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Development of Multi-Component Reactions using Catalytically Generated Allyl Metal Reagents Nicklas Selander Licentiate Thesis Department of Organic Chemistry Stockholm University, Sweden June 2008 Phil. Licentiate seminar will be held Friday 27 June 2008 at 10.00 in Magnélisalen Kemiska Övningslaboratoriet Svante Arrhenius väg 12A Abstract This licentiate thesis is based on the development of catalytic reactions for the synthesis and application of organometallic reagents. By use of palladium pincer-complex catalysts, we have developed an efficient procedure for the synthesis of allylboronates starting from allylic alcohols. These reactions were further extended by including various one-pot multi-component reactions, using the in situ generated allylboronates. Furthermore, novel unsymmetrical palladium pincer-complexes were synthesized and studied in auto-tandem catalysis. II Table of Contents ABSTRACT............................................................................................................................................ II TABLE OF CONTENTS .....................................................................................................................III LIST OF PUBLICATIONS ................................................................................................................. IV LIST OF ABBREVIATIONS ................................................................................................................V 1. INTRODUCTION .............................................................................................................................. 1 1.1 MULTI-COMPONENT REACTIONS .................................................................................................... 1 1.2 ALLYLIC ORGANOMETALLIC REAGENTS ......................................................................................... 2 1.2.1 ALLYLBORONATE REAGENTS IN ORGANIC SYNTHESIS ................................................................ 3 1.2.2 SYNTHESIS OF ALLYLBORONATES ............................................................................................... 4 1.3 PALLADIUM PINCER-COMPLEXES ................................................................................................... 5 2. PALLADIUM PINCER-COMPLEX-CATALYZED BORYLATION OF ALLYLIC ALCOHOLS (PAPERS I-II).................................................................................................................. 7 2.1 ALLYLIC ALCOHOLS AS SUBSTRATES IN THE CATALYTIC BORYLATION REACTION ....................... 7 2.2 SELECTIVITY AND SUBSTITUENT EFFECTS IN THE BORYLATION REACTION .................................... 9 2.3 SOLVENT EFFECTS – METHANOL AS CO-SOLVENT .......................................................................... 9 2.4 ACTIVATION OF THE HYDROXY GROUP ........................................................................................ 10 2.5 STRATEGIES FOR FINE-TUNING THE CATALYTIC ACTIVITY OF PINCER-COMPLEXES .................... 11 2.5.1 SYNTHESIS AND CHARACTERIZATION OF METHOXY SUBSTITUTED PINCER-COMPLEXES .......... 12 2.5.2 APPLICATION OF METHOXY SUBSTITUTED PINCER-COMPLEXES IN CATALYTIC ARYLATION OF VINYL EPOXIDE AND BORYLATION OF CINNAMYL ALCOHOL ............................................................. 12 3. ONE-POT ALLYLATION OF CARBONYL COMPOUNDS VIA TRANSIENT ALLYLBORONATES GENERATED BY PALLADIUM-CATALYZED SUBSTITUTION OF ALLYLIC ALCOHOLS (PAPERS III-V).......................................................................................... 15 3.1 ONE-POT ALLYLATION OF ALDEHYDES ........................................................................................ 16 3.2 ONE-POT ALLYLATION OF KETONES ............................................................................................ 20 3.3 ONE-POT SYNTHESIS OF Α-AMINO ACIDS VIA IN SITU GENERATED ALLYLBORONATES................. 21 3.4 COUPLING OF CATALYTICALLY GENERATED ALLYLBORONATES WITH IN SITU HYDROLYZED ACETALS............................................................................................................................................. 24 3.5 MECHANISTIC ASPECTS OF THE ONE-POT ALLYLATION OF CARBONYL COMPOUNDS .................. 28 4. SYNTHESIS AND TANDEM CATALYTIC PERFORMANCE OF SYMMETRICAL AND UNSYMMETRICAL SULFUR-CONTAINING PALLADIUM PINCER-COMPLEXES (PAPER VI) .......................................................................................................................................................... 32 4.1 SYNTHESIS OF THE UNSYMMETRICAL PC(H)S-PINCER PRO-LIGAND AND THE PCS-COMPLEXES . 33 4.2 CATALYTIC PERFORMANCE OF SULFUR- AND PHOSPHOROUS-BASED PINCER-COMPLEXES AS PRECATALYST IN AN ALDOL CONDENSATION ........................................................................................... 35 4.3 SCS- AND PCS-PINCER-COMPLEXES AS CATALYSTS FOR TANDEM CATALYSIS ........................... 36 4.4 MECHANISTIC CONSIDERATIONS OF THE TANDEM COUPLING REACTION ..................................... 39 5. GENERAL CONCLUSIONS AND OUTLOOK ........................................................................... 42 6. ACKNOWLEDGEMENTS ............................................................................................................. 43 7. REFERENCES.................................................................................................................................. 44 III List of Publications The thesis is based on the following papers, referred to by their roman numerals 1-VI. I. V. J. Olsson, S. Sebelius, N. Selander and K. J. Szabó: Direct Boronation of Allyl Alcohols with Diboronic Acid Using Palladium Pincer-Complex Catalysis. A Remarkably Facile Allylic Displacement of the Hydroxy Group under Mild Reaction Conditions. J. Am. Chem. Soc. 2006, 128, 4588-4589. II. J. Aydin, N. Selander and K. J. Szabó: Strategies for Fine-tuning the Catalytic Activity of Pincer-Complexes. Tetrahedron Lett. 2006, 47, 8999-9001. III. N. Selander, S. Sebelius, C. Estay and K. J. Szabó: Highly Selective and Robust Palladium-Catalyzed Carbon-Carbon Coupling between Allyl Alcohols and Aldehydes via Transient Allylboronic Acids. Eur. J. Org. Chem. 2006, 40854087. IV. N. Selander, A. Kipke, S. Sebelius and K. J. Szabó: Petasis Borono-Mannich Reaction and Allylation of Carbonyl Compounds via Transient Allyl Boronates Generated by Palladium Catalyzed Substitution of Allyl Alcohols. An Efficient One-Pot Route to Stereodefined α-Amino Acids and Homoallyl Alcohols. J. Am. Chem. Soc. 2007, 129, 13723-13731. V. N. Selander and K. J. Szabó: Single-pot Triple Catalytic Transformations Based on Coupling of in situ Generated Allyl Boronates with in situ Hydrolyzed Acetals. Chem. Commun. 2008, DOI: 10.1039/b804920c. VI. M. Gagliardo, N. Selander, N. C. Mehendale, G. v. Koten, R. J. M. Klein-Gebbink and K. J. Szabó: Catalytic Performance of Symmetrical and Unsymmetrical Sulfur-Containing Pincer Complexes: Synthesis and Tandem Catalytic Activity of the First PCS-Pincer Palladium Complex. Chem. Eur. J. 2008, 14, 4800-4809. Not included in this thesis: N. Selander and K. J: Szabó: Efficient Synthesis of α-Amino Acids via Organoboronate Reagents. ACS Symposium Series: “Current Frontiers in Asymmetric Synthesis and Application of alpha-Amino Acids. Eds: V. A. Soloshonok and K. Izawa, 2008, in press. IV List of Abbreviations cat catalyst dba dibenzylideneacetone DMSO dimethylsulfoxide L. A. Lewis acid MeOH methanol p-TsOH para-toluenesulfonic acid RT room temperature THF tetrahydrofuran TS transition state V 1. Introduction One of the most attractive tools in modern organic chemistry is the use of multi-step onepot procedures1-7 to construct densely functionalized compounds starting from simple precursors. This strategy is widely adopted by Nature, but in traditional organic synthesis, complex molecules are usually built up by stepwise formation of the individual bonds in the target structure. By using the multi-component approach, in which several reaction steps are performed in the same reaction vessel, the amount of solvents, waste and labor can be reduced. Thus, the higher efficiency is favorable from both an environmental and economical point of view. In particular, multi-component synthesis involving transition metal catalysis is a powerful combination of synthetic efficiency and highly selective transformations. Since the catalytically generated intermediates (such as organometallic compounds) need not to be isolated, but react with other components present in the reaction mixture, cumbersome purification of highly reactive species can be avoided. This thesis is focused on development of selective multi-component reactions in which an allyl metal reagent is generated in situ by palladium-catalysis. 1.1 Multi-Component Reactions In the past decades, the development of effective multi-component based synthesis has played an important role to achieve high atom economy and sustainable chemistry.1-7 The major challenges in this field are compatibility between the reagents and catalysts present to prevent catalyst inhibition and unwanted side-reactions. Furthermore, the timematching of the distinct reactions are important to avoid high concentrations of reactive intermediates which can lead to decomposition or side-reactions. The classifications found in the literature are often non-consistent and distinguishing terms such as domino, cascade, one-pot and tandem reactions (or catalysis) sometimes cause confusion. Several definitions have been proposed,2-6 and the most important ones are presented here. The term domino reactions was first defined by Tietze2 as “a process involving two or more bond-forming transformations (usually C-C bonds) which take place under the same reaction conditions without adding additional reagents and catalysts, and in which the subsequent reactions result as a consequence of the functionality formed in the previous step”. Cascade reactions usually refer to multiple domino sequences. When multi-component reactions involve transition metal-catalyzed processes, additional definitions are found.3-6 A thorough taxonomy of tandem catalysis has been reviewed by Fogg and co-workers.4 Accordingly, in tandem or domino catalyses, all catalytic species must be present from the outset. When only one catalytic transformation is performed, followed by another stoichiometric transformation, the tandem concept is not valid, but the process is a domino reaction. The definition of domino reactions proposed by Tietze2 can also be extended to catalytic protocols where the transformations are performed by a single catalytic mechanism. Tandem catalysis is defined as coupled catalyses in which sequential catalytic elaborations of the substrate occurs via two or more mechanistically distinct processes. Three different categories are proposed; Orthogonal, assisted and auto-tandem catalysis. 