新型2-芳氨基嘧啶衍生物的合成

通过间羟基苯硼酸与2,4-二氯嘧啶的Suzuki反应及其后酚羟基的烷基化得到4-芳基-2-氯嘧啶衍生物. 然后, 采用Pd(PPh3)4/dppf催化剂, 在温和的条件下实现了4-芳基-2-氯嘧啶类化合物和芳香胺的偶联. 合成了3个结构新颖的2-芳氨基嘧啶类化合物. 中间体及产物的结构均经由IR, 1H NMR, 13C NMR, MS和元素分析表征而予以证实.     

生物合理设计光系统Ⅱ抑制剂研究(Ⅴ)——取代苯甲酰胺基丙烯酸乙酯和新型嘧啶酮类化合物的合成及其Hill反应抑制活性

基于Dl蛋白结构模型,设计并合成了取代苯甲酰胺基丙烯酸乙酯及有关成环化合物嘧啶酮,通过X射线衍射确定了2-芳基-5-乙氧甲酰基-6-甲硫基-4-嘧啶酮的结构.生物活性测定结果表明,部分化合物显示出一定的Hill反应抑制活性.     

生物合理设计光系统Ⅱ抑制剂研究(Ⅴ)──取代苯甲酰胺基丙烯酸乙酯和新型嘧啶酮类化合物的合成及其Hil反应抑制活性

基于Dl蛋白结构模型,设计并合成了取代苯甲酰胺基丙烯酸乙酯及有关成环化合物嘧啶酮,通过X射线衍射确定了2-芳基-5-乙氧甲酰基-6-甲硫基-4-嘧啶酮的结构.生物活性测定结果表明,部分化合物显示出一定的Hill反应抑制活性.     

嘧啶的研究:氯和硫醇嘧啶类的作用:4-甲基-5-正丙基-6-氨基-2-氧嘧啶的合成

1. 2-乙硫基-4-甲基-5-正丙基-6-氯代嘧啶在甲醇溶液与甲醇钠相互作用,和在乙醇溶液与乙醇钠互相作用,分别得到相应的嘧啶-甲醚及嘧啶-乙醚。2. 氯对2-乙硫基-4-甲基-5-正丙基-6-氯代嘧啶,2-乙硫基-4-甲基-5-正丙基-6-甲氧基嘧啶及2-乙硫基-4-甲基-5-正丙基-6-乙氧基嘧啶起作用,得到相应的嘧啶砜,用氯在水溶液中氧化硫醇嘧啶化合物(Ⅰ),此反应是特殊的,对嘧啶环中的双键没有影响,祇有硫醇基团氧化而得到相应的稳定的嘧啶砜(Ⅱ)。3. 将醇氨与2-乙磺醯基-4-甲基-5-正丙基-6-氯代嘧啶作用时,对于2-位上的磺醯基不起反应,取代于6-位的氯被置换为氨基而得到2-乙磺醯基-4-甲基-5-正丙基-6-氨基嘧啶。4. 硷对2-乙磺醯基-4-甲基-5-正丙基-6-乙氧基嘧啶及2-乙磺醯基-4-甲基-5-正丙基-6-甲氧基嘧啶作用,分别得到2-氧代-4-甲基-5-正丙基-6-乙氧基嘧啶及2-氧代-4-甲基-5一正丙基-6-甲氧基嘧啶,因此,嘧啶砜中在2-位的磺醯基与硷反应时被置换为羟基,而取代于6-位的乙氧基和甲氧基则不起反应。5. 叙述了一种合成2-氧代-4-甲基-5-正丙基-6-氨基嘧啶(或1,2-二氢化-2-酮-4-氨基-5-正丙基-6-甲基嘧啶)的新方法。     

N-(4,6-二甲氧基嘧啶-2-基)-N'-磷酰基脲类衍生物的合成及生物活性

利用二氯代磷酰基异氰酸酯与4,6-二甲氧基-2-氨基嘧啶的加成反应合成了中间体N-(4,6-二甲氧基嘧啶-2-基)-N'-二氯代磷酰基脲(Ⅰ).Ⅰ与2倍的醇或胺反应得到对称双取代磷酰基脲类化合物Ⅱa_Ⅱi;Ⅰ与1倍的胺反应得到氯代磷酰基脲类化合物Ⅲa_Ⅲe,再与1倍的醇反应则得到不对称双取代磷酰基脲类化合物Ⅳa_Ⅳg.生物活性测定结果表明,化合物Ⅱ、Ⅲ和Ⅳ均显示一定除草活性.     

