酸性条件下多苯基取代环戊二烯的氧化扩环反应

报道了空气(或氧气)存在的条件下,由高氯酸引发多苯基取代环戊二烯发生新颖的碳-碳键断裂扩环反应,在此反应中,氧原子插入到环戊二烯环中形成相应的六元环吡喃盐类化合物.分别用红外光谱、核磁共振氢谱、碳谱、质谱以及元素分析对所得化合物进行了表征.     

A Ring-Enlargement Reaction Yielding 1,2,5-Benzothiadiazonin-6-one 1,1-Dioxides

At room temperature or under reflux in MeCN, 3-amino-2H-azirines 2 and 3,4-dihydro-2H-1,2-benzothiazin-3-one 1,1-dioxide ( 4 ) give 1,2,5-benzothiadiazonin-6-one 1,1-dioxides 5 in fair-to-good yield (Scheme 2). The structure of this novel type of heterocyclic compounds has been established by X-ray crystallography of 5a (Fig.). A ring expansion via a zwitterionic intermediate of type A ' is proposed as the reaction mechanism of the formation of 5 .     

Structures and Mutagenic Properties of Products Obtained by C-Nitrosation of Opipramol

Reaction of the tricyclic psychotropic drug opipramol ( 1 ) with an excess of HNO₂ affords a product mixture mutagenic for Salmonella typhimurium. The main product is a tetracyclic furoxan 2 (yield ca. 80%), resulting from nitrosation at C(10) and C(11) of 1 . Compound 2 is not mutagenic. The essential mutagen is a nitroarene 3 formed via contraction of the central ring of 1 , and nitrosation at C(2). Its yield is extremely low (<0.1%). Nitroarenes have previously not been encountered as mutagenic products of the interaction of drugs with nitrite.     

The Crystal and Molecular Structures of Two Acid-Catalysed Rearrangement Products of Taxochinon

The structures of two acid catalysed rearrangement products of taxochinone ( 1 ) have been determined by X-ray analysis. One of the products turned out to be a 20 (10→9) abeo-abietane ( 2 ), the other an optically inactive phenalenone ( 3 ). Crystals of the former compound, C₂₀H₂₆O₃, belong to space group P2₁2₁2₁ with four molecules per cell and the structure was refined with 879 significant reflexions to R = 0.032. Crystals of the latter compound, C₂₀H₂₂O₂, belong to space group P2₁/c with 12 molecules per cell and the structure was refined with 1823 significant reflexions to R = 0.058.     

Reactivity of Organolithium Reagents to 2,3,4,5-Tetraphenylcyclopentadienone and Crystal Structures of Addition Products

The conjugate addition reactions of four organolithium reagents to 2,3,4,5-tetraphenylcyclopentadienone (tetracyclone) were investigated to reveal the reactivity of organolithium reagents to tetracyclone. The results show that 1,2-addition products 2,3,4,5-tetraphenyl-1-(2-thienyl)-2,4-cyclopentadien-1-ol(1), 1-n-butyl-2,3,4,5-tetraphenyl-2,4-cyclopentadien-1-ol(2) and 1,2,3,4,5-pentaphenyl-2,4-cyclopentadien-1-ol(3) were synthesized in excellent yields while tetracyclone reacted with 2-thienyllithium, n-butyllithium and phenyllithium, respectively. Interestingly, three 1,2-, 1,4- and 1,6-addition isomers 1-tert-butyl-2,3,4,5-tetraphenyl-2,4-cyclopentadien-1-ol(4), 4-tert-butyl-2,3,4,5-tetraphenyl-2-cyclopenten-l-one(5) and 2-tert-butyl-2,3,4,5-tetraphenyl-3-cyclopenten-l-one(6), were simultaneously obtained by the conjugate addition reaction of tert-butyllithium with larger steric hindrance to tetracyclone. Compounds 1-6 were characterized by ¹H and ¹³C NMR spectra, Fourier transform infrared(FTIR) spectra and mass spectra(MS). The crystal and molecular structures of compounds 1, 2 and isomers 5, 6 were determined by X-ray single crystal diffraction technique. The results imply that the steric hindrance of tert-butyllithium probably play a key role in controlling the conjugate addition reaction. The conjugate addition mechanism of organolithium reagents to tetracyclone was proposed.     

Ring-Enlargement and Ring-Opening Reactions of 1,2-Thiazetidin-3-one 1,1-Dioxides with Ammonia and Primary Amines as Nucleophiles

The N-benzyl- and N-alkyl-substituted 1,2-thiazetidin-3-one 1,1-dioxides 1b – d reacted readily with NH₃ and primary amines via ring opening. The reaction with NH₃ proceeded at −78°→room temperature yielding ring-opened adducts via nucleophilic attack of NH₃ at the sulfonyl group, whereas the reactions with amines at room temperature yielded products via attack at the carbonyl group. The N-unsubstituted analogue 1a , when reacted with benzylamine in refluxing EtOH, also gave a product of ring opening via nucleophilic attack at the carbonyl group of 1a . The transamidation-like reactions of the 2-(aminoalkyl)-1,2-thiazetidin-3-one 1,1-dioxides 19a – d proceeded via six-, seven-, and eight-membered intermediates, giving the ring-enlarged eight-, nine-, and ten-membered products 21 – 24 (Schemes 8 and 9), respectively, in 42 – 87% yields. The products resulted from the nucleophilic attack of the amino group of the side chain at the carbonyl C-atom. The structure of the eight-membered product 24 with an asymmetrically situated methyl substituent was established by X-ray crystallography.     

