5-氨基-6-硝基-[1,2,5]噁二唑并[3,4-b]吡啶-1-氧化物的合成新方法

以2,6-二氯吡啶为起始原料, 经肼基化、还原、硝化、Nietzki-Dietschy环合4步反应得到5-氨基-6-硝基-[1,2,5]噁二唑并[3,4-b]吡啶-1-氧化物。 结合反应机理讨论了还原、硝化、Nietzki-Dietschy环合反应的影响因素,获得了合成5-氨基-6-硝基-[1,2,5]噁二唑并[3,4-b]吡啶-1-氧化物的最佳工艺条件,目标产物的总收率为59.2%。 用1H NMR、MS和IR谱对5-氨基-6-硝基-[1,2,5]噁二唑并[3,4-b]吡啶-1-氧化物的结构进行了表征。     

5-取代氧化呋咱并[3,4-b]吡啶衍生物的合成与表征

以廉价易得的2,6-二氯吡啶为原料,经过硝化、叠氮化、热解环化步骤得到中间体[1,2,5]噁二唑并[3,4-e]四唑并[1,5-a]吡啶-3-氧化物(4b),再与浓硫酸/硝酸钾、甲醇钠和甲胺水溶液反应分别得到5-取代的氧化呋咱并[3,4-b]吡啶衍生物5~7。 研究了化合物4b结构的稳定性,发现其中的氧化呋咱环在强酸性、强碱性和弱碱性条件下较稳定,而吡啶环与叠氮基形成的四唑环结构则不太稳定。     

7-氨基-6-硝基-[1,2,5]噁二唑并[3,4-b]吡啶-1-氧化物的胺化开环反应及产物的抗肿瘤活性

7-氨基-6-硝基-[1,2,5]噁二唑并[3,4-b]吡啶-1-氧化物(1)与胺在温和条件下反应,氧化呋咱环开环,释放一分子次硝酸,得到了蓝绿色的开环产物2-胺取代的-3-亚硝基-4-氨基-5-硝基吡啶5a~5f.发现化合物1中的6-位硝基对其氧化呋咱开环起到关键作用.利用~1H NMR,~(13)C NMR和HRMS对目标化合物进行了结构表征.用四甲基偶氮唑盐(MTT)法测试了目标化合物体外抑制人肺癌细胞株(H522)和脑胶质瘤细胞株(U87)两种肿瘤细胞的增殖活性.测试结果显示,所有目标化合物均表现较强的体外肿瘤细胞抑制活性.     

10-氯-5-二乙氧基甲基-1,3-二甲基色烯并[4,3-d]吡唑并[3,4-b]吡啶-6(3H)-酮的合成和晶体结构

利用L-脯氨酸催化的5-氯水杨醛(1)与6-甲基-4-羟基吡喃酮(2)的缩合反应及硫酸铜催化下与1,3-二甲基-5-氨基吡唑(3)的串联反应,合成得到了10-氯-1,3-二甲基-5-(2-氧代丙基)色烯并[4,3-d]吡唑并[3,4-b]吡啶-6(3H)-酮(4)和10-氯-5-二乙氧基甲基-1,3-二甲基色烯并[4,3-d]吡唑并[3,4-b]吡啶-6(3H)-酮(5).化合物5的结构通过单晶X射线衍射法确定:晶体属于三斜晶系,空间群P-1;相对分子质量Mr=803.68;晶胞参数a=1.03160(10)nm,b=1.42900(13)nm,c=1.44268(15)nm;V=1.9448(3)nm~3;Z=2;晶胞密度Dc=1.372g/cm~3;吸收系数μ=0.228mm-1;单胞中电子的数目F(000)=840.晶体结构用直接法解出,经全矩阵最小二乘法对原子参数进行修正,最终的偏离因子为R=0.0681,w R=0.2051.在晶体结构中色烯环与吡啶环及吡唑环近似于共平面.     

改进的2-巯基-5-甲氧基咪唑并[4,5-b]吡啶合成法

以2,6-二氯吡啶为起始原料,经甲氧基化、硝化、氨基化、还原及成环5步反应得到2-巯基-5-甲氧基咪唑并[4,5-b]吡啶,总收率45.7%。重点比较了2-氯-6-甲氧基吡啶和2,6-二氯吡啶硝化反应条件及收率的差异,讨论了水合肼、NaOH的用量对目标产物收率的影响。用1HNMR、MS和IR测试技术对目标产物结构进行了表征。     

5(4H)-吡啶酮并氧化呋咱及其核苷衍生物的合成及结构表征

设计了一个新化合物——5(4H)-吡啶酮并氧化呋咱(4H,5H-[1,2,5]噁二唑[3,4-b]吡啶-5-酮-1-氧化物),对它的合成方法及四乙酰核糖核苷衍生物的合成进行了研究.合成产物及中间体经1HNMR、质谱和元素分析进行了结构鉴定.     

