Catechol-O-methyltransferase-Inhibiting Pyrocatechol Derivatives: Synthesis and Structure-Activity Studies

3-Nitro- and 3-cyanopyrocatechols bearing electron-withdrawing substituents at C(5) have been found to inhibit the enzyme catechol-O-methyltransferase. Structure-activity studies are discussed on the basis of the pharmocological data of 50 compounds (cf, Chapt. 4, Tables 1–7). Some 3-nitro-5-aroylpyrocatechols (Type A², Table 1) fulfil the requirements for a clinical candidate, being orally active, specific, reversible, and relatively short-acting. The chemical work involved is illustrated by describing a choice of exemplary syntheses, dealing with compounds 9, 11, 14, 18, 22, 24, 25, 35, 41 , and 42 (Chapt. 5, Schemes 1–10).     

Discodermolide及其衍生物三维定量构效关系的研究

Discodermolide是一种新颖的作用于微管蛋白的抗肿瘤化合物, 具有良好的药用前景. 为了设计出药效更好的类似物, 我们用比较分子力场分析(CoMFA)和比较分子相似性指数分析(CoMSIA)对discodermolide及其衍生物进行了三维定量构效关系(3D-QSAR)的研究, 并建立了相关的预测模型. 其中, CoMFA模型的交叉验证相关系数(q2)为0.592, 非交叉验证相关系数(r2)为0.982, 标准偏差(SEE)为0.094, F值为119.761; CoMSIA模型的q2为0.544, r2为0.980, SEE为0.098, F值为108.715. 计算结果表明, 获得的CoMFA和CoMSIA模型具有良好的预测能力, 可以应用于指导该类化合物的设计.     

Asymmetric Synthesis of Aminophosphonic Acids and Trifluoromethylated Derivatives Thereof

Various approaches leading to chiral aminophosphonic acids were described. Catalytic asymmetric-induced addition of dialkylphosphite to chiral aldimine gives low ee. value. The diastereoselective alkylation of bicyclic phosphonamide derived from anilinomethylpyrrolidine and followed by subsequent reactions provide much better results. 1,3-Proton Schiff reaction was applied successfully for chiral trifluoromethylated f - and/or g -aminophosphonic acids.     

EHMO和模式识别法研究芬太尼衍生物的构效关系

自Hansch等创立QSAR法以来,药物构效关系的研究已获得较大的进展。本文将模式识别法用于芬太尼衍生物构效关系的研究,将该类药物的分子结构看作与生物活性具有对应关系的表现形式——模式,以药物分子结构中有关取代基的多个量子化学参数为数量化的模式向量成分。将已知生物活性的药物作为模式识别训练点,则所得模式识别分类图反映了该类药物的生物活性与其量子化学结构特征参数间的统计学意义的关系。它既可用来探寻高效药物的结构参数,又能预测新设计药物生物活性的等级或类别。     

一种新三维描述子用于Nevirapine类抗艾滋病药物定量构效关系的研究

运用三维全息原子场作用矢量(3D-HoVAIF)对33个Nevirapine类抗艾滋病药物进行了定量构效关系(QSAR)研究。采用偏最小二乘回归(PLSR)建立定量构效关系模型,同时采用内部及外部双重验证的方法对所得模型稳定性能进行深入分析和检验,所建模型的复相关系数(Rcum2)、留一法(LOO)交互校验(CV)复相关系数(Qcum2)和外部样本校验复相关系数(Qext2)分别为0·835、0·530和0·518。结果表明,3D-HoVAIF能较好表征Nevirapine类抗艾滋病药物分子结构信息,且所建模型具有较好稳定性能和预测能力。     

取代芴—9—羧酸酯衍生物的合成

报道了以９，１０－菲醌为起始原料，通过在碱性条件下重排，再经过氯化、酯化及Ｎ杂环取代反应，合成了２０个新的含氮杂环芴－９－羧酸酯类似物，其结构经ＩＲ，＾１Ｈ ＮＭＲ及元素分析所证实。并对其合成方法进行了研究。同时还对合成的新化合物的抗霉菌生物活性进行了简单的测定。     

Quantitative Studies on Structure－Activity Relationships （QSAR） of Cytokinin－Active Phenyl Urea Derivatives（PUD）

