Synthesis of a small library of oximes and phenylhydrazones of phenyl ketone C-glycosides

An efficient and convenient route was developed for the synthesis of oximes, the corresponding O-methylated oximes, and phenylhydrazones from phenyl ketone C-glycosides in medium to high yields. The broad substrate and reagent scope of this method expands the potential of applying phenyl ketone C-glycosides to the synthesis of important bioactive molecules.     

E- and Z-isomerism of 2-acetylthiophene oximes

A study on the oximation of a number of 2-acetylthiophenes in order to ascertain the validity of contradictory results previously described is reported. The fact that the steric hindrance is smaller in 2-acetylthiophenes unsubstituted at position-3 than in acetylbenzenes allows in these cases the formation of Z oximes, which even can predominate on the E oximes in the case of a + M substitution at position-5. In the paper is also shown that the E/Z ratio of 2-acetylthiophene oximes can be deduced from the ¹H-nmr spectrum of the crude oxime mixture.     

Stereospecific 1,4‐Metallate Shift Enables Stereoconvergent Synthesis of Ketoximes

Reported herein is a stereospecific 1,4‐metallate rearrangement for single‐geometry ketoxime synthesis from oxime chlorides and arylboronic acids. This strategy exhibits broad substrate scope with excellent stereoselectivity under mild reaction conditions. In comparison with the conventional approaches, each configuration of unsymmetric diaryl oximes, as well as the thermodynamically less stable Z isomer of aryl alkyl ketoximes can be selectively and exclusively obtained. The reactivities of unsymmetric diaryl oximes and the Z isomer of aryl alkyl oximes, a class of underexplored molecules, enables efficient access to the corresponding isoquinolines, isoquinoline N‐oxides, and amides having a single configuration.     

Divergent Synthesis of Oxa-Cyclic Nitrones through Gold(I)-Catalyzed 1,3-Azaprotio Transfer of Propargylic α-Ketocarboxylate Oximes: Experimental and DFT Studies

1,3-Azaprotio transfer of propargylic α-ketocarboxylate oximes, a new type of alkynyl oximes featuring an ester tether, has been explored by taking advantage of gold catalysis. The incorporation of an oxygen atom to the chain of alkynyl oximes led to the formation of two different oxa-cyclic nitrones. It was found that internal alkynyl oximes with an E-configuration deliver five-membered nitrones, whereas terminal alkynyl oximes with an E-configuration afford six-membered nitrones. DFT calculations on four possible pathways supported a stepwise formation of C−N and C−H bonds, in which a 1,3-acyloxy-migration competes with the 1,3-azaprotio-transfer, especially in the case of internal alkynyl oximes. The relative nucleophilic properties of oxygen in the carbonyl group and the nitrogen in the oxime, the electronic effects of alkynes, and the influence of the ring system have been investigated computationally.     

新的α-单取代环十二酮肟的合成及晶体结构

单晶X射线衍射分析表明,几个新的α-单取代环十二酮与氨衍生物羟胺发生反应得到三种母体构象分别为[3333]和[2334],而取代基为边外向或角反向的α-单取代环十二酮肟.利用底物的"角位羰基参与反应"原理,"记忆效应"及进攻试剂与底物是否形成氢键解释了这一实验结果.通常取代基体积较大以及α-取代基与羰基形成分子内氢键情况下,试剂从空间障碍小以及远离氢键的一面进攻羰基生成α-角反取代环十二酮肟;当试剂与底物的取代基之间能够形成强的分子间氢键时,生成α-边外取代环十二酮肟;当试剂与底物的取代基之间只能形成弱的分子间氢键以及底物的取代基较小时,试剂从两面进攻羰基同时生成α-角反取代环十二酮肟和α-边外取代环十二酮肟.     

Reactions of N-heteroarylformamide oximes and N-heteroarylacetamide oximes with N,N-dimethylformamide dimethyl acetal. Synthesis of 2-methyl-s-triazolo[1,5-x]azines and N-methylcyanoaminoazines

N-Heteroarylformamide oximes 3 (R ? H) were converted with N,N-dimethylformamide dimethyl acetal (DMFDMA) into N-heteroaryl-N-methylcyanoamino compounds 5 , as the main products. In some instances N-heteroarylcyanoamino compounds 4 , cyanoimino compounds 7 , and some other products, such as 9 and 10 were also formed. On the other hand, N-heteroarylacetamide oximes 3 (R ? CH₃) were cyclized under the same reaction conditions into 2-methyl-s-triazolo[1,5-x]azines ( 6 ). N-Heteroarylacetamide O-methyl oximes 11 and 12 were prepared from the corresponding acetamidines 2 (R ? CH₃) and O-methylhydroxylamine.     

α-单取代环十二酮肟及缩氨基硫脲的合成及晶体结构

单晶X射线衍射分析表明, α-单取代环十二酮与氨衍生物羟胺和氨基硫脲发生缩合反应得到两种母体构象均为[3333], 而取代基为边外向或角反向的α-单取代环十二酮肟或缩氨基硫脲. 利用底物的“角位羰基参与反应”原理, “记忆效应”及进攻试剂与底物是否形成氢键解释了这一实验结果. 通常情况下, 试剂从空间障碍小的一面进攻羰基而生成α-角反取代环十二酮肟或缩氨基硫脲. 当试剂与底物的取代基之间能够形成分子间氢键时, 则生成α-边外取代环十二酮肟或缩氨基硫脲.     

