A novel synthesis of 2‐vinyldihydropyrans and dihydro‐1,4‐oxazines (morpholine derivatives) from alkynals and alkynones has been developed. The cyclizations require a mild generation of catalytic ruthenium carbenes from terminal alkynes and (trimethylsilyl)diazomethane followed by trapping with carbonyl nucleophiles. Mechanistic aspects of the new cyclizations are discussed. 相似文献
Ru nanoparticles (RuNPs) stabilized by non‐isolable chiral N‐heterocyclic carbenes (NHCs), namely SIDPhNp ((4S,5S)‐1,3‐di(naphthalen‐1‐yl)‐4,5‐diphenylimidazolidine) and SIPhOH ((S)‐3‐((1S,2R)‐2‐hydroxy‐1,2‐diphenylethyl)‐1‐((R)‐2‐hydroxy‐1,2‐diphenylethyl)‐4,5‐dihydro‐3H‐imidazoline), have been synthesized through a new procedure that does not require isolation of the free carbenes. The obtained RuNPs have been characterized by state‐of‐the‐art techniques and their surface chemistry has been investigated by FTIR and solid‐state MAS NMR upon the coordination of CO, which indicated the presence of free and reactive Ru sites. Their catalytic activity has been tested in various hydrogenation reactions involving competition between different sites, whereby interesting differences in selectivity were observed, but no enantioselectivity. 相似文献
The reactivity of Fischer alkenyl carbenes toward 8‐azaheptafulvenes is examined. Alkenyl carbenes react with 8‐azaheptafulvenes with complete regio‐ and stereoselectivity through formal [8+3] and [8+2] heterocyclization reactions, which show an unprecedented dependence on the Cβ substituent at the alkenyl carbene complex. Thus, the formal [8+3] heterocyclization reaction is completely favored in carbene complexes that bear a coordinating moiety to give tetrahydrocyclohepta[b]pyridin‐2‐ones. Otherwise, alkenyl carbenes that lack appropriate coordinating groups undergo a formal [8+2] cyclization with 8‐azaheptafulvenes to give compounds that bear a tetrahydroazaazulene structure. A likely mechanism for these reactions would follow well‐established models and would involve a 1,4‐addition/cyclization in the case of the [8+2] cyclization or a 1,2‐addition/[1,2] shift–metal‐promoted cyclization for the [8+3] reaction. The presence of a coordinating moiety in the carbene would favor the [1,2] metal shift through transition‐state stabilization to lead to the [8+3] product. All these processes provide an entry into the tetrahydroazaazulene and cycloheptapyridone frameworks present in the structure of biologically active molecules. 相似文献
Another way to dienes : The ruthenium‐catalyzed 6‐endo‐cycloisomerization of 1,5‐enynes gives the corresponding 1,3‐cyclohexadienes in high to excellent yields. This novel synthetic and catalytic method constitutes another way to selectively prepare 1,3‐cyclohexadienes, this cyclic diene skeleton being a core subunit in many natural products and a useful building block for a variety of organic transformations.
The methylation of the uncoordinated nitrogen atom of the cyclometalated triruthenium cluster complexes [Ru3(μ‐H)(μ‐κ2N1,C6‐2‐Mepyr)(CO)10] ( 1 ; 2‐MepyrH=2‐methylpyrimidine) and [Ru3(μ‐H)(μ‐κ2N1,C6‐4‐Mepyr)(CO)10] ( 9 ; 4‐MepyrH=4‐methylpyrimidine) gives two similar cationic complexes, [Ru3(μ‐H)(μ‐κ2N1,C6‐2,3‐Me2pyr)(CO)10]+( 2 +) and [Ru3(μ‐H)(μ‐κ2N1,C6‐3,4‐Me2pyr)(CO)10]+ ( 9 +), respectively, whose heterocyclic ligands belong to a novel type of N‐heterocyclic carbenes (NHCs) that have the Ccarbene atom in 6‐position of a pyrimidine framework. The position of the C‐methyl group in the ligands of complexes 2 + (on C2) and 9 + (on C4) is of key importance for the outcome of their reactions with K[N(SiMe3)2], K‐selectride, and cobaltocene. Although these reagents react with 2 + to give [Ru3(μ‐H)(μ‐κ2N1,C6‐2‐CH2‐3‐Mepyr)(CO)10] ( 3 ; deprotonation of the C2‐Me group), [Ru3(μ‐H)(μ3‐κ3N1,C5,C6‐4‐H‐2,3‐Me2pyr)(CO)9] ( 4 ; hydride addition at C4), and [Ru6(μ‐H)2{μ6‐κ6N1,N1′,C5,C5′,C6,C6′‐4,4′‐bis(2,3‐Me2pyr)}(CO)18] ( 5 ; reductive dimerization at C4), respectively, similar reactions with 9 + have only allowed the isolation of [Ru3(μ‐H)(μ3‐κ2N1,C6‐2‐H‐3,4‐Me2pyr)(CO)9] ( 11 ; hydride addition at C2). Compounds 3 and 11 also contain novel six‐membered ring NHC ligands. Theoretical studies have established that the deprotonation of 2 + and 9 + (that have ligand‐based LUMOs) are charge‐controlled processes and that both the composition of the LUMOs of these cationic complexes and the steric protection of their ligand ring atoms govern the regioselectivity of their nucleophilic addition and reduction reactions. 相似文献