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新型含芴基的富勒烯衍生物的合成

以2,7-二溴芴酮为起始原料,经Suzuki偶合、腙化和1,3-偶极环反应合成了3种新型的含芴基的富勒烯衍生物,其结构经UV-Vis,1H NMR,13C NMR,FT-IR和MALDI-TOF-MS表征。     

末端基团对芴类衍生物分子非线性光学性质的影响

通过采用预估矫正的时域有限差分方法数值求解速率方程-光场强度方程,研究了纳秒激光脉冲在具有不同末端基团的对称性芴类衍生物分子2,7-双(4′-(二甲基氨基)苯乙烯基)-9-氢-芴(F1分子)和2,7-双(4′-硝基苯乙烯基)-9-氢-芴(F2分子)中的动力学传播过程以及光限幅效应,分析了两种分子的光限幅特性随传播距离(z)、粒子数密度(N)以及脉冲宽度(τ)的变化情况,并且拟合了两种分子的动态双光子吸收(TPA)截面。计算结果表明,该系列分子具有较大的双光子吸收截面以及较好的光限幅效应。此外,F2分子的末端基团―NO2与F1分子的末端基团―N(CH3)2相比具有更强的得电子能力,因而使得F2分子具有更大的跃迁偶极矩,双光子吸收截面增大,光限幅效应更为明显。     

神经肽FF的构效关系研究

多肽在机体中具有重要的生理功能,并且它具有化学合成和修饰的便利性,因此它吸引了越来越多的化学、生物学及其交叉领域研究人员的研究兴趣。神经肽FF(NPFF)作为阿片调节肽在阿片耐受等药理学方面具有重要的调节作用,然而迄今为止仍缺乏NPFF受体高选择性的激动剂和拮抗剂,从而阻碍了NPFF药理学功能及其作用机制的研究。本文简述了NPFF的发现,并综述了近几年来在NPFF的前体、受体和生理学功能等方面所取得的最新进展,结合本实验室的工作重点介绍了NPFF构效关系方面的研究,并展望了该研究方向今后的发展趋势。     

STAT3环烷烃并噻吩类衍生物抑制剂的三维定量构效关系研究

本文对STAT3抑制剂的化学结构与生物活性之间的关系进行研究。采用三维定量构效关系(3D-QSAR)中的比较分子力场分析(CoMFA)和比较分子相似性指数分析(CoMSIA)方法针对52个STAT3抑制剂建立3D-QSAR模型,阐明了抑制剂化学结构与其生物活性之间的关系。所构建的CoMFA模型交叉验证系数为0.548,非交叉验证系数为0.754,标准偏差为0.278,显著系数为58.297;所构建的CoMSIA模型交叉验证系数为0.892,非交叉验证系数为0.597,标准偏差为0.192,显著系数为57.794。结果显示CoMFA和CoMSIA模型具有良好的稳定性和预测能力。3D-QSAR模型等势图提供的相关场信息对新型STAT3抑制剂的设计具有指导意义。     

Structure-Activity Relationship of NF023 Derivatives Binding to XIAP-BIR1

Inhibitors of Apoptosis Proteins (IAPs) are conserved E3-ligases that ubiquitylate substrates to prevent apoptosis and activate the NF-kB survival pathway, often deregulated in cancer. IAPs-mediated regulation of NF-kB signaling is based on the formation of protein complexes by their type-I BIR domains. The XIAP-BIR1 domain dimerizes to bind two TAB1 monomers, leading to downstream NF-kB activation. Thus, impairment of XIAP-BIR1 dimerization could represent a novel strategy to hamper cell survival in cancer. To this aim, we previously reported NF023 as a potential inhibitor of XIAP-BIR1 dimerization. Here we present a thorough analysis of NF023 binding to XIAP-BIR1 through biochemical, biophysical and structural data. The results obtained indicate that XIAP-BIR1 dimerization interface is involved in NF023 binding, and that NF023 overall symmetry and the chemical features of its central moiety are essential for an efficient interaction with the protein. Such strategy provides original hints for the development of novel BIR1-specific compounds as pro-apoptotic agents.     

