反-1,2-双[2-(5-取代苯基恶唑基)]环丙烷的合成与光性能的研究

合成了8个反 -1,2-双[2-(5-取代苯基恶唑基)]环丙烷和2个1,2-双[2-取代苯基恶唑基)]乙烷,其中9个为新化合物.讨论了化合物的结构与其电子光谱及荧光量子产率间的关系.发现恶唑环与三元环间存在一定程度的共轭,并解释了上述化合物荧光量子产率较低的现象.     

5-苯基-2-(2'-苯基啉基-5')1,3,4-二唑及其5-对位取代苯基衍生物的研究

合成了十三个未见报道的5-苯基-2-(2'-苯基唑基-5')1,3,4-二唑及其5-对位取代苯基衍生物. 测试了它们的紫外光谱、荧光光谱、荧光量子产率和激光转换效率, 发现化合物的γmax^u^v和νmax^u^v与Hammett取代基常数|σρ^+|有线性关系, 化合物分子受激发后结构的平面性增加.     

5-取代苯胺基-6-苯基-1, 2, 4-三嗪-3-硫酮的合成

苯甲酰基-N-取代苯基硫代甲酰胺和氨基硫脲反应, 首先在酸性介质中形成缩氨基硫脲, 然后在碱性介质(pH=8~9)中环化, 生成5-取代苯胺基-6-苯基-1, 2, 4-三嗪-3-硫酮。本文合成10个新的该类杂环化合物。     

2-氰基-3-取代丙烯酸(2-乙氧基乙基)酯的合成及除草活性

设计并合成了11个2-氰基-3-取代苯胺基-3-甲硫基丙烯酸(2-乙氧基乙基)酯(2)和11个2-氰基-3-取代苯基脲基丙烯酸(2-乙氧基乙基)酯(5)两类光合作用光系统Ⅱ(PSⅡ)电子传递抑制剂,目标化合物的结构均经1H NMR,13C NMR和质谱分析确证,生物活性测试结果表明:部分化合物2对双子叶杂草表现出良好的选择性和除草活性,化合物5苯环上间位有取代基时有一定的除草活性.     

2-[4-取代苯基-2-氧-3-酰氨基-1-吖丁啶基]-2-苯基乙酸类化合物的合成

用叠氮钠和D-苯基甘氨酸为原料合成了2-[4-取代苯基-2-氧-3-酰氨基-1-吖啶基]-2-苯基乙酸类化合物. 在叠氮乙酰氯和亚胺化合物在三乙胺存在下在-78℃时进行环缩合反应, 可导致立体专一性合成顺-甲基-2-(4-取代苯基-2-酮-3-叠氮-1-吖啶基)-2-苯基乙酸, 催化氢化或硫化氢可减少叠氮基和得到氨基β-内酰胺后者被酰化生成α-酰氨基-β-内酰胺, 在温和碱性条件下选择性地氢化酯基既不会影响β-内酰胺环, 又不全影响酰胺侧链. 合成了二十个标题化合物, 其中九个被表明对β-内酰胺酶有抑制活性.     

1-取代-4,5-二(4-氯苯基)咪唑的合成和结构表征

合成了6种1-取代-4,5-二(4-氯苯基)咪唑.以对氯苯乙酸和氯苯为原料,经Friedel-Crafts酰基化反应、二氧化锡氧化、与多聚甲醛和乙酸铵环合制备了中间体4,5-二(4-氯苯基)咪唑(5),5再经取代得到3个1-取代-4,5-二-(4-氯苯基)咪唑类化合物6a-c.6a再分别与液体胺经亲核取代反应得到3个1-取代乙酰胺类-4,5-二-(4-氯苯基)咪唑类化合物7a-c.目标化合物结构用核磁共振氢谱和红外光谱进行了表征.     

酰氨基硫脲及有关的杂环衍生物的研究 I:1-氰乙酰基-4-芳基氨基硫脲及有关的杂环衍生物的合成

合成了九个1-氰乙酰基-4-芳基氨基硫脲类化合物和四个3-氰甲基-4-芳基-1,2,4-三唑啉与硫酮类化合物和四个2-苯基氨基-5-取代-1,3-噻二唑类化合物.并初步研究了这些化合物的抗结核菌活性和植物生长促进作用.     

5-苯基-2-(2’-苯基(口恶)唑基-5’)1,3,4-(口恶)二唑及其5-对位取代苯基衍生物的研究

合成了十二个未见报道的5-苯基-2-(2’-苯基(口恶)唑基-5’)1,3,4-(口恶)二唑及其5-对位取代苯基衍生物。测试了它们的紫外光谱、荧光光谱、荧光量于产率和激光转换效率,发现化合物的(?)和(?)与 Hammett 取代基常数|σ_p~+|有线性关系,化合物分子受激发后结构的平面性增加。     

1-对甲苯基-5-取代苯基亚胺基-1,2,3-三唑甲酸/甲酰胺的合成及生物活性研究

以对甲基苯胺为原料,经过重氮化反应生成对甲基叠氮苯(1).在强碱性条件下,1分别与氰基乙酸乙酯、氰基乙酰胺反应,制得中间体1-对甲苯基-5-氨基-1,2,3-三唑甲酸乙酯(2)和1-对甲苯基-5-氨基-1,2,3-三唑甲酰胺(5);中间体2经水解生成1-对甲苯基-5-氨基-1,2,3-三唑甲酸(3),进而在弱酸性条件下与取代苯甲醛反应得到6个未见文献报道的目标化合物1-对甲苯基-5-取代苯基亚胺基-1,2,3-三唑甲酸(4a～4f),5与取代苯甲醛反应得到6个未见文献报道的目标化合物1-对甲苯基-5-取代苯基亚胺基-1,2,3-三唑甲酰胺(6a～6f),化合物的结构均经IR,1H NMR,13C NMR确证.初步生物测试表明,12个化合物均表现出良好的抑菌活性,其中化合物4d～4f和6d～6f对金黄色葡萄球菌、白色念球菌的最小抑菌浓度(MIC)值为2～8μg/mL,抗菌效果优于氟康唑和三氯生.     

3-取代胺甲基-5-连三唑基-1, 3, 4-恶二唑-2-硫酮的合成

2-苯基-1,2,3-三唑-4-甲酰肼(1)在CS~2/KOH作用下环化得到5-(2-苯基-1,2,3-连三唑-4-基)-1,3,4-恶二唑-2-硫酮(2),2经Mannich反应合成得到标题化合物3-(取代胺甲基-5-(2-苯基-1,2,3-连三唑-4-基)-1,3,4-恶二唑-2-硫酮(3)。     

Sulfoxide stretching mode as a structural reporter via dual-frequency two-dimensional infrared spectroscopy

The S=O stretching mode in sulfoxides, having a frequency in the 950-1150?cm(-1) range, is tested as a structural label via dual-frequency two-dimensional infrared (2DIR) spectroscopy. The properties of this structural reporter are studied in several compounds, including (4,4(')-dimethyl-2,2(')-bipyridyl)(o-methylsulfinylbenzoate) ruthenium II, [Ru(dmb)(2)(BzSO)](+), (RuBzSO), octylsulfinylpropionic acid (OSPA), and o- and p-methylsulfinyl-benzoic acid (oMSBA and pMSBA). The mode assignment in the fingerprint region for these compounds is made using a combination of density functional theory calculations and 2DIR and relaxation-assisted 2DIR (RA 2DIR) spectroscopies. The SO stretching mode frequency and IR intensity demonstrate substantial sensitivity to the molecular structure. Multiple cross peaks of the C=O and S=O stretching modes with modes in the fingerprint region (930-1450?cm(-1)) were recorded. The 2DIR and RA 2DIR spectra focusing at interactions of a high-frequency mode of a ligand with the modes in the fingerprint region provide a spectral fingerprint of a compound and help mode assignment in the often congested fingerprint region. The cross-peak amplitudes in oMSBA, pMSBA, and OSPA were compared with the theoretical predictions based on the computed values for the off-diagonal anharmonicities and a reasonable match is found. The SO stretching mode provides means for assigning other modes in the fingerprint region and constitutes a promising structural reporter for the 2DIR and RA 2DIR spectroscopy measurements.     