微波辐射促进选择性合成4,6-二芳基-3,4-二氢嘧啶-2(1H)-酮和嘧啶-2(1H)-酮

探讨了在微波加热条件下,芳香醛、取代苯乙酮和尿素的三组分反应在N,N-二甲基甲酰胺(DMF)中制得4,6-二芳基-3,4-二氢嘧啶-2(1H)-酮类化合物,收率为68%～84%.若在反应体系中加入三甲基氯硅烷,该三组分反应则高产率(66%～87%)地生成相应的脱氢产物4,6-二芳基嘧啶-2(1H)-酮类化合物.该反应具有反应条件温和、产物收率高、操作方便等优点,为4,6-二芳基-嘧啶-2(1H)-酮类药物中间体的合成提供了一条全新的路线.     

2-苯甲酰基嘧啶类化合物的合成与生物活性

2-嘧啶氧基-N-芳基苄胺类化合物结构经过两次骨架结构优化后得到2-苯甲酰基嘧啶类化合物二次先导结构.在二次先导结构基础上,共设计并合成了36个化合物,所有化合物结构经1H NMR、13C NMR、HRMS确认,并进行了室内杀菌活性筛选,对各部位取代基进行了逐次优化.结果表明2-苯甲酰基嘧啶类化合物中R1取代基以2位卤素或烷基取代的苯环或杂环活性最好;中间苯环6位引入氟原子活性保持;嘧啶环4,6位甲氧基取代活性较好,5位甲基取代活性大大降低;羰基被还原为羟基后活性消失.其中2,3-二氯-N-[2-(4,6-二甲氧基嘧啶-2-甲酰基)苯氧基]-N-甲基苯甲酰胺(4AHl)、2,5-二氯-N-[2-(4,6-二甲氧基嘧啶-2-甲酰基)苯氧基]-N-甲基苯甲酰胺(4AHn)及N-[2-(4,6-二甲氧基嘧啶-2-甲酰基)-3-氟苯氧基]-N,2-二甲基苯甲酰胺(4AFd)对黄瓜白粉病的杀菌活性与对照样苯菌酮相当.     

嘧啶的研究:氯和硫醇代嘧啶类的作用,4-甲基-5-乙基-6-氨基-2-氧嘧啶的合成

(1)2-乙硫醇基-4-甲基-5-乙基-6-氯代嘧啶和醇钠在醇溶液中反应,则生成它相应的乙硫醇-嘧啶-醚类。(2)2-乙硫醇-嘧啶类有下列结构:式中 X 为卤素或烷氧基。它很容易和氯互相作用,形成嘧啶一砜。(3)当2-乙磺醯-嘧啶类和醇钠及碱作用时,则嘧啶中的乙磺酰基在所有的情况下都相似于一个易于被烷氧基和羟基所置换的卤原子。然而氨和氯-乙磺酰-嘧啶反应时,则氯原子为氨基取代,而乙磺酰基仍然是不作用的。(4)叙述了两种新的合成4-甲基-5-乙基-6-氨基-2-氧-嘧啶的方法。     

嘧啶的研究:氯对硫醇嘧啶的作用2-酮-4-氨基-5,6-二甲基-1,2-二氢-嘧啶的合成

1.甲醇鈉對於2-乙硫醇基-4,5-二甲基-6-氯代嘧啶在甲醇溶液中生成相應的乙硫醇基嘧啶甲醚。 2.氯對於2-乙硫醇基-4,5-二甲基嘧啶衍生物(I),在水溶液中的作用是特殊的,嘧啶中的不飽和現象不被氯化反應改變而硫醇基團被氧化,形成穩定相應嘧啶碸的衍生物(II),因此製備了2-乙磺醯基-4,5-二甲基-6-甲氧基嘧啶和2-乙磺醯基-4,5-二甲基-6-氯代嘧啶. 3.2-乙硫醇-4,5-二甲基-6-甲氧基嘧啶在甲醇中進行氯化反應,現象甚複雜,並且嘧啶碸的產量很低,2-乙硫醇-4,5-二甲基-6-甲氧基嘧啶在甲醇中被氯氧化,首先形成嘧啶碸,後者並不穩定,再與氯作用形成乙磺醯氯和2-氯代-4,5-二甲基-6-甲氧基嘧啶。 4.嘧啶碸與鹼作用,乙磺醯基被羥基取代,同時在嘧啶環6位上的乙氧基保留,因此2-乙磺醯基-6-甲氧基-4,5-二甲基嘧啶與鹼作用,形成2-酮-5,6-二甲基-4-甲氧基-1,2-二氫嘧啶。 5.酒精-氨的溶液作用在氯代乙磺醯基嘧啶得到氨基-乙磺醯基嘧啶,在氯代乙磺醯基嘧啶中,嘧啶環上2位的乙磺醯基仍保留,而6位土的氯被氨基取代。 6.本文敘述了合成4,5-二甲基-2-氧代-6-氨基嘧啶(或2-酮-4-氨基-5,6-二甲基-1,2-二氫化嘧啶)的新方法。     