芴衍生物的合成、结构与蓝色(λmax=418nm)双光子荧光

分别以二苯胺和咔唑为端基,以芴为共轭桥, 合成了两个对称型芴衍生物:2,7-二-(N,N-二苯胺基)-9,9-二乙基芴[2,7-bis(N,N-diphenylamino)-9,9-diethyl-fluorene,简称DPDEF]和2,7-二咔唑基-9,9-二乙基芴(2,7-dicarbazol-9'-yl-9,9-diethyl-fluorene,简称DCDEF).用四圆X射线衍射方法测定了其晶体结构.DPDEF单晶属于单斜晶系,C2/c空间群.晶胞参数:a=2.8649(4) nm, b=0.85111(9) nm, c=2.7012(4) nm, β=100.982(11)º, V=6.4657(14) nm³, Z=8, D_c=1.144 g·cm^-3, R=0.0581. DCDEF单晶属于单斜晶系,P2₁/c空间群.晶胞参数:a=0.92794(12) nm, b=0.88561(9) nm, c=3.7236(4) nm, β=96.914(9)º, V=3.0378(6) nm³, Z=4, D_c=1.208 g*cm^-3, R=0.0652.晶体中DPDEF和DCDEF的芴桥具有很好的平面性,构成芴桥的两个苯环平面之间的夹角分别仅为3.0º和5.8º.在波长为730 nm的飞秒脉冲激光激发下,化合物DPDEF在THF中发出强的蓝色双光子上转换荧光(λ_max=418 nm),测得双光子吸收截面为15 GM.     

Simple and Efficient Method for Obtaining Fluorene and Spirobifluorene Bromide Derivatives

A mild, simple, and efficient synthetic procedure for the preparation of 2-monobromo-, 2,7-dibromo-, and 2,2′,7,7′-tetrabromo-substituted spirobifluorene derivatives and their key intermediates, 2-monobromo- and 2,7-dibromo-substituted fluorene compounds, has been developed. The oxidative bromination of fluorene and spirobifluorene was achieved using NaBr/H₂O₂ as the bromine source. High conversion of the starting materials was achieved together with good selectivities under optimized reaction conditions.     

Synthesis,Cytotoxicity, and Structure-Activity Relationships of New Oxaliplatin Derivatives

Summary. In order to setup structure-activity relationships and to explore the possibilities of improving the anticancer activity of oxaliplatin, which was recently approved for combination chemotherapy of metastatic colorectal cancer, new oxaliplatin analogues have been synthesized. The cytotoxicity was determined in nine human tumor cell lines and revealed a comparable or even higher cytotoxic potency in leukemia, ovarian and colon cancer cell lines in the case of small substituents at position 4 of the cyclohexane-1,2-diamine ligand. Introduction of bigger substituents at this position and thereby increasing the steric demand of the diamine ligands and the lipophilicity of the oxaliplatin derivatives resulted in platinum complexes with reduced cytotoxic properties.     

新型长共轭结构芴类化合物的合成及其发光性能

通过Heck偶联反应合成了3个新的长共轭结构芴类衍生物(3a～3c),其结构经1H NMR,IR和元素分析表征.测定了3在THF溶液中电子吸收和光致发光性能.结果发现3呈现高的发光强度,D-π-D型化合物比A-π-A型化合物荧光发光强度高,对产生这一光谱行为的主要原因进行了分析.     

斑蝥素衍生物的合成、抗肝癌活性及构效关系研究

斑蝥素衍生物具有结构多样性和良好的抗肝癌活性。本文以呋喃、顺丁烯二酸酐为原料,合成了35个斑蝥素衍生物。以顺铂为阳性对照药,经MTT法测试了所合成化合物对人肝癌HepG2细胞的体外抗肿瘤活性。结果表明,化合物6d、6f、6g、6h、6i的抗肝癌活性与顺铂相当,其中,斑蝥素酰亚胺类化合物具有较好的抗肝癌活性,且当取代基为吸电子基或含氮杂环时化合物显现出较强的抗肝癌活性,该类化合物具有潜在的抗肝癌应用价值。     

Structure-Activity Relationship of Insecticidal Steroids. X. Androstane and Pregnane Derivatives

The androstane and pregnane steroids 1-10 were verified to have insecticidal activity for larvae of the Colorado beetle Leptinotarsa decemlineata. Insect growth and development regulators were found among these compounds.