人参中达玛烷型皂苷的化学转化产物结构和转化途径研究

利用高效液相色谱-电喷雾-多级串联质谱(HPLC-ESI-MSⁿ)技术分析人参中3种达玛烷型皂苷(三七皂苷R₁,人参皂苷Rd、20(S)-Rg₃)在12-磷钨酸环境中转化的产物结构和转化途径。由原人参三醇型皂苷R₁转化获得9种产物:20(S)-25-OH-R₂、20(R)-25-OH-R₂、25-OH-T₅、20(S)-R₂、20(R)-R₂、20(S)-25-epoxy-R₂、20(R)-25-epoxy-R₂、T₅、3β,12β-二羟基-6α-(2-O-β-D-吡喃木糖基-β-D-吡喃葡糖氧基)达玛烷-20(22),24-二烯。由原人参二醇型皂苷Rd和20(S)-Rg₃转化得到10种产物:20(S)-25-OH-Rg₃、20(R)-25-OH-Rg₃、25-...     

The Structures of Some Products from the Photodegradation of the Pluramycin Antibiotics Hedamycin and Kidamycin

The photolability of the antitumor antibiotic hedamycin ( 1 ) was investigated by irradiation in different solvents in the presence or in the absence of oxygen. The products formed were separated chromatographically and their structures determined by NMR spectroscopy. Photolysis of 1 in the presence of oxygen gave only one isolable product, photohedamycin A ( 3 ), where ring E of hedamycin had been transformed into an enol ether. The reaction in the absence of oxygen yielded the photohedamycins B, C, and D ( 5, 6 , and 7 , respectively). In these compounds, one of the epoxides of hedamycin had been opened reductively, and in photohedamycin D ( 7 ) the substituent at C(8) - originally ring E of hedamycin - was now acyclic. In addition to these compounds, the photolyses yielded a large number of unstable minor products, which could not be isolated.     

Synthesis and Crystal Structures of the Reaction Products of the Magnesium Acenaphthenediimine Complex with Tosyl Azide

Russian Journal of Coordination Chemistry - The reaction of [(Dpp-Bian)Mg(THF)3] (I) (Dpp-Bian is 1,2-bis[(2,6-diisopropylphenyl)imino]acenaphthene) with tosyl azide (TosN3) affords the binuclear...     

Recent Advances in Discovery of Lead Structures from Microbial Natural Products: Genomics- and Metabolomics-Guided Acceleration

Natural products (NPs) are evolutionarily optimized as drug-like molecules and remain the most consistently successful source of drugs and drug leads. They offer major opportunities for finding novel lead structures that are active against a broad spectrum of assay targets, particularly those from secondary metabolites of microbial origin. Due to traditional discovery approaches’ limitations relying on untargeted screening methods, there is a growing trend to employ unconventional secondary metabolomics techniques. Aided by the more in-depth understanding of different biosynthetic pathways and the technological advancement in analytical instrumentation, the development of new methodologies provides an alternative that can accelerate discoveries of new lead-structures of natural origin. This present mini-review briefly discusses selected examples regarding advancements in bioinformatics and genomics (focusing on genome mining and metagenomics approaches), as well as bioanalytics (mass-spectrometry) towards the microbial NPs-based drug discovery and development. The selected recent discoveries from 2015 to 2020 are featured herein.     

Interpretation of Retention Indices in Gas Chromatography for Establishing Structures of Isomeric Products of Alkylarenes Radical Chlorination

By an example of previously uncharacterized products obtained by alkylarenes radical chlorinationwas demonstrated that combination of various interpretation methods applied to the retention indices (RI) inthe gas chromatography on the standard nonpolar phases (comparison of RI of products, initialcompounds, characteristics of succession of the chromatographic elution of the structural isomers with theuse of estimation of molecular dynamic parameters, application of the additive schemes to RI calculation, and using of structural analogy CH₃Cl for testing the results obtained) permitted unambiguous identification of the structure even without data of mass spectrometry.     

Structures of Addition Products of Acetylenedicarboxylic Acid Esters with Various Dinucleophiles. An application of C,H-spin-coupling constants

Heterocyclic compounds obtained by addition of acetylenedicarboxylic acid esters to thioureas, cyclic amidines and o-difunctionalized aromatic systems have been studied by ¹³C-NMR. In particular, C, H-spin-coupling constants over two and three bonds were used to differentiate between the various constitutional isomers and to establish the configuration of trisubstituted exocyclic C, C-double bonds. The configurational significance and diagnostic value of vicinal cis and trans C,H-spin coupling is again demonstrated in the present series.     

