Palladium-catalyzed reactions of cyclopropanols bearing oxazoline directing group

Cyclopropanols bearing oxazoline directing group were investigated in palladium-catalyzed reactions. When the directing group and cyclopropanol unit were bonded through two- or three-carbon spacer, formation of unusual products was observed. Oxidative ring opening proceeded with uncommon regioselectivity providing linear enones as main products. The reaction of such cyclopropanols with aryl iodides and silver acetate furnished diarylated α-methylene ketones, which cannot be obtained from cyclopropanols lacking oxazoline ring under the same conditions.     

Site‐Selective Approach to β‐Fluorination: Photocatalyzed Ring Opening of Cyclopropanols

To expand upon the recent pioneering reports of catalyzed sp³ C?H fluorination methods, the next rational step is to focus on directing “radical‐based fluorination” more effectively. One potential solution entails selective C?C bond activation as a prelude to selective fluorination. Herein, we report the tandem photocatalyzed ring‐opening/fluorination reactions of cyclopropanols by 1,2,4,5‐tetracyanobenzene (TCB) and Selectfluor to afford a process tantamount to site‐selective β‐fluorination of carbonyl‐containing compounds. This new approach provides a synthetically mild and operationally simple route to otherwise difficult‐to‐prepare β‐fluorinated products in good yields and with good‐to‐excellent regioselectivity. Remarkably, substrates that contain other usually reactive (e.g., benzylic) sites undergo ring‐opening fluorination preferably. The versatility of this method to give cyclic β‐fluorides from tertiary cyclopropanols and γ‐fluoro alcohols is also highlighted.     

Total syntheses via cyclopropanols

Cyclopropanols are readily available via the Kulinkovich cyclopropanation, the Simmons-Smith reaction, and other synthetic methods. Due to their intrinsic ring stains, cyclopropanols and their derivatives are highly reactive and can be converted to different structural scaffolds which are frequently found in many natural products. In this review, we highlight the applications of various cyclopropanol ring opening/expansion/fragmentation reactions in the total syntheses of natural products.     

Cis-homo addition-1,4 thiophile d'organomagnesiens avec des composes thiocarbonyles comportant un groupe carbonyle en β: Synthese stereoselective d'alcoylthio-2 et de bis (alcoylthio)-2,2 cyclopropanols

Aliphatic Grignard reagents react stereoselectively with β thioxo carbonyl compounds to give substituted cis 2-alkylthio or 2,2-bis (alkylthio) cyclopropanols with good yields. Two types of non-enethiolisable thiocarbonyl compounds of formulae MeCOC(Me)₂CSR undergo this reaction a thioketone (R = Me) and a number of dithioesters (R = SMe, SEt, S iso Pr). The cis configuration of cyclopropanols has been assigned by ¹H NMR-Eu(fod)₃. The cyclopropane ring closure is a concerted cis-1,4-homo addition.     

Synthesis of α-methyl ketones by a selective, iridium-catalyzed cyclopropanol ring-opening reaction

A mild method for synthesizing α-methyl ketones from substituted cyclopropanols is reported. This process, catalyzed by [Cp∗IrCl₂]₂, cleaves cyclopropanol rings regioselectively and more efficiently than the other conditions examined. While tertiary cyclopropanols afford α-methyl ketones, secondary cyclopropanols and cyclopropyl silyl ethers are less reactive and yield other isomerization products.     

Copper(I)‐Catalyzed Chemoselective Coupling of Cyclopropanols with Diazoesters: Ring‐Opening C−C Bond Formations

Reported herein is an exceptional chemoselective ring‐opening/C(sp³)−C(sp³) bond formation in the copper(I)‐catalyzed reaction of cyclopropanols with diazo esters. The conventional O−H insertion product is essentially suppressed by judicious choice of reaction conditions. DFT calculations provide insights into the reaction mechanism and the rationale for this unusual chemoselectivity.     

