2-甲氧/乙氧羰基-4-氟苯基-1,5-苯并硫氮杂的合成、抑真菌活性及构效关系

以高活性的2-甲氧/乙氧羰基-4-(4-氟苯基)-1,5-苯并硫氮杂A和B为模型化合物,设计合成了11个含氟杂衍生物3a~3k,考察了它们对白色念珠菌和新生隐球菌的抑菌活性.研究结果表明,2-甲氧/乙氧羰基-4-(2-氟苯基)/(3-氟苯基)/(2,4-二氟苯基)-1,5-苯并硫氮杂3a,3b,3d~3f对新生隐球菌有很强的抑菌活性,3c的活性中等,而7位氯代杂3g~3k基本无活性;上述杂对白色念珠菌均无活性.在此基础上,进一步测试了高活性杂3a,3b,3d~3f对新生隐球菌的抑菌浓度梯度、最小抑菌浓度(MIC)和最小杀菌浓度(MFC),发现其MIC和MFC均远低于对照药氟康唑.为了考察杂3a~3f的药效基团,又设计合成了4类杂衍生物4a~4f,5a~5f,6a~6f和7a~7c,通过对其抑菌活性的评价,发现分子中2-甲氧/乙氧羰基和亚胺官能团对杂3a~3f的抑真菌(新生隐球菌)活性起关键作用,硫原子被氧原子或氮原子代替后原杂的活性降低.     

手性2-甲氧羰基-4-氟苯基-1,5-苯并硫氮杂卓的不对称合成及抑真菌活性

以(R)/(S)-4-苄基-2-噁唑烷酮为手性助剂,采用不对称合成方法制备了18个具有光学活性的2-甲氧羰基-4-氟苯基-1,5-苯并硫氮杂卓类化合物9a~9i和14a~14i,经HPLC分析e.e.值较为理想;通过核磁共振谱、红外光谱和高分辨质谱表征了其结构,通过单晶X射线衍射法确定化合物9h的相对构型;用抑菌圈法测试了目标化合物对新生隐球菌的抑菌活性.研究结果表明,由S型手性助剂诱导不对称合成的杂卓对新生隐球菌的抑制作用普遍高于由R型手性助剂诱导合成的杂卓及外消旋体.测试了抑菌活性较好的化合物14a~14f的最小抑菌浓度(MIC)和最小杀菌浓度(MFC),发现其对新生隐球菌的MIC和MFC均低于抗真菌药物氟康唑.     

C(3)-1,2,4-三氮唑取代的1,5-苯并硫氮杂■的合成及抑菌活性

设计合成了3类C(3)-1,2,4-三氮唑取代的1,5-苯并硫氮杂■化合物,2,3-二氢/2,5-二氢/2,3,4,5-四氢-3-(1,2,4-三氮唑)-4-芳基-1,5-苯并硫氮杂■.研究了中间体及目标产物的合成条件,确定了其中2个副产物的结构.目标产物的抑菌活性测试表明,2,3-二氢/2,5-二氢-3-(1,2,4-三氮唑)-4-芳基-1,5-苯并硫氮杂■对新生隐球菌和白色念珠菌表现出很高的抑制作用,在200μg/disc的浓度下,有4个化合物对新生隐球菌的抑制作用高于对照药物氟康唑,有3个化合物对白色念珠菌的抑制活性高于对照药物氟康唑.初步抑真菌构效关系研究表明,1,2,4-三氮唑环和C=N双键是2,3-二氢-3-(1,2,4-三氮唑)-4-芳基-1,5-苯并硫氮杂■抑真菌活性的关键药效团.     

C(2)-酰胺基-4-芳基-1,5-苯并硫氮杂的合成及抑菌活性的研究

设计合成了三类C(2)酰胺基取代的1,5-苯并硫氮杂衍生物:2-酰胺基(N-芳基)-4-芳基-1,5-苯并硫氮杂、2-酰胺基(N-烷基)-4-芳基-1,5-苯并硫氮杂和2-酰胺基(N,N-二烷基)-4-芳基-1,5-苯并硫氮杂,其结构用元素分析,IR,MS及1H NMR确证.测定了目标化合物的抑真菌活性,结果表明部分化合物对新生隐球菌具有中等强度的抑真菌活性.还研究了2-酰胺基-4-芳基-1,5-苯并硫氮杂的合成反应条件.     