金属硫氰酸根配合物FeHg(SCN)~4, MnHg(SCN)~4的合成、晶体结 构与非线性光 学性质的研究

合成了配合物晶体FeHg(SCN)~4和MnHg(SCN)~4。用单晶X射线衍射方法测定了这两个晶体的结构。以尿素为标准样品用粉末晶体倍频1064nm的Nd:YAG激光,测得其倍频光强度分别为:FeHg(SCN)~4,0.6倍于尿素;MnHg(SCN)~4,50倍于尿素,后者显示了作为新的非线性光学材料的发展前景。     

Ballistic energy transport along PEG chains: distance dependence of the transport efficiency

Dual-frequency relaxation-assisted two-dimensional infrared (RA 2DIR) spectroscopy was used to investigate energy transport in polyethylene glycol (PEG) oligomers of different length, having 0, 4, 8, and 12 repeating units and end-labeled with azido and succinimide ester moieties (azPEGn). The energy transport initiated by excitation of the N≡N stretching mode of the azido group in azPEGn in CCl(4) at ca. 2100 cm(-1) was recorded by probing the C=O stretching modes (reporters) of the succinimide ester moiety. Sensitive to the excess energy delivered to the reporter modes, RA 2DIR permits observation of both the through-bond and through-solvent energy transport contributions. The cross-peak data involving the reporter modes with different thermal sensitivity and the data for mixtures of compounds permitted concluding that through-bond energy transport is the dominant mechanism for most cross peaks in all four azPEGn compounds. The through-bond energy transport time, evaluated as the waiting time at which the cross peak maximum is reached, was found to be linearly dependent on the chain length of up to 60 ?, suggesting a ballistic energy transport regime. The through-bond energy transport speed determined from the chain-length dependence of T(max) in CCl(4) is found to be ca. 450 m s(-1). The cross-peak amplitude at the maximum decays exponentially with the chain length; a characteristic decay distance is found to be 15.7 ± 1 ?. The cross-peak amplitude at zero waiting time, determined by the end-to-end distance distribution, is found to decay with the chain length (L) as ～L(-1.4), which is close to predictions of the free flight chain model. The match indicates that the end-group interaction does not strongly perturb the end-to-end distribution, which is close to the ideal random coil distribution with the Gaussian probability density.     

释放显影抑制剂型成色剂在彩色影像形成过程中的动力学研究 Ⅱ.DIR和DIAR成色剂对染料影像形成的主反应的影响

继前文测定了成染料成色剂、DIR和DIAR成色剂与QDI的偶合反应的速率常数的基础上,本文进一步研究了DIR和DIAR成色剂对染料影像形成的主反应的作用.研究结果表明其作用(1)DIR或DIAR参与与成染料成色剂竞争QDI的反应,从而控制了QDI在显影银周围的扩散距离,同时也影响了染料的形成速率;(2)DIR和DIAR成色剂在与QDI反应后所释放的显影抑制剂抑制了卤化银的显影进程,从而控制了QDI的形成速率.两种作用的结果都使染料云的尺寸减小.本文还比较了体系中加入等摩尔(mol)量的带有相同抑制基团的DIR或DIAR成色剂的情况下,它们对主反应的影响,结果表明无论是对QDI的竞争作用或对显影的抑制作用,其作用大小都取决于它们与QDI反应的表现速率常数K值.     

