海绵Spongia sp.中一个新的D环为吡啶环的降海绵烷型二萜（英文）

在对一种Spongia属海绵的化学成分研究中,分离得到一个新的降海绵烷型二萜dinorspongiapyridine(1)和四个已知化合物2～5.通过核磁共振波谱、单晶X-ray衍射以及对比文献的方法,确定了这些化合物的结构及其绝对构型.化合物1是首次发现的D环为吡啶环的3,4-裂环-3,19-双降海绵烷型二萜类化合物,并对其细胞毒活性进行了测试.此外,对化合物1的生物合成途径也进行了探讨.     

中国南海海绵Seletta tenuis Lindgren中24-亚甲基-27-甲基胆甾醇的结构鉴定

自七十年代以来,已从海绵中发现了许多结构独特的、具有强烈生理活性的新化合物,有些已发展成为特效的药物。我们在研究中国南海海绵生物活性成分的过程中,从南海海绵Seletta teuuis Lindgren中分离出24-亚甲基-27-甲基胆甾醇(1)。虽然这个化合物已由De Luca等于1972年从海绵(Aplysina aerophoba)中发现了它。次     

南海海绵Biemna fortis化学成份的研究(一)

从中国南海海绵Biemnafortis的乙酸乙酯可溶部分中分离得到化合物 2 4 -甲基胆甾 - 7 2 2E -二烯 - 3β,5α -二羟基 - 6-酮 ,其结构由IR、MS、1 HNMR等分析手段得以确定     

南中国海星骨海绵Stelletta sp.中的三萜化合物

最近,我们又从采自广西涠洲岛海域的星骨海绵Stelletta sp.中分离得到3个黄色三萜色素1,2和3(见下式).通过IR,UV,MS和1D NMR,2D NMR等方法测定了它们的结构,并对化合物1的所有C和H进行了指认.同时,通过X射线单晶衍射分析测定了化合物1的立体化学结构.初步的药理实验表明,这3个化合物对P388肿瘤细胞均有很强的抑制活性,ED₅₀值依次为0.01,0.5和1.0μg/mL,提示Stelletta属海绵中的这类三萜具有很好的药用开发前景.     

沐浴海绵Spongia zimocca aubspecles irregularia(Lendenfeld)中的含氮化合物

从沐浴海绵Spongia zimocca aubspecles irregularia(Lendenfeld)分离和处理得到3种含氮化合物,通过波谱法鉴定化学结构,化合物1为新的神经酰胺N-2-(1,3-二羟基-十五烷基)-2′,20′-二十一酰胺,2为神经酰胺(E)-N-2-(1,3-二羟基-4-十八烯基)-十六酰胺,3为醋酸胍.     

海绵Phacelliafusca中含氮化合物的分离与结构鉴定

从采自中国南海西沙群岛海域的海绵Phacellia fusca Schmidt中得到4个含氮 化合物。经~1H NMR,~(13)C NMR,HMQC,HMBC,~1H-~1HCOSY,FABMS和EIMS等光谱分析 ，确证其结构分别为：N,N'-二[2-乙氧基-1（Z）-乙烯基]脲（1），2- Bromoaldisin(2),Aldisin(3)Dibromophakellin盐酸盐(4)。其中化合物1为一具有 对称结构的新脲类化合物，命名Phacelliaurea A；化合物4是首次从该海绵中分离 得到的已知胍基生物碱，首次报到了它的~(13)C NMR数据及其归属。     

海绵Phacellia fusca Schmidt中一个结构新颖的脑甙类化合物

从采自中国南海西沙群岛海域的海绵Phacellia fusca Schmidt中得到了一种结构新颖的脑甙类化合物 Phacelliacerebroside A.经¹HNMR、¹³CNMR, HMQC、¹H-¹HCOSY、NOE、FABMS和GC-MS 等光谱分析,确证其结构为长链碱(LCB)含3个自由羟基的α-葡萄糖苷神经酰胺,命名为 Phacelliacerebroside A.这是Phakellia sp.海绵中首次报道的脑甙类化合物.     

