L-谷氨酸桥联的卟啉二联体的合成和表征及其CD光谱研究

通过L-谷氨酸(乙酰基保护)与二氯亚砜反应制备的二酰氯和单羟基卟啉(M-PH₂)反应,合成了L-谷氨酸桥联的卟啉二联体,用红外光谱、 电子吸收光谱、 核磁共振氢谱、 元素分析和质谱对化合物的结构加以确证,通过圆二色谱(CD)研究了化合物的手性特征.     

烟酸-卟啉二元化合物的合成、表征及其电化学性质

通过亲核取代反应合成了3个新的烟酸-卟啉二元化合物, 并用红外光谱、紫外-可见光谱、核磁共振氢谱、元素分析和质谱对化合物的结构进行确认, 通过循环伏安法研究了其电化学性质.     

Nucleophilic substitution in 4-bromo-5-nitrophthalodinitrile: VIII. Synthesis of 4-(benzotriazol-1-yl)-5-[4-(1-methyl-1-phenylethyl)phenoxy]phthalodinitrile and phthalocyanines on its basis

Nucleophilic aromatic substitution of the bromine atom in 4-bromo-5-nitrophthalodinitrile by a 2-aminophenylamine residue followed by conversion of the resulting compound to 4-(1-benzothiazol-1-yl)-5-nitrophthalodinitrile and nucleophilic substitution of the nitro group by a 4-(1-methyl-1-phenylethyl)-phenoxy group gave 4-(benzotriazol-1-yl)-5-[4-(1-methyl-1-phenylethyl)phenoxy]phthalodinitrile. The latter product was reacted with certain metal acetates and chlorides to obtain the corresponding metal complexes of octasubstituted phthalocyanines. Spectral properties of the complexes were studied.     

Synthesis of b-Cyclodextrin Bonded Metal Porphyrins

6-Deoxy- 6-iodo-b -cyclodextrin (1) reacted with 5-(p-aminophenyl)-10,15,20-triphenyl porphyrin(2), 5-(p-aminophenyl)-10,15,20-triphenyl nickel(II) porphyrin [NiⅡTPPNH2P] (3), 5-(p-aminophenyl)-10,15,20-triphenyl manganese(Ⅲ) porphyrin [MnⅢTPPNH2P] (4) and 5-(p-aminophenyl)-10,15,20-triphenyl carbonyl ruthenium porphyrin [RuⅡ(CO)TPPNH2P] (5) to generate the compounds 6-9, respectively. Those new compound 5-9 have been identified by 1H NMR, IR, MS and UV-visible spectra and elemental analysis.     

卟啉化合物研究(Ⅸ)——聚5-邻丙烯酰胺苯基-10,15,20-三苯基卟啉及其钴配合物的合成

将丙烯酰氯和5-邻氨基苯基-10,15,20-三苯基卟啉(Ⅰ)相连合成了5-邻丙烯酰胺苯基-10,15,20-三苯基卟啉(Ⅱ)。在引发剂作用下,Ⅱ进一步聚合,生成聚5-邻丙烯酰胺苯基-10,15,20-三苯基卟啉(Ⅲ),同时还合成了单体和聚合物的钴配合物。通过元素分析、核磁共振谱、红外光谱和可见吸收光谱对单体和聚合物的结构进行了鉴定。     

卟啉化合物的研究(ⅩⅩ)——5-(p-十六烷氧基苯基)-10,15,20-三苯基卟啉和5-(p-十六羰酰氧苯基)-10,15,20-三苯基卟啉的合成及光电性质的研究

在卟啉的苯环上接上4～30个碳的长链,则其光电化学性能增强,并成为性能良好的充电导膜材料及照相感光材料。为此,本文合成了5-(p-十六烷氧基苯基)-10,15,20-三苯基卟啉(Ⅱ)和5-(p-十六羰酰氧苯基)-10,15,20-三苯基卟啉(Ⅲ),合成路线如下:     

Nucleophilic substitution of hydrogen in meso-nitroaryl-substituted porphyrins—unprotected at the NH-centers in the core ring

Unprotected 5-(4-nitrophenyl)-10,15,20-triphenylporphyrin and 5,10-bis(4-nitrophenyl)-15,20-diphenylporphyrin react in the presence of a base at low temperature with carbanions (which bear a leaving group X at the carbanionic center) affording vicarious nucleophilic substitution of hydrogen (VNS) products in good yields (50-89%). The reactivity is explained in terms of the predominance of the porphyrin N-anion resonance forms at this temperature.     