Synthesis and Structures of New Oxidation/ Cycloaddition Products of λ3‐Cyclodiphosphazanes

Reaction of the cyclodiphosphazane [(OC₄H₈N)P(μ‐N‐t‐Bu)₂P(HN‐t‐Bu)] ( 1 ) with an equimolar quantity of diisopropyl azodicarboxylate afforded the phosphinimine product [(OC₄H₈N)P(μ‐N‐t‐Bu)₂P=N‐t‐Bu)(N(CO₂ ‐i‐Pr)NHCO₂‐i‐Pr] ( 6 ) having a P^III‐N‐P^V skeleton. Similar products [(t‐BuNH)P(μ‐N‐t‐Bu)₂P=N‐t‐Bu)(N(CO₂Et)NHCO₂Et] ( 7 ) and [(CO₂‐i‐Pr)HNN(CO₂‐i‐Pr)](t‐BuN=P(μ‐N‐t‐Bu)₂POCH₂CMe₂CH₂O[P(μ‐N‐t‐Bu)₂P=N‐t‐Bu)(N(CO₂‐i‐Pr)NH(CO₂‐i‐Pr)] ( 8 ) were spectroscopically characterized in the reaction of [(t‐BuNH)P‐N‐t‐Bu]₂ ( 2 ) and [(t‐BuNH)P(μ‐N‐t‐Bu)₂POCH₂CMe₂CH₂OP(μ‐N‐t‐Bu)₂P(NH‐t‐Bu)] ( 3 ) with diethyl‐ and diisopropyl azodicarboxylate, respectively. By contrast, the reaction of [(μ‐t‐BuN)P]₂[O‐6‐t‐Bu‐4‐Me‐C₆H₂]₂CH₂ ( 4 ) and [(C₅H₁₀N)P‐μ‐N‐t‐Bu]₂ ( 5 ) with diisopropyl azodicarboxylate afforded the mono‐ and bis‐oxidized compounds [(O)P(μ‐N‐t‐Bu)₂P][O‐6‐t‐Bu‐4‐Me‐C₆H₂]₂CH₂ ( 9 ) and [(C₅H₁₀N)(O)P‐μ‐N‐t‐Bu]₂ ( 10 ), respectively. Oxidative addition of o‐chloranil to 7 and its DIAD analogue [(t‐BuNH)P(μ‐N‐t‐Bu)₂P=N‐t‐Bu)(N(CO₂‐i‐Pr)NHCO₂‐i‐Pr] ( 11 ) afforded [(C₆Cl₄‐1, 2‐O₂)(t‐BuNH)P(μ‐N‐t‐Bu)₂P=N‐t‐Bu)(N(CO₂R)NHCO₂R] [R = Et ( 12 ) and i‐Pr ( 13 )] containing tetra‐ and pentacoordinate P^V atoms in the cyclodiphosphazane ring. The structures of 6 , 9 , 12 and 13 have been confirmed by X‐ray structure determination. For comparison, the X‐ray structure of the double cycloaddition product [(C₆Cl₄‐1, 2‐O₂)(t‐BuNH)PN‐t‐Bu]₂ ( 14 ), obtained from the reaction of 2 with two mole equivalents of o‐chloranil is also reported.     

Structures and Anticoagulant Activities of the Partially Mild Acidic Hydrolysis Products of the Fucosylated Chondroitin Sulfate from Sea Cucumber Pearsonothuria graeffei

Fucosylated chondroitin sulfate from Pearsonothuria graeffei (fCS-Pg) is a unique glycosaminoglycan (GAG), which was reported to have potent antithrombotic and anticoagulant activities. In the present study, the native fCS-Pg was hydrolyzed by mild acid to improve its bioavailability. The structures of the acid-released and acid-resistant sulfated fucose branches of fCS-Pg before and after acidic hydrolysis were characterized by nuclear magnetic resonance spectroscopy (NMR) technology. The results showed the acid-released fucose residues included both α- and β-fucose conformation, containing 2,4-di-O-sulfated fucose (Fuc2,4S), 3,4-di-O-sulfated fucose (Fus3,4S), 3-O-sulfated fucose (Fuc3S), and 4-O-sulfated fucose (Fuc4S), with a mole ratio of 6:26:22:46, respectively. Their difference to the native fCS-Pg in the sulfation pattern of the backbone could be due to selective removal of the sulfated groups during the release of the fucose branches by acid. For the acid-resistant part, the sulfation patterns of fucose were similar to the native polysaccharides, but the signal strength of Fuc3,4S was obviously decreased, whereas Fuc2,4S was kept unchanged, indicating Fuc3,4S is more liable to acid. The anticoagulant activities of the acid-resistant part were tested in vitro, and the results showed that partial degradation could result in significant reduction of anticoagulant activity, which could help to lower the risk of bleeding when developing fCS as an antithrombotic drug.