氘代AZD9291的合成

吲哚和2,4-二氯嘧啶经偶联反应制得3-(2-氯嘧啶-4-基)-1H-吲哚(1); 1与CD₃I 经取代反应制得3-(2-氯嘧啶-4-基)-1-(甲基-d₃)-吲哚(2); 2经两步亲核取代反应制得N′-(2-二甲基氨基乙基)-2-甲氧基-N′-甲基-N-{［4-(1-(甲基-d₃)吲哚-3-基)］嘧啶-2-基}-5-硝基苯-1,4-二胺(4); 4经还原反应后,与氯丙酰氯发生缩合反应合成了氘代AZD9291,总收率8.5%,其结构经¹H NMR, ¹³C NMR和ESI-MS表征。     

Synthesis of imidazo[1,5-c]pyrimidine derivatives

Two complementary procedures, each starting from 6-aminomethyluracil ( 2 ), have been used to prepare imidazo[1,5-c]pyrimidines with a variety of substituents at positions 3, 5, 6, and 7. The starting material, 2 , can be readily prepared from commercially available 6-chloromethyluracil by reaction with anhydrous ammonia. In the first procedure, 2 is acylated and then cyclodehydrated by reaction with phosphorus oxychloride to give a separable mixture of a 3-substituted 5,7-dichloroimidazo[1,5-c]pyrimidine and a 3-substituted 7-chloroimidazo[1,5-c]pyrimidin-5(6H)-one. The relative product distribution is subject to some control by the choice of the acyl substituent on the starting uracil. The resulting dichloro compounds were derivatized by reaction at the 5-position with various nucleophiles, although the 7-chloro substituent is unreactive. An alternative synthetic method proceeds from 2 in six efficient steps (protection as the phthalimide, chlorination, nucleophilic substitution, deprotection, acylation, and cyclodehydration) to 3-substituted-5,7-bis(methylthio)imidazo[1,5-c]pyrimidines. These compounds may also be derivatized by nucleophilic substitution at the 5-position.     

Pyrrolopyrimidine nucleosides. XIII. Synthesis and chemical reactivity of certain selenopyrrolo[2,3-d]pyrimidine nucleosides

5-Cyano-7-(β-D-ribofuranosyl)pyrrolo[2,3-d]pyrimidin-4-selone ( 1 ) has been prepared via a reaction of the appropriate 4-chloro compound with sodium hydrogen selenide. Alkylation of 2 under basic conditions has provided certain 4-substitutedseleno-5-cyano-7-(β-D-ribofuranosyl)-pyrrolo[2,3-d]pyrimidines. 5-Cyano-4-methylseleno-7-(β-D-ribofuranosyl)pyrrolo[2,3-d]pyrimidine was allowed to react with hydroxylamine and hydrazine. The products obtained and reaction course were compared to those obtained from identical reactions using the corresponding sulfur analog.     

Azolopyrimidines and pyrimidoquinazolines from 4-chloropyrimidines

5-Cyano-3,4-dihydro-6-phenyl-2-substitutedpyrimidin-4-ones 1a-c reacted with phosphorus oxychloride to give the corresponding 4-chloropyrimidine derivatives IIa-c . Compounds IIa-c reacted with aniline and hydrazine to yield the 4-anilino, IIIa,e , and 4-hydrazino, IIIb-d derivatives. The 4-hydrazino analogues IIIb,c could be converted into the triazolo[4,3-c] and tetrazolo[4,5-c]pyrimidines IV and V by the action of carbon disulphide and nitrous acid, respectively. The reaction of IIb,c with phenylhydrazine afforded directly the 5-amino-4,6-diphenyl-6H-2-substitutedpyrazolo[3,4-d]pyrimidines VIa,b . The 4-chloro derivative IIa reacted with antrhanilic acid to form the 5-cyano-2,4-diphenyl-6-(o-carboxyphenylamino)pyrimidine VIII , which could be cyclised into the 4-cyano-1,3-diphenyl-10H-pyrimido[6,1-b]quinazolin-10-one IX by heating with acetic anhydride.     

Exceptional stereoselectivity in the synthesis of 1,3,4-trisubstituted 4-carboxy beta-lactam derivatives from amino acids

[reaction: see text] The base-promoted cyclization of optically pure N-(p-methoxybenzyl)-N-(2-chloro)propionyl amino acid derivatives resulted in a diastereo- and enantioselective approach to valuable 1,3,4,4-tetrasubstituted beta-lactams. The stereochemical outcome of the reaction is exclusively governed by the configuration of the N-(2-chloro)propionyl moiety.     

Substitutions nucleophiles d'amines sur les halogeno-1 cycloalcenes en presence de bases dans le tetrahydrofuranne

Condensations of amines with 1-chloro cycloheptene in the presence of complex base (NaNH₂-t-BuONa) lead to mixtures of enamines and 1,2-cycloheptadiene dimer. Under the same conditions, 2-chloro and 3-chloro bicyclo [3.2.1] oct-2 enes yield only enamines via bicyclo [3.2.1] oct-2 yne. The mechanism of these reactions depends not only upon the halogeno derivatives but also upon “reaction media.” The general problem of the interpretation of elimination-addition reactions is discussed.     

Novel Aspects of the Reaction of 3-(Benzimidazol-2-yl)-2-iminocoumarins with Aromatic Aldehydes

The reaction of 3-(benzimidazol-2-yl)-2-iminocoumarins with aromatic aldehydes has been studied. The condensation products 7-aryl-7H-benzo[4,5]imidazo[1,2-c]benzopyrano[3,2-e]pyrimidines or 3-(benzimidazol-2-yl)coumarins are formed depending on the nature of the substituent in the starting 2-iminocoumarin and aldehyde. In DMF medium, 7-aryl-7H-benzo[4,5]imidazo[1,2-c]benzopyrano[3,2-e]pyrimidines isomerize to the corresponding 7-aryl-14H-benzo[4,5]imidazo[1,2-c]benzopyrano[3,2-e]pyrimidines. The effect of the substituent on the isomerization process has been studied and the reaction mechanisms are discussed.     

Palladium-catalyzed ortho-selective C–H bond chlorination of aromatic ketones

A palladium-catalyzed ortho-selective C–H bond chlorination reaction for the preparation of 2-chloro aromatic ketones was described. Both electron-withdrawing and electron-donating groups on the aromatic rings are well tolerated under the optimized conditions. The 2-chloro aromatic ketones obtained by our method could be applied to synthesize the derivatives of 1H-indazole or benzo[d]isoxazole.     

Studies on phenothiazines. Part 11. Synthesis and spectral studies of substituted 1-chloro/methyl/nitrophenothiazines

Synthesis of the title compounds by the Smiles rearrangement has been reported. 1-Nitrophenothiazines have been prepared by the reaction of 2-amino-3-chloro/methyl/methoxythiophenol with substituted o-halonitrobenzenes in ethanolic sodium hydroxide, in which Smiles rearrangement occurs in situ. 1-chloro/methyl-7-substituted phenothiazines have been prepared by Smiles rearrangement of 3-chloro/methyl-2-formamido-2′-nitro-4′-substituted diphenyl sulphides. The latter were prepared by the formylation of the diphenyl sulphides obtained by the condensation of 2-amino-3-chloro/methylthiophenols with substituted o-halogenonitrobenzenes in ethanolic sodium acetate. Spectral studies are also included.     

Selective reductive cleavage of 2-(phenylthio)pyrimidines for efficient synthesis of 2-(H)pyrimidines

A reaction method is described for selective reductive cleavage of 2-(phenylthio)pyrimidines using Pd(OAc)₂ and Et₃SiH to produce 2-(H)pyrimidines. The reaction proceeds efficiently with a wide range of 2-(phenylthio)pyrimidines. Considering the ready availability of 2-(arylthio)pyrimidines derived from oxidative CS cross coupling of 3,4-dihydropyrimidin-1H-2-thiones (DHPMs), this method unambiguously provides a shortcut to the preparation of 2-(H)pyrimidines with unprecedented diversity.     

Solvent-free synthesis of dibenzo[b,j][1,10]phenanthroline derivatives using Eaton’s reagent as catalyst

A new class of dibenzo[b,j][1,10]phenanthrolines has been prepared. The synthon acridones were achieved in very good yield by a one-pot reaction of 2-amino-5-chloro or 2′-chloro/flouro-substituted benzophenones with 1,2-cyclohexanedione in the presence of freshly prepared Eaton’s reagent (phosphorus pentoxide–methanesulfonic acid) without solvent, through Friedländer synthesis. Then these intermediates were reacted with 2-amino-3,5-dibromobenzaldehyde to afford 1,3-dibromo-10-chloro-8-aryl-6,7-dihydrodibenzo[b,j][1,10]phenanthroline. Also an one-pot reaction between 2?mol of 2-amino-5-chloro aryl benzophenones with 1?mol of 1,2-cyclohexanedione to get 3,10-dichloro-5,8-diaryl-6,7-dihydrodibenzo[b,j][1,10]phenanthroline has also been reported. The newly synthesized structures of the compounds were deduced by spectroscopic techniques.