Transmetalation

Transmetalation (alt. spelling: transmetallation) is a type of organometallic reaction that involves the transfer of ligands from one metal to another. It has the general form: Transmetalation (alt. spelling: transmetallation) is a type of organometallic reaction that involves the transfer of ligands from one metal to another. It has the general form: where R and R′ can be, but are not limited to, an alkyl, aryl, alkynyl, allyl, halogen, or pseudo-halogen group. The reaction is usually an irreversible process due to thermodynamic and kinetic reasons. Thermodynamics will favor the reaction based on the electronegativities of the metals and kinetics will favor the reaction if there are empty orbitals on both metals. There are different types of transmetalation including redox-transmetalation and redox-transmetalation/ligand exchange. During transmetalation the metal-carbon bond is activated, leading to the formation of new metal-carbon bonds. Transmetalation is commonly used in catalysis, synthesis of main group complexes, and synthesis of transition metal complexes. There are two main types of transmetalation, redox-transmetalation (RT) and redox-transmetalation/ligand-exchange (RTLE). Below, M1 is usually a 4d or 5d transition metal and M2 is usually a main group or 3d transition metal. By looking at the electronegativities of the metals and ligands, one can predict whether the RT or RTLE reaction will proceed and what products the reaction will yield. For example, one can predict that the addition of 3 HgPh2 to 2 Al will yield 3 Hg and 2 AlPh3 because Hg is a more electronegative element than Al. In redox-transmetalation a ligand is transferred from one metal to the other through an intermolecular mechanism. During the reaction one of the metal centers is oxidized and the other is reduced. The electronegativities of the metals and ligands is what causes the reaction to go forward. If M1 is more electronegative than M2, it is thermodynamically favorable for the R group to coordinate to the less electronegative M2. In redox-transmetalation/ligand exchange the ligands of two metal complexes switch places with each other, bonding with the other metal center. The R ligand can be an alkyl, aryl, alkynyl, or allyl group and the X ligand can be a halogen, pseudo-halogen, alkyl, or aryl group. The reaction can proceed by two possible intermediate steps. The first is an associative intermediate, where the R and X ligands bridge the two metals, stabilizing the transition state. The second and less common intermediate is the formation of a cation where R is bridging the two metals and X is anionic. The RTLE reaction proceeds in a concerted manner. Like in RT reactions, the reaction is driven by electronegativity values. The X ligand is attracted to highly electropositive metals. If M1 is a more electropositive metal than M2, it is thermodynamically favorable for the exchange of the R and X ligands to occur. Transmetalation is often used as a step in the catalytic cycles of cross-coupling reactions. Some of the cross-coupling reactions that include a transmetalation step are Stille cross-coupling, Suzuki cross-coupling, Sonogashira cross-coupling, and Negishi cross-coupling. The most useful cross-coupling catalysts tend to be ones that contain palladium. Cross-coupling reactions have the general form of R′–X + M–R → R′–R + M–X and are used to form C–C bonds. R and R′ can be any carbon fragment. The identity of the metal, M, depends on which cross-coupling reaction is being used. Stille reactions use tin, Suzuki reactions use boron, Sonogashira reactions use copper, and Negishi reactions use zinc. The transmetalation step in palladium catalyzed reactions involve the addition of an R–M compound to produce an R′–Pd–R compound. Cross-coupling reactions have a wide range of applications in synthetic chemistry including the area of medicinal chemistry. The Stille reaction has been used to make an antitumor agent, (±)-epi-jatrophone; the Suzuki reaction has been used to make an antitumor agent, oximidine II; the Sonogashira reaction has been used to make an anticancer drug, eniluracil; and the Negishi reaction has been used to make the carotenoid β-carotene via a transmetalation cascade. Lanthanide organometallic complexes have been synthesized by RT and RTLE. Lanthanides are very electropositive elements. Organomercurials, such as HgPh2, are common kinetically inert RT and RTLE reagents that allow functionalized derivatives to be synthesized, unlike organolithiums and Grignard reagents. Diarylmercurials are often used to synthesize lanthanide organometallic complexes. Hg(C6F5)2 is a better RT reagent to use with lanthanides than HgPh2 because it does not require a step to activate the metal. However, phenyl-substituted lanthanide complexes are more thermally stable than the pentafluorophenyl complexes. The use of HgPh2 led to the synthesis of a ytterbium complex with different oxidation states on the two Yb atoms: