Activation of Mononuclear Arene Ruthenium Complexes for Catalytic Propargylation Directly with Propargyl Alcohols

Abstract: by activation of the propargylic alcohol, leading to the carbonyl ligand formation via allenylidene and alkenyl-hydroxycarbene intermediates. The generation of the catalytically active species requires a short initial thermal activation to induce decoordination of the p-cymene ligand. The in situ generated catalyst has been applied to catalytic transformations of alkynes and propargylic alcohols: propargylation of furans, propargyl ether synthesis from internal and terminal propargylic alcohols with propargyl,… Show more

“…Moreover complexes containing phosphine ligands continue to enjoy immense popularity in connection with homogenous catalysis and organometallic chemistry [18e23]. A large number of ruthenium complexes with arene ligands have been employed in different catalytic reactions including allylic alkylation [24], amination [25], cyclization [26], cycloisomerization of dienes [27] and hydroformylation [28] and transfer hydrogenation.…”

Ruthenium(II) half-sandwich complexes containing thioamides: Synthesis, structures and catalytic transfer hydrogenation of ketones

“…Moreover complexes containing phosphine ligands continue to enjoy immense popularity in connection with homogenous catalysis and organometallic chemistry [18e23]. A large number of ruthenium complexes with arene ligands have been employed in different catalytic reactions including allylic alkylation [24], amination [25], cyclization [26], cycloisomerization of dienes [27] and hydroformylation [28] and transfer hydrogenation.…”

Ruthenium(II) half-sandwich complexes containing thioamides: Synthesis, structures and catalytic transfer hydrogenation of ketones

“…b) The reactions of cycloalkanols gave a small amount of phenylsulfanylethynylcycloalkenes 5. 46) formed the reaction with other thiols such as 2-thienyl, naphthyl, p-chlorophenyl and cyclohexylthiol and obtained satisfactory results (entries 2-5, Table 4). A variety of propargyl alcohols bearing the substituents such as R 1 ϭ2-thienyl, 1-naphthyl and benzodioxol-5-yl produced some propargyl sulphides 8ba-8gc in moderate to high yields (entries [6][7][8][9][10][11].…”

Lewis Acid-Catalyzed Propargylic Etherification and Sulfanylation from Alcohols in MeNO2-H2O

“…Because an excess of water is present in the reaction media, complex Q can undergo the Markovnikov addition of water to the coordinated carbon-carbon triple bond to afford the corresponding enones via intermediates R and S. The formation of penyne Q is supported by the fact that if the catalytic process is performed in anhydrous THF, the corresponding free 1,3-enynes can be isolated from the reaction media via demetalation of Q. 51b 52 Thus, using 5 mol% of this complex, the terminal alkynol 1,1-diphenylprop-2-yn-1-ol [i.e., HC≡CC(OH)Ph 2 ] was selectively converted into 3,3-diphenylprop-2-enal (i.e., HCOCH=CPh 2 ) in 89% yield after only 5 minutes in refluxing THF. Remarkably, in contrast to the aforementioned ruthenium-based systems, this precatalyst is also active with internal alkynols and is able to isomerize 1,3-diphenylprop-2-yn-1-ol [i.e., PhC≡CC(OH)HPh] into a mixture of (Z)-and (E)-chalcone (i.e., PhCOCH=CHPh), albeit in moderate yield (49%), after 12 hours.…”

Ruthenium-Catalyzed Isomerizations of Allylic and Propargylic Alcohols in Aqueous and Organic Media: Applications in Synthesis