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Reaction Mechanisms Before we get into the synthetic chemistry it is a good idea to first become familiar with some of the more importatn reaction mechanisms available to transition metals. We will see these again and again as we continue in the course. I. Ligand Substitution M + L1 L2 M L2 + L1 Both associative (SN2-like) and dissociative (SN1-like) mechanisms are possible II. Oxidative Addition/Reductive Elimination often polarized, "electrophilic" M(n) + oxidative addition A B metal has been formally oxidized A M(n+2) reductive elimination usually low-valent (n = 0,1), "nucleophilic" metal coordinatively unsaturated B M–A and M–B bonds are usually strong, complex coordinatively saturated Reaction Mechanisms III. Migratory Insertion & Elimination X L L M Y M Y note cis relationship X M Y X note empty coordination site IV. Nucleophilic Attack on Ligands Coordinated to Metal reactive to nucleophiles (electron-deficient) M + X Y X Y Nuc– M unreactive to nucleophiles (electron-rich) very reactive to other electrophiles, reactivity increased if electron-deficeint M X Y Nuc often this process results in "reductive elimination" of the metal Reaction Mechanisms V. Transmetallation M1 R + M2 X + M2 R M1 X almost always the rate-limiting step, usually the culpret when catalytic processes fail M1 = Mg, Zn, Zr, B, Hg, Si, Sn, Ge M2 = transition metal VI. Electrophilic Attack on Metal Coordinated Ligands Several different reaction modes are known, will explore further later M R + E E M R Nuc– reductive elimination E R Nuc inverstion at R R retention at R attack can directly cleave M–R bond or can happen α, β, or γ to the metal Ligand Substitution Though we will be concerning ourselves more with the reactivity and synthetic utility of organimetallic complexes, understanding the mechanisms available for ligand substitution is critical to understanding how the complexes react. M L1 + L2 M L2 + L1 Associative Mechansim (SN2-like) – typically occurs with coordinatively unsaturated complexes; exemplified by 16-electron, square planar, d8 metals (Ni(II), Pd(II), Pt(II), Rh (I), Ir (I)) Lc LT M X Lc square planar (16 e–) +Y apical attack Lc LT Y M X Lc square pyramidal (18 e–) Lc LT M Lc X Lc Y LT trigonal bipyramidal (18 e–) Factors that influence the rate: – identity of the metal – identy of incoming and outgoing ligands – identy of the trans ligand ("trans effect") M X Y Lc –X apical exit Lc LT M X Y Lc Ligand Substitution Though we will be concerning ourselves more with the reactivity and synthetic utility of organimetallic complexes, understanding the mechanisms available for ligand substitution is critical to understanding how the complexes react. + L1 M L2 M L2 + L1 Dissociative Mechansim (SN1-like) – typically occurs with 18 electron coordinatively saturated complexes; often slower that associative substitution; exemplified by M(0) metal carbonyl complexes – CO +L Ni(CO)4 Ni(CO)3 LNi(CO)3 (d10, 18 e–) (d10, 16 e–) (d10, 18 e–) The rate can be accelerated by bulky ligands (loss of labile ligand relieves steric strain). This is particularly noticeable with phosphines and can be measured by the "cone angle". The electronics of the phosphine can be changed (idenpendently from sterics) by substitution. R R R P M cone angle (Θ) R θ OMe OPh Ph o-tolyl Cy t-Bu 107 128 145 194 170 182 νco (cm-1) 2079 νco (cm-1) is determined with Ni(CO)3L and is a 2085 measurement of the amount of backbonding. More 2069 donating L, more backbonding and νco decreases. – 2056 2056 Hartwig, Organotransition Metal Chemistry, 2010, pp 37–38. Ligand Substitution A "full dissociation" is not always necessary to open coordination site on an 18-electron complex. Sometimes a polydendate ligand can "slip" and free up a coordination site. This can explain some observations seen with ligands such as η3-allyl, η5-cyclopentadienyl, and η6-arene complexes. By slipping to a lower hapticity, a coordination site (or two) is opened. M M η3-allyl (2 sites) η1-allyl (2 sites) M M M η6-arene (3 sites) η4-arene (2 sites) η2-arene (1 site) +L Mn(CO)3 Mn(I), d6 18 e– Mn(CO)3 Mn(I), d6 16 e– – CO L Mn(CO)3 Mn(CO)2L Oxidative Addition/Reductive Elimination Reactions of this type are central to the synthetic utility of transition metals complexes and relies on the ability of metals to easily and reversably change oxidation states (compare to what is takes to change oxidation state of C). M(n) + oxidative addition A B A M(n+2) reductive elimination B The terms "oxidative addition" and "reductive elimination" are generic and refer only to the process of changing the oxidation state of the metal. The exact