含有芳杂环及酯基结构的1H-2,5-二氢-1,5-苯并二氮杂?类化合物的合成、抑菌活性及构效关系

以2-(2-噻唑基)-3-乙酯基-4-甲基-1H-2,5-二氢-1,5-苯并二氮杂?(A)为模型化合物,设计合成了3个系列30种1H-2,5-二氢-1,5-苯并二氮杂?类衍生物2~6,其结构通过核磁共振波谱、红外光谱、质谱和元素分析确证.采用常规滤纸片扩散法测试了其对真菌(新生隐球菌标准株、临床株、白色念珠菌标准株)和细菌(大肠杆菌标准株和金黄色葡萄球菌标准株)的抑菌活性.研究结果表明,大多数化合物对所测试的菌种都表现出很好的抑制作用,且抑真菌能力大于抑细菌能力;通过对活性较高的化合物2-(2-噻唑基)-3-乙酯基-4-乙基-8-甲基-1H-2,5-二氢-1,5-苯并二氮杂?(4b)和2-(2-噻唑基)-3-乙酯基-4-乙基-8-氟-1H-2,5-二氢-1,5-苯并二氮杂?(4c)的最小抑菌浓度(MIC)和最小杀菌浓度(MFC)测试,发现其对白色念珠菌的MIC和MFC都远低于标准药物氟康唑.进一步构效关系研究表明C-2位的2-噻唑基,C-4位的CH_3、CH_2CH_3和C-8位的CH_3都是该类化合物抑菌的必需基团.     

含1,2,3-三氮唑结构的1,5-苯并硫氮杂?的合成及其抑真菌活性

设计合成了三类含1,2,3-三氮唑结构的1,5-苯并硫氮杂?化合物3-(1H-1,2,3-三氮唑)-4-芳基-2,5-二氢-1,5-苯并硫氮杂?(5a～5f)、3-(2H-1,2,3-三氮唑)-4-芳基-2,3-二氢-1,5-苯并硫氮杂?(6a～6f)和3-(1H-1,2,3-三氮唑)-4-芳基-2,3,4,5-四氢-1,5-苯并硫氮杂?(7a～7f).研究了中间体及目标产物的合成条件,分离出其中两个副产物并进行了结构确定.目标产物的抑真菌活性测试表明,化合物5a～5f对真菌具有良好的抑制作用,对新生隐球菌的抑制效果尤为突出.初步抑真菌构效关系研究表明, 1H-1,2,3-三氮唑环和C=C双键是化合物5a～5f抑真菌活性的关键官能团.     

2-烷氧羰基烷基/正丁基-4-芳基-1,5-苯并硫氮杂类化合物的合成及抑菌活性的研究

设计、合成了三类2位取代-1,5-苯并硫氮杂衍生物:2-烷氧羰基甲基-4-芳基-1,5-苯并硫氮杂、2-烷氧羰基乙基-4-芳基-1,5-苯并硫氮杂和2-正丙基-4-芳基-1,5-苯并硫氮杂.所有目标化合物结构经过元素分析,IR,MS,HRMS及1H NMR确证.研究了2-烷氧羰基烷基/正丁基-4-芳基-1,5-苯并硫氮杂的合成反应条件,测定了目标化合物的抑真菌活性.通过对该类化合物抑真菌活性的评价,进一步明确乙酯基在1,5-苯并硫氮杂1的生物活性中所起的作用.     

七元杂环——Ⅰ.2,4-二取代-2,3,4,5-四氢一苯骈(1:5)硫氮杂

2-甲基-4-苯基-2,3-二氢一苯骈(1:5)硫氮杂()的盐酸盐和2,2,4-三甲基-2,3-二氢一苯骈(1:5)硫氮杂()分别用硼氢化钠处理,制得相应的四氢化物,作为合成精神病安定剂的原料。 2-甲基-4-苯基-2,3-二氢一苯骈(1:5)硫氮杂()的盐酸盐在温和条件下,遇氢氧化钠水溶液发生开环作用得到β-(邻氨基苯硫基)苯基丙基甲酮,后者受无水氯化氢的作用又环化为原料,用化学方法和红外光谱证实了上述化合物的结构。     

