Synthesis of difunctional 1,4-dimethyl-1,4-disilacyclohexanes

Transformations of HVinSiCl₂, HVinSi(Me)Cl, HVinSi(Me)Ph, and HVinSi(Me)NEt₂ in the presence of Pt catalyst were studied. In dilute solutions, the reaction gave a mixture of structural and stereoisomers of five- and six-membered disilacyclanes, resulting from intramolecular cyclization of the initially formed linear dimer. In the case of methyl(phenyl)disilacyclane, the structural isomers were separated andtrans-1,4-dimethyl-1,4-diphenyl-1,4-disilacyclohexane was isolated. The reaction of this product with HCl in the presence of AlCl₃ followed by hydrolysis resulted in the synthesis oftrans-1,4-dichloro- andtrans-1,4-dihydroxy-1,4-dimethyl-1,4-disilacyclohexanes. The structures of the structural and stereoisomers synthesized were confirmed by¹H,¹³C, and²⁹Si NMR and IR spectroscopies and mass spectrometry. Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 9, pp. 1734–1738, September, 1999.     

Synthesis of Asymmetric 4H-1, 3, 2-Benzodioxaphosphorin 2-Sulfides from Intramolecular Cyclization Reaction

Avarietyofbiologicalactivitiesofsome4H-l,3,2-benzodioxaphosphorin2-sulfideshavebeenreported,forexampletheinsecticideSalithionl.Thecyclicphosphonothionateshavebeenpreparedbyintermolecularcondensationofphosphorodichloridothioateswithsalicylalcoholoritsderivativesinthepresenceofabase=,andbyintramolecularcyclizationreactionofthesalicylalasthestartingmaterial3.However,theintramolecularcyclizationreactionofthe2-hydrobenzophenonesandstereochemicalstudieshavenotbeenreported.Wenowdescribeanewsynthesis…     

Convenient one-pot synthesis of functionalized cyclopentene via Sm/TMSCl/t-BuOH system mediated hydrodimerization cyclization of gem-diactivated alkene

Functionalized cyclopentenes could be prepared through Sm/TMSCl/t-BuOH mediated hy-drodimerization cyclization of gem-diactivated alkene in one-pot at mom temperature. The trans- or trans, transform isomer is in the majority and the major product was isolated from its stereoisomers through the fractional crystallization method.     

丁苯橡胶的阳离子环化

应用一氯二乙基铝和苄基氯催化剂体系进行了丁苯橡胶的阳离子环化反应。研究了反应温度、苄基氯／一氯二乙基铝比例、溶剂、原胶浓度对环化的影响。发现通过控制苄基氯／一氯二乙基铝比,可在高温（１２０℃）、高原胶浓度（２～４％ｗ／ｖ）下进行丁苯橡胶的环化,制得特性粘度较原胶有大幅度降低,可溶性无凝胶的环化丁苯胶。通过对红外光谱、＾１Ｈ－ＮＭＲ谱初步解析,证实了环化反应的发生。     

Synthesis of 4,5,6-trisubstituted 3-cyanopyridine-2(1H)-thiones based on α-substituted β-diketones

5-Substituted 3-cyano-4,6-dimethylpyridine-2(lH)-thiones were synthesized by the re action of a-substituted -diketones with cyanothioacetamide in the presence of triethyl amine. The compounds synthesized were converted into thieno[2,3-blpyridines by treatment with organic halides and KOH.Translated fromlzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 11, pp. 2719–2721, November, 1996.     

Synthesis and conformational analysis by 1H NMR and restrained molecular dynamics simulations of the cyclic decapeptide [Ser-Tyr-Ser-Met-Glu-His-Phe-Arg-Trp-Gly]