mechanism by which this occurs can vary. Oxidative Addition (OA) Metal must be coordinatively unsaturated and relatively electron rich (nucleophilic) and usually in low oxidation state (0, +1). σ-Donor ligands (PR3, R–, and H–) facilitate OA. π-Acceptor ligands (CO, CN–, alkenes) suppress OA. By the formalism used to assign oxidation state, the metal has lost two electrons during the above process (the metal has been oxidized) Metals that most commonly undergo OA reactions (other are certainly known): d10: Ni(0), Pd(0) → d8: Ni(II), Pd(II) d8: Rh(I), Ir(I) → d6: Rh(III), Ir(III) Exact mechanism by which the OA occurs depends on the nature of the substrate. Oxidative Addition/Reductive Elimination Nonpolar Electrophiles O Common examples: H2, R–H, Ar–H, R3Si–H, R3Sn–H, R2B–H, R3Sn–SnR3, R2B–BR2, RC H Generally undergo OA by concerted, one-step "insertion" mechanism. The configuration of any stereocenters would be expected to be retained. May require dissociation of a ligand from the initial complex. A–B LnM LnM A A A LnM B LnM B B "agostic" interaction (2 e–, 3 center bond) cis stereochemistry (kinetic) Examples: OC Ph3P Ir PPh3 Cl H2 H Ph3P Ph3P Ph3P Rh H Ir CO PPh3 Ph3P Cl Ph3P PPh3 Cl RCHO Ph3P Rh H PPh3 Cl PPh3 Rh R Ph3P Cl O R2BH Ph3P Ph3P H Rh Cl PPh3 BR2 Oxidative Addition/Reductive Elimination Polar Electrophiles Common examples: HX, X2, R–X, R(O)X, Ar–X, Two mechanisms are possible. One is analagous to reactions with nonpolar electrophiles (direct insertion). The other is an ionic, two-step SN2 mechanism, where the metal functions as a nucleophile and donates two electrons in the process. The configuration of any stereocenters would be expected to be inverted in this case. The structure of the electrophile determines which is active. Mn C X M C X M(n+2) C relative rates: Me > primary > secondary >> tertiary I > Br ~ OTs > Cl >> F phosphines promote with greater basicity giving faster rates X X M C Oxidative Addition/Reductive Elimination Polar Electrophiles, cont'd Examples: L OC Ir inversion Cl CH3I L CH3 L Cl Ir L OC I D Pd(0) Pt-Bu2Me H t-Bu TsO H trans (kinetic) Br Ph trans D t-Bu H TsO D Br L2Pd L2Pd H D L2Pd Br L2Pd + H Ph trans (retention) Ph ONa Ph Fe(CO)5 d8, 18 e– Ph Na2[Fe(CO)4]2– Collman's reagent "supernucleophile" R X Na[RFe(CO)4]– Further reactions possible Oxidative Addition/Reductive Elimination Polar Electrophiles, cont'd There are also examples of reactions that cannot be explained by either of these mechanisms (concerted or SN2). These have been rationalized by a radical-chain mechanism. R X hν or R O2R R + LnMn R M(n+1)Ln X R M(n+1)Ln + X R R M(n+2)Ln + R sequential 1e– oxidations, net 2e– oxidation of metal Oxidative Addition/Reductive Elimination M(n) + A oxidative addition A B M(n+2) reductive elimination B Reductive Elimination (RE) The reverse of oxidative addition. Concerted mechanism proceeds with retention of any stereochemical information. Nucleophilic attack on the ligand would invert the configuration. Factors that influence: – First row metals faster than second row, faster than third row – Electron-poor complexes react faster than electron-rich – Sterically hindered complexes reacter faster – H reacts faster than R – complexes with 1 or 3 L-type ligands faster than 2 or 4 Geometry of the complex is also quite important Ph Ph P Me Pd Me P Ph Ph fast Me Me Me Ph2P Pd Me Δ PPh2 no reaction Migratory Insertion & Eliminations Migratory Insertion In this process an unsaturated ligand (CO, RNC, alkene, alkyne) inserts into an existing M-ligand bond. The two ligands involved must be cis to one another. These are usually reversible processes. At the end of the reaction the metal is left with an empty coordination site. X L L M Y M Y X M Y X General examples: R L +L LnM R LnM C C O +L LnM A O B trans LnM A +L B R L LnM A A H trans cis R LnM H R R = aryl, alkyl, H L R B B Migratory Insertion & Eliminations Eliminations are the reverse reaction of migratory insertion and can occur one after the other. The group being eliminated does not have to be the one that participated in the insertion. There are several types of eliminations. β-Hydride Elimination (BHE) If an alkyl metal complex has hydrogens b to the metal, then this type of elimination is likely to occur. However, the β-hydrogens usually must be syn coplanar to the metal. Also the metal usually must have an open coordination site. H LnM LnM LnM H H syn coplanar BHE from transition metal-alkoxides and -amines are also important Me O LnM Me H O LnM Me +L Me H O L LnM H + M–H without using H2 β-Eliminations of alkoxides and halides are known. Me Me Migratory Insertion & Eliminations Eliminations are the reverse reaction of migratory insertion and can occur one after the other. The group being eliminated does not have to be the one that participated in the insertion. There are several types of eliminations. α-Hydride Elimination (AHE) Elimination of an α-hydrogen from metal alkyl complexes. This forms a carbene. Much slower than β-elimination processes and usually only occur when BHE is not possible. More common with early transition metals (d0, group 4 and 6), but can happen with later metals. H LnM H H H LnM Often induced by ligand exchange processes. Cp Me3P V t-Bu t-Bu + Me Me2P PMe2 Me Cp V P P Me Me t-Bu + tBuCH3 + PMe3 Nucleophilic Attack on Coordinated Ligands Many different kinds of examples of this. From our prespective the more important ones involve attack on M–CO complexes and M–alkene/alkyne complexes. Attack on Metal-Bound Carbonyl – The nucleophile is typically strong nucleophiles, like RLi LnM C O RLi O LnM Ln is good π-acceptor (another CO) usually quite stable and can be further manipulated R acyl "ate" complex Attack on M–C σ-Bonds – Such bonds are often intermediates in catalytic reactions. The carbon can be sp2 or sp3 hybridized. Nucleophilc reactions with η3-allyl complexes fall in this category. Can also be considered as a "reductive elimination" process. X L L ROH Pd Ar PdLn O + ArCO2R Nuc Nuc– M M + HX Nucleophilic Attack on Coordinated Ligands Many different kinds of examples of this. From our prespective the more important ones involve attack on M–CO complexes and M–alkene/alkyne complexes. Attack on M–C π-Bonds – By ligating the metal, alkenes and alkynes usually become electrophilic. This makes then susceptible to nucelophilic attack. Depending on how the nucleophile reacts, the addition can be syn or anti. Nuc Nuc– "external" addition of nucleophile product of anti addition (most common pathway) M M Nuc– insertion M Nuc "internal" addition of nucleophile product of syn addition M Nuc Other nucleophilic reactions will be covered as needed Transmetallation Importance is growing as this is a key step in useful methods for constructing C–C bonds, particularly such bonds that are difficult to forge by other means. However, the exact mechanism by which transmetallation occurs is not well understood and seems to be quite dependent on the metal species. M1 R + M2 X M2 R + M1 X M1 = Mg, Zn, Zr, B, Hg, Si, Sn, Ge M2 = transition metal Generally speaking, transmetallation involves replacing the halide or pseudohalide in a transition metal (M2) complex with the organic group of a "main group" organometallic (M1) reagent. This step is almost always the rate-limiting step and is usually the culpret when cross-coupling reactions fail. This is an equilibrium, so to ensure success both partners must gain some thermodynamic benefit. Often this can be enhanced by appropriate "activation" of the main group element. Isomeric integrity (cis, trans) is usually maintained when R is an olefin. With alkyl metals the situation is more complicated. With polar solvents, alkylstannanes can transmetallate with inversion of configuration (open transition state?), but in less polar solvents retention is seen (closed transition state?). However, aliphatic organoboron reagents tend to proeed with retention. R R L Pd L C SnBu3 L Pd C X SnBu3 L X proposed open t.s. leading to inversion similar mechanisms could be drawn with other metals under apprpriate activation proposed open t.s. leading to retention Electrophilic Attack on Coordinated Ligands Several different reactivity modes depending on the metal, ligand, and electrophile involved. More specific examples will be discussed as needed. Electrophilic cleavage of σ-alkyl metal bonds – Note metal is removed. R + M E+ Fe(CO)2Cp Me R M+ + E retention at R DCl D Me + CpFe(CO)2Cl Attack at α-position – Forms carbenes Ph M CHPh + Ph3C+ H M C Ph M C R + H H TfO– TMSOTf OC OC Fe CH2OH M C H+ CH2Cl2 –90 ºC OC OC Fe + CH2 Me3SiOH Electrophilic Attack on Coordinated Ligands Several different reactivity modes depending on the metal, ligand, and electrophile involved. More specific examples will be discussed as needed. Attack at β-position M H + Ph3C+ M M E E+ + M R M R E+ + M C E vinylidene MeOTf OC Mn OC Mn C Me OC OC CO2Me O CO2Me O OMe Me3OBF4 (OC)5W (OC)5W Ph (OC)5W Ph Ph Electrophilic Attack on Coordinated Ligands Several different reactivity modes depending on the metal, ligand, and electrophile involved. More specific examples will be discussed as needed. Attack at γ-position M + E+ R2 R1 + R3CHO SnBu3 M + R2 OH PdCl2(PPh3)2 R3 likely involves formation of M E A η1-allyl M B R1 intermediate B A Cp(CO)3Mo Cp(CO)3Mo + ArSO2NCO Me Me B M A N O SO2Ar