CO2 activation by electrogenerated divalent samarium for aryl halide carboxylation.

The reductive carboxylation of aryl halides has been investigated using a samarium electrode as a sacrificial anode to yield the corresponding benzoic acids, providing a smooth strategy for CO2 activation. Carboxylation occurred after an efficient reduction of carbon dioxide mediated by an electrogenerated Sm(ii)-complex acting as a strong monoelectronic reductive reagent.

Chemoselective guest-triggered shaping of a polynuclear CuII calix[6]complex into a molecular host.

A new calix[6]arene scaffold bearing a tris-imidazole binding site at the small rim and three tetradentate aza ligands at the large rim was synthesized. The system binds three CuII ions at the large rim sites and is unable to bind a fourth one, which remains in solution. The charge repulsion between the complexes, together with the flexibility of the scaffold, disorganizes the small rim site for binding and prevents its use for host-guest studies. Although the presence of MeCN or DMF guests does not alter this state, the addition of a heptylamine guest, which further displays Brønsted basicity, restores its receptor ability by stabilizing the extra CuII ion at the tris-imidazole site with concomitant guest encapsulation and binding of an exo hydroxo ligand. This chemoselective nuclearity switch yields a tetranuclear complex in which the guest backbone is preorganized in front of three potentially reactive Cu(ii) complexes, reminiscent of polynuclear CuII enzyme active sites.

Three roles for the fluoride ion in palladium-catalyzed Hiyama reactions: transmetalation of [ArPdFL2] by Ar'Si(OR)3.

From the kinetic data on the transmetalation/reductive elimination in fluoride-promoted Hiyama reactions, obtained using electrochemical techniques, it has been established that fluoride ions play three roles. F(-) reacts with trans-[ArPdBrL2] (L=PPh3) to form trans-[ArPdFL2], which reacts with Ar'Si(OMe)3 in the rate-determining transmetalation, whereas trans-[ArPdBrL2] does not react with Ar'Si(OMe)3. F(-) reacts with Ar'Si(OMe)3 to deliver the unreactive silicate Ar'SiF(OMe)3(-), thus leading to two antagonistic kinetic effects. In addition, F(-) catalyzes the reductive elimination from intermediate trans-[ArPdAr'L2].

Large yet flexible N-heterocyclic carbene ligands for palladium catalysis.

A straightforward and scalable eight-step synthesis of new N-heterocyclic carbenes (NHCs) has been developed from inexpensive and readily available 2-nitro-m-xylene. This process allows for the preparation of a novel class of NHCs coined ITent ("Tent" for "tentacular") of which the well-known IMes (N,N'-bis(2,4,6-trimethylphenyl)imidazol-2-ylidene), IPr (N,N'-bis(2,6-di(2-propyl)phenyl)imidazol-2-ylidene) and IPent (N,N'-bis(2,6-di(3-pentyl)phenyl)imidazol-2-ylidene) NHCs are the simplest and already known congeners. The synthetic route was successfully used for the preparation of three members of the ITent family: IPent (N,N'-bis(2,6-di(3-pentyl)phenyl)imidazol-2-ylidene), IHept (N,N'-bis(2,6-di(4-heptyl)phenyl)imidazol-2-ylidene) and INon (N,N'-bis(2,6-di(5-nonyl)phenyl)imidazol-2-ylidene). The electronic and steric properties of each NHC were studied through the preparation of both nickel and palladium complexes. Finally the effect of these new ITent ligands in Pd-catalyzed Suzuki-Miyaura and Buchwald-Hartwig cross-couplings was investigated.

Mechanism of palladium-catalyzed Suzuki-Miyaura reactions: multiple and antagonistic roles of anionic "bases" and their countercations.

In Suzuki-Miyaura reactions, anionic bases F(-) and OH(-) (used as is or generated from CO3(2-) in water) play multiple antagonistic roles. Two are positive: 1) formation of trans-[Pd(Ar)F(L)2] or trans-[Pd(Ar)-(L)2(OH)] (L = PPh3) that react with Ar'B(OH)2 in the rate-determining step (rds) transmetallation and 2) catalysis of the reductive elimination from intermediate trans-[Pd(Ar)(Ar')(L)2]. Two roles are negative: 1) formation of unreactive arylborates (or fluoroborates) and 2) complexation of the OH group of [Pd(Ar)(L)2(OH)] by the countercation of the base (Na(+), Cs(+), K(+)).

Autocatalytic intermolecular versus intramolecular deprotonation in C-H bond activation of functionalized arenes by ruthenium(II) or palladium(II) complexes.

The activation of the C-H bond of 1-phenylpyrazole (2) and 2-phenyl-2-oxazoline (3) by [Ru(OAc)2(p-cymene)] is an autocatalytic process catalyzed by the co-product HOAc. The reactions are indeed faster in the presence of acetic acid and water but slower in the presence of a base K2CO3. A reactivity order is established in the absence of additives: 2-phenylpyridine>2-phenyl-2-oxazoline>1-phenylpyrazole (at RT). The accelerating effect of added acetate ions reveals an intermolecular deprotonation after C-H bond activation by a cationic Ru(II) center (SE 3 mechanism). The reactions of 1-phenylpyrazole and 2-phenyl-2-oxazoline first lead to the neutral cyclometalated complexes A2 and A3 ligated by one acetate. The latter dissociate to the cationic complexes B2(+) and B3(+), respectively, and acetate. A slow incorporation of one or two D atoms into 2, 3, and 2-phenylpyridine (1) was observed in the presence of deuterated acetic acid. The "reversibility" of the C-H bond activation/deprotonation takes place from the cationic complexes Bn(+) (n=1-3). They are also involved in oxidative additions to PhI, which are rate-determining and lead to the mono- and bis-phenylated products at high temperatures. A general mechanism is proposed for the arylation of arenes 1-3 catalyzed by [Ru(OAc)2(p-cymene)]. In contrast, the reaction of Pd(OAc)2 with 2-phenylpyridine (1), is much faster: Pd(OAc)2>[Ru(OAc)2(p-cymene)]. Since the kinetics is not affected by added acetates, the reaction proceeds through a CMD mechanism assisted by a ligated acetate (intramolecular process) and is irreversible. A bis-cyclometalated Pd(II)^Pd(II) dimer D'1 is formed whose bielectronic electrochemical oxidation leads to a [Pd(III)^Pd(III)](2+) dimer, in agreement with the result of a reported chemical oxidation used in arene functionalizations catalyzed by Pd(OAc)2.

