5-(取代吡唑基-4-次甲基)(硫代)巴比妥酸的合成

以冰乙酸为催化剂,将取代吡唑甲醛和巴比妥酸或硫代巴比妥酸在无水乙醇中进行Knoevenagel缩合反应,合成了6个5-（取代吡唑基-4-次甲基）（硫代）巴比妥酸。标题化合物经IR、1^HNMR、元素分析确证结构。     

5-（吲哚基-3-次甲基）（硫代）巴比妥酸的合成

以冰乙酸为催化剂,吲哚-3-甲醛与巴比妥酸或硫代巴比妥酸在无水乙醇中进行Knoevenagel缩合,合成了5-(吲哚基-3-次甲基)巴比妥酸或5-(吲哚基-3-次甲基)(硫代)巴比妥酸,其结构经1H NMR和IR表征.     

巴比妥酸-NO_2~--铁(Ⅱ)-CPB显色体系光度测定巴比妥酸的研究

本文对巴比妥酸－ＮＯ－２－铁（Ⅱ）－ＣＰＢ显色体系进行了研究,建立了一种测定巴比妥酸的分光光度法,该法巴比妥酸含量在１．０×１０－６～２．０×１０－５ｇ／ｍＬ范围内符合比尔定律。方法简便、快速且具有良好的选择性及重现性,用于巴比妥类药物合成样中巴比妥酸的测定,回收率在９０．２％～１０２．１％     

巴比妥酸—NO2^—2铁（Ⅱ）—CPB显色体系光度测定巴比妥酸的研究

本文对巴比妥酸－ＮＯ＾－２－铁（Ⅱ）－ＣＰＢ显色体系进行了研究,建立了一种测定巴比妥酸的分光光度法,该法巴比妥酸含量在１．０＊１０＾－６－２．０＊１０＾－５ｇ／ｍＬ范围内符合比尔定律。     

钌（Ⅱ）－联吡啶－巴比妥酸－Ce（Ⅳ）化学发光体系测定巴比妥酸的研究

利用巴比妥酸对Ｃｅ（Ⅳ）氧化钌（Ⅱ）－联吡啶化学发光反应的增强作用，建立了痕量巴比妥酸的自动脉冲注射化学发光测定法方法的检出限为１０×１０－９ｇ／ｍＬ，线性范围为５０×１０－８－６．２×１０－５ｇ／ｍＬ巴比妥酸的衍生物如巴比妥、苯巴比妥和戊巴比妥对Ｃｅ（Ⅳ）氧化钌（Ⅱ）联吡啶化学发光反应无增强作用据此对合成样中巴比妥酸作选择性检测探讨了巴比妥酸的增强机理     

巴比妥酸在药物合成上的应用

本文综述了巴比妥酸在药物合成上的应用与进展。通过巴比妥酸的烃化、卤化、环化、缩合、光解、螯合等反应得到的一些衍生物具有重要的生理活性，可用作镇静剂、麻醉剂、安眠药、抗肿瘤药、抗菌素等。参考文献２６篇。     

室温离子液体促进的5-亚芳基巴比妥酸衍生物的合成

在室温离子液体1-丁基-3-甲基咪唑四氟硼酸盐([bmim]BF₄)存在下, 采用室温研磨和微波辐射的方法, 由芳香醛和巴比妥酸或硫代巴比妥酸经Knoevenagel缩合反应, 制备了相应的5-亚芳基巴比妥酸或5-亚芳烃基硫代巴比妥酸衍生物. 在室温研磨条件下反应2 h, 产率为78%～96%, 在微波辐射功率为160 W时反应20 s, 产率为82%～98%, 产物结构经¹H NMR确证.     

研磨法制备5－芳叉巴比妥酸

将巴比妥酸、芳香醛与无水ZnCl2于研钵中，室温研磨5min后放置，得到缩合 产物5－芳叉巴比妥酸，收率90％－97％。该法反应条件温和、操作简便、收率高。     

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.     

巴比妥酸与芳香醛的固相反应研究

固相有机化学反应作为绿色化学的重要组成部分是近年来发展起来的新领域 [1,2 ] .固相有机化学反应中 ,反应物分子受晶格的控制 ,运动状态受到很大限制 ,因此表现出比溶液更高的反应效率及反应选择性[3～ 6] .巴比妥酸具有生理活性 ,且有较高的化学反应活性 ,尤其是 C5位的氢 ,由于受相邻两个羰基的吸电子作用而具有较强的酸性 ( p H=4.0 0 ) .因此 ,巴比妥酸与芳香醛易发生 Knoevenagel型缩合反应 ,生成 C5取代的衍生物 - 5 -亚烃基巴比妥酸 .这类缩合反应在溶液中很容易发生 [7,8] ,近年来又发现在蒙脱土 KSF存在下 [9] 及无载体条件下…     

Synthesis of cyclic bis- and trismelamine derivatives and their complexation properties with barbiturates

Cyclic bis- and trismelamine derivatives were prepared from cyanuric chloride by stepwise substitutions with appropriate amines. The complexation abilities of these melamine derivatives with barbituric acid derivatives were evaluated by UV-vis spectroscopy and (1)H NMR. The structure was also confirmed by X-ray crystallography. Both the acyclic and the cyclic bismelamine derivatives formed a 1 : 1 complex via six hydrogen bonds with barbituric acid derivatives. van't Hoff analyses on the complexation of the bismelamines with the barbituric acid derivative revealed that the complexation of the cyclic bismelamine was entropically favored and enthalpically less favored process than those of the acyclic bismelamine. X-Ray crystallographic analysis and (1)H NMR studies revealed that the cyclic trismelamine bound one barbituric acid derivative into the cavity via six hydrogen bonds by two melamine moieties and another barbituric acid via three hydrogen bonds by the residual melamine moiety.     

Preparation of 5,5′‐pyrilidene and 5,5′‐quinolidene bis‐barbituric acid derivatives

NMR reaction following experiments were used to find optimal conditions for the barbituric acid double addition to aromatic and heteroaromatic carboxaldehydes. It was established that aromatic aldehydes with electron‐donating substituents such as hydroxy, methoxy, and dimethylamino produce only the single addition barbituric acid adduct (barbituric acid benzylidenes). If these electron‐donating substituents are transformed into electron‐withdrawing substituents by virtue of protonation (NMe₂ to NHMe₂⁺) then the double barbituric acid adduct becomes the sole product of the reaction. This is also true regardless of the reaction media if strong electron‐withdrawing substituents (such as a nitro group) are present. Considering that the reactive species for nitrogen containing aromatic heterocycles are actually the conjugated acids (electron deficient molecule) only the double barbituric acid adducts are isolated. All synthetic procedures presented are applicable to multi‐gram scale preparations of double barbituric acid adducts.     

The influence of solvent molecules on NMR spectrum of barbituric acid in the DMSO solution

This work shows the modification of barbituric acid (BA) chemical shifts by dimethylsulphoxide (DMSO) molecules. The discussed changes are caused by creation of the H-bonded associates formed by barbituric acid with DMSO in solution. Free molecule of barbituric acid, the cluster of BA with two DMSO molecules and two different clusters of BA with four DMSO units are taken into consideration. The chemical shifts of these systems have been calculated and the obtained results have been compared with experimental data. Theoretical calculations predict a significant downfield shift for imino protons of barbituric acid involved in intermolecular-N-H...DMSO hydrogen bonds. The influence of the solvent molecules on other nuclei chemical shifts, especially protons of barbituric acid methylene group, is also reported. The calculations have involved Hartree-Fock and several Density Functional Theory methods. All methods correctly describe experimental ¹H and ¹³C NMR spectra of barbituric acid. The best consistence between experiment and theory is observed for the BLYP functional. Four approximations of magnetic properties calculations embedded in the Gaussian’98 package have been tested. The results of the performed calculations indicate that from a practical point of view the GIAO method should be preferred.     

Transition metal free reductive dimerization of nitrogen containing barbituric acid benzylidenes

Through the NMR monitoring of the reactive intermediates in the condensation of barbituric acid with nitrogen containing heterocyclic 2‐carboxaldehydes, a synthetic procedure was developed for the preparation of each of the intermediates. The simple high yield procedure for the preparation of the reductive dimer from corresponding barbituric acid benzylidenes was developed, although we were not able to elucidate the source of the reduction. The structure of the dimer was confirmed by X‐ray analysis.     

几种具有电子给-受体结构的两亲性化合物的合成及鉴定

设计并合成了3种含有巴比妥酸基团的具有电子给-受体结构的两亲性有机分子,经元素分析、红外光谱、核磁共振谱确定了其结构,研究了醛与巴妥酸缩合的条件及醛的反应活性与其IR、NMR谱的关系.     

Green chemistry multicomponent protocol for formylation and Knoevenagel condensation for synthesis of (Z)-5-arylaminomethylene pyrimidine 2, 4, 6-trione derivatives in water

A green, efficient, and novel one-pot multicomponent protocol was developed to achieve stereoselective (Z)-5-(arylpropenylidine)-2,4,6-pyrimidinetrione derivatives using a three-component reaction involving appropriate aromatic amines, formic acid, and barbituric acid using water as green solvent by conventional thermal heating process. In this way, N-formylation of various amines takes place. The resulted different formamides undergo Knoevenagel condensation with active methylene group containing compound, that is, barbituric acid. The newly synthesized compounds were characterized by spectral analysis (Fourier Transform Infrared [FT-IR], 1H nuclear magnetic resonance [NMR], 13C NMR, Heteronuclear Multiple-Bond Correlation [HMBC], Mass, UV spectroscopy) and elemental analysis. The multicomponent reactions (MCRs) showed good stereoselectivity.     

Azines and Azoles: CXX. Synthesis of Acyclic Analogs of N1-Ribosides of Barbituric Acid and Its 5-ylidene Derivatives

The reaction of 2,4,6-tris(trimethylsiloxy)pyrimidine with 2-oxabutane-1,4-diyl diacetate in methylene chloride in methylene chloride in the presence of SnCl₄ proceeds regioselectively to form 1-[(2-acetoxyethoxy)methyl]barbituric acid. The latter is readily deacetylated to a free acyclic analog of N-ribosides of barbituric acid. 1-[(2-Acetoxy- and 2-hydroxyethoxy)methyl]barbituric acids easily react with aromatic and heterocyclic aldehydes in water and organic solvents, forming 5-ylidenebarbituric acids. The structure of the products was proved by ¹H NMR and UV spectroscopy. Certain of the products exhibit a moderate antimicrobial and antiviral activity.     

Reaction of Barbituric, 2-Thiobarbituric Acids and Their Derivatives with 2-Carboxybenzaldehyde and Opianic Acid: Synthesis and Tautomerism of 5-(3'-Oxo-1',3'-dihydroisobenzofuran-1'-yl)barbituric Acids and Their 2-Thio Analogs

The reaction of barbituric, N-alkylbarbituric acids, and their 2-thio analogs with carboxybenzaldehyde and 2-carboxy-3,4-dimethoxybenzaldehyde leads to the formation of the corresponding 5-(3'-oxo-1',3'-dihydroisobenzofuran-1'-yl)barbituric and 2-thiobarbituric acids, the structures of which were studied by ¹H and ¹³C NMR spectroscopy and mass spectrometry. In DMSO the derivatives of barbituric acid exist in the form of mixtures of the ketone and enol tautomers, while their 2-thio analogs exist in the enol form. In chloroform the tautomeric equilibrium is displaced fully toward the ketone form.