新型不对称卟啉配体及其锌配合物的合成与荧光性能

以3,5-二羟基苯甲酸丙酯和5-(4-硝基)苯基-10,15,20-三苯基卟啉为起始原料,合成了新型的不对称卟啉配体——5-[4-(3,5-二-十六烷氧基苯甲酰亚胺基)苯基]-10,15,20-三苯基卟啉(1)及其锌配合物(2),其结构经UV-Vis,1H NMR,IR和元素分析表征。用荧光激发光谱研究了1和2的荧光性能,结果表明:在激发波长为420 nm时,1和2的荧光发射峰分别在650 nm,709 nm和600 nm,644 nm。     

Novel routes to 1,2,3,4-tetrahydropyrrolo[1,2-a]pyrazines and 5,6,9,10,11,11a-hexahydro-8H-pyrido[1,2-a]pyrrolo[2,1-c]pyrazines

Condensation reactions of benzotriazole and 2-(pyrrol-1-yl)-1-ethylamine (1) with formaldehyde and glutaric dialdehyde, respectively, afforded intermediates 2 and 6. Subsequent nucleophilic substitutions of the benzotriazole group in 2 and 6 with Grignard reagents, sodium cyanide, and sodium borohydride gave 1,2,3,4-tetrahydropyrrolo[1,2-a]pyrazines 3a-e, 4, 5 and 5,6,9,10,11,11a-hexahydro-8H-pyrido[1,2-a]pyrrolo[2,1-c]pyrazines 7a-c, 8, 9, respectively, in good yields.     

Titrations in non-aqueous media: potentiometric investigation of symmetrical and unsymmetrical tetra-aryl porphyrins with 4-nitrophenyl and 4-aminophenyl substituents in nitrobenzene solvent

The basicity of the symmetrical and unsymmetrical tetraphenylporphyrins, namely 5,10,15,20-tetraphenylporphyrin (I) (references), 5-(4-nitrophenyl)-10,15,20-triphenylporphyrin (II), a mixture of 5,10-bis(4-nitrophenyl)-15,20-diphenylporphyrin and 5,15-bis(4-nitrophenyl)-10,20-diphenylporphyrin (III), 5,10,15-tris(4-nitrophenyl)-20-phenylporphyrin (IV), 5,10,15,20-tetrakis(4-nitrophenyl)porphyrin (V), 5-(4-aminophenyl)-10,15,20-triphenylporphyrin (VI), a mixture of 5,10-bis(4-aminophenyl)-15,20-diphenylporphyrin and 5,15-bis(4-aminophenyl)-10,20-diphenylporphyrin (VII), 5,10,15-tris(4-aminophenyl)-20-phenylporphyrin (VIII) and 5,10,15,20-tetrakis(4-aminophenyl)porphyrin (IX), was investigated potentiometrically in nitrobenzene solvent. This investigation showed that these compounds are basic rather than acidic. Although they can not be titrated even with tetrabuthylammonium hydroxide, they can easily be titrated with perchloric acid to give well shaped and stoichiometric end-points. In addition they all undergo two proton reactions per porphyrin molecule. However, compounds VI, VII, VIII and IX each shows a second end-point to give three, four, five and six proton reactions, respectively, per porphyrin molecule. Half neutralization potentials (measures of their basicity) of these compounds are: I=368, II=409, III=432, IV=461, V=520, VI=340, VII=302, VIII=238 and IX=225 mV versus Ag/AgCl in methanol. These potentials clearly indicate that, if para-hydrogen with respect to the porphyrin core of tetraphenylporphyrin (I) is replaced with an acidifying nitro group (II, III, IV and V) the basicity of I decreases. This decrease is approximately proportional to the number of nitro groups. Each nitro group decreases the half neutralization potential by about 35 mV. On the other hand, if para-hydrogen indicated above is replaced with a basifying amino group (VI, VII, VIII and IX) the basicity increases. This increase is also approximately proportional to the number of amino groups. Each amino group increases the half neutralization potential by about 36.7 mV. The values 35 and 36.7 mV indicate that in nitrobenzene solvent the electron releasing power of an amino group to the porphyrin system is a little stronger than the electron withdrawing power of a nitro group from the porphyrin system. All these observations reveal that the nitrogen atoms at the core of the porphyrin molecules are strongly influenced by changes at the periphery of the molecules, which is a very good indication that the substituted phenyl groups and the cores of the porphyrins are nearly in the same plane.     

