then synthesized by polymerization of methacrylic acid initiated with G3-X. The number-average degree of polymerization of PMAA segment was estimated to be 10. The pK_a value for G3-PMAA was evaluated to be 7.3 that is somewhat higher than that (6.8) of the corresponding linear PMAA with the same segment length, indicating the interaction of PMAA segments caused by assembling them at the dendrimer surface. When the diameter of G3-PMAA in aqueous solution at various pHs was measured by a dynamic light scattering, G3-PMAA was found to self-aggregate in a pH region, where the PMAA segment took a hydrophobic, compact coil conformation. Subsequently, the interaction of a fluorescent probe (1-anilino-8-naphthalenesulfonic acid ammonium salt (ANS)) with G3-PMAA was examined by means of fluorescence spectroscopy. As a result, ANS was found to bind to the hydrophobic site of G3-PMAA aggregates at lower pH, and to be released into water phase at higher pH.     

利用SHIP－IN－BOTTLE技术在NaY分子筛中合成Ru_8（CO）_（12）原子簇

利用ＳＨＩＰ－ＩＮ－ＢＯＴＴＬＥ技术在ＮａＹ分子筛中合成Ｒｕ_８（ＣＯ）_（１２）原子簇肖丰收，徐如人，何亚男，丁红，张艳秋（吉林大学化学系，长春，１３００２３）关键词原子簇，Ｒｕ_３（ＣＯ）_１２，ＮａＹ分子筛，钌，羰基在多相催化研究中，金属羰基簇合物...     

Crossed Molecular Beams and Theoretical Studies of the O(3P)+1,2-Butadiene Reaction: Dominant Formation of Propene+CO and Ethylidene+Ketene Molecular Channels

Detailed understanding of the mechanism of the combustion relevant multichannel reactions of O(³P) with unsaturated hydrocarbons (UHs) requires the identification of all primary reaction products, the determination of their branching ratios and assessment of intersystem crossing (ISC) between triplet and singlet potential energy surfaces (PESs). This can be best achieved combining crossed-molecular-beam (CMB) experiments with universal, soft ionization, mass-spectrometric detection and time-of-flight analysis to high-level ab initio electronic structure calculations of triplet/singlet PESs and RRKM/Master Equation computations of branching ratios (BRs) including ISC. This approach has been recently demonstrated to be successful for O(³P) reactions with the simplest UHs (alkynes, alkenes, dienes) containing two or three carbon atoms. Here, we extend the combined CMB/theoretical approach to the next member in the diene series containing four C atoms, namely 1,2-butadiene (methylallene) to explore how product distributions, branching ratios and ISC vary with increasing molecular complexity going from O(³P))+propadiene to O(³P)+1,2-butadiene. In particular, we focus on the most important, dominant molecular channels, those forming propene+CO (with branching ratio ∽0.5) and ethylidene+ketene (with branching ratio ∽0.15), that lead to chain termination, to be contrasted to radical forming channels (branching ratio ∽0.35) which lead to chain propagation in combustion systems.     

Novel Dendritic Naproxen Prodrugs with Poly(aspartic Acid) Oligopeptide: Synthesis and Hydroxyapatite Binding in Vitro

Abstract

Novel bone-targeting prodrugs containing dendritic naproxen and poly(aspartic acid) oligopeptide were synthesized in a convergent approach and were characterized by NMR, mass spectral, and elemental analysis techniques. The modified naproxen prodrugs showed a high affinity to hydroxyapatite in vitro and provided an effective entry for the synthesis of a dendritic naproxen–poly(aspartic acid) oligopeptide conjugates used for bone targeting.     

乳液聚合法制备P(St/BA)-KAl(OH)2CO3纳米复合物

利用乳液聚合法制备了一种含KAl(OH)2CO3纳米粒子的聚苯乙烯／丙烯酸丁酯复合物．Zeta电位、粒径分布、扫描电镜(SEM)和透射电镜(TEM)等分析表明KAl(OH)2CO3粒子能够稳定地分散于苯丙乳液的乳胶粒中,形成核一壳结构．热失重(TG)分析表明KAl(OH)2CO3粒子的加入能提高复合物的热稳定性,使其在阻燃涂料领域有着潜在的应用前景．     

Synthesis and Crystal Structure of 3-（1-Ethyl-1H-indole-3-carbonyl）aminopropionic Acid

3-(1-Ethyl-1H-indole-3-carbonyl)aminopropionic acid has been synthesized by alkylation of 3-(1H-indole-3-carbonyl)aminopropionic acid methyl ester with bromoethane,follo-wed by saponifying and acidating,in 89.0% yield.Its crystal structure was gotten and determined by X-ray diffraction method.The crystal is of orthorhombic,space group P212121 with a = 8.9490(12),b = 11.1010(15),c = 13.0475(18) ,V = 1296.2(3) 3,Z = 4,Dc = 1.334 g/cm3,λ = 0.71073 ,μ(MoKα) = 0.095 mm-1,Mr = 260.29 and F(000) = 552.The structure was refined to R = 0.0306 and wR = 0.1445 for 2612 observed reflections with I 2σ(I).In the crystal structure,molecules are linked to each other through hydrogen bonds of N(2)-H(2)···O(1) and O(3)-H(3)···O(1),generating a three-dimensional network.     

