Alkynes propargyl activation

AgN02, MeOH, H2O, 24°, cool to 0°, add KCN, then HCl, 96% yield." The reduced electron density of the propargylic alkyne directs the electrophilic silver to the other alkyne and activates it for cleavage. 

AgNOs, MeOH, H2O, 24°C, cool to 0°C, add KCN, then HCl, 96% yield. The reduced electron density of the propargylic alkyne directs the electrophilic silver to the other alkyne and activates it for cleavage. These conditions also resulted in the removal of a primary TBDMS group. AgOTf can also be used, but other inert salts such as AgCl are ineffective. A procedure that does not require the use of cyanide has been developed. The process uses water as a cosolvent with acetone. Since nitric acid is generated in the reaction, TBDMS ethers were also cleaved. 

Tosylates were recently added to the family of viable migrating groups for such reactions. Gonzalez and co-workers were able to engage these substrates in different inter- and intramolecular cascade reactions, thereby expanding the scope of both NHC-Au catalysts and propargyl-activated alkynes. ... 

The heterogeneous catalytic system iron phthalocyanine (7) immobilized on silica and tert-butyl hydroperoxide, TBHP, has been proposed for allylic oxidation reactions (10). This catalytic system has shown good activity in the oxidation of 2,3,6-trimethylphenol for the production of 1,4-trimethylbenzoquinone (yield > 80%), a vitamin E precursor (11), and in the oxidation of alkynes and propargylic alcohols to a,p-acetylenic ketones (yields > 60%) (12). A 43% yield of 2-cyclohexen-l-one was obtained (10) over the p-oxo dimeric form of iron tetrasulfophthalocyanine (7a) immobilized on silica using TBHP as oxidant and CH3CN as solvent however, the catalyst deactivated under reaction conditions. 

Another example of the addition of terminal alkynes to C=N in water is the coupling of alkynes with in-situ-generated A-acylimines (Eq. 4.32) and A-acyliminium ions (Eq. 4.33). In 2002, Li et al. developed a coupling reaction of alkynes with A-acylimines and A-acyliminium ions mediated by Cu(I) in water to generate propargyl amide derivatives.57 Either an activated imine derivative or imininum derivative was proposed as the intermediate, respectively. 

The key feature of the first total synthesis of (+)-homopumiliotoxin 223G 418 was a Lewis acid-induced, chelation-controlled propargylation of the trifluoroacetate salt of (. )-2-acetyl pi peri dine 415, derived from iV-Cbz-L-pipecolinic acid. Alkyne 416 thus formed was transformed after several steps into 417, which was cyclized by activation of the primary hydroxyl with the carbon tetrabromide-triphenylphosphine system to give the natural product (Scheme 98) <1998TL2149>. 

The high-valent metal species required for activation of an alkyne has also been generated by the oxidative addition to an allylic or propargylic system. For example, with an allyl aryl ether as the substrate, this type of reaction achieves a cycloisomerization that occurs through an 0- to C-allyl migration (Equation (92)) 323,324 similarly, (9-propargyl derivatives lead to a mixture of allenyl and propargyl products (Equation (93)).325,326... 

Similar to the CuOTf/PyBox system, the CuBr/QUINAP system also gave high enantioselectivities of the three component reactions to construct propargyl amines from aldehydes, amines, and alkynes (Scheme 5.6). In this system various aldehydes including aromatic aldehydes and aliphatic aldehydes could be used and a wide range of chiral propargyl amines were prepared in good yields and enantioselectivities. Mechanistic studies showed that the dimeric Cu/QUINAP complex is the catalytically active species that differs from the previous reaction. 

This overview impressively demonstrates that Bi(III) salts are not only versatile Lewis acid catalysts for the activation of cr-donors, including benzyl and propargyl alcohols, but also efficient catalysts for the activation of Ji-donors such as styrenes or alkynes. In recent years, various environmentally benign bismuth-catalyzed methods have been developed for the alkylation of arenes, heteroarenes,... 

Quite recently, some mononuclear ruthenium complexes such as [(p-cymene)RuX-(CO)(PR3)]OTf (X = Cl, OTf, R = Ph, Cy) have been found to work as catalysts for the propargylation of aromatic compounds such as furans, where some ruthenium complexes were isolated as catalytically active species from the stoichiometric reactions of propargylic alcohols (Scheme 7.27) [31]. The produced active species promoted the propargylation of furans vdth propargylic alcohols bearing not only a terminal alkyne moiety but also an internal alkyne moiety, indicating that this propargylation does not proceed via allenylidene complexes as key intermediates. 

Catalytic transformations of alkynes have recently led to tremendous developments of synthetic methods with useful applications in the synthesis of natural products and molecular materials. Among them, the selective activations of terminal alkynes and propargylic alcohols via vinylidene- and allenylidene-metal intermediates play an important role, and have opened new catalytic routes toward anti-Markovnikov additions to terminal alkynes, carbocyclizations or propargylations, in parallel to the production of new types of molecular catalysts. 

The impressive activity achieved by Teles catalyst was improved some years later by the use of CO as an additive [92]. In this study, Hayashi and Tanaka reported a TOF of 15600h 1, at least two orders of magnitude higher than [as-PtCl2(tppts)2], for the hydration of alkynes, providing an alternative synthetic route to the Wacker oxidation. Although several solvents were tested, the best results were obtained with aqueous methanol, and sulfuric acid or HTfO as acidic promoters. Unlike Utimoto s observation, in this case terminal propargylic alcohols partially (17-20%) delivered anti-Markovnikov product, in addition to the Markovnikov species. Some years before, Wakatsuki et al. had already reported the anti-Markovnikov hydration of terminal alkynes catalyzed by ruthenium(II) [93]. 

In Section 6.3.6, it was emphasized that C02 and secondary amines could add to terminal alkynes in the presence of ruthenium catalysts to afford carbamates. Under comparable conditions (393-413 K, 5 MPa Ru-catalysts), primary amines will afford symmetrical disubstituted ureas in moderate yield [131]. It is worth noting that although the final urea does not contain the starting alkyne, its catalytic formation requires, besides the Ru-catalyst, the presence of a stoichiometric amount of a 1-alkyne (e.g., a propargylic alcohol). A possible mechanism (Scheme 6.32) for this catalytic reaction may involve activation of the alkyne at the metal center, a nucleophilic addition of the carbamate to the activated alkyne to produce... 

Shortly after this initial success, the isolation of optically active propargyl alcohols in up to 99 % ee could be effected by the use of stoichiometric amounts of (-i-)-N-methyl ephedrine (1) (Eq. 7). A wide range of aldehydes and acetylenes participate in this addition reaction affording the product alcohols in generally high yields, especially when using aldehydes that are Ca-branched (Eq. 8). Of additional importance, the reaction can be performed with functionalized alkynes, which... 

Computational studies performed on both reactions, leading either to dienyl esters or to alkenylidenecyclobutenes, show that the biscarbene ruthenium intermediate requires a high activation energy to produce the cyclobutadiene complex from terminal alkynes whereas with propargyl alcohols this step occurs readily [25],... 

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