肽核酸骨架分子键联卟啉的合成及结构表征

以5,10,15-三苯基-20-(4-羧基苯基)卟啉和5,10,15-三苯基-20-(4-羟基苯基)卟啉为原料, 分别与N-(Boc-氨乙基)甘氨酸乙酯(3)及其衍生物4作用, 得到了两种肽核酸骨架分子键联卟啉化合物6和8. 中间体和目标化合物均由紫外-可见光谱、红外光谱、核磁共振光谱、质谱及元素分析所确证. 目标化合物的荧光光谱测试结果表明, 肽核酸单元分子的链接对卟啉分子的荧光波长和强度影响不大.     

几种取代胡椒醛缩合不对称卟啉化合物的合成及结构表征

利用微波加热法, 以6-硝基胡椒醛、两种R取代苯甲醛(R＝H, Cl)、吡咯为原料, 在丙酸中缩合, 合成了两种新的不对称卟啉化合物5-(2-硝基-4,5-亚甲二氧基)苯基-10,15,20-三苯基卟啉(2)和5-(2-硝基-4,5-亚甲二氧基)苯基-10,15, 20-三对氯苯基卟啉(3). 将2和3还原得到了化合物5-(2-氨基-4,5-亚甲二氧基)苯基-10,15,20-三苯基卟啉(4)和5-(2-氨 基-4,5-亚甲二氧基)苯基-10,15,20-三对氯苯基卟啉(5). 新化合物结构分别经UV-Vis, IR, ¹H NMR及元素分析所证实. 荧光测试表明, 几个化合物都有比较好的荧光强度, 且氨基取代化合物的荧光强度比相应的硝基化合物的大.     

Competitive nucleophilic substitution reactions of methylsulfonyl and nitro derivatives of polychloropyridines

2,6-Di(methylsulfonyl)-3,4,5-trichloropyridine (II) and 4-nitro-2,6-di(methyl-sulfonyl)-3, 5-dichloropyridine (IX) were synthesized, and their reactions with nucleophilic reagents were studied. It was found that the methylsulfonyl groups are replaced on reaction with alkali and sodium alkoxides; on reaction with amines, the chlorine atoms are replaced in the case of II and the nitro group is replaced in the case of IX. The nitro and methylsulfonyl groups are simultaneously replaced in the reaction of excess sodium methoxide with IX.Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 6, pp. 802–806, June, 1975.     

酰胺基卟啉的制备,光谱及电化学性质研究

合成了未见文献报道的5-(4-异烟酸酰亚胺基)苯基-10,15,20-三苯基卟啉配体(H2P)及其锌配合物(ZnP),并通过紫外-可见光谱、红外光谱、核磁共振氢谱、元素分析等测试方法对化合物的结构加以确认.研究表明,配体和配合物的拉曼光谱有很大区别,卟啉配体的循环伏安曲线与氨基卟啉和锌配合物不同,卟啉环的氧化还原峰位都有移动.差热研究表明,卟啉配体410oC开始分解,显示了很高的热稳定性.     

Synthesis of some multi-β-substituted cationic porphyrins and studies on their interaction with DNA

A series of multi-β-substituted cationic porphyrins, 2,3,12,13-tetraphenyl-5-(N-trimethyl-4-ammoniumphenyl)-10,15,20-triphenylporphyrin 2; 2,3,12,13-tetramethyl-5-(N-trimethyl-4-ammoniumphenyl)-10,15,20-triphenylporphyrin 3; 2,3,7,8,12,13,17,18-octaphenyl-5-(N-trimethyl-4-ammoniumphenyl)-10,15,20-triphenylporphyrin 4, and 2,3,7,8,12,13,17,18-octaphenyl-5,10-di(N-trimethyl-4-ammoniumphenyl)-15,20-diphenylporphyrin 5, have been synthesized. Their photooxidative abilities and interaction with DNA were investigated by UV, fluorescence, CD, and gel electrophoresis. It is found that substituents at β-position of the porphyrins have significant effect on interactions and binding mode of the porphyrins with DNA. Increasing positive charges in the porphyrins strengthen their interactions with DNA.     