1 In orthogonal tandem catalysis, two different catalysts transform the substrate simultaneously. If one catalyst is able to perform two or more mechanistically distinct processes in concert, auto-tandem catalysis is operating. The catalyst can also be triggered by an additional reagent to be able to perform a second catalytic transformation, referred to as assisted tandem catalysis (Figure 1).4 Are all precatalysts present at outset? No One-pot multicatalytic reaction Yes Is more than one catalytic mechanism required? No Yes Is a single (pre)catalyst used? No Cat. A Cat. A Domino A' + B B' ( cascade ) A catalysis Mech. A Mech. A Cat. A A Orthogonal catalysis Yes Cat. B A' Mech. A No Is a trigger used to change the mechanism or to transf orm the catayst? Yes Auto-tandem catalysis Trigger Cat. A Assisted-tand em catalysis A A' Mech. A Cat. A (A') B' Mech. B Cat. B A' Mech. A Mech. B Cat. A A B' B' Mech. B TANDEM CATALYSES Figure 1. Overview of one-pot processes involving multiple catalytic transformations. Throughout this thesis, we employ this subset of definitions when applicable. 1.2 Allylic Organometallic Reagents Allylic organometallic reagents are extensively used as carbanion equivalents in organic synthesis. Their additions to aldehyde, ketone and imine electrophiles provide a valuable route to homoallylic alcohols and amines (Scheme 1). 8-14 O OH R2 2 H R1 M 1 NR3 R2 4 R1 NHR 3 R2 3 H R2 5 R1 Scheme 1. Allylation of aldehydes and imines using allylic organometallic reagents. These C-C bond forming reactions are complementary to the aldol reactions, and the introduction of a double bond in the products offers an important synthetic advantage. A wide array of metals has been utilized with different levels of selectivity. 2 1.2.1 Allylboronate Reagents in Organic Synthesis The main focus of this thesis is directed to the synthesis and highly selective transformations of allylboronates. The allylation of aldehydes by allylboronates leading to homoallylic alcohols is an important C-C bond forming reaction. Several attractive properties of allylboronates account for their popularity as synthetic intermediates in organic synthesis.8-62 Their high diastereoselectivity in the coupling reactions with aldehydes is predictable and often superior to other allylating reagents. Moreover, the allylboronates are easy to handle and less sensitive to oxidation and rearrangements than allylboranes such as 6a. The stability and reactivity of allylboron derivatives have been studied by Brown and co-workers.63 It was concluded that the stability and reactivity are highly dependent on the groups directly attached to the boron atom. Thus, the oxygen substituents found in allylboronic acids (6b) and allylboronic acid esters (6c) are important to decrease the electrophilicity of boron by donation (nπ-pπ) of electrons into the unoccupied pπ-orbital of boron. The pinacol allylboronic esters (6c) are more stable than the corresponding allylboronic acids (6b), and can be purified by column chromatography. The allylboronic acids (6b) are not stable under solvent-free conditions30,47 but can be transformed into the corresponding potassium trifluoro(allyl)borates (6d),43,44,64,65 which are isolatable air- and moisture stable species (Figure 2). OH B OH < B 6a O B < 6b < O BF3K 6c 6d Figure 2. Relative stability of allylboronic derivatives. The high diastereoselectivity in the coupling of allylboronates with aldehydes is a result of an internal activation of the aldehyde functionality by the empty pπ-orbital of boron. The addition proceeds via a compact six-membered ring transition state, where the geometry of the olefin bond determines the diastereoselectivity66 (Scheme 2). Type II L.A. O Type I OR B OR RE RCHO 2 RZ 6e RE OR B OR OH R O R E RZ 7a 4 RZ R RE R H M RZ 7b M: Si, Sn Scheme 2. Allylation of aldehydes via type I (7a) and type II (7b) mechanisms. Allylboronates add to aldehydes by a “type I” (7a) mechanism67 with high diastereoselectivity. Thus, E-allylboronate gives the anti product 4, and Z-allylboronate gives the syn isomer of 4. In contrast, allylic silanes and stannanes require an external Lewis acid activation via an open transition state 7b (type II), reducing the diastereoselectivity and predictability. 3 Although allylboronates are self-activating in their coupling with aldehydes, Hall and coworkers found that the addition of a Lewis acid catalyzes the reaction.16-20,23,24,27,28,40 It was shown that the Lewis acid interacts with the lone-pairs of the boronate oxygen (7c) and thereby renders the boron more electron deficient (Figure 3). By using chiral Brønsted acids,23,27 moderate levels of enantioselectivity were induced. Alternatively, chirality can be induced by employment of chiral diol-based boronates.17,19,20,31,40,47,49,61 RE OR B OR R O L.A RZ 7c Figure 3. Proposed Lewis acid activation in the allylation of aldehydes. Allylation reactions using imines as electrophiles, obtaining homoallylic amines have also been reported.29,31,45,58,68 Perhaps the most elegant and synthetically powerful development in this field is based on in situ generation of imines. Petasis and coworkers69-73 have shown that vinylboronic acids add to imines formed in situ from various amines (9) and glyoxylic acid (2a), to give un-natural α-amino acid derivatives (10). Virtually all types of organoboronates (8) undergo the Petasis reaction (Also referred to as the Petasis Borono-Mannich reaction), including vinyl-,70,72,74,75 aryl-72,74,76 and allylboronates46,51,52 (Scheme 3). Very recently, Schaus77 reported an asymmetric version of the Petasis reaction of vinylboronates. R-B(OH) 2 + R'2NH + HOOC-CH=O 8 9 2a NR´2 R 10 COOH Scheme 3. General scheme for the Petasis reaction affording α-amino acids. Allylation of ketones is generally much slower than the allylation of aldehydes, and the selectivity is highly dependent on the relative size of the ketone substituents. Chelating groups such as amines in α-position to the ketone functionality were shown to enhance the reactivity.41,42 Furthermore, asymmetric allylation of ketones, using chiral phosphorus-based ligands57 or diols have been reported.59,62 Kobayashi and co-workers have also found that InI catalyzes the allylboration of ketones. It was shown that allylboronates could be added to a variety of ketones under mild conditions.53 The scope of this protocol was recently extended to include N-acylhydrazones as electrophiles.55,56 1.2.2 Synthesis of Allylboronates Several methods for the synthesis of allylboronates have been reported.15,29,31,38,48,49,63,78102 The boronate functionality can either be introduced directly into the substrate (direct methods), or an organoboronate can be modified to construct an allylic system (indirect methods). In the context of this thesis, the direct methods are the most relevant, but also more synthetically interesting and general. 4 Simple, non-functionalized allylboronates such as allyl- and crotylboronates can readily be prepared by addition of reactive allylic organometallic reagents 1 such as allyllithium78-82 allyl-Grignard-49,63,78,83 or allylpotassium48,82,84-89 reagents to trialkoxyborates (11). With substituted allylic reagents, the stereo- and regioselectivity is sometimes low, giving a mixture of products 6f and 6g by metallotropic rearrangement (Scheme 4). R2 M B(OR)3 1 R 1 M = Li, Mg, K OR B OR + 2 R 11 R1 OR B OR R1 R2 6g 6f Scheme 4. Synthesis of allylboronates using highly reactive allyl metal reagents. However, the harsh conditions and the stereochemical instability66 associated with this type of reagents, limits the synthetic scope of the procedure. A more versatile strategy in the synthesis of functionalized allylboronates is the use of transition metal based catalytic transformations.29-31,38,90-103 Miyaura and co-workers96 have shown that allylic acetates 12 can be employed in a palladium-catalyzed substitution reaction using bis(pinacolato)diboron 14 to yield functionalized allylboronic esters 6h (Scheme 5). R OAc 12 [Pd(dba)2]cat O O B B O 14 O R L Pd L 13 R O B R O 6h + 15 Scheme 5. Palladium-catalyzed substitution of allylic acetates. The reaction proceeds via mono-allyl palladium intermediate 13. A drawback with this process is the formation of varying amounts of the dimer 15, resulting from transmetallation of the product to the mono-allyl palladium intermediate 13 followed by reductive allyl-allyl coupling. Notably, formation of this by-product was not observed when the borylation was carried out in the presence of an electrophile.29,31,38 1.3 Palladium Pincer-Complexes The development of highly selective and effective transition metal catalysts is an important field in organic chemistry.104-108 A key property of such catalysts is a welldefined metal-ligand bonding, which can be achieved by the use of so called “pincercomplexes”.109-121 A plethora of pincer-complexes with several different metals have been synthesized, and this thesis is focused on the application of palladium pincercomplexes (16) as highly selective catalysts in organic transformations (Figure 4). 