微波辐射下硅磺酸催化的香豆素并[4,3-d]吡唑并[3,4-b]吡啶的高效合成

在硅磺酸催化下,通过微波辐射的3-酰基香豆素与5-氨基吡唑的反应,一步高产率地合成了一系列香豆素并[4,3-d]吡唑并[3,4-b]吡啶衍生物.该方法具有反应时间短(20~30 min)、选择性好、产率高、操作简单和环境友好等优点.产物的结构经红外光谱、核磁共振谱及高分辨质谱予以确定.     

微波辐射下磷酸改性铌酸催化的香豆素修饰吡唑并[3,4-b]吡啶衍生物的高效合成

香豆素和吡唑并[3,4-b]吡啶骨架广泛存在于具有生物活性的天然化合物中,在药物化学中也被广泛用作药物核心单元,具有极其重要的作用.以磷酸改性铌酸作为催化剂,通过微波辐射下醛、香豆素衍生物、5-氨基吡唑的三组分反应一锅法高产率地合成一系列香豆素修饰的吡唑并[3,4-b]吡啶衍生物.该反应一步完成,具有催化剂和溶剂对环境友好,操作简单等优点.产物的结构经红外光谱、核磁共振谱及高分辨质谱予以确定.     

4-氯-2-甲基吡啶并[3,2-d]嘧啶的合成

吡啶并嘧啶类衍生物具有较好的生物活性,4-氯-2-甲基吡啶并[2,3-d]嘧啶是一种重要的医药中间体,已报道的合成方法成本较高且操作繁琐,不适合工业化生产.本文以2-氯-3-硝基吡啶为起始原料,经取代、还原、环合等5步反应得到目标化合物,产物结构经1 H NMR,13C NMR和MS确证,总收率为33％.该路线具有成本...     

嘧啶并呋咱核苷衍生物的制备及其活性初探

4H,6H-[1,2,5]噁二唑并[3,4-d]嘧啶-5,7-二酮1-氧化物(1)和6-甲基-4H,6H-[1,2,5]噁二唑并[3,4-d]嘧啶-5,7-二酮1-氧化物(2)是一氧化氮(NO)供体, 将它们分别在无溶剂条件下与高温熔融的全乙酰基保护的核糖、木糖、葡萄糖进行糖基化反应, 分别得到相应的噁二唑并[3, 4-d]嘧啶核苷类化合物7, 9～12, 化合物7经NH₃-MeOH处理, 去O-乙酰基制得8, 这些新型核苷化合物可作为潜在的NO供体. 部分此类化合物的生物活性研究表明, 嘧啶并呋咱核苷衍生物具有抗病毒、抗肿瘤活性, 为研究抗病毒、抗肿瘤药物提供了新结构类型的候选化合物.     

异色满并[4,3-b]喹啉衍生物的合成

早在1931年,Hetherington等从念珠状曲菌(Aspergillus Cand inin)和土曲菌(Asperillus tereus)等菌类中分离出带有异色满(Isochroman)环系结构的左旋抗菌素橘霉素(C itrinin),后来又相继发现诸多带有异色满环系的天然产物[1-3],新近在软木木质素中也发现了多种具有异色满结构的     

苯并咪唑并[2,1-b]噻唑衍生物的合成

以2-巯基咪唑类化合物为原料,室温下与含有端基炔的二芳基高碘盐反应,一步合成苯并咪唑并[2,1-b]噻唑衍生物,其结构经¹H NMR、¹³C NMR、 单晶X-衍射和HR-MS表征。在最佳反应条件［n(2-巯基苯并咪唑)/n(二芳基高碘盐)=1/1,二氯甲烷为溶剂,反应12 h］下,目标化合物的产率最高为84%。同时对该反应的机理进行了详细探讨,并采用MTT法研究了目标化合物对人肝癌细胞（HepG2）生长情况的影响。结果表明：当浓度为4 μg/mL时,化合物3b具有较强的抑制HepG2细胞增殖的活性,抑制率为52%。     

Mono- and penta-addition of enol silyl ethers to [60]fullerene

The reaction of 1-alkoxy-1-siloxyethene with [60]fullerene in 20% DMSO/chlorobenzene at ambient temperature under an oxygen atmosphere gave a penta-addition product, while the reaction of 1-alkoxy-1-siloxyalkenes or 1,2-siloxyalkenes under argon gave monoaddition products. The new method has merits over the previously reported syntheses of these compounds in that the synthesis does not require the use of heavy metals or photolysis conditions, and it can be carried out under simple and mild conditions.     

