ABSTRACT
The use of well-defined palladium(ii) complexes as precatalysts for C-X cross-coupling reactions has improved the use of palladium catalysts in organic synthesis including large-scale processes. Whereas sophisticated Pd(ii) precursors have been developed in the past years to facilitate catalyst activation as well as the handling of systems with more advanced monophosphine ligands, we herein report that simple PdCl2 complexes function as efficient precatalysts for ylide-substituted phosphines (YPhos). These complexes are readily synthesized from PdCl2 sources and form unprecedented monomeric PdCl2 complexes without the need for any additional coligand. Instead, these structures are stabilized through a unique bonding motif, in which the YPhos ligands bind to the metal through the adjacent phosphine and ylidic carbon site. DFT calculations showed that these bonds are both dative interactions with the stronger interaction originating from the electron-rich phosphine donor. This bonding mode leads to a remarkable stability even towards air and moisture. Nonetheless, the complexes readily form monoligated LPd(0) complexes and thus the active palladium(0) species in coupling reactions. Accordingly, the YPhos-PdCl2 complexes serve as highly efficient precatalysts for a series of C-C and C-X coupling reactions. Despite their simplicity they can compete with the efficiency of more complex and less stable precatalysts.
ABSTRACT
We report a series of ruthenium complexes with a tetradentate N,S-donor ligand, 2,11-dithia[3.3](2,6)pyridinophane (N2S2), that undergo single and double deprotonation in the presence of a base leading to the deprotonation of one or both pyridine rings. Both singly and doubly deprotonated complexes were structurally characterized by single-crystal X-ray diffraction. The NMR spectra are indicative of the dearomatization of one or both pyridine rings upon the deprotonation of the CH2-S arm, similar to the dearomatization of phosphine-containing pincer ligands. The deprotonated (N2S2)Ru complexes did not show appreciable catalytic or stoichiometric reactivity in transfer hydrogenation, hydrogenation and dehydrogenation of alcohols, and attempted activation of H2, CO2, and other substrates. Such a lack of reactivity is likely due to the low stability of the deprotonated species as evident from the structural characterization of one of the decomposition products in which shrinkage of the macrocyclic ring occurs via picolyl arm migration.
Subject(s)
Ruthenium , Carbon Dioxide , Hydrogenation , Ligands , Pyridines/chemistry , Ruthenium/chemistryABSTRACT
The development of homogeneous catalysts is strongly connected to the design of new, sophisticated ligands, which resolve limitations of a given reaction protocol by manipulating the electronic properties of the metal and its spatial environment. Phosphines are a privileged class of ligands that find applications in many catalytic transformations, ranging from hydrogenation reactions to hydroformylation and coupling chemistry. For many years, chemists have been trying to improve the efficiency, selectivity, and application of coupling reactions. The use of highly electron-rich and bulky phosphines was often associated with increased selectivity and efficiency and led to the development of a vast variety of electron-rich alkyl-substituted phosphines. However, this concept of increasing the ligand donor strength reaches its limits with the use of trialkyl-substituted phosphines with tri-tert-butylphosphine thus being one of the most active ligands for many years. In the course of our research efforts to use the special donor strength of ylides to stabilize electron-deficient, low-valent main group compounds, we realized that ylide-substituted phosphine (YPhos) ligands possess remarkably strong donor abilities. Moreover, the YPhos ligands are highly tunable by changing the nature of the groups on the phosphonium, phosphine, or central ylidic carbon atom. We thus obtained a ligand platform with donor capabilities ranging from PCy3 to even stronger donor abilities than N-heterocyclic carbenes, while being more sterically demanding than simple phosphines as well as many well-known biarylphosphine ligands.These properties led us to explore the applicability of the YPhos ligands in catalysis. In a series of recent reports, our group applied YPhos ligands in gold and palladium catalyzed reactions at catalytic loadings applicable for medium- to large-scale applications. The increased donor strength and unique architecture allowed for remarkable activities in a series of transformations at mild reactions conditions. For gold(I)-catalyzed reactions, we obtained turnover numbers (TONs) for the hydroamination of phenylacetylene with aniline of over 20â¯000. Also, more complex reactions were easily catalyzed with efficiencies greater than those of other known gold(I) catalysts. Similar efficacies were found in a series of palladium-catalyzed coupling reactions. In Buchwald-Hartwig aminations, unprecedented activities for the amination of aryl chlorides were reached at room temperature. The speed of formation of the catalytically active mono-YPhos palladium species allowed for some of the amination reactions to be completed in only a few minutes. Adjustment of the ligand design enabled the use of a large variety of different aryl and alkyl amines of different steric demands. Furthermore, the YPhos ligands in general showed high activities and selectivity in the coupling of a variety of carbon nucleophiles with aryl chlorides, bromides, and triflates. This enabled the development of efficient reaction protocols for the α-arylation of unhindered ketones and the coupling of Grignard and zinc reagents as well as the first efficient coupling of chloroarenes with alkyllithium compounds. This Account summarizes the recent development of YPhos ligands and their application in gold and palladium catalysis. We also hope to stimulate further use of this ligand platform in catalysis in the future.