5 R BF4PhSe Pd Cl SePh MeS 16a Pd SMe NCMe BF4PhS 16b Pd PPh 2 NCMe 16c Figure 4. Selected palladium pincer-complexes applied in this thesis. Due to the tri-coordinated ligand in the palladium pincer-complexes, the air-, moistureand thermal stability is high. Moreover, the single free coordination site is important to give robust, selective and predictable catalytic properties. Several ligands with the general structure [C6H3(CH2E)2-2,6]- have been utilized. Usually, the pincer-complexes are classified according to the hetero-atoms (E) in the side-arms of the pincer-ligand and the ipso atom (e.g. complex 16a119,122 is a SeCSe-pincer, E=Se). Another attractive feature of the pincer-complexes is the tunability of the ligand. By varying the side-arms, counter ions and aromatic backbones, the reactivity and selectivity in catalytic transformations can be altered. Furthermore, asymmetric induction by chiral ligands,123,124 and immobilization of the catalyst on a solid support125,126 have also been reported. A large number of synthetic applications using palladium pincer-complexes can be found in the literature. In the Szabó group, palladium pincer-catalysts have been used in the synthesis and transformations of organometallic reagents.30-35,37,110,123,124,127-135 As pointed out in Chapter 1.2, allylboronates are highly important reagents in organic synthesis and therefore selective methods for preparation of functionalized allylboronates are of high interest. It was shown30 that palladium pincer-complex 16a catalyses the boronate transfer from tetrahydroxydiboron (19) to allylic acetates 12, vinyl cyclopropanes 17 and aziridines 18. The initial products of these highly selective reactions are the allylboronic acids 6i, but due to their instability under solvent-free conditions, 30,47 they where instead isolated as the corresponding potassium trifluoro(allyl)borates 6j (Scheme 6). R OAc 12 EtOOC COOEt PhSe 17 Ph OH B OH Q HO Ts N 18 Pd SePh Cl 16a [ ]cat OH B B HO 19 OH 6i KHF2 Q BF3K 6j Scheme 6. Palladium pincer-complex-catalyzed synthesis of functionalized allylborates. A clear advantage of the rigid pincer architecture in these transformations is that the allylallyl coupling product 15 (Scheme 5) can be completely avoided. 6 2. Palladium Pincer-Complex-Catalyzed Borylation of Allylic Alcohols (Papers I-II) As mentioned in the introduction, allylboronates are important synthetic intermediates in organic synthesis. However, many of the existing protocols require either harsh conditions or rather exotic precursors. Thus, the functional group tolerance is sometimes low, and the poor availability of the starting materials limits the synthetic scope. Therefore, development of selective methods to prepare functionalized allylboronates from easy accessible starting materials is highly important. Allylic alcohols are one of the most attractive and readily available substrates that undergo palladium-catalyzed allylic displacement reactions.10,107,136-143 Unfortunately, the hydroxy group is one of the most reluctant leaving group in substitution reactions; and therefore, application of harsh reaction conditions, use of Lewis acids or other additives are required in these processes.136,143 However, employment of these reaction conditions and reagents precludes the efficient synthesis of unstable allyl metal derivatives, such as allylboronates, in high isolated yields. 2.1 Allylic Alcohols as Substrates in the Catalytic Borylation Reaction Previously, the Szabó group30 has shown that allylic acetates could be used as precursors in the palladium pincer-complex-catalyzed synthesis of allylboronic acids (Scheme 6). In these reactions, DMSO was used as solvent. Inspired by these results, we studied the possibility to use allylic alcohols as substrates instead of allylic acetates. We found that under the same reaction conditions used for allylic acetates, the conversions of the allylic alcohols were low. However, using methanol as a co-solvent we observed that the conversions of the allylic alcohols were significantly accelerated. Very recently, we found33 that the hydroxy to boronate substitution can be achieved under mild conditions using a wide variety of allylic alcohols 20 and diboronic acid (also called tetrahydroxydiboron, 19) with 5 mol% pincer-complex 16a in a mixture of DMSO and MeOH (Scheme 7). R HO OH 20 + OH B B HO 19 OH PhSe Pd SePh Cl [16a]cat R B(OH) 2 21a-j DMSO/MeOH KHF2 R BF3K 22a-j Scheme 7. Direct borylation of allylic alcohols. This method can be used for regio- and stereoselective synthesis of functionalized allylboronic acids 21a-j. As allylboronic acids are not sufficiently stable under solvent free conditions,30,47 compounds 21a-j were converted30,43-45,65,99,144 to their potassium trifluoro(allyl)borate derivatives 22a-j, which are useful precursors in Lewis acid and 7 transition metal-catalyzed allylation reactions.32,44,144 Because of the mild reaction conditions and the use of the highly selective (and readily available37,119) pincer-complex catalyst 16a, the products 22a-j were isolated in high yields (Table 1). Commonly used palladium(0) sources, such as Pd2(dba)3 and Pd(PPh3)4, were found to be inefficient as catalysts in the presented reactions. Table 1. Palladium-catalyzed direct borylation of allylic alcohols.a Entry 1 Ph Ph 4 OH 20a OH 2c 3 Cond. [oC/h] Substrate C5H11 C3H7 5 40/16 Allylboronic Acid Ph 40/7 50/16 B(OH)2 C5H11 21b OH 50/16 C3H7 20d OH B(OH)2 C3H7 OH 40/21 BnO 21f HO OH 20/16 HO 94 BF3K B(OH) 2 B(OH) 2 22f HO 87 BF3K 74 22g OH 87 OH B(OH)2 21h COOMe 10e BF3K 22h COOMe COOMe 50/24 20j 82 OH B(OH)2 21i OH EtOOC 20k 40/20 92 BF3K 40/16 20i 98 22e BnO 21g OH 20h HO BF3K 22d B(OH)2 60/16 90 BF3K 21e BnO 22c B(OH)2 21d OH BF3K 22b 21c 50/16 20g 11e 92 86 22a C5H11 20c 20f 9d BF3K 22a 20b OH 6 8c Ph 21a 20e 7 B(OH)2 21a Yieldb Product EtOOC 21j a EtOOC B(OH) 2 BF3K 22i 22j BF3K 77 Unless otherwise stated, the reactions of 19 and the corresponding substrates 20 were conducted in the presence of 16a (5 mol% ) in a mixture of DMSO and MeOH. After the indicated reaction times, aqueous KHF2 was added. b Isolated yield. c MeOH was used as solvent. d A mixture of DMSO and water was used as solvent. e p-toluenesulfonic acid 2.5 mol% (entry 11) or 5 mol% (entry 10) was used as co-catalyst. 8 2.2 Selectivity and Substituent Effects in the Borylation Reaction The regioselectivity in the borylation reactions (Scheme 7, Table 1) was excellent, as isomeric allylic alcohols 20a and 20b give the same regioisomer 22a. Similarly, the branched alcohol 20c and the linear alcohol 20d provide linear allylboronates 22b and 22c, respectively. Unsubstituted cyclic alcohol 20f reacted smoothly providing the corresponding boronate 22e in excellent yield. Allylic substitution in the presence of hydroxy or benzyloxy substituents leads to an increased reactivity, as substitution of 20g-i proceeded at lower temperature (20-40 °C) than the corresponding reaction of the alkyl substituted analogues 20c-f (40-60 °C). The relatively low temperature is also essential for the high isolated yields of the products, since allylic hydroxyboronates 22g-h very easily undergo hydroxy-boronate elimination to give the corresponding 1,3diene. Compounds 20g-h reacted with excellent regioselectivity to give linear products 20f-g. Interestingly, substitution of 20h resulted in mono-borylated product 22g, and thus the reaction can be used for desymmetrization of bisallyl alcohols. Borylation of cyclic substrate 20i provides a single diastereomer 22h indicating that the reaction is both regio- and stereoselective. The substitution pattern of 22h clearly shows that the reaction proceeds with allylic rearrangement and with anti substitution. For acyclic primary dialcohol 20h the borylation reaction affords the corresponding linear product 22g, however in case of cyclic analogue 20i, the directing effect of the hydroxy group leads to formation of the 1,2-substituted product 22h. Formation of this regioisomer is particularly surprising, since usual palladium-catalyzed reactions via allylpalladium complexes bearing electron-withdrawing substituents usually gives the other regioisomer, the 1,4-substituted product.107,145-147 In the presence of ester groups (20j-k), the rate of the borylation reaction drops considerably. However, we found that addition of catalytic amounts (3-5 mol %) of strong acid, such as p-toluenesulfonic acid (p-TsOH) accelerated the conversion of 20j-k, affording the corresponding borylated products 22i and 22j. Again, 22i was obtained as a single diastereomer, clearly indicating that the borylation reactions proceed with high trans regioselectivity. 2.3 Solvent Effects – Methanol as Co-solvent We found that a DMSO/MeOH mixture is indispensable to achieve high reaction rates and high yields.33 When the reactions were performed in DMSO solely, low conversions (about 5-20%) of the allylic alcohols were observed. On the other hand, catalyst 16a is poorly soluble in methanol, and therefore, only the most reactive allylic alcohols 20h-i react using methanol as solvent. As mentioned above, allylic hydroxyboronates tend to decompose to 1,3-dienes. For 20h this decomposition could to a large extent be avoided using methanol as solvent, increasing the yield of the borylation reaction. We found that in a DMSO/water mixture the conversion of 20i is slower than that in methanol; however, the corresponding boronated product 21h/22h could be obtained in high yield, indicating that 21h is stable in the presence of water as a co-solvent. 