含1,2,3-三氮唑结构的1,5-苯并硫氮杂[艹卓]的合成及其抑真菌活性

设计合成了三类含1,2,3-三氮唑结构的1,5-苯并硫氮杂[艹卓]化合物3-(1H-1,2,3-三氮唑)-4-芳基-2,5-二氢-1,5-苯并硫氮杂[艹卓](5a^5f)、3-(2H-1,2,3-三氮唑)-4-芳基-2,3-二氢-1,5-苯并硫氮杂[艹卓](6a^6f)和3-(1H-1,2,3-三氮唑)-4-芳基-2,3,4,5-四氢-1,5-苯并硫氮杂[艹卓](7a^7f).研究了中间体及目标产物的合成条件,分离出其中两个副产物并进行了结构确定.目标产物的抑真菌活性测试表明,化合物5a^5f对真菌具有良好的抑制作用,对新生隐球菌的抑制效果尤为突出.初步抑真菌构效关系研究表明, 1H-1,2,3-三氮唑环和C=C双键是化合物5a^5f抑真菌活性的关键官能团.     

2-取代苯基-3-(N,N-二甲基甲酰胺基)-4-甲基-1,5-苯并硫氮杂?的合成及抑菌活性

将N,N-二甲基甲酰胺基引入1,5-苯并硫氮杂?,设计合成了6个2-取代苯基-3-(N,N-二甲基甲酰胺基)-4-甲基-1,5-苯并硫氮杂?化合物,研究了它们的合成反应条件,发现其为动力学控制产物.生物活性研究表明,目标化合物对真菌和细菌都有明显的抑制作用,尤其是对新生隐球菌和大肠杆菌有突出的抑制效果.     

二氧化碳和丙烯直接合成甲基丙烯酸的NiPMo/TiO2催化剂的研究

用溶胶-凝胶法以磷钼酸(MPA)的镍盐溶液水解钛酸四丁酯制备了NiPMo/TiO2催化剂.使用ICP、 XRD、 TG-DTA、 IR、 TPD-MS和微反应技术研究了催化剂的化学组成、热稳定性、化学吸附性质和催化反应性能.杂多钼酸盐与TiO2通过O2-在TiO2表面发生了键合.在623 K下,杂多阴离子仍保持原有的Keggin结构.CO2在Lewis酸位Ni(Ⅱ)和Lewis碱位Ni-O-Mo的桥氧协同作用下生成CO2卧式吸附态Ni(Ⅱ)←O-(CO)←(O--Ni).丙烯有多种吸附态在催化剂上吸附.在563 K、 1 MPa和空速1500 h-1的反应条件下,丙烯的摩尔转化率为3.2%,产物MAA选择性为95%.     

Synthesis of 1-benzyloxypyrazin-2(1H)-one derivatives

Different approaches for the synthesis of 1-benzyloxypyrazin-2(1H)-one derivatives from simple amino acids have been investigated. A library of 33 precursors for the preparation of N-hydroxy pyrazinones was obtained in moderate to good yields.     

α-Amino acid derived enaminones and their application in the synthesis of N-protected methyl 5-substituted-4-hydroxypyrrole-3-carboxylates and other heterocycles

A new and simple synthesis of novel N-protected methyl 5-substituted-4-hydroxypyrrole-3-carboxylates, which exist in equilibrium with their 4-oxo tautomers, has been developed in two steps starting from N-protected α-amino acids. The key intermediates are enaminones, which can also be isolated, characterized, and used for the construction of other functionalized heterocycles, before they spontaneously decompose to pyrrole products. 4-Hydroxypyrroles are prone to partial aerial oxidation but can be efficiently alkylated or reduced to stable polysubstituted pyrrolidine derivatives.     

Specific intramolecular aromatic CH insertion of diazosulfonamides

The chemoselectivity in the intramolecular CH insertion of various diazosulfonamides has been experimentally studied. The results reveal that the aliphatic 1,4-, 1,5-, or 1,6-C(sp³)?H insertions of diazosulfonamides are not accessible, while the aromatic 1,5-C(sp²)?H insertion can be realized specifically by adjusting the diazo-adjacent group. In addition, the general chemoselectivities in the intramolecular CH insertions of diazosulfonyl compounds are summarized. Generally, diazosulfones undergo both aromatic 1,5-C(sp²)?H and aliphatic 1,5- and 1,6-C(sp³)?H insertions, while diazosulfonates undergo aliphatic 1,5- and 1,6-C(sp³)?H insertions. However, diazosulfonamides only undergo aromatic 1,5-C(sp²)?H insertion.     