Subject(s)
Palladium , Phosphines , Catalysis , Gold , Ligands , Palladium/chemistry , Phosphines/chemistryABSTRACT
Phosphorus ylides are 1,2-dipolar compounds with a negative charge on the carbon atom. This charge is stabilized by the neighbouring onium moiety, but can also be shifted towards other substituents thus making ylides strong π donor ligands and hence ideal substituents to stabilize reactive compounds such as cations and low-valent main group species. Furthermore, the donor strength and the steric properties can easily be tuned to meet different requirements for stabilizing reactive compounds and for tailoring the properties and reactivities of the main group element. Although the use of ylide substituents in main group chemistry is still in its infancy, the first examples of isolated compounds impressively demonstrate the potential of these ligands. This review summarizes the most important discoveries also in comparison to other substituents, thus outlining avenues for future research directions.
ABSTRACT
Single and double dearomatization of pyridine rings was observed in MnI complexes with an N2S2 pyridinophane ligand via deprotonation of one or two CH2 arms, respectively. In contrast to other N,S-donor pincer-like systems, the dearomatized (N2S2)Mn species were found to be stable, with the dearomatization being reversible.
ABSTRACT
A ruthenium(II) complex bearing a naphthyridine-functionalized pyrazole ligand catalyzes oxidant-free and acceptorless selective double dehydrogenation of primary amines to nitriles at moderate temperature. The role of the proton-responsive entity on the ligand scaffold is demonstrated by control experiments, including the use of a N-methylated pyrazole analogue. DFT calculations reveal intricate hydride and proton transfers to achieve the overall elimination of 2 equiv of H2.
ABSTRACT
The NiII complex 1 containing pyridyl- and hydroxy-functionalized N-heterocyclic carbenes (NHCs) is synthesized and its catalytic utility for the selective nitrile hydration to the corresponding amide under base-free conditions is evaluated. The title compound exploits a hemilabile pyridyl unit to interact with a catalytically relevant water molecule through hydrogen-bonding and promotes a nucleophilic water attack to the nitrile. A wide variety of nitriles is hydrated to the corresponding amides including the pharmaceutical drugs rufinamide, Rifater, and piracetam. Synthetically challenging α-hydroxyamides are accessed from cyanohydrins under neutral conditions. Related catalysts that lack the pyridyl unit (i.e., compounds 2 and 4) are not active whereas those containing both the pyridyl and the hydroxy or only the pyridyl pendant (i.e., compounds 1 and 3) show substantial activity. The linkage isomer 1' where the hydroxy group is bound to the metal instead of the pyridyl group was isolated under different crystallization conditions insinuating a ligand hemilabile behavior. Additional pKa measurements reveal an accessible pyridyl unit under the catalytic conditions. Kinetic studies support a ligand-promoted nucleophilic water addition to a metal-bound nitrile group. This work reports a Ni-based catalyst that exhibits functional hemilability for hydration chemistry.
ABSTRACT
The utility and selectivity of the catalyst [Ru(COD)(L(1))Br2] (1) bearing a fused π-conjugated imidazo[1,2-a][1,8]naphthyridine-based abnormal N-heterocyclic carbene ligand L(1) is demonstrated toward selective oxidation of CâC bonds to aldehydes and C≡C bonds to α-diketones in an EtOAc/CH3CN/H2O solvent mixture at room temperature using a wide range of substrates, including highly functionalized sugar- and amino acid-derived compounds.