9 2.4 Activation of the Hydroxy Group In order to gain insight into the activation of the hydroxy group, we carried out competitive borylation experiments monitored by 1H-NMR (Figure 5). We have previously shown30 that cinnamyl acetate can be converted into cinnamylboronic acid 21a in the presence of catalytic amounts of 16a and 19 (Scheme 6). Surprisingly, under the same reaction conditions, cinnamyl alcohol 20a was converted significantly faster to boronic acid 21a, than cinnamyl acetate. Thus, 20a was converted quantitatively to 21a in 8 hours, while its acetate derivative was still present in the reaction mixture after 11 hours. Addition of 5 mol% of p-TsOH had a dramatic effect on the rate of the reaction, as borylation of 20a was complete in two hours, accounting for a 4-fold acceleration of the reaction. Allylboronic acid 21a was surprisingly stable even in the presence of p-TsOH, as in 9 hours only 5% of 21a was decomposed. The S-shaped curve obtained for cinnamyl alcohol (•) indicates that the reaction requires an induction period, such as activation of the hydroxy group. Alternatively, an auto-catalytic process with respect to increasing acid concentration operates (Figure 5). formation of 21a [%] 100 50 t [hours] 0 2 4 6 8 10 12 Figure 5. Formation of cinnamylboronic acid 21a from cinnamyl alcohol 20a (• , ∆) and cinnamyl acetate (□) using 19 and 5 mol % of 16a in DMSO-d6/MeOH-d4 at 55 °C. Effects of addition of 5 mol% p-TsOH (∆). The above studies clearly indicate that under the employed reaction conditions, the hydroxy group of the alcohol is converted to an excellent leaving group, which is easier to displace than the acetate functionality. A possible explanation is that 19 acts as a Lewis-acid catalyst by interacting with the free electron-pairs of the oxygen of 20a-k. A similar activation is suggested in the Tamaru reaction, employing BEt3 for activation of allylic alcohols.136-138 On the other hand, boronic acids are far less efficient Lewis-acids than alkyl (or halo) boranes. Therefore, we envision another type of activation of the hydroxy group, involving formation of allylboronic acid ester 24 (Scheme 8). This esterification is probably facilitated by inclusion of a methanol molecule in the sixmembered ring transition state (23) of the process. In 24, the hydroxy group is converted to a better leaving group, and moreover, the cleavage of the B-B bond is also facilitated by coordination of the water molecule produced in the esterification. Application of catalytic amounts of p-TsOH is supposed to catalyze the ester formation. 10 R Me O H H OH 20 + + MeOH R HO OH B B HO 19 OH - MeOH R O OH 24 O O H B OH B(OH)2 23 B OH2 B(OH) 2 Scheme 8. Proposed activation of the allylic alcohols. In summary, we have shown that allylic alcohols can be converted to functionalized allylboronates using diboronic acid 19 and catalytic amounts of pincer-complex 16a. The above presented robust catalytic transformation employs the least expensive allylic precursors reported for synthesis of functionalized allylboronates, and therefore this method is also a good example for synthesis of highly value added chemicals. 2.5 Strategies for Fine-Tuning the Catalytic Activity of Pincer-Complexes As discussed in Chapter1.3, one of the most important features of pincer-complexes is the strong terdentate coordination between the metal and the pincer-ligand. Thus, when a pincer-complex is the active catalyst in a transformation, the ligand remains tightly bound to the metal center for the entire reaction, which allows an efficient transmission of the ligand effects to the catalyst. Accordingly, the activity and selectivity of pincer-complex catalysts are expected to be efficiently fine-tuned by substituents in the pincer-ligand. However, the electronic effects of the ligand may also depend upon the location of the substituent in the pincer-complex catalyst. Our previous results30,33,130 suggested that the catalytic activity of 16a can be increased for several catalytic transformations by increasing the electron density on palladium. These studies inspired us to prepare several analogues (16d-f) of 16a (Figure 6) to investigate the electronic effects of electron donating methoxy substituents upon the catalytic activity of the complex in the borylation of allylic alcohols and the arylation of vinyl epoxides.130 OMe PhSe Pd Cl 16d OMe SePh Se MeO Pd Cl Se Se 16e OMe MeO Pd Cl 16f Se OMe Figure 6. Methoxy substituted palladium pincer-complexes applied in this study. In complex 16d, the methoxy substituent is located para to the metal, while in 16e the side arms are substituted. Expecting a synergic effect on the methoxy substitution, we also prepared complex 16f, substituted in the para position and also on the side-arms. 11 2.5.1 Synthesis and Characterization of Methoxy Substituted Pincer-Complexes Pincer-complexes 16d-f were synthesized by a slightly modified version of the procedure reported by Yao and co-workers.119 Dibromoxylene derivatives 25a-b were reacted with the appropriate diselenide (26a or 26b) to obtain pro-ligands 27b-d, which underwent a transcyclometallation reaction111,114 with 28 to give complexes 16d-f in good to excellent yields (Scheme 9). R R R' Br 26a R = H 26b R' = OMe Br 25a R = H 25b R = OMe N Pd Se 2 Se Se Cl 2 28 NaBH4 AcOH R' 16d-f yield 70-96% R' 27b R = OMe, R' = H 27c R = H, R´= OMe 27d R = R' = OMe Scheme 9. Synthesis of methoxy substituted palladium pincer-complexes. Characterization of the complexes by 77Se-NMR spectroscopy revealed an interesting trend. The 77Se-NMR shift values obtained for 16a132 (427.1 and 424.9 ppm) and 16d (427.1 and 425.7 ppm) were almost identical, while methoxy substitution of the sidearms led to an increase of the shielding of the selenium nuclei (16e, 420.5 and 419.3 ppm; 16f, 420.7 and 419.1 ppm). This indicates that only methoxy substitution of the side-arms affects the electron-density of the selenium atoms. Note that the two 77Se-NMR shift values for each complex 16a,d-f is a consequence of the two diastereomeric forms of the complexes (about 1:1 ratio). 2.5.2 Application of Methoxy Substituted Pincer-Complexes in Catalytic Arylation of Vinyl Epoxide and Borylation of Cinnamyl Alcohol Previously, we have shown that pincer-complex 16a catalyzes the ring opening of vinyl epoxides and aziridines with organoboronic acids.130 In this reaction, an electron-rich palladium centre was expected to increase the catalytic activity of the applied pincercomplex. Therefore, we investigated the effects of the methoxy substituted pincer-ligands on the catalytic ring opening of vinyl epoxide 29a with phenylboronic acid (30) (Scheme10). Ph O + PhB(OH)2 29a 30 OH [16a,d-f ]cat THF/H2O Cs2CO3 Ph Ph 31 Scheme 10. Palladium pincer-complex-catalyzed opening of vinyl epoxide. 12 The progress of the reaction (formation of 31) was monitored by 1H-NMR spectroscopy (Figure 7). 100 + + + + + + + + + + + + + + Formation of 31 [%] + + 50 + + x 0 +x 0 x x 1 2 x x x x x x x x x x x x x x t [hours] 3 4 5 6 7 8 9 10 Figure 7. Catalytic phenylation of 29a affording 31 at room temperature. Catalysts (2.5 mol %): 16a (•), 16d (+), 16e (x), and 16f (■). Under the reaction conditions applied, the complete conversion of 29a to 31 required about 10 hours using the parent catalyst 16a. Application of 16d led to a dramatic (4fold) acceleration of the process, which was completed in only two hours. Surprisingly, methoxy substitution on the side-arms of the catalyst led to a weak deactivating effect. Complex 16e proved to be slightly less reactive than the parent complex 16a, and the trimethoxy substituted catalyst 16f was less efficient than the mono-methoxy complex 16d. Subsequently, we also studied the rate of borylation of cinnamyl alcohol 20a with diboronic acid 19, in the presence of catalytic amounts of 16a, d and f (Table 1, entry 1 and Scheme 11). Ph OH 20a + HO HO B B 19 OH [16a,d,f] cat OH DMSO/MeOH Ph B(OH)2 21a Scheme 11. Palladium pincer-complex-catalyzed borylation of cinnamyl alcohol. The reaction was completed in about 8 hours using the parent catalyst 16a. Similar to the catalytic arylation of 29a, the borylation reaction was significantly accelerated using para-methoxy complex 16d. Although the acceleration in the borylation reaction was less extensive than in the ring-opening process, the catalytic transformation with the methoxy complex 16d proceeded about twice as fast as with the parent catalyst 16a. On the other hand, the reaction rate was unaffected by the methoxy substituents on the side-arms, as the reaction was completed about as quickly with 16f as with 16d (Figure 8). 13 100 + + + + + + + + + + + + Formation of 21a [%] + 50 + + + + + 0 + + 0 2 + t [hours] 4 6 8 10 12 Figure 8. Catalytic borylation of 20a to obtain cinnamylboronic acid 21a at 55°C. Catalysts (5 mol%): 16a (•), 16d (+), and 16f (■). The above results clearly indicate that the catalytic activity of pincer-complex 16a can be efficiently fine-tuned by para-substitution of the complexes. The 77Se-NMR shifts (see above) indicate that methoxy substitution of the side arms (16e and 16f) increases the electron density on the selenium atom. Nevertheless, complexes 16e and 16f do not display higher reactivity than the corresponding analogues 16a and 16d. Accordingly, the most efficient fine-tuning of the catalytic activity of pincer-complexes can be achieved by para-substitution of the aromatic ring, while substitution of the side-arms has much weaker effects on the catalytic activity. These results are also in line with previous studies on the electronic and magnetic properties of pincer-complexes. Van Koten and co-workers111 have shown that the 195Pt-NMR shifts and the natural charges on the platinum atom are in excellent correlation with the Hammet substituent constants of the para-substituents in platinum pincer-complexes. In summary, we have shown that in arylation and borylation reactions, the catalytic activity of pincer-complex 16a can be effectively increased by para-methoxy substitution of the catalyst (16d). On the other hand, methoxy substitution of the side-arms does not increase the catalytic activity of the complexes or even has a slight deactivation effect. These substituent effects probably apply to other pincer-complex-catalyzed substitution reactions, in which charge accumulation on the metal atom is required to increase the catalytic activity of the complex. 