The fragmentation of ortho-methoxyphenyl-2-propanone oximes and related compounds–further examples of an ortho-effect

An [M ? 31]⁺ ion was a prominent fragment in the mass spectra of three ortho-methoxy-phenyl-2-propanone oximes and is shown to be due to the expulsion of a methoxyl radical from the molecular ion as a result of an ortho-effect. In contrast, an [M ? 31]⁺ ion was absent from the spectra of a structurally related ketone and a hydroxylamine, and was not observed in the spectra of meta- and para-methoxyphenyl-2-propanone oximes.     

Oximes of azolecarbaldehydes and Δ2-azolinecarbaldehydes and their derivatives

The configurational (kinetic) stability of the anionic and zwitterionic forms of 1-methylpyrazolecarbaldehyde oximes and 1-methylimidazolecarbaldehyde oximes and their quaternary ammonium derivatives in aqueous solutions has been established. In an acid medium, isomerization takes place and an E-Z equilibrium of the cations of the oximes is established. The changes in the relative thermodynamic stabilities of the stereoisomers of the heteroaromatic carbaldehyde oximes as functions of the size and nature of the ring, the position of the oxime group, and the steric loading are due to spatial factors and electrostatic interactions. To substantiate the preferred conformations of the Z aldehyde oximes the differences in the values of the chemical shifts of the protons of the ring and the rates of their deuterium exchange have been used.For Communication II, see [1],Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 9, pp. 1176–1180, September, 1973.     

Chemistry of N,N‐Bis(silyloxy)enamines,Part 5

Aliphatic nitro compounds can be considered as good precursors of a wide variety of α‐azolyl‐substituted oximes. The double silylation of convenient aliphatic nitro compounds and the subsequent N,C‐coupling of the resulting N,N‐bis(silyloxy)enamines 3 with N‐silylated azoles 4 lead to the formation of the silylated α‐azolyl‐substituted oximes 6 , which can be smoothly desilylated to give the target α‐azolyl‐substituted oximes 5 . The mechanism of the key step of this process – N,C‐coupling – includes the generation of corresponding conjugated nitrosoalkenes 7 (Schemes 4 and 5). The contribution of the chain mechanism in the overall process is considered as well. The studies of the scope and limitations of this reaction, as well as the optimization of its conditions were accomplished. The configuration of the CN bond in oximes was established by NMR.     

First Representatives of O-(2-Vinyloxyethyl)oximes

Previously unknown ketone and acetaldehyde O-(2-vinyloxyethyl)oximes were synthesized in 22-88% by reaction of the corresponding oximes with 2-chloroethyl vinyl ether in the system KOH-DMSO.     

Use of Zeolite Catalysts for Efficient Synthesis of Benzoxazoles via Beckmann Rearrangement

Substituted benzoxazoles have been synthesized in very good yields starting from o-acylphenol oximes via Beckmann rearrangement using zeolite catalysts.     

Die heterolytische Fragmentierung von Benzoin-O-(carbamoyl)oximen

The Heterolytic Fragmentation of Benzoin-O-(carbamoyl)oximes While the known heterolytic fragmentation reactions give only three, thermal decomposition of benzoin-O-(carbamoyl)oximes results in at least four fragments: nitrile or isocyanide, carbonyl compound, CO₂ and amine. This exception is due to the transformation of the nucleofugal group 3 into the unstable carbamic acid and its decomposition (s. Scheme 1). Since only the configuration of benzoin (E)-O-(carbamoyl)oximes is satisfactory for concerted reactions, we conclude that the nitrile producing fragmentation of these (E)-compounds is concerted, whereas in the isocyanide producing fragmentation of the corresponding (Z)-compounds several steps are involved. – In contrast to the benzoin-O-(carbamoyl)oximes the pyrolysis of benzil-(E)-O-(methylcarbamoyl)oxime starts with the elimination of methyl isocyanate and the following fragmentation is that of the oxime.     

Copper‐Catalyzed Skeletal Rearrangements of O‐Propargylic Oximes via Cleavage of a Carbon–Oxygen Bond

In this account, we describe recent developments in copper‐catalyzed skeletal 2,3‐rearrangement reactions of O‐propargylic oximes to form four‐membered cyclic nitrones, pyridine N‐oxides, and amidodienes via N‐allenylnitrone intermediates. The sequence of events leading up to our encounter with O‐propargylic oximes is also presented.     

Polycyclic N‐Heterocyclic Compounds. Part 78: Synthesis of N‐[2‐([1,2,4]Oxadiazol‐5‐yl)cyclohepten‐1‐yl]formamide Oximes and Their Evaluation as Inhibitors of Platelet Aggregation

N‐[2‐([1,2,4]Oxadiazol‐5‐yl)cyclohepten‐1‐yl]formamide oximes were synthesized by fusion of (6,7,8,9‐tetrahydro‐5H‐cyclohepta[1,2‐d]pyrimidin‐4‐yl)amidines with hydroxylamine hydrochloride through a subsequent rearrangement reaction. Effects of the products as well as the structurally related N‐[4‐([1,2,4]oxadiazol‐5‐yl)‐2,3‐dihydro[1]benzoxepin‐5‐yl]formamide oximes and N‐[4‐([1,2,4]oxadiazol‐5‐yl)‐2,3‐dihydro[1]benzothiepin‐5‐yl]formamide oximes on platelet aggregation were evaluated.     

Reinvestigation of the rearrangement of 2-acetylbenzofuran oxime tosylate

The acetal, resulting from the rearrangement of anti-2-acetylbenzofuran oxime tosylate (I) was proved to be a mixture of trans- (IX) and cis- (X) 2,3-dihydro-2-acetyl-2,3-dimethoxybenzofuran. The structure of these isomers as well as that of their oximes XI and XII was elucidated by ir, nmr, and mass spectral investigation and by the ir and nmr spectra of the benzoyl (XIII and XIV) and acetyl (XV and XVI) derivatives of the oximes. A new reaction mechanism concerning the rearrangement process is discussed.     

Cytotoxicity of cobalt complexes of furan oximes in murine and human tissue‐cultured cell lines

The copper complexes of 2‐furaldehyde and furan oximes have previously demonstrated potent cytotoxicity, L1210 DNA synthesis inhibition, DNA topoisomerase II inhibition and DNA fragmentation. Currently a series of cobalt metal complexes of 2‐furaldehyde oximes were compared with copper complexes of furan oximes to determine whether the type of metal is important to the cytotoxicity and mode of action of the complexes. The cobalt complexes of furan oximes, like the copper complexes, were shown to be cytotoxic to suspended tumor cell lines, e.g. leukemias, lymphomas, acute monocytic leukemia and HeLa‐S³ uterine carcinoma. The cobalt complexes did not demonstrate dramatic cytotoxicity against the growth of tumors derived from solid human tumor lines. The cobalt complexes preferentially inhibited L1210 DNA synthesis, followed by inhibition of RNA and protein synthesis from 25 to 100 µM over 60 min. These agents, like the copper complexes of 2‐furaldehyde and furan oximes, were inhibitors of DNA polymerase α activity and de novo purine synthesis with marginal inhibition of ribonucleoside reductase and dihydrofolate reductase activities with DNA fragmentation. Unlike the copper complexes, the cobalt complexes did not inhibit L1210 DNA topoisomerase II activity but did reduce thymidylate synthetase activity. Thus, varying the type of metal within the complexes of 2‐furaldehyde and furan oximes produces differences in both cytotoxicity and mode of action. Copyright © 1999 John Wiley & Sons, Ltd.     

Behaviour of the Primary Nitro Group Under Denitration Conditions

ABSTRACT

Treatment of per-O-acetylated or acetalated glycosylnitromethanes derived from the common hexoses and pentoses with tributyltin hydride and a catalytic amount of a radical initiator [1,1′-azobis(cyclohexanecarbonitrile)] in refluxing benzene easily afforded the corresponding glycosylmethanal oximes in 84-97% yields. Per-O-acetylated C-β-glycopyranosylmethanal oximes were employed for synthesis of versatile C-β-glycopyranosyl cyanides of the β-D-gluco, β-D-manno, β-D-galacto, β-D-xylo, and β-L-rhamno configurations.     

Equilibres conformationnels de glucides au niveau de liaisons σ sp2-sp3 C-C. III Dérivés d'oximes d'aldéhydo-sucres utilisation de tris-dipivaloylméthanato-europium

A series of sugar oximes and O-methyloximes of the general formula RCH?NOR′ (R′ ? H, CH₃) have been studied by PMR. spectroscopy. These compounds exist in solution as a mixture of the syn and anti isomers. The conformational equilibrium of the syn isomers seems to consist exclusively of the eclipsed rotamers, whereas for the anti isomers there appears to be a significant contribution from bisecting rotamers. Using tris-dipivaloylmethanato-europium it is found that the α proton of the anti oximes is much more deshielded than the corresponding proton of the syn isomers, which means that the downfield shift of a particular proton does not depend exclusively on its distance from the oxygen of the oxyimino group.     

15N chemical shifts of a series of isatin oxime ethers and their corresponding nitrone isomers

In this article, we describe the characteristic ¹⁵N chemical shifts of isatin oxime ethers and their isomer nitrone. These oxime ethers and nitrones are the alkylation reaction products of isatin oximes. In our study, the ¹⁵N chemical shifts observed in these oxime ethers were in the 402–408 (or 22–28) ppm range, although those for their corresponding nitrone series were in the 280–320 (or ?100 to ?60) ppm range. This remarkable difference in ¹⁵N NMR chemical shift values could potentially be used to determine the O‐ versus N‐alkylation of oximes, even when only one isomer is available. In this paper, the differences in ¹⁵N NMR chemical shifts serve as the basis for a discussion about how to distinguish both regioisomers derived from the oximes alkylation. Copyright © 2010 John Wiley & Sons, Ltd.