南海海绵Pseudoceratina purpurea活性成分的研究(Ⅰ)

从中国南海海绵Pseudoceratina purpurea的乙酸乙酯萃取部分提纯 出两个化合物,应用IR,1H-NMR,MS等波谱技术确定它们为正十六酸和 3-β-5-烯-谷甾醇。     

海绵Polymastia Sobustia的化学成份研究

首次报道从中国南海海绵Polymastiasobustia中分离得到5个纯化合物,经过MS,IR,1^HNMR,13^CNMR(DEPT),HMQC和HMBC等波谱技术鉴定为：豆甾-5-烯-7-羰基-3β-甾醇(1),N-(1-羟甲基-2,6-二羟基)十七烷基-5-羟基二十四脂肪酰胺(2),胸腺嘧啶(3),尿嘧啶(4),对羟基苯甲酸(5);其中化合物1和化合物2为新化合物。     

南海黄蜂海绵中系列长链甲基酮成分分析

从中国南海海绵Spheciospongia Vagabunda乙酸乙酯萃取部分中分离出一组混合物,应用^13HNMR,^13CNMR,H-HCOSY和GC／MS等光谱分析技术对它们的结构进行了分析,主要为一些长链甲基酮化合物。共鉴定出二十四碳烯-2-酮异构体、二十四碳二烯-2-酮和二十四碳烯-2-酮等14种化合物,其中4种化合物的双键位置有待于进一步确定。     

Cordycedipeptide A, a new cyclodipeptide from the culture liquid of Cordyceps sinensis (Berk.) Sacc

A new cyclodipeptide named as cordycedipeptide A, a new natural compound and two known compound were isolated from the culture liquid of Cordyceps sinensis (BERK.) SACC. Their structures were elucidated as 3-acetamino-6-isobutyl-2,5-dioxopiperazine (1), 3-isopropyl-6-isobutyl-2,5-dioxopiperazine (2) and 3,6-di(4-hydroxy)benzyl-2,5-dioxopiperazine (3) by 1D and 2D-NMR techniques. The cytotoxic assay showed compound 1 had the cytotoxic activities to L-929, A375, and Hela.     

Synthesis, Crystal Structure and DNA Binding Studies of α,α'-Bis(3,5-bismethyl-1-pyrozolyl)- carbene-acetyl-isopropenyl Hydrazine

The title compound α,α'-bis(3,5-bismethyl-pyrozole-N-yl)-carbene-acetyl-isopro-penyl hydrazine (C16H22N6O, Mr = 314.40) has been prepared. It was characterized by elemental analysis as well as IR, MS, 1H-NMR and 13C-NMR spectra. Its crystal structure was determined by single-crystal X-ray diffraction, getting the following data: triclinic, space group P1 with a = 6.9734(16), b = 10.773(3), c = 12.001(3) A, α = 75.311(4), β = 82.695(4), γ = 77.143(4)°, Z = 2, V = 847.9(3) A3, Dc : 1.231 g/cm3, F(000) = 336 and μ(MoKα) = 0.082 mm-1 (λ = 0.71073 A). The results of crystal structure determination show that there exist intermolecular and intramolecular hydrogen bonds, resulting in a two-dimensional supramolecular framework of the title compound. The binding of the title compound to DNA was investigated by absorption, emission, and viscosity measurements. The title compound shows absorption hyperchromicity accompanied by a blue shift at about 254 nm. The binding constant Kb for the title compound has been determined to be 1.89 × 104 M-1 from absorption measurements. The addition of the title compound to DNA pretreated with EB causes appreciable reduction in the emission intensity, indicating that the DNA-bound EB fluorophore is partially replaced by the title compound. The value of K is 3.093 × 104 M-1. The relative viscosity of DNA decreased with the addition of the title compound. Results suggest that the title compound binds to DNA with a non-classical intercalative or groove interaction mode. The observed efficient nuclease activity of the title compound is interesting and may have further influences on the chemistry of DNA minor groove binders.     

WYE‐120318, a ring contraction product of methylnaltrexone,and structure revision of coniothyrione

A contracted ring degradation product, WYE‐120318 (compound 2), was discovered during the development phase for methylnaltrexone bromide (compound 1) drug substance. The compound was isolated by high‐performance liquid chromatography fractionation, and its structure was determined by spectroscopic data analyses. WYE‐120318 is formed from methylnaltrexone through a benzyl‐benzilic acid type rearrangement reaction to yield an α‐hydroxy‐cyclopentanecarboxylic acid substructure. The proposed structure and the formation mechanism are confirmed by the synthesis of WYE‐120318 from methylnaltrexone (compound 1). A similar benzyl‐benzilic acid type rearrangement reaction can be envisioned as the biological origin of remisporine A (compound 3), a naturally occurring cyclopentadienyl compound that autocatalytically dimerizes to remisporine B (compound 4). The structure of remisporine A was deduced from its dimer 4. Coniothyione (compound 5) can be considered as the first example of a stable natural product bearing the remisporine A skeleton. However, the regiochemistry of the chlorosubstitution in the coniothyrione structure needs to be revised to compound 6 on the basis of the nuclear magnetic resonance data and biogenesis analysis. Copyright © 2012 John Wiley & Sons, Ltd.     