非对称氮杂环丙烷的亲核开环反应及其区域选择性

本文系统地总结了各类亲核试剂对非对称氮杂环丙烷(吖丙啶)的亲核开环反应及开环的区域选择性.氮杂环丙烷亲核开环的区域选择性是一种空间效应和电子效应平衡的结果,非芳基和非烯基取代的氮杂环丙烷的亲核开环通常发生在氮杂环丙烷取代少的碳原子上,空间效应起主导作用;而芳基和烯基取代的氮杂环丙烷的亲核开环通常发生在氮杂环丙烷芳甲位和烯丙位的碳原子上,电子效应起主导作用,烯基取代的氮杂环丙烷的亲核开环还可以发生在烯基的β-碳原子上;分子内的亲核开环反应主要受成环时环大小的控制,成环时的倾向是五元环>六元环>七元环.对于亲核试剂,一般的亲核试剂也同时受电子效应和空间效应的影响; 而亲核性强的亲核试剂通常只受空间效应的影响.容易生成稳定自由基的亲核试剂容易发生单电子转移机理的开环反应,生成相当于亲核试剂进攻氮杂环丙烷中取代多的碳原子得到的开环产物.     

Gold(I)-catalyzed ring expansion of cyclopropanols and cyclobutanols

The rearrangement of 1-alkynyl cyclobutanols and cyclopropanols to alkylidene cycloalkanones catalyzed by cationic triarylphosphine gold(I) complexes is described. The reaction tolerates terminal alkynes as well as alkyl, aryl, and halo-substitution at the acetylenic position and stereoselectively provides a single olefin isomer. The gold(I)-catalyzed rearrangement is stereospecific with regard to substituents on the ring, thus providing a practical method for the stereoselective synthesis of highly substituted cyclopentanones from cyclopropanols. The reaction stereoselectively provides a single olefin isomer and is stereospecific with regard to substituents on the ring via sequential gold(I)-catalyzed ring expansion reactions.     

Synthesis and radical ring opening behaviour of 1,1-difluoro-2-heptyl-2-vinylcyclopropane and some of its isomers

The syntheses and characterisations of 1,1-difluoro-2-heptyl-2-vinylcyclopropane and some of its isomers are described together with attempts to effect free radical ring opening polymerisation. We have recently shown that the parent monomer, 1,1-difluoro-2-vinylcyclopropane, undergoes predominantly 1,4-addition ring opening in contrast to the more usual 1,5-ring opening of other substituted vinylcyclopropanes and we find that the same anomalous behaviour occurs in this work confirming the influence of fluorine on the course of cyclopropane ring opening proposed by Dolbier. The presence of an alkyl chain modifies the ratios of 1,4- to 1,5-ring opening compared to that found in the unsubstituted parent monomer. In addition an the unexpected behaviour of different alkyl substituted buta-1,3-dienes towards difluorocarbene addition is described.     

Ring-opening of tertiary cyclopropanols derived from β-diketones

The ring-opening reaction of 1,2-disubstituted cyclopropanols, prepared from β-diketones, mediated by Cu(NO₃)₂, p-TsOH, and NaOH is reported. The Cu(II)-mediated ring-opening of cyclopropanols gave α-methylene-γ-diketones in good yields. The reaction took place at the less substituted carbon of the cyclopropanols, involving mild conditions and a simple procedure. The reaction induced by p-TsOH in CH₂Cl₂ afforded α-methyl-γ-diketones as the major product with minor amounts of δ-diketones. The 2,3,5-trisubstituted furans were obtained in high yields when the ring-opening reaction was mediated by p-TsOH in methanol under reflux conditions. In the presence of sodium hydroxide the reaction proceeded smoothly in preference to the formation of δ-diketones, particularly for substrates with an aromatic group on the cyclopropane.     

非对称环硫乙烷的区域选择性亲核开环反应

环硫乙烷与它的氧类似物环氧乙烷和氮类似物氮杂环丙烷一样,是一类重要的有机合成中间体,在医药和农用化学品工业领域也得到广泛应用。通过开环和异构化反应,还广泛用于制备硫醇和硫醚等含硫化合物。本文总结了常用亲核试剂对非对称环硫乙烷的亲核开环反应及其区域选择性。环硫乙烷的亲核开环反应通常只受空间效应影响,亲核试剂进攻非对称环硫乙烷位阻小的碳原子,对于烯基取代的环硫乙烷有时可以进攻烯基的β碳原子发生SN2’开环反应。强亲核性的亲核试剂容易致使环硫乙烷脱硫生成烯烃,而亲核性相对较弱的亲核试剂容易发生多聚反应生成多硫醚。在Lewis酸存在下,电子效应会对开环反应的区域选择性产生影响,甚至起主导作用。虽然烷基取代环硫乙烷在Lewis酸存在下的开环仍然主要发生在其取代基少的碳原子上(位阻控制),但受电子效应影响,芳基和烯基取代环硫乙烷的亲核开环,其亲核试剂一般倾向于进攻环硫乙烷的芳甲位和烯丙位碳原子(电子效应控制)。     