5-(色酮基-3-次甲基)(硫代)巴比妥酸的合成

将巴比妥酸或硫代巴比妥酸、3-甲酰基色酮在乙酸-乙酸酐溶液(含乙酸酐10%)中进行缩合反应,制备了5-(色酮基-3-次甲基)(硫代)巴比妥酸.并经元素分析,IR,1H NMR及13C NMR确证了产物的结构.     

Synthesis and Tumor Cytotoxicity of Novel 1, 2, 3-Triazole-substituted 3-Oxo-oleanolic Acid Derivatives

Fifteen novel 3-oxo-oleanolic acid esters bearing aryl substituted 1,2,3-triazolyl methyl moiety were synthesized via the method of Copper(I)-catalyzed Huisgen cycloaddition. The cytotoxicity evaluation results of these compounds against five human tumor cell lines show that most of these compounds presented potent activity and selectivity against A375-S2 and HT1080 cells. Compound 6c, with a p-NO₂ at the bezene ring, possesses the best inhibitory activity against A375-S2(IC₅₀=2.82 μmol/L) and HT1080(IC₅₀=1.69 μmol/L).     

Novel tetradentate diamine dioxime ligands: synthesis,characterization and in vivo behavior of their 99mTc‐complexes

Two novel diamine dioxime ligands, 4,7‐diaza‐3,8‐diethyldecane‐2,9‐dione bis oxime (3) and 4,9‐diaza‐3,10‐diethyldodecane‐2,11‐dione bis oxime (5), were synthesized in order to develop new brain perfusion imaging agents, based on ^99mTc(V)‐complexes. The synthesis involved condensation of 2‐hydroxyimino‐3‐pentanone with appropriate diamine in protic solvent which afforded the bis imine adducts. Subsequent reduction of imine functional groups yielded a diastereoisomeric mixture of 3 and 5. UV–visible, IR, ¹H NMR, ¹³C NMR and elemental analysis were used to characterize the structures of the synthesized compounds. ^99mTc‐complexes of both diamine dioximes were prepared and radiolabeling conditions optimized to give the maximum yield. Physicochemical parameters of the labeled complexes as well as and their biodistribution in rats were investigated. Both compounds (3 and 5) formed ^99mTc‐complexes with a net charge of zero, determined by electrophoresis. The resultant lipophilic ^99mTc‐complexes of 3 and 5 were readily formed at pH ~9.0 within 10 min at room temperature with yields of 90% and 95%, respectively. The ^99mTc‐3 complex was found to be stable within 1 h, while ^99mTc‐5 was stable for a few hours. A significant brain uptake of ^99mTc‐3 (2.1% injected dose) and ^99mTc‐5 (1.8% injected dose) complexes, 2 min after injection, is in accordance with their lipophilicity. The present study suggests that both ligands are promising candidates as new ^99mTc‐based brain‐imaging agents. Copyright © 2012 John Wiley & Sons, Ltd.     

Synthesis of poly(propylene imine) dendrimers via homogeneous reduction process using lithium aluminium hydride: Bioconjugation with folic acid and doxorubicin release kinetics

The heterogeneous reduction process for synthesis of poly(propylene imine) (PPI) dendrimer has been replaced by a novel and homogeneous process. Accordingly, to prepare half generations, acrylonitrile was added to amine groups via Michael addition reaction. Then, nitrile groups were reduced via homogeneous hydrogenation using lithium aluminium hydride to synthesize fifth‐generation PPI dendrimers with ethylenediamine core. Also, peripheral primary amine groups were conjugated with folic acid (FA). Fourier transform infrared and ¹³C NMR spectroscopies and gel permeation chromatograph y were used to prove the synthesis of the various structures. Finally fifth‐generation and FA‐conjugated fifth‐generation PPI dendrimers were loaded with doxorubicin and exposed to environments with different pH values to examine the release properties of the structures. Also, drug release kinetics was investigated by fitting experimental data with various release models. The synthesized dendritic structures showed Higuchi model release behaviour due to better solubility of drug in release media with respect to dendrimer cavities.