Mechanistic origin of antagonist effects of usual anionic bases (OH-, CO3(2-)) as modulated by their countercations (Na+, Cs+, K+) in palladium-catalyzed Suzuki-Miyaura reactions.

The mechanism of the reaction of trans-ArPdBrL(2) (Ar=p-Z-C(6)H(4), Z=CN, H; L=PPh(3)) with Ar'B(OH)(2) (Ar'=p-Z'-C(6)H(4), Z'=H, CN, MeO), which is a key step in the Suzuki-Miyaura process, has been established in N,N-dimethylformamide (DMF) with two bases, acetate (nBu(4)NOAc) or carbonate (Cs(2)CO(3)) and compared with that of hydroxide (nBu(4)NOH), reported in our previous work. As anionic bases are inevitably introduced with a countercation M(+) (e.g., M(+)OH(-)), the role of cations in the transmetalation/reductive elimination has been first investigated. Cations M(+) (Na(+), Cs(+), K(+)) are not innocent since they induce an unexpected decelerating effect in the transmetalation via their complexation to the OH ligand in the reactive ArPd(OH)L(2), partly inhibiting its transmetalation with Ar'B(OH)(2). A decreasing reactivity order is observed when M(+) is associated with OH(-): nBu(4)N(+) > K(+) > Cs(+) > Na(+). Acetates lead to the formation of trans-ArPd(OAc)L(2), which does not undergo transmetalation with Ar'B(OH)(2). This explains why acetates are not used as bases in Suzuki-Miyaura reactions that involve Ar'B(OH)(2). Carbonates (Cs(2)CO(3)) give rise to slower reactions than those performed from nBu(4)NOH at the same concentration, even if the reactions are accelerated in the presence of water due to the generation of OH(-). The mechanism of the reaction with carbonates is then similar to that established for nBu(4)NOH, involving ArPd(OH)L(2) in the transmetalation with Ar'B(OH)(2). Due to the low concentration of OH(-) generated from CO(3)(2-) in water, both transmetalation and reductive elimination result slower than those performed from nBu(4)NOH at equal concentrations as Cs(2)CO(3). Therefore, the overall reactivity is finely tuned by the concentration of the common base OH(-) and the ratio [OH(-)]/[Ar'B(OH)(2)]. Hence, the anionic base (pure OH(-) or OH(-) generated from CO(3)(2-)) associated with its countercation (Na(+), Cs(+), K(+)) plays four antagonist kinetic roles: acceleration of the transmetalation by formation of the reactive ArPd(OH)L(2), acceleration of the reductive elimination, deceleration of the transmetalation by formation of unreactive Ar'B(OH)(3)(-) and by complexation of ArPd(OH)L(2) by M(+).

Kinetic data for the transmetalation/reductive elimination in palladium-catalyzed Suzuki-Miyaura reactions: unexpected triple role of hydroxide ions used as base.

The mechanism of the reaction of trans-[ArPdX(PPh(3))(2)] (Ar=p-Z-C(6)H(4); Z=CN, F, H; X=I, Br, Cl) with Ar'B(OH)(2) (Ar'=p-Z'-C(6)H(4); Z'=CN, H, OMe) has been established in DMF in the presence of the base OH(-) in the context of real palladium-catalyzed Suzuki-Miyaura reactions. The formation of the cross-coupling product ArAr' and [Pd(0)(PPh(3))(3)] has been followed through the application of electrochemical techniques. Kinetic data have been obtained for the first time, with determination of the observed rate constant, k(obs), of the overall reaction. trans-[ArPdX(PPh(3))(2)] is not reactive in the absence of the base. The base OH(-) plays three roles. It favors the reaction: 1) by formation of trans-[ArPd(OH)(PPh(3))(2)], a key complex which, in contrast to trans-[ArPdX(PPh(3))(2)], reacts with Ar'B(OH)(2) (rate-determining transmetalation), and 2) by unexpected promotion of the reductive elimination from the intermediate trans-[ArPdAr'(PPh(3))(2)], which generates ArAr' and a Pd(0) species. Conversely, the base OH(-) disfavors the reaction by formation of the unreactive anionic Ar'B(OH)(3)(-). As a consequence of these antagonistic effects of OH(-), the overall reactivity is controlled by the concentration of OH(-) and passes through a maximum as the concentration of OH(-) is increased. Therefore, the base favors the rate-determining transmetalation and unexpectedly also the reductive elimination.

Aryl sulfoxides from allyl sulfoxides via [2,3]-sigmatropic rearrangement and domino Pd-catalyzed generation/arylation of sulfenate anions.

Allylic sulfoxides, via [2,3]-sigmatropic rearrangement and oxidative addition of the resulting allylic sulfenate esters to Pd(0), are found to be excellent precursors of sulfenate anions. This hitherto unknown reactivity is applied in a new Pd(0)-catalyzed domino sequence involving sulfenate anion generation followed by arylation to afford aryl sulfoxides.