Photosensitized [4+2]- and [2+2]-Cycloaddition Reactions of N-Sulfonylimines

The synthesis of polycyclic compounds is of high interest due to the prevalence of these motifs in drugs and natural products. Herein, we report on the stereoselective construction of 3D bicyclic scaffolds and azetidine derivatives by modulation of N-sulfonylimines to achieve either [4+2]- or [2+2]-cycloaddition reactions. The utility of the method was established by further modulation of the product. Mechanistic studies are also included, which support reaction via Dexter energy transfer.     

Thermal unimolecular isomerization of 1,4-dimethylbicyclo[2.2.0]hexane, 1,4-dimethylbicyclo[2.1.1]hexane,and 1,4-dimethylbicyclo[2.1.0]pentane

The thermal isomerization of the title compounds was studied in the vapor phase. Over the temperature range from 445.1 to 477.5°K, 1,4-dimethylbicyclo[2.2.0]hexane underwent a homogeneous unimolecular reaction to 2,5-dimethyl-1,5-hexadiene, the rate constants being represented by the equation: k = 1.86 × 10¹¹ exp (?31000 ± 1800/RT) sec^?1. Over the temperature range from 630.0 to 662.2°K, 1,4-dimethylbicyclo[2.1.1]-hexane also underwent a unimolecular isomerization to the same product, the rate constants being given by the equation: k = 8.91 × 10¹⁴ exp (?56000 ± 900/RT) sec^?1. The pyrolysis of 1,4-dimethylbicyclo[2.1.0]pentane gave 1,3-dimethylcyclopentene-1 and 2,4-dimethyl-1,4-pentadiene in the ratio of 9:1. The former reaction was influenced by surface effects but the latter was not. The rate constants for the formation of 2,4-dimethyl-1,4-pentadiene fitted the equation: k = 1.66 × 10¹⁷ exp (?57400 ± 3100/RT) sec^?1. The effect of the two methyl groups at the bridgehead positions in these molecules in influencing the rate of decomposition is discussed in terms of the non-bonded repulsive forces between the substituents.     

Kinetically and thermodynamically controlled synthesis of tetraoxa[14]metacyclophanes and hexaoxa[16]metacyclophanes

The nucleophilic aromatic substitution of 1,5-difluoro-2,4-dinitrobenzene with 2-propylresorcinol in Et₃N/CH₃CN produces a mixture of syn and anti conformers of the cyclic tetramer and the cyclic hexamer with a kinetically controlled product distribution. Moreover, the reaction in DMF was catalyzed by CsF to also produce a mixture of these cyclic oligomers. In this case, however, the C-O bond is cleaved by the fluoride ion and the cyclization reaction is reversible; therefore, in the presence of excess CsF, the thermodynamically favored product (syn-isomer of cyclic tetramer) is obtained as the major product. The structures of the two conformational isomers of cyclic tetramers were determined by X-ray crystallography.     

Electrophilic acetylation and bromination reactions of benzo[b]naphtho[2,3-e][1,4]dioxin

The reactivity of benzo[b]naphtho[2,3-e][1,4]dioxin in the electrophilic aromatic substitution reactions has been studied. Friedel-Crafts acetylation resulted in the formation of three out of the possible five monoacetylated products, with the acetyl group located in positions 8 (major), 7 and 6 (minor) of the heterocycle. In the bromination reaction a higher selectivity was observed with the 6-bromo derivative found as the only monobrominated product and the 6,11-dibromo derivative found as the only polybrominated product. A ratio of unreacted heterocycle:6-bromo:6,11-dibromo derivatives in the bromination reaction has been found to depend strongly on the reaction conditions and on the heterocycle:bromine ratio.     

Polyethylene glycol-promoted synthesis of pyrimido[1,2-a]benzimidazole and pyrano[2,3-c]pyrazole derivatives in water

Synthesis of pyrimido[1,2-a]benzimidazole and pyrano[2,3-c]pyrazole derivatives were achieved using polyethylene glycol (PEG-400) as promoting reaction medium in water under catalyst-free conditions at reflux and room temperature, respectively. The structure of pyrimido[1,2-a]benzimidazole was confirmed using ¹H NMR, ¹³C NMR, DEPT, and HMBC experiments. The promising points for the present methodology are efficiency, generality, high yield, short reaction time, cleaner reaction profile, ease of product isolation, simplicity, potential of recycling reaction medium, and finally agreement with green chemistry protocols.     

1,2,3-benzotriazines. IV. The chemical reactivity of benzimidazo[1,2-c] [1,2,3]benzotriazine

The reactions of benzimidazo[1,2-c][1,2,3]benzotriazine (1) with fluoroboric acid, potassium iodide and phenyl isothiocyanate are described. The structure of the phenyl isothiocyanate product is elucidated by chemical and spectroscopic techniques. The reaction of 1 with alcoholic potassium hydroxide is shown to proceed by a free radical mechanism. The structure of the compound formed from 1 and sodium diethyl malonate is investigated by spectroscopic methods. The reduction and photochemical reactivity of 1 are also discussed.