Selective tandem enyne metathesis for the synthesis of functionalized cycloheptadienes

The regio- and site-selective ring expansion of dienes and the regioselective ring expansion of substituted cyclopentenes provide 1,3-cycloheptadienes by enyne metathesis under methylene-free conditions. Site-selectivity results from differential ring strain among two different cycloalkenes in diene reactants. The high regioselectivity found in the ring expansion of tetrahydroindene (THI) is explained on the basis of a selective ring opening by the second generation Grubbs' ruthenium carbene complex. The ring opening of substituted cyclopentenes and cyclopentene contained in a bicyclic ring system was also achieved. The ring expansion of bicyclic dienes provided seven-membered dienes contained in the bicyclo[5.2.0]nonane ring system. Details of the structural analysis are also discussed. A mechanistic analysis is provided to account for the data presented herein.     

Polyfunctional intermediates for the preparation of liquid-crystalline and anisotropic materials

This paper describes the polyfunctional intermediates for the preparation of various anisotropic and liquid-crystalline compounds with different combinations of cyclic, bridge, terminal fragments and lateral substituents. Both chiral and nonchiral nematic, smectic mesomorphic and anisotropic compounds can be prepared by the transformations of the corresponding 3,6-disubstituted cyclohex-2-enones, trans-2,5-disubstituted cyclohexanones, 3,5-disubstitiuted 2-isoxazolines, substituted cyclohex-2-enonyl 2-isoxazolines, 1,2-disubstitiuted cyclopropanols and substituted unsaturated epoxyketones.     

Intramolecular hetero-Michael addition of beta-hydroxyenones for the preparation of highly substituted tetrahydropyranones

Structurally diverse beta-hydroxyenones are shown to undergo nonoxidative 6-endo-trig ring closure to form highly substituted tetrahydropyranones. Amberlyst-15, Al(ClO(4))(3) x 9 H(2)O and [Pd(MeCN)(4)](BF(4))(2) were found to be suitable catalysts for these intramolecular conjugate additions, preventing side reactions, such as dehydration or retroaldolisation. The use of [Pd(MeCN)(4)](BF(4))(2) is particularly effective, as this palladium-mediated reaction is under kinetic control and generates tri- and tetrasubstituted tetrahydropyranones with high levels of diastereocontrol. In the presence of the Lewis acid Al(ClO(4))(3) x 9 H(2)O, the reaction proceeded with a similar level of diastereocontrol; however, in contrast to [Pd(MeCN)(4)](BF(4))(2), this catalyst can promote enolisation. The palladium-mediated reaction was also found to be compatible with an enantioenriched beta-hydroxyenone substrate, giving no loss of enantiopurity upon ring closure. The most distinctive synthetic development to emerge from this new chemistry is the possibility to access tri- and tetrasubstituted 2,6-anti-tetrahydropyranones from anti-aldol precursors. These compounds are particularly difficult to access by using alternative methodologies. Two modes of activation were envisaged for the ring closure, involving metal coordination to either the C=C or C=O functional groups. Experimental results suggest that C=O coordination was the preferred mode of activation for reactions performed in the presence of Al(ClO(4))(3) x 9 H(2)O or [Pd(MeCN)(4)](BF(4))(2).     

Silicon-assisted ring opening of donor-acceptor substituted cyclopropanes. An expedient entry to substituted dihydrofurans

[reaction: see text]. (tert-butyldiphenylsilyl)methylcyclopropanes undergo ring opening to furnish substituted dihydrofurans in good to excellent yields on treatment with TiCl4 in dichoromethane. The silicon that assists the regioselective ring opening is retained in the product to allow further functional group manipulations.     