A general and convenient synthesis of 4-(tosylmethyl)semicarbazones and their use in amidoalkylation of hydrogen,heteroatom, and carbon nucleophiles

A general synthesis of previously unknown semicarbazone-based α-amidoalkylating reagents, 4-(tosylmethyl)semicarbazones, has been developed. The synthesis involved three-component condensation of semicarbazones of aliphatic or aromatic aldehydes with the same or other aldehydes and p-toluenesulfinic acid. The scope and limitations of this reaction were investigated. The compounds obtained were demonstrated to be an efficient α-(4-semicarbazono)alkylating agents. They were reacted with H- (sodium borohydride), O- (sodium methylate), S- (sodium phenylthiolate), N- (pyrrolidine, sodium succinimide), P- (trialkyl phosphites), and C-nucleophiles (sodium diethyl malonate) to give the corresponding products of the tosyl group substitution, 4-substituted semicarbazones, including analogues of nitrofurazone. Among the prepared compounds tested in vitro for antibacterial and antifungal activity, three nitrofuryl-containing semicarbazones exhibited high biological activities with minimum inhibitory concentration (MIC) values of 8–32 μg/mL.     

Toward new camptothecins. Part 6: Synthesis of crucial ketones and their use in Friedländer reaction

In the context of the preparation of camptothecin and luotonin A analogs, the synthesis of some key keto-precursors and their use in Friedländer condensation are described. This paper also focuses on the stability of these keto intermediates and emphasizes the major differences between indolizinones and pyrroloquinazolinones series. Noteworthy is also the report of some original structures isolated as by-products of some experiments.     

Synthesis of novel chiral bidentate hydroxyalkyl-N-heterocyclic carbene ligands and their application in palladium-catalyzed Mizoroki–Heck couplings and asymmetric addition of diethylzinc to benzaldehyde

A small library of new chiral bidentate hydroxyalkyl-imidazolium salts 1 is conveniently synthesized on multi-gram scale from inexpensive and commercially available chiral pool amino acids. The corresponding carbenes, generated by deprotonation of imidazolium salts 1, in combination with palladium(II) chloride were tested in the Mizoroki–Heck coupling reaction. The most significant results in terms of yields and reactivities were achieved with low catalyst loading. The catalytic activities of these imidazolium salts were also investigated in the asymmetric addition of diethylzinc to benzaldehyde. The use of MgO nanoparticles as an additive in conjunction with these ligands played a crucial role in increasing the efficiency of these reactions.     

N-Heterocyclic carbene-palladacyclic complexes: synthesis,characterization and their applications in the C-N coupling and α-arylation of ketones using aryl chlorides

N-Heterocyclic carbene-palladacyclic complexes 3 were successfully achieved in a one-pot procedure under mild conditions. The structure of 3a was unambiguously confirmed by X-ray single crystal diffraction and it was an active catalyst in the Buchwald-Hartwig amination and α-arylation of ketones even at very low catalyst loadings (0.01?mol%).     

Iodine-mediated oxidative Pictet-Spengler reaction using terminal alkyne as the 2-oxoaldehyde surrogate for the synthesis of 1-aroyl-β-carbolines and fused-nitrogen heterocycles

An efficient iodine-mediated oxidative Pictet-Spengler reaction in dimethyl sulphoxide (DMSO) using terminal alkynes as the 2-oxoaldehyde surrogate for the synthesis of aryl (9H-pyrido[3,4-b]indol-1-yl)methanones is described. The scope of the protocol includes the total synthesis of Fascaplysin, Eudistomins Y₁ and Y₂. The methodology is extended for preparing pyrrolo[1,2-a]-quinoxaline and indolo[1,5-a]quinoxaline derivatives. The utility of 1-aroyl-β-carbolines was demonstrated by performing palladium-catalyzed β-carboline directed ortho-C(sp2)-H functionalization of the phenyl ring with thiomethyl (SMe) group using DMSO as source and for accessing 4-aryl-canthin-6-ones.     

Facile synthesis of bicyclic 1-arylpyrazol-5-ones

In this Letter, we described a facile method for constructing fused bicyclic 1-arylpyrazol-5-one ring system. We employed various methylene-containing carboxylic acids as the substrates and proved that the pyrazolone ring closure requires activated methylene group in intermediate II. Accordingly, a series of structurally diversified, fused bicyclic 1-arylpyrazol-5-ones was prepared in moderate to high yields using the requisite substrates.