14 3. One-Pot Allylation of Carbonyl Compounds via Transient Allylboronates Generated by Palladium-Catalyzed Substitution of Allylic Alcohols (Papers III-V) The synthetic applications of allylboronates as allylating reagents were discussed in Chapter 1.2. An important feature of these reagents is their highly selective and effective carbon-carbon formation in coupling reactions with carbonyl compounds such as aldehydes, ketones and imines. As a consequence, there is a high current demand for new efficient synthetic procedures providing functionalized allylboronates. However, development of these procedures raise two important synthetic issues: (i) the synthetic procedures have to be highly stereo- and regioselective, and have to tolerate many functionalities; and (ii) the prepared functionalized allylboronates are required to be stable under the purification and isolation procedures, yet sufficiently reactive in the desired allylation reactions. The development of transition metal based synthesis of functionalized allylboronates29-31,38,90-103 is an important strategy to address problem (i) above. Considering the relatively low stability of the functionalized allylboronates, their isolation and purification often becomes a major issue [(ii) above], which may encumber the synthetic application of allylboronates. Allylboronic acids are more reactive allylating reagents46,63 than allylboronate esters, however, these species rapidly decompose (probably oxidize) under solvent free conditions.30,31,34,47 An attractive solution for the above purification issues is the development of one-pot procedures, in which the transient allylboronates are not isolated but directly reacted with the corresponding allyl acceptors.29,31,99,103,148 Development of these procedures requires highly selective formation of allylboronates and carefully designed reaction conditions to avoid undesired side products in the multi-component processes. In Chapter 2, a versatile method for preparation of functionalized allylboronates, starting from allylic alcohols, was presented. We have found35,37 that this efficient borylation procedure can be integrated in a one-pot sequence for stereo- and regioselective carboncarbon bond coupling of allylic alcohols 20 and aldehydes 2, ketones 32 or in situ generated imines (from 9 and 2a) (Scheme 12). R2-CHO 2b-e OH R2 R1 4a-i OH + 14/19 R1 20 O O B B 14 [16a,b] cat [p -TsOH] cat O HO O HO B B 19 OH R1 B(OH)2 21 not isolated OH R 3R4CO 32a-b [InI]cat R 5-NH2 9a-c HOOC CHO 2a OH R4 R3 R1 4j-l NHR 5 COOH R1 10a-h Scheme 12. One-pot transformations of in situ generated allylboronic acids. 15 The selective coupling reactions proceed via palladium pincer-complex- (16a,b) (Figure 4.) catalyzed generation of transient allylboronic acids 21 using bis(pinacolato)diboron (14) or diboronic acid (19) as boronate source. These transient intermediates are proved to be reasonably acid, base, alcohol, water and air stable species, which allows a high level of compatibility with the reaction conditions of the allylation of various aldehyde/ketone and imine electrophiles. The regio- and stereoselectivity of the reaction is excellent, as almost all products are formed as single regio- and stereoisomers. 3.1 One-Pot Allylation of Aldehydes Allylation of aldehydes using allylic alcohol as allylating reagent is a highly efficient and attractive synthetic route to functionalized homoallylic alcohols. Allylic alcohols are one of the least expensive and most accessible allylating agents, and therefore carbon-carbon couplings between allylic alcohols and aldehydes represent excellent examples for value added synthesis. However, a usual problem with these types of reactions is the activation of the allylic carbon-oxygen bond of the alcohol functionality. Many excellent solutions for this problem were presented by using palladium-catalyzed substitution9,10,13 of the in situ activated hydroxy group of the allylic alcohols. The most important strategies for activation of the hydroxy group136,149 involve application of SnCl2,139,150-152 BEt3,153-155 Et2Zn156 and various indium salts.157-159 As these transformations involve a two step procedure using Lewis acids and/or reductive organometallic reagents, the functional group tolerance of the reaction may be problematic. Another problem is often the unsatisfactorily low stereoselectivity of the reaction. The majority of these selectivity problems can be avoided by converting the hydroxy group of the allylic alcohol to a boronate. In these reactions the hydroxy group is activated by diboronic acid (Chapter 2.4), which does not affect the usual functional groups, and therefore the reaction tolerates carbonyl, cyano, aromatic halogenide and nitro groups. As the allylation proceeds via a cyclic six-membered ring TS (Scheme 2),15,18,66 the coupling of the transient allylboronate with aldehydes proceeds with a remarkably high stereoselectivity. In fact, all the presented coupling reactions of aldehydes with in situ generated allylboronates provided a single diastereomer without traces of the other isomer. Considering the allylation reactions of aldehydes with allylic alcohols, we have also extended the synthetic scope of the reactions, by application of commercially easily available diboronate 14 and a new SCS-catalyst, 16b, to accelerate the rate of the reactions (Scheme 12). The coupling reaction between the corresponding allylic alcohol 20 and aldehyde 2 can be performed as an operationally simple one-pot, one-step procedure. Accordingly, in a typical reaction, reactants 20, 14/19 and 2 and catalysts 16a-b119,122,135 (5 mol%) and pTsOH (5-20 mol%) were dissolved in a mixture of DMSO and methanol (1:1) at the outset of the reaction. After the allotted reaction times given in Table 2, the coupling products (4a-i) were isolated in good to excellent yields (Table 2). 16 Table 2. Representative entries for allylation of aldehydes via transient allylboronates.a Entry 1 b Alcohol Aldehyde Diboron Cat. O Ph OH 2f 20a 20a 3 20a 4 20a Ph 2b 2b O 5 19 16a 40/16 19 16a 40/48 14 16a 50/24 19 16a 40/16 Product OH OH C5H11 16b 14 16a 19 2e OH Br 4c OH 50/36 69 C5H11 4d OH 7 8 BnO 87 87 O 20e 96 50/24 20c OH 4a 4a 4b OH Ph 2d 88 e 93 2d 6g Ph Ph 14 Yield 4a OH Br O 20a Cond.d Ph 2b 2c c 2b 16a 77 50/16 NO2 4e OH 19 16a Ph 40/16 20g NO2 96 4f BnO OH 9g 20g 2d 19 16a 50/36 78 BnO OH 10 H 2b 19 16a 50/36 4g OH Ph 93 11 COOMe 20j 20j 2b 14 16a 50/48 4h 92 12 20j 2b 14 16b 50/6 4h OH 87 2b 19 16a 60/16 Ph 82 13 OH 20l COOMe 4h 4i In a typical reaction 20, 14/19 (1.2 equiv.) and 2 (1.2 equiv.) were dissolved in a DMSO/MeOH mixture in the presence of catalytic amounts of 16a/b and p-TsOH (each 5 mol%). b When 14 was applied, 8.0 equiv. of water and 20 mol% of p-TsOH were used. c Catalyst. d Temperature/time [°C]/[h]. e Isolated yield. f Without addition of p-TsOH . g 3.0 equiv. of aldehyde was used. a 17 We have found that primary, secondary, cyclic and acyclic alcohols react with an excellent stereo- and regioselectivity to give the branched homoallylic products exclusively. In the described processes, the homoallylic alcohol products 4a-d,f-h were obtained as single diastereomers. The reactions from acyclic allylic alcohols 20a,c,g, give the anti products, as the transformations proceed via allylboronic acids 21a,b,f (See Table 1) in which the geometry of the double bond is trans. The reaction proceeds readily and with high diastereoselectivity even for cyclic allylic alcohols as 20j. In these reactions the double bond in the cyclic allylboronic acid intermediate 21i (Table 1) has cis geometry, and thus the new carbon-carbon bond forms with syn diastereoselectivity. It is remarkable that starting from 20j, a selective tandem stereoinduction can be achieved, providing the product as a single diastereomer out of the four possible (Table 2, entry 10). The excellent stereoselectivity is a consequence of the highly stereoselective formation of the allylboronic acid intermediate 21i (Table 1) and the subsequent selective coupling with the aldehyde. Furthermore, the high selectivity was maintained even for tertiary alcohols. The reaction of alcohol 20e with aldehyde 2e resulted in formation of the branched isomer 4e exclusively, creating a new quaternary carbon center (Table 2, entry 7). As shown in Chapter 2, the transient allylboronic acids derived from the alcohols in Table 2 can be isolated and fully characterized. Probably, the only exception is the dienylboronic acid intermediate (21l) formed by borylation of 20l (Table 2, entry 13), which resisted all attempts to isolation. However, due to the one-pot/one-step conditions, the unstable 21l intermediate was allowed to react directly with 2b after its formation, and thus the corresponding product 4i could be isolated in high yield. As previously communicated,30,33 the efficient borylation procedures are based on application of diboronic acid 19, which is a highly efficient reagent in the pincercomplex-catalyzed transformation of allylic alcohols (Chapter 2) and other easily accessible substrates. Furthermore, the only by-product using 19 is non-toxic boric acid. Unfortunately, the poor commercial availability of 19 can be considered as a limiting factor and therefore we studied the possibility to replace 19 with commercially available bis(pinacolato)diboron 14. In general, diboronic reagent 14 performs much less efficiently in the pincer-complex-catalyzed borylation reactions, than 19 does.30 Accordingly, using 14 under the standard reaction conditions described above, the conversion into the homoallylic product 4 is low. We have reasoned that the in situ hydrolysis of 14 to 19 could help to improve the performance of the bispinacolato reagent 14 in the coupling reactions. We have previously reported33 that addition of water does not inhibit the robust borylation process of allylic alcohols. However, the catalytic reactions are slightly slowed down, and hence the in situ hydrolysis of 14 to 19 has to be done by addition of as small amount of water as possible. Our optimization studies showed that the best results were achieved by addition of 8 equivalents of water and increasing the amount of p-TsOH to 20 mol%. This modification did not affect the isolated yields in the coupling reaction significantly. However, the required reaction times were usually longer with 14, than with 19 (c.f entries 1 and 3, or 10-11 in Table 2). This is probably because of the decelerating effect of water in the borylation process. 