不对称酰胺基卟啉及其锌配合物的合成,表征及光谱研究

以CH2Cl2为溶剂,通过5-(4-氨基)苯基-10,15,20-三苯基卟啉(MATPP)与异烟酸直接反应得到一种不对称酰胺基卟啉配体(H2P),并合成了其锌配合物(ZnP),利用紫外-可见光谱、红外光谱、核磁共振氢谱、元素分析等测试方法对化合物的结构加以确认.同时,结合光谱法初步研究了卟啉的自聚合性质.研究表明,紫外-可见光谱显示了卟啉的J-聚合特征,荧光量子产率由于自聚合而降低.     

Iodine-catalyzed one-pot synthesis of unsymmetrical meso-substituted porphyrins

The wide range use of 5-(4-nitrophenyl)-10,15,20-triphenylporphyrin is well established, but its synthesis requires two steps and is not very practical. This article describes an iodine-catalyzed one-pot synthesis of this unsymmetrical porphyrin that uses commercial reagents and reactants as such, without prior distillation. Unsymmetrical mono functionalized porphyrins with various functional groups have also been obtained to validate this method. The influence of electronic effects of functional groups (donor or acceptor) has also been studied.     

4-氟-1,2-二氢-3,6-哒嗪二酮及其衍生物的合成

本文报导了4-氟-1,2-二氢-3,6-哒嗪二酮(Ⅱ)及其衍生物3,6-二氯-4-氟哒嗪(Ⅲ)、3-甲氧基-4-氟-6-氯哒嗪(Ⅳ)、3-邻甲苯氧基-4-氟-6-氯哒嗪(Ⅵ)、1-苯基-3-羟基-4-氟-6-哒嗪酮(Ⅶ)等五种新化合物的合成,探讨了(Ⅲ)同亲核试剂的反应性能和部分化合物的药理实验结果.     

meso-三嗪取代苯基卟啉的简单一锅合成

报道一种以羟基卟啉与三嗪和其它亲核试剂为原料一锅法高产率合成不对称多取代三嗪卟啉化合物的简单方法. 研究了2,4,6-三氯三嗪与羟基卟啉、醇和胺通过分级亲核取代反应合成不对称2,4,6-取代三嗪卟啉的方法和反应条件. 以2,4,6- 三氯三嗪和5-(4-羟基)苯基-10,15,20-三苯基卟啉反应生成卟啉单取代二氯三嗪, 然后进一步与醇或胺反应合成了7个三嗪卟啉新化合物, 产物经元素分析, MS, 1H NMR和UV-Vis进行结构表征.     

Nucleophile-mediated ring expansion of 4-chloromethyl- and 4-mesyloxymethyl-5-tosyl-1,2,3,4-tetrahydropyrimidin-2-ones to 6-tosyl-2,3,4,5-tetrahydro-1H-1,3-diazepin-2-ones: effect of the leaving group and the substituent at C6

A five-step synthesis of 4-chloromethyl- and 4-mesyloxymethyl-5-tosyl-1,2,3,4-tetrahydropyrimidin-2-ones has been developed. The reaction of N-[(2-benzoyloxy-1-tosyl)ethyl]urea with sodium enolates of α-tosylketones followed by cyclization-dehydration, and debenzoylation gave 4-hydroxymethyl-5-tosyl-1,2,3,4-tetrahydropyrimidin-2-ones, which were transformed into the 4-chloromethyl- or 4-mesyloxymethyl-derivatives. Treatment of the latter with nucleophilic reagents, such as sodium cyanide, sodium diethyl malonate, sodium thiophenolate, or potassium phthalimide, afforded the corresponding 4,7-disubstituted 6-tosyl-2,3,4,5-tetrahydro-1H-1,3-diazepin-2-ones as a result of ring expansion. The effect of the leaving group and the substitution at the position C6 on the reactivity of the pyrimidines is discussed.