基于结构设计合成新型喹啉类分泌型PLA2抑制剂

磷脂酶A2(PLA2)在很多人类疾病的病理研究中起重要作用,是药物化学研究所的热点之一。因此,发展新型的PLA2抑制剂对生物有机研究和临床应用均有重要意义。我们设计合成分泌型PLA2的非底物类似物以寻找新型PLA2抑制剂。本文基于结构设计并合成了喹啉－4－乙酰胺作为PLA2抑制剂,目标化合物结构经1^HNMR,IR,MS和元素分析确认,初步活性检测显示该类化合物具有较好体外活性及动物活性。     

New N1-(4-aryloxybenzyl)uracils containing N3-positioned 4-(trimethyleneoxy)benzoic acid moiety,and study of their antiviral activity against SARS-CoV-2 and influenza virus

New title uracil derivatives, 4-{3-[2,6-dioxo-3-(4-aryl-oxybenzyl)-3,6-dihydropyrimidin-1(2H)-yl]propoxy}benzoic acids and their butoxy homologues, were obtained in three steps using 2,4-bis(trimethylsilyloxy)pyrimidine, 4-aryloxy-benzyl bromides and methyl 4-(ω-bromoalkoxy)benzoates as the key reactants. The compounds were studied as inhibitors of H1N1 influenza virus and SARS-CoV-2 R replication in MDCK and Vero E6 cell cultures, respectively, which revealed that the tested compounds had high levels of anti-SARS-CoV-2 activity.     

α- and β-Glucosidase inhibitors: chemical structure and biological activity

Glycoside trimming enzymes are crucially important in a broad range of metabolic pathways, including glycoprotein and glycolipid processing and carbohydrate digestion in the intestinal tract. Amongst the large array of enzymes, glucosidases are postulated to be a powerful therapeutic target since they catalyze the cleavage of glycosidic bonds releasing glucose from the non-reducing end of an oligo- or polysaccharide chain involved in glycoprotein biosynthesis. Glucosidase inhibitors are currently of interest owing to their promising therapeutic potential in the treatment of disorders such as diabetes, human immunodeficiency virus (HIV) infection, metastatic cancer, and lysosomal storage diseases. Glucosidase inhibitors have also been useful in probing biochemical pathways and understanding structure-activity relationship patterns required for mimicking the enzyme transition state. Amongst the various types of glucosidase inhibitors, disaccharides, iminosugars, carbasugars, thiosugars, and non-sugar derivatives have received great attention. This review is aimed at highlighting the main chemical classes of glucosidase inhibitors, as well as their biological activities toward α- and β-glucosidases, but it is not intended to be an exhaustive review on the subject. Inhibition data on the compounds covered in this review are included in a tabular form as an Appendix, where the type of each glucosidase associated with a specific inhibitor is also given.     

2-芳胺基-5-[5'-氨基-1'-(4''-氯苯基)-1', 2', 3'-三唑-4'-基]——-1, 3, 4-恶二唑的合成

利用1-[5'-氨基-1'-(4'-氯苯基)-1', 2', 3'-三唑-4'-甲酰基]-4-芳基氨基硫脲在汞盐Hg(OAc)2-HOAc中加热缩合, 制得11种新的2-芳胺基-5-[5'-氨基-1'-(4'-氯苯基)-1', 2', 3'-三唑-4'-基]---1, 3, 4-恶二唑。所有化合物的结构经元素分析, IR、MS以及1H NMR确认。选择代表物作生测试验, 结果表明, 2b, 2k中MIC3.1mg/L时, 对大肠杆菌及金黄色葡萄球菌繁殖有明显抑制。     

Tyrosol 1,2,3-triazole analogues as new acetylcholinesterase (AChE) inhibitors

The present work proposed the preparation of triazolic analogues of tyrosol, a biophenol found in olive oil and whose wide range of bioactivities has been the target of many studies. We obtained fifteen novel tyrosol derivatives and the compounds of the series were later evaluated as acetylcholinesterase (AChE) inhibitors. The study of AChE inhibition is important for the development of new drugs and pesticides, and especially the research for managing Alzheimer's disease. The most active compound, namely 7-({1-[2-(4-hydroxyphenyl)ethyl]-1H-1,2,3-triazol-4-yl}methoxy)-4-methyl-2H-chromen-2-one (30), showed IC₅₀ value of 14.66 ± 2.29 μmol L⁻¹. Docking experiments corroborated by kinetic assay are suggestive of a competitive inhibition mechanism. Derivatives interacted with amino acids from the AChE active site associated to the development of Alzheimer's disease. The results indicate that the compounds synthesized have a high potential as prototypes for the development of new acetylcholinesterase inhibitors.