Summary The design of enzyme mimics with therapeutic and industrial applications has interested both experimental and computational chemists for several decades. Recent advances in the computational methodology of restrained molecular dynamics, used in conjunction with data obtained from two-dimensional ¹H NMR spectroscopy, make it a promising method to study peptide and protein structure and function. Several issues, however, need to be addressed in order to assess the validity of this method for its explanatory and predictive value. Among the issues addressed in this study are: the accuracy and generizability of the GROMOS peptide molecular mechanics force field; the effect of inclusion of solvent on the simulations; and the effect of different types of restraining algorithms on the computational results. The decapeptide Ser-Tyr-Ser-Met-Glu-His-Phe-Arg-Trp-Gly, which corresponds to the sequence of ACTH_1–10, has been synthesized, cyclized, and studied by two-dimensional ¹H NMR spectroscopy. Restrained molecular dynamics (RMD) and time-averaged restrained molecular dynamics (TARMD) simulations were carried out on four different distance-geometry starting structures in order to determine and contrast the behavior of cyclic ACTH_1–10 in vacuum and in solution. For the RMD simulations, the structures did not fit the NOE data well, even at high values of the restraining potential. The TARMD simulation method, however, was able to give structures that fit the NOE data at high values of the restraining potential. In both cases, inclusion of explicit solvent molecules in the simulation had little effect on the quality of the fit, although it was found to dampen the motion of the cyclic peptide. For both simulation techniques, the number and size of the NOE violations increased as the restraining potential approached zero. This is due, presumably, to inadequacies in the force field. Additional TARMD vacuum-phase simulations, run with a larger memory length or with a larger sampling size (16 additional distance-geometry structures), yielded no significantly different results. The computed data were then analyzed to help explain the sparse NOE data and poor chymotryptic activity of the cyclic peptide. Cyclic ACTH_1–10, which contains the functional moieties of the catalytic triad of chymotrypsin, was evaluated as a potential mimic of chymotrypsin by measurement of the rate of hydrolysis of esters of L-and d-phenylalanine. The poor rate of hydrolysis is attributed to the flexibility of the decapeptide, the motion of the side chains, which result in the absence of long-range NOEs, the small size of the macrocycle relative to that of the substrate, and the inappropriate orientation of the Gly, His, and Ser residues. The results demonstrate the utility of this method in computer-aided molecular design of cyclic peptides and suggest structural modifications for future work based on a larger and more rigid peptide framework.     

One-pot synthesis of [1,2,4]Triazolo[1,5-a]pyridines from azines and benzylidenemalononitriles via copper-catalyzed tandem cyclization

A simple and efficient copper-catalyzed tandem radical cyclization reaction has been discovered for the synthesis of triaryl [1,2,4]triazolo[1,5-a]pyridines from easily accessible azines and benzylidenmalononitriles. The new transformation involves multiple CH/CC bonds cleavage and CC/CN bonds formation, with extrusion of gaseous hydrogen and methane. A wide variety of substrates with different functional groups could be converted into the corresponding products in good yields. The fused heterocycles have strong blue fluorescence with large Strokes shifts and high quantum yields.     

Novel tricyclic diamines 2. Synthesis of 1,7-diazaisoadamantane, 1,5-diazaisoadamantane and 1,6-diazahomobrendane

Three novel tricyclic diamines (1,7-diazaisoadamantane, 1,5-diazaisoadamantane and 1,6-diazahomobrendane) were prepared. A flexible synthetic strategy was employed which used flat, aromatic azaindoles as the starting materials. The requisite azaindoles were prepared by a tandem Sonogashira coupling/intramolecular cyclization reaction. Ring saturation, appropriate functionalization and intramolecular alkylation provided the three novel tricyclic diamines cores.     

Recent advances in Garratt-Braverman cyclization: Mechanistic and synthetic explorations

Garratt-Braverman cyclization has emerged as one of the simplest synthetic tool to construct two consecutive CC bonds leading to the formation of various important structural scaffolds having significance in the field of therapeutics and material science. The strategic design of suitable precursor for this cycloaromatization reaction involves the deep understanding of reaction pathways involving diradicals and ions. On the other hand, the reaction offers an unprecedented mechanistic paradox for the chemists to solve. This report aims at outlining the recent mechanistic and synthetic developments with special emphasis on the research outcomes from our laboratory.     

Catalyst-free three-component approach to efficient synthesis of chromeno[4,3-b]pyrrol-4(1H)-one derivatives

A mild, efficient, and environmentally benign one-pot synthesis of functionalized chromeno[4,3-b]pyrrol-4(1H)-ones by a three-component domino reaction of 4-aminocoumarins, arylglyoxal monohydrates, and 1,3-dicarbonyl compounds in refluxing ethanol without the use of catalyst is reported. The present protocol features operational simplicity, short reaction time, good yields, and the absence of aqueous workup procedure and chromatographic separation.