18 Although the coupling reactions can be carried out in the absence of p-TsOH (Table 2, entry 2), the reaction proceeds much faster when catalytic amounts of p-TsOH is present in the reaction mixture (c.f. Table 2, entries 1-2). As pointed out in Chapter 1-2,21,24,28,33 the addition of p-TsOH has an important catalytic effect in the borylation reaction as well as in the allylation of aldehydes. Accordingly, in the procedures when bispinacolato derivative 14 is used as borylation agent, p-TsOH catalyses three distinct processes under the applied one-pot conditions: (i) hydrolysis of 14 to 19 in the presence of water, (ii) borylation of alcohol 20 to allylboronate 21 and (iii) allylation of aldehyde 2 with 21. Some structural features in the alcohol substrates, such as the presence of carboxy functionality and the cyclic topology of the substrate (20j), leads to a decrease in reactivity.33 As application of 14 in place of 19 leads to a further slowdown of the processes, some of the reactions required extended reaction times (e.g. Table 2 entry 11). We attempted to accelerate these reactions by employing other catalysts. It was found that application of SCS-catalyst 16b135 instead of 16a119 led to a much faster coupling reaction, without significant decrease of the yields. For example, the coupling reaction of cyclic substrate 20j with benzaldehyde (2b) using 14 as boronate source required 48 h using 16a as catalyst (Table 2, entry 11), while the same reaction with 16b could be completed in only 6 h (Table 2, entry 12). The obtained stereodefined and densely functionalized homoallylic products involve functionalities that directly can be employed in further catalytic processes. For example, applying 4-pentenal (2d) as aldehyde component with alcohols 20a, 20c and 20g we could perform an operationally simple one-pot synthesis of stereodefined 1,7-dienes (4c, 4d and 4g). These products can easily be cyclized (Scheme 13), affording stereodefined cyclohexene derivatives (33a-c) using Grubbs RCM procedure. 50,160 OH [34]cat CH2Cl2 Z OH Z 4c Z= Ph 33a yield (%) 96 4d Z= C5H11 33b 89 4g Z= CH2OBn 33c 97 Mes N N Mes Cl Ph Ru Cl PCy3 34 Scheme 13. Synthesis of stereodefined cyclohexenes from the products of the one-pot allylation of 2d with various allylic alcohols. In conclusion, functionalized regio- and stereodefined homoallylic alcohols may easily be prepared from aldehydes and allylic alcohols via catalytic generation of allylboronates in a one-pot sequence. The reaction displays a high functional group tolerance and broad synthetic scope, involving primary, secondary and tertiary alcohols with both cyclic and acyclic architecture. By a slight change of the reaction conditions, the one-pot procedures were performed using commercially readily available bis(pinacolato)diboron (14) in place of diboronic acid (19). Furthermore, a sulfur-based pincer-complex catalyst 16b was introduced as a complement for the very efficient and easily accessible complex 16a. 19 3.2 One-Pot Allylation of Ketones Although allylboronates do not react directly with ketone substrates,10,13 these transformations can be performed by activation of one of the reactants.42,53,57 Recently, Kobayashi and Schneider53,55,56 reported an operationally simple and elegant way to activate of allylboronates by using InI as catalyst. We have found that application of InI catalysis can also be employed for activation of allylboronic acids generated in situ from allylic alcohols (Table 3). Table 3. One-pot allylation of ketones using InI as co-catalyst.a Entry Ketone Alcohol O 1 Ph OH Ph 32a 20a 2 c Diboron Cat.b Cond. 19 16a 50/16 4j 72 e OH O 20a 19 16a 50/16 73 Ph 4k OH OH C5H11 20c Ph Ph 32b 3 Yield d Product OH 32b 19 16a 50/16 86 C5H11 4l In a typical reaction 20, and 19 (1.2 equiv.) were dissolved in a DMSO/MeOH mixture in the presence of catalytic amounts of 16a and p-TsOH (each 5 mol%). After the borylation was completed, 32a/b (1.2 equiv) and InI (20 mol%) were added. b Catalyst. c Temperature/time [°C]/[h]. d Isolated yield. e Formation of 10 % of the syn diastereomer was also observed. a The reaction was conducted similarly to the allylation of aldehydes, except that the ketone substrate (32a-b) and InI (20 mol%) was added after completion of the borylation step. This slight modification was necessary to avoid deactivation of catalyst 16a by InI in the borylation reaction. The limited number of reactions we have carried out with alcohols 20a and 20b with ketones 32a-b suggest a broad synthetic scope. The regioselectivity of the process is excellent, as the branched allylic isomer with a new quaternary carbon center is formed as the only product. The diastereoselectivity of the coupling of 20a and acetophenone (32a) is still high (Table 3, entry 1), as the two diastereomers are formed in a 9:1 ratio. As expected,10,13,161 this level of stereoselectivity is somewhat lower than in the corresponding reaction with benzaldehyde (Table 2, entry 1). The high regio- and stereoselectivity and the high yield in the presented reactions clearly shows that the one-pot allylation reactions using alcohols as allyl sources can easily be extended to ketone substrates as well. Although, the above results clearly demonstrate the benefits of the operationally simple multi-component coupling of easily available allylic alcohols and carbonyl compounds, we wished to further extend the synthetic scope of the reaction by integrating the Petasis Borono-Mannich reaction46,51,52,69-77as a crucial segment in our one-pot approach. 20 3.3 One-Pot Synthesis of α-Amino Acids via in situ Generated Allylboronates Petasis and co-workers69-73 have reported a new powerful three component method for coupling of alkenylboronic acids with amines and aldehydes to obtain homoallylic amines, including α-amino acids.162-169 This efficient coupling reaction have found many applications,70,72,74,170-173 and recently, it was also extended by Kobayashi and Thadani and their co-workers46,51,52 to coupling of allylboronates with aldehydes and ammonia. These reactions proceed with high regio- and stereoselectivity, however the synthetic scope is limited by the poor availability of functionalized allylboronates. Therefore, we decided to extend the three-component Petasis Borono-Mannich reaction to a four component coupling, involving in situ generation of the allylboronate component. As far as we know, allylic alcohols were not previously used as reagents in the allylation of imine substrates. Furthermore, the Petasis Borono-Mannich reactions were not carried out with in situ generated organoborane substrates either. We found that several elements of the above described coupling of alcohols and aldehydes can be employed in combination with the Petasis reaction. The most important difference was that amines 9a-c and glyoxylic acid (2a) were not added at the outset of the coupling reaction, but after completion of the borylation process. Addition of the amine component in the beginning of the reaction inhibited the formation of allylboronate 21. Thus, the synthesis of α-amino acids 10a-h from allylic alcohols 20 could be performed as a sequential one-pot reaction, where the in situ generated allylboronic acids were coupled with in situ formed imines 35a-c (Scheme 14). O OH + H O 2a R' OH 20 NR -H2O R-NH2 9a-c 14/19 + [16a,b] cat [p -TsOH]cat H OH not isolated O 35a-c NHR R' B(OH)2 21 not isolated R' COOH 10a-h Scheme 14. In situ formation of imines used in the Petasis reaction with in situ generated allylboronates. The structural diversity of the amino acid products 10a-h is created by the various substituents of the allylboronates 21 that can be prepared from simple precursors without cumbersome isolation and handling of the allylboronate reagents. First we studied the substrate scope of the reactions. It was found that primary (20a,g), secondary (20c,k,m) and tertiary (20e) alcohols perform equally well in the reactions, and that benzyloxy (20g) and carbethoxy/methoxy (20k,m) groups are tolerated (Table 4). 21 Table 4. Petasis Borono-Mannich reaction with in situ generated allylboronates.a Entry 1 Alcohol c d e Diboronb Cat. Cond. A Cond. B Amine Ph Ph OH H 2N 20a Ph 19 16a 40/16 HN 25/16 9a 2 3 H 2N OH 40/16 25/16 9b 19 16a 50/16 HN 25/8 9a 9a 19 14 16b 16b 50/4 50/4 25/16 25/16 19 16a 50/16 25/8 10c 10c OMe 20c H 2N HN 9c 9a 52 C5H11 10d Ph 19 16a 50/16 HN 25/24 Ph 8 BnO OH HN 9a 19 16a 40/8 25/16 Ph COOH 10f 20g BnO OH EtOOC 19 16a 50/16 25/16 MeOOC 9a 19 16a 50/16 25/16 Ph COOH 78 10g EtOOC O OH 75 Ph HN 9a 20k 10 60 COOH 10e Ph 20e 9 OMe 83 77 COOH OH 7 75 C5H11 10c 20c 20c 6 Ph COOH 20c 4 5 78 COOH 10b Ph Ph 9a C5H11 16a 76 COOH 10a Ph HN 19 Yield Ph Ph 20a f Product Ph Ph N Ph 80 COOH 10h 20m In a typical reaction 20 and 14/19 (1.2 equiv.) were dissolved in a DMSO/MeOH mixture in the presence of catalytic amounts of 16a/b and p-TsOH (each 5 mol%). After the allotted times (cond. A), 9 (2.0 equiv.) was added followed by addition of 2a (1.5 equiv.) and the reaction was continued for the times and temperatures given in column cond. B. b When 14 was applied, 8.0 equiv. of water and 20 mol% of p-TsOH were used. c Catalyst. d Temperature/time [°C]/[h] for the borylation reaction e Temperature/time [°C]/[h] for the allylation reaction f Isolated yield. All products except 10h were isolated as HCl salts. a 22 In the four-component coupling reactions we observed a stereo- and regioselectivity equivalent to the analogue coupling reaction of allylic alcohols and aldehydes. Hence, αamino acid derivatives (10a-h) were formed as single regio- and stereoisomers from readily available alcohols and amines. The benzhydryl (10a,c,e-h) and anilyl (10b) derivatives could be purified by silica gel chromatography with addition of HCl to the eluent. However, methoxy-anilyl derivative 10d displayed some tendency for decomposition and therefore it was purified by recrystallization. Accordingly, the presented reactions provide an easy access to stereodefined analogues and homologues of natural amino acids, such as phenylalanine (10a,b), isoleucine (10c,d), valine (10e), serine (10f), glutamic acid (10g) and pyroglutamic acid (10h). An interesting domino reaction can be triggered by using ester functionalized allylic alcohols 20k and 20m as precursors. When ethyl ester derivative 20k was reacted under the standard reaction conditions, glutamic acid analogue 10g was formed with high selectivity and in high yield. However, upon heating, product 10g underwent lactam formation reaction, affording pyroglutamic acid derivative 10h. Interestingly, starting from methyl ester derivative 20m, the corresponding glutamic acid analogue (10g) could not be isolated, as it underwent spontaneous cyclization affording 10h as the final product of the process. Accordingly, the reaction of 20m, 19, 9a and 2a triggers a spectacular four-step cascade, which can be performed as a one-pot reaction (Scheme 15). Ph OH ROOC HN 1) 19/[16a]ca t/[p -TsOH]c at Ph COOH 2) 9a + 2a 20k: R=Et 20m: R=Me NH2 10g, R=Et yield 78 % ROOC COOH HOOC L-Glutamic acid R=Me O N Lactam formation O Ph Ph COOH 10h yield 80 % NH COOH L-Pyroglutamic acid Scheme 15. Lactam formation in the Petasis reaction of ester substituted allylic alcohols, obtaining glutamic and pyroglutamic acid derivatives. In the coupling reactions we have employed benzyl and aryl amines 9a-c, which proved to be beneficial to avoid allylic rearrangement of the products. According to Kobayashi and co-workers,52 branched homoallylic α-amino acids with unprotected amino groups show a tendency for rearrangement to the corresponding linear isomers via aza-Cope rearrangement. This process is most extensive for products formed with quaternary carbon center,52 such as 10e (Table 4, entry 7), but even in this case, formation of the linear isomer could be avoided completely. 