New compounds in ring‐opening reaction of 5‐substituted epoxyisoindolines

Methoxy or nitro group present in the furan ring of tertiary alkenylfurfurylamine changes the expected results of both, the intramolecular [4+2]cycloaddition and the acid catalyzed ring‐opening reaction of the derived oxatricycloadduct. With a 5‐methoxy group, in addition to the expected 5‐methoxyisoindoline 3 , the corresponding hydroxy derivative 5 was obtained. On the other hand a 5‐nitro group changes the outcome of the reaction even more profoundly. Instead of the expected 5‐nitroisoindoline 12 , 5‐nitro‐substituted epoxy‐isoindoline 6 submitted to ring‐opening reaction with the mixture of hydrobromic and acetic acid, yielded the mixture of bromo‐substituted epoxy compounds 7,8, 9 and/or bromo‐substituted isoindolines 10 and 11 .     

Reactions of halogenoquinolizinium bromides with diethylamine

The reactions of quinolizinium bromide (QB) and its four monobromo derivatives with diethylamine have been investigated. For Br in position 2 or 4, substitution is the main process, whereas for Br in positions 1 and 3 quantitative ring opening is found. The substituted pyridylbutadienes formed by ring opening, are cis-trans-butadienes, which isomerize into the all-trans forms. The steric cours of the ring opening is explained.     

非对称环氧乙烷的区域选择性亲核开环反应

本文总结了常用亲核试剂对非对称环氧乙烷的亲核开环反应及其区域选择性。强亲核性的亲核试剂通常只受空间效应影响,进攻非对称环氧乙烷位阻小的碳原子,对于烯基取代环氧乙烷还可以进攻烯基的β-碳原子发生S_N2'开环反应,其他亲核试剂同时受空间效应和电子效应的影响,对于烷基环氧乙烷通常进攻其取代少的碳原子, 空间效应起主导作用,而对芳基和烯基取代环氧乙烷开环反应通常发生在环氧乙烷芳甲位和烯丙位的碳原子上, 电子效应起主导作用。在质子酸或强Lewis酸存在下,虽然单烷基环氧乙烷的开环仍然发生在其取代少的碳原子上,但对于芳基、烯基和同碳双取代环氧乙烷,亲核开环反应将主要受电子效应控制,一般亲核试剂倾向于进攻环氧乙烷的芳甲位、烯丙位或多取代的碳原子。分子内的亲核开环反应主要受成环时环大小的控制, 成环时的倾向是五元环> 六元环> 七元环。环氧乙烷亲核开环的区域选择性是环氧乙烷和亲核试剂空间效应和电子效应平衡的结果。     

Theoretical calculational investigation on the regioselectivity of the ring opening of thiiranes with ammonia and amines

The course, especially the regioselectivity, of the nucleophilic ring opening of thiiranes with ammonia and amines was investigated with the density functional theory (DFT) calculation. In the ring-opening reaction, thiiranes could be attacked on either their less or more substituted carbon atoms. The analyses of the potential energy surfaces, the bond lengths, and charges of key species in both pathways indicate that alkyl-substituted thiiranes are attacked dominantly on their less substituted ring carbon atom, whereas arylthiiranes are on their more substituted one due to the existence of the p-π conjugative effect, which stabilizes the transition states generated in the reaction. Furthermore, the Lewis acid can modulate the regioselectivity. However, the steric hindrance of nucleophiles and solvents affect the regioselectivity slightly as they show similar influence on both pathways, despite the fact that they can put an impact on the energy. NBO and MO analyses also support the substituent-depended regioselectivity. This is the first DFT calculational investigation on the regioselective ring opening of thiiranes and provides a rational explanation for the experimental results. The theoretical investigation gives a general understanding and a rule for the rationale and prediction of the regioselectivity in the nucleophilic ring opening of thiiranes, even other three-membered heterocycles.     

Facile synthesis of 2-substituted 1,2-dihydro-1-naphthols and 2-substituted 1-naphthols

[reaction: see text] The palladium-catalyzed ring opening of dimethoxy oxabenzonorbornadiene with aryl or vinyl halides occurred under very mild conditions to give substituted 1,2-dihydronaphthols that were oxidized with IBX to furnish substituted naphthols in excellent overall yields.