New cadmium thio- and selenocyanato coordination compounds: structural snapshots on the reaction pathway to more condensed anionic networks

In this contribution several new coordination compounds on the basis of cadmium(II) thio- and selenocyanate with pyrimidine as co-ligand were prepared and investigated for their structural, thermal and spectroscopic properties. The reaction of cadmium(II) thiocyanate with pyrimidine leads to the formation of four compounds, which from a structural point of view are closely related. In the most pyrimidine-rich 1 : 2 compound [Cd(NCS)(2)(pyrimidine)(2)](n) (1A) (1 : 2 = ratio between metal salt and the co-ligand pyrimidine) the Cd cations are linked by the pyrimidine ligands into layers and are additionally coordinated by two terminal N-bonded anions. In the 2 : 3 compound {[Cd(NCS)(2)](2)(pyrimidine)(3)}(n) (1B) the Cd cations are linked into chains by μ-1,3 bridging thiocyanato anions, which are connected into layers by only half of the pyrimidine ligands, whereas the other co-ligands are only terminal coordinated. Further reduction of the pyrimidine content leads to the formation of the 1 : 1 2D compound [Cd(NCS)(2)(pyrimidine)](n) (1CI) in which the terminal N-bonded thiocyanato anions become bridging. Surprisingly, crystallization experiments lead to the formation of an additional pyrimidine-deficient intermediate of composition {[Cd(NCS)(2)](3)(pyrimidine)(2)}(n) (1D), in which some of the μ-1,3 coordinated anions transform into μ-1,1,3 bridging thiocyanato anions. Consequently the four structures can be used as snapshots of intermediates on the way to a more condensed thiocyanato coordination network. In contrast, with cadmium selenocyanate only two different compounds were obtained. The 1 : 2 compound [Cd(NCSe)(2)(pyrimidine)(2)](n) (2A) is not isotypic to 1A and shows a completely different coordination topology whereas the pyrimidine-deficient 1 : 1 compound (2B) shows a more condensed network with μ-1,3 coordinating selenocyanato anions. On heating, the 1 : 2 compound 1A decomposes into Cd(NCS)(2)via a new polymorphic modification (1CII) as intermediate which is metastable, whereas the 1 : 2 selenocyanato compound 2A transforms into the 1 : 1 compound 2B on heating which cannot be obtained phase pure under these conditions. If faster heating rates are used, there are indications for the formation of a 3 : 2 compound, which is amorphous to X-rays. The results are compared with those obtained for related thio- and selenocyanato coordination polymers with pyridine, pyridazine and pyrazine as co-ligand. Moreover, their impact on the structures and thermal reactivity of analogous paramagnetic compounds is discussed in detail. Based on the structural data of compound 1D the unknown structures of two intermediates were determined, which are formed in the thermal decomposition reaction of the Mn and Fe thiocyanato pyrimidine coordination polymers, reported recently.     

Structure elucidation of a novel analog of sildenafil detected as an adulterant in a dietary supplement using LC-UV and LC/MS

A sildenafil-related compound was detected in a dietary supplement marketed as an aphrodisiac. The compound was detected during analysis of the dietary supplement using LC-UV and LC/electrospray ionization-MS. The structure of the compound was established using high resolution MS, NMR spectrometry, and X-ray crystal structure analysis. The compound was identified as 5-(5-((3,5-dimethylpiperazin-1-yl)sulfonyl)-2-ethoxyphenyl)-l-methyl-7-((1-methyl-4-nitro-1H-imidazol-5-yl)thio)-3-propyl-1H-pyrazolo[4,3-d] pyrimidine. Based on this structure, the compound was named nitroprodenafil. The dietary supplement was found to contain 90 mg nitroprodenafil/capsule. This article describes the structural characterization of a new sildenafil-related compound. The compound was detected during analysis of a dietary supplement using LC-UV and LC/electrospray ionization (ESI)-MS. The structure was established using high resolution MS (HRMS), NMR spectrometry, and X-ray crystal structure analysis. The structures of methisosildenafil, thiomethisosildenafil, and this new analog, named nitroprodenafil (21), are shown in Figure 1. In the Demizu et al. report, the compound is named mutaprodenafil instead ofnitroprodenafil. Considering the naming right, the authors of this paper think the use of mutaprodenafil is appropriate as the compound name, although nitroprodenafil is used.     