23 Similarly to the coupling reactions of alcohols and aldehydes (Table 2), the four component coupling reactions proceed smoothly when diboronic acid 19 is replaced with bis(pinacolato)diboron 14 (Table 4, entry 5). The required modifications of the reaction conditions, such as addition of water (8 equiv.) and increasing the catalyst loading of pTsOH (20 mol%) gave comparable isolated yields (c.f. Table 4, entries 3-5). Use of diboronic acid 19 (either directly or in situ hydrolyzed from 14) to generate the transient allylboronic acids 21 is probably an important factor to obtain high yield and reactivity in the Petasis reaction. Thadani and co-workers46 have pointed out that the analogue coupling reactions of (isolated) allylboronates with ammonia and aldehydes proceed most efficiently when allylboronic acids are used instead of allylboronic esters. This can be explained by the fact63 that allylboronic acids are more reactive in allylation reactions, than the allylboronic ester analogues. To conclude this part, we have demonstrated that the palladium pincer-complexcatalyzed borylation of allylic alcohols can be combined with the Petasis BoronoMannich reaction. The products of these one-pot multi-component reactions are densely functionalized stereodefined α-amino acids which are useful drug intermediates162-169 3.4 Coupling of Catalytically Generated Allylboronates with in situ Hydrolyzed Acetals As a part of our research program focused on development of one-pot reactions based on catalytically generated allylboronates, we have studied the possibility to use in situ hydrolyzed acetals as electrophiles. This approach is particularly useful when the acetals are more stable or more easily accessible than the requisite aldehyde. Moreover, this method gives access to novel stereodefined homoallylic alcohols, epoxides and amino alcohols. Indeed, we have found that under the reaction conditions of pincer-complex(16a-b) catalyzed borylation with bis(pinacolato)diboron (14) or diboronic acid (19), various acetals, 36a-e can readily be hydrolyzed by water in the presence of catalytic amounts of p-TsOH. (Scheme 16). R OH 14/19 + [16a,b]cat 20 R OAc 12 EtOOC COOEt + OR'' R''O R' 36 [p-TsOH]cat DMSO/MeOH/H2O OH R' R 4m-u 17 Scheme 16. One-pot allylation of in situ hydrolyzed acetals. In these processes, a broad variety of allylic substrates, including allylic alcohols (20), acetates (12) and vinyl cyclopropane (17), can be used. The overall reaction results in functionalized, regio- and stereodefined homoallylic alcohols (4). A typical reaction could be performed as a real one-pot process by mixing diboronate 14/19, pincer-catalyst 16a/b, acetal 36 and allylic substrate 12/17/20 in a mixture of DMSO, methanol and water to obtain the homoallylic alcohol products (4) in good to excellent yields (Table 5). 24 Table 5. Selective one-pot allylation of in situ hydrolyzed acetals.a Entry 1 Substrate Acetal OEt OH Ph EtO 20a 2 3d 4e NHTs MeO MeO 70/24 16a 16a 16a Ts N 92 89 4n OH 50/16 81 4o Ph OH Cl 36c Cl Yieldc 4m 70/24 Ph OMe 20a 16a Product OH NHTs Ph OH OMe 20a Cond.b 36a OEt Ts N EtO 36b 20a Cat 70/24 Ph 36d 78 4p O 5 e,f 20a 36d 16a 70/24 OH H 6 36a 16b Ph OH 29b NHTs 76 70/24 COOMe 20j 4q COOMe O 7 68 36a 12a 16b 70/16 16a 70/24 4q 73 O 8 OH OMe 36e 20n OAc 9g MeO 36a OH NHTs 70/24 12b SiMe3 11 12b 78 SiMe3 4s OH 10g 4r OH 16b 74 36b 16b 70/24 Ts N 73 SiMe3 4t OH Ts N EtOOC COOEt 36b 16b 17 70/24 COOEt 69 COOEt 4u Unless otherwise stated, the allylic substrate, 14 (1.2 equiv.) and 36 (1.2 equiv.) were dissolved in a DMSO/MeOH/H2O mixture in the presence of catalytic amounts of 16a/b (5 mol%) and p-TsOH (20 mol%). b Temperature/time [°C]/[h].c Isolated yield d Sequential one-pot reaction was performed e 50 mol%) p-TsOH was used f After in situ formation of 4p, KOH was added. g 19 and 20 mol% LiOAc was used in a sequential one-pot reaction. a 25 The use of acetals is advantageous from a synthetic point of view, since the aldehydes formed by hydrolysis of these acetals are either difficult to access (36a,b), unstable (36d) or difficult to handle (36c,e). Protected amino aldehydes 36a,b reacted smoothly under standard reactions conditions, providing ready access to various functionalized stereodefined amino alcohols 4m,n,q,s-u. Chloro substituted acetal 36d was used to prepare chlorohydrins such as 4p. By addition of base, chlorohydrin 4p can easily be converted to the corresponding epoxide 29b (Table 5, entry 5) without isolation of 4p. Thus, this procedure, involving hydrolysis of acetal 36d, borylation of alcohol 20a, their coupling to obtain 4p and the subsequent epoxide formation (29b), can be considered as a four-step, one-pot sequence. Another synthetically important transformation can be achieved using dimethoxy methane 36e, which is easier to handle and less toxic than formaldehyde. The overall result of this one-pot reaction is a homologization of the allylic substrate with allyl shift (Table 5, entry 8). Although the majority of the reactions could be performed as the above described real one-pot procedure, a sequential approach had to be applied in a few cases. Acrylaldehyde formed by hydrolysis of 36c inhibited catalyst 16, and therefore 36c was added after completion of the catalytic borylation process (Table 5, entry 3). Likewise, silyl substituted substrate 12b undergoes rapid Peterson elimination even under mild acidic conditions, and consequently, p-TsOH and acetals 36a-b had to be added after borylation of 12b (Table 5, entries 9-10). Under the neutral borylation conditions, bis(pinacolato)diboron (14) was not suitable as a boronate source, and therefore in the reactions with 12b, diboronic acid 19 was used. Interestingly, the corresponding allylboronate30 with an allylsilane functional group is stable under the mildly acidic conditions of the acetal hydrolysis and the densely functionalized products 4s-t were isolated in high yields. The above described procedure involves three individual reactions performed in concert. The first process is based on our catalytic borylation of allylic substrates (Chapter 2), to give allylboronates. As previously discussed, these processes are accelerated by catalytic amounts of p-TsOH, and can also be performed in the presence of water. These reaction components can also be used for the in situ hydrolysis of acetals 36. The aldehydes formed in this process immediately react with the allylboronate in a highly regio- and stereoselective process (Scheme 17). [p-TsOH]cat OR'' R''O R OH 20 R OAc 12 EtOOC COOEt H2O R' 36 14/19 + [16a,b] cat [p -TsOH]cat DMSO/MeOH/H2O R'CH=O not isolated 2 OH R B(OH)2 21 not isolated R' R 4m-u 17 Scheme 17. One-pot coupling of catalytically generated allylboronates and in situ hydrolyzed acetals. 26 This approach ensures that unstable or highly reactive aldehydes formed from 36 do not accumulate in the reaction mixture, leading to a smooth reaction without decomposition or catalyst inhibition. Accordingly, the homoallylic product 4 is formed as a single regioand stereoisomer, without significant formation of by-products, indicating that both the borylation and allylation processes are highly selective. Overall, the reaction can be classified as cooperative concerted catalysis3-6 involving a catalytic action by palladium pincer-complex 16 on the allylic substrate and by p-TsOH on both the allylic substrate and on acetal 36, followed by coupling of the transient allylboronate and aldehyde intermediates. Accordingly, the presented new one-pot procedure involves three perfectly synchronized catalytic actions, of which two are catalyzed by p-TsOH and one is catalyzed by pincer-complex 16. The stereo- and regiodefined products obtained in the above described operationally simple procedures are useful intermediates for advanced organic synthesis. This can be demonstrated by synthesis of stereodefined heterocyclic compounds174-177 from 4n,t,u using Hoveyda-Grubbs catalyst160,178 37 (Scheme 3). This ring-closing metathesis reaction does not affect the stereocenters of the dienes, thus it can be employed for synthesis of stereodefined azepines 38a-c, which are analogues of potent glycosidase and protein kinase inhibitors.174-176 OH Ts N R OH [37]cat R 4n R=Ph 4t R=CH2SiMe3 4u R=CH2CH(COOEt) 2 NTs yield (%) 38a 95 38b 92 38c 94 Mes N Ru Cl O i-Pr N Mes Cl 37 Scheme 18. Synthesis of stereodefined azepines by ring-closing metathesis. In summary, we have devised a new one-pot procedure for allylation of in situ hydrolyzed acetals using easy accessible substrates, such as allylic alcohols, acetates and vinylcyclopropanes. This procedure involves three individual processes under the same reaction conditions: borylation of the allylic substrates, hydrolysis of the acetals and highly selective carbon-carbon bond formation by the in situ generated allylboronates and aldehydes. This sequence of fully compatible cooperative processes involves three perfectly synchronized catalytic actions by p-TsOH and palladium-pincer-complex 16. The reaction is particularly useful for in situ generation and application of unstable and sensitive aldehydes. Because of the one-pot approach, all discrete reactions share the same solvent and at least two purification steps can be avoided. 