A series of six‐ and seven‐membered expanded‐ring N‐heterocyclic carbene (er‐NHC) gold(I) complexes has been synthesized using different synthetic approaches. Complexes with weakly coordinating anions [(er‐NHC)AuX] (X?=BF4?, NTf2?, OTf?) were generated in solution. According to their 13C NMR spectra, the ionic character of the complexes increases in the order X?=Cl?<NTf2?<OTf?<BF4?. Additional factors for stabilization of the cationic complexes are expansion of the NHC ring and the attachment of bulky substituents at the nitrogen atoms. These er‐NHCs are bulkier ligands and stronger electron donors than conventional NHCs as well as phosphines and sulfides and provide more stabilization of [(L)Au+] cations. A comparative study has been carried out of the catalytic activities of five‐, six‐, and seven‐membered carbene complexes [(NHC)AuX], [(Ph3P)AuX], [(Me2S)AuX], and inorganic compounds of gold in model reactions of indole and benzofuran synthesis. It was found that increased ionic character of the complexes was correlated with increased catalytic activity in the cyclization reactions. As a result, we developed an unprecedentedly active monoligand cationic [(THD‐Dipp)Au]BF4 (1,3‐bis(2,6‐diisopropylphenyl)‐3,4,5,6‐tetrahydrodiazepin‐2‐ylidene gold(I) tetrafluoroborate) catalyst bearing seven‐membered‐ring carbene and bulky Dipp substituents. Quantitative yields of cyclized products were attained in several minutes at room temperature at 1 mol % catalyst loadings. The experimental observations were rationalized and fully supported by DFT calculations. 相似文献
The transition‐metal‐catalyzed direct synthesis of amides from alcohols and amines is herein demonstrated as a highly environmentally benign and atom‐economic process. Among various catalyst systems, in situ generated N‐heterocyclic carbene (NHC)‐based ruthenium (Ru) halide catalyst systems have been proven to be active for this transformation. However, these existing catalyst systems usually require an additional ligand to achieve satisfactory results. In this work, through extensive screening of a diverse variety of NHC precursors, we discovered an active in situ catalyst system for efficient amide synthesis without any additional ligand. Notably, this catalyst system was found to be insensitive to the electronic effects of the substrates, and various electron‐deficient substrates, which were not highly reactive with our previous catalyst systems, could be employed to afford the corresponding amides efficiently. Furthermore, mechanistic investigations were performed to provide a rationale for the high activity of the optimized catalyst system. NMR‐scale reactions indicated that the rapid formation of a Ru hydride intermediate (signal at δ=?7.8 ppm in the 1H NMR spectrum) after the addition of the alcohol substrate should be pivotal in establishing the high catalyst activity. Besides, HRMS analysis provided possible structures of the in situ generated catalyst system. 相似文献
Tying up loose ends : The reaction of bisallenes tethered with N‐(p‐tolylsulfonamide) in the presence of a cationic gold N‐heterocyclic carbene catalyst gave new cycloisomerization products, 6,7‐dimethyleneazabicyclo[3.1.1]heptanes, in high yields (see scheme; IPr=N,N′‐bis(2,6‐diisopropylphenyl)imidazol‐2‐ylidene).
Cross‐coupling carbenes : The coupling of a propargylic ester with a diazoalkane in the presence of [RuCl(cod)Cp*] catalyst leads to the formation of functionalized conjugated dienes with high stereoselectivity. The reaction involves the cross‐coupling of a vinylcarbene fragment, arising from a ruthenium‐catalyzed propargylic ester rearrangement, with a diazoalkane carbene.
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