Synthesis, structural characterization, and Monte Carlo simulation of the magnetic properties of two new alternating MnII azide 2-D honeycombs. Study of the ferromagnetic ordered phase below 20 K

Reaction of MnII and pyridine derivatives such as 4-methylpyridine (4-Mepy) and 4-ethylpyridine (4-Etpy) led to the new two-dimensional systems trans-[Mn(4-Mepy)2(N3)2]n (1) and trans-[Mn(4-Etpy)2(N3)2]n (2). Compound 1 crystallizes in the triclinic system, P1 group (a = 9.269(2) A, b = 9.635(3) A, c = 18.860(4) A, Z = 4), and compound 2 crystallizes in the monoclinic system, P2(1)/c group (a = 14.416(3) A, b = 8.515(2) A, c = 15.728(4) A, Z = 4). The two compounds show honeycomb structures based on dinuclear Mn-(mu-N3)2-Mn subunits linked to the four nearest-neighbor similar subunits by four end-to-end single azido bridges, but whereas the subunits of compound 1 show the end-to-end Mn-(mu 1,3-N3)2-Mn kind of bridges, compound 2 prefers the end-on Mn-(mu 1,1-N3)2-Mn fragment. Magnetically, compound 1 is an alternating 2-D system with two different antiferromagnetic interactions, whereas compound 2 corresponds to a two-dimensional ferro-antiferromagnetic system showing spin canting and permanent magnetization below 20 K. The coupling constant parameters J1 = -10.1 cm-1, J2 = -4.7 cm-1, and g = 2.019 for 1 and J1 = -5.3 cm-1, J2 = 2.9 cm-1, and g = 2.016 for 2 have been obtained from calculations using the Monte Carlo method based on the Metropolis algorithm.     

A new labdane diterpene from the flowers of Solidago canadensis

A new labdane diterpene, 9alpha,16xi-dihydroxy-6-oxo-7,13-labdadien-15,16-olide (solicanolide, 1) and six known compounds identified as quercetin (2), 3-O-caffeoylquinic acid (3, neochlorogenic acid), 5-O-caffeoylquinic acid (4, chlorogenic acid), 4,5-di-O-caffeoylquinic acid (5), 3,5-di-O-caffeoylquinic acid (6) and 3,4-di-O-caffeoylquinic acid (7) were isolated from the flowers of Solidago canadensis. To our knowledge, compound 7 was isolated for the first time in S. canadensis. This work describes the isolation of compounds 1-7 and the structure elucidation of a new compound identified as compound 1. Solicanolide (1) showed cytotoxic activity against A549 (IC(50): 13+/-2 microM), DLD-1 (IC(50): 26+/-2 microM) and WS1 (IC(50): 17+/-1 microM) cell lines.     

四(5-氟尿嘧啶-1-基乙酰氧基苯基）卟啉及其锌配合物的合成

以二环己基碳二亚胺为脱水剂,meso-四(对羟基苯基)卟啉与5-氟尿嘧啶-1-基乙酸反应,合成了一种新型meso-四[4-(5-氟尿嘧啶-1-基乙酰氧基)苯基]卟啉化合物(A),产率12.7%;将其与乙酸锌反应得到其锌配合物(B),产率30.8%。 通过1H NMR、IR、MS、UV-Vis及元素分析确证了卟啉化合物A及其锌配合物B的结构。     

1-methyl-2-undecyl-4(1H)-quinolone as an irreversible and selective inhibitor of type B monoamine oxidase

The inhibitory compound of monoamine oxidase (MAO) activity was isolated from the CH(2)Cl(2) fraction of the fructus of Evodia rutaecarpa and identified as 1-methyl-2-undecyl-4(1H)-quinolone (1). Compound 1 showed a selective inhibition of type B MAO (MAO-B) activity with the IC(50) value of 15.3 microM using a substrate kynuramine, but did not inhibit type A MAO (MAO-A) activity. The kinetic analysis using Lineweaver-Burk plots indicated that compound 1 competitively inhibited MAO-B activity with the K(i) value of 9.91 microM. The inhibition of MAO-B by compound 1 was found to be irreversible by dialysis of the incubation mixture. These results suggest that compound 1 is a potent irreversible inhibitor of MAO-B, and may regulate catecholamine content in the neurons.     

Structure Comparison of Benzothiazepine Derivatives

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