27 3.5 Mechanistic Aspects of the One-Pot Allylation of Carbonyl Compounds In this chapter, several applications of catalytically generated allylboronates have been presented. All of these one-pot reactions are based on the versatile palladium pincercomplex-catalyzed borylation of allylic substrates presented in Chapter 2. In this section, some general mechanistic aspects of these transformations will be discussed. Although the in depth mechanistic details of the distinct chemical reactions involved in the above one-pot procedures are not fully understood, the consecutive processes and their connectivity can be described based on the above studies and literature reports on allylation reactions with allylboronates.9,10,13-15,52,66,70,72,179 Accordingly, the coupling reaction of allylic alcohols and corresponding electrophiles is initiated by the activation of the hydroxy functionality of 20 with diboronic acid 19 as proposed in Chapter 2. Diboronic acid 19 is either present as a reactant or it is generated by hydrolysis of 14. It was found that under the reaction conditions when 14 is used as a boronate source (i.e. in the presence of 8 equiv. of water and 20 mol% of p-TsOH), immediate formation of free pinacol can be observed. Hydrolysis of 14 to 19 under these conditions is probably an equilibrium process, as after extended reaction times the ratio of the boron bound and free pinacol (3:1) is about constant. We have previously suggested (Chapter 2) that the activation of the hydroxy group of 20 takes place by formation of boronic ester 39 (Figure 9). This is a very mild way of activation compared to the analogue SnCl2,139,150-152 BEt3,153-155 Et2Zn156 and indium157-159 based methods, which explains the broad synthetic scope and high functional group tolerance of the above presented reactions. R 2-CHO 2 + H2O 1 R 1 R 21 B(OH)2 + B(OH) 3 PhSe Pd SePh L 16g B2pin2 14 O OH B B HO OH 39 [p -TsOH]cat H2O B2(OH) 4 19 OH R2 4 + B(OH) 3 Allylation Activation Borylation R1 OH 20 R1 R1 R1 40 O 40 HO B L + H2O PhSe Pd SePh O B L HO B(OH)2 16h Figure 9. Plausible mechanism for the allylation of aldehydes using allylic alcohols. 28 The detailed mechanism of the catalytic formation of 21 from 39 is a subject of ongoing and future studies, however, we strongly suggest that the catalytic transfer of the boronate group from diboronic acid 19 or its derivatives (such as 14) proceeds by a similar mechanism as the analogue stannylation process. Previously, Szabó and co-workers127,131 have shown that hexamethylditin (dimetallic analogue of 19) readily reacts with pincercomplexes under stoichiometric conditions to give an η1-coordinated mono-stannyl pincer-complex, which is the tin analogue of 16h. Subsequent DFT modeling studies have shown that the stannyl group is easily transferred from palladium to the allylic position of unsaturated carbons.131 Accordingly, we suppose that the boronate group is transferred from diboronate 19 to catalyst 16g, affording η 1-boronato complex 16h. Subsequently, the boronato group substitutes the activated hydroxy group of 40 to give allylboronic acid 21 and boric acid. In the absence of aldehydes or other electrophiles, these allylboronic acid derivatives (21) can also be isolated, as described in Chapter 2. Using functionalized allylic alcohols, the borylation reaction takes place with an excellent stereo- and regioselectivity, which is very important for the subsequent allylation processes. The borylation reaction shows a clear preference for formation of the linear allylboronates, as both primary (e.g. 20a) and secondary (e.g. 20b) allylic alcohols give the corresponding terminally borylated products (Chapter 2). The next step of the process is the allylation of aldehyde 2, which proceeds with an excellent stereo- and regioselectivity, as the reaction takes place via a six-membered ring TS (Scheme 2).13,15,66,180 The very high stereoselectivity is probably explained by the fact that in the TS, the carbonyl oxygen of the aldehyde (2) and the boron atom of the allylboronate comes to a very close proximity.66,180 As the metal atoms (Si, Sn, Zn, etc) in other widely used allyl metal species are derived from higher periods of the periodical table, such close proximity between the reactants in the TS of the allylation cannot be realized.66 Therefore, the stereoselectivity in the allylation of electrophiles is much higher with allylboronates than with any other allyl metal species. Obviously, the high stereoselectivity of formation of the homoallylic products 4 is based on the availability of regio- and stereodefined allylboronic acids (21), which is delivered by the efficient pincer-complex-catalyzed borylation reaction. Moreover, in this chapter, we have also shown that acetals can be readily used as aldehyde sources. The in situ hydrolysis of the acetals is fully compatible with the catalytic borylation process, giving access to other functionalized electrophiles. Using ketones as substrates, Kobayashi and Schneider53 suggested that allylboronates are activated by InI followed by electrophilic coupling with the carbon atom of the keto functionality. In the presented reactions (Chapter 3.2, Table 3) involving ketones 32a-b allylboronic acid 21 is supposed to be activated in a similar way, and the TS geometry of the allylation is probably similar to that of the corresponding reaction with aldehydes. While the coupling of allylic alcohols with aldehydes is based on three stoichiometric components and involves two core processes (Figure 9), the use of allylic alcohols as substrates in the Petasis Borono-Mannich reaction is a four component (20, 14/19, 9 and 2a) reaction in at least three different processes: the borylation (20 → 21), imine formation (9 + 2a → 35) and allylation (21+ 35 → 10) (Figure 10). 29 HOOC-CH=NR2 R 2-NH2 + HOOC CHO 9 35 2a Imine f ormation + H2O 1 R 21 B(OH) 2 + B(OH) 3 16g NHR2 COOH R1 Allylation Borylation 10 + B(OH) 3 R1 O 40 16h B L + H2O HO Figure 10. Allylboronates derived from allylic alcohols in the Petasis reaction. The borylation process takes place similarly to the above described mechanism. However, as mentioned in Chapter 3.3, the amine component 9 and glyoxylic acid 2a cannot be added to the reaction mixture at the outset. Addition of 9 inhibits the borylation process, probably by coordination to the palladium atom of pincer-complex 16g. This coordination hinders the transmetallation of diboronate 19 to form 16h, which prevents formation of 21. On the other hand, addition of 2a alone leads to allylation of the aldehyde functionality providing the homoallylic alcohol as product. Formation of imine 35 and its addition to organoboronates is still a subject of mechanistic studies.15,170 Similarly to the studies with isolated vinyl and allylboronates, we have also observed that addition of 2a and 9 separately gives higher yields than addition of imine 35 formed in a separate process. This suggests precoordination of 9 to the boron atom of 21. Then, this imine-boronate complex undergoes the allylation process affording product 10. Coordination of 9 to 21 may explain the fact that in the presented reactions, we could not observe allylation of aldehyde 2a, whereas the in situ formation of 35 is an equilibrium process. Considering that the regio- and stereoselectivity in the formation of amino acids (10) is similar to the allylation of aldehydes, we suppose a similar type of TS structure in both processes. In the one-pot reactions we use p-TsOH as an additive, which was an important key for an efficient conversion of some allylic alcohols (Chapter 2). The acid may also be beneficial in the allylation reactions. Although allylboronates are self-activating with aldehydes, recent studies revealed16,17,40,181 that Lewis acids accelerate this reaction via activation of the allylic component as discussed in Chapter 1. This activation may be particularly important for allylation of deactivated aldehydes with sterically hindered allylboronates. We have also shown that the sulfur-based catalyst 16b, in which the counter ion is loosely coordinated, can be used to obtain faster conversions. A possible explanation of this acceleration effect can be ascribed to a facile transmetallation of the diboronic reagent due to the more accessible palladium atom in 16b. Another possibility is that 16b acts as a Lewis-acid catalyst in the allylation process. 30 In this Chapter it was shown that homoallylic alcohols and amino acids can efficiently be prepared from allylic alcohols via transient allylboronates in a one-pot sequence. The high level of compatibility of the borylation procedure with allylation of various electrophiles forms the basis of the above described reactions. This compatibility relies on three main factors: (a) the high selectivity of the pincer-complex catalyst, which does not undergo further reactions with the allylboronic acid products or other components; (b) use of 14/19 as boronate source, allowing that the only by-product of the borylation reaction is unreactive (and non-toxic) boric acid; (c) the high reactivity of the in situ formed allylboronic acids, which is accompanied with a fairly high chemical inertness, such as their acid, base, water and air stability and tolerance of alcohol as co-solvent. The reactions have a broad synthetic scope involving cyclic and acyclic alcohols, aromatic and aliphatic aldehydes, ketones and in situ formed imines. The mild conditions for activation of the allylic alcohols allow a wide range of functionalities, resulting in densely functionalized products. Due to the high regio- and stereoselectivity both in the formation of the allylboronates and in the allylation reaction, the final products are obtained as single regio- and stereoisomers. 31 4. Synthesis and Tandem Catalytic Performance of Symmetrical and Unsymmetrical Sulfur-Containing Palladium Pincer-Complexes (Paper VI) As pointed out in Chapter 1.3, palladium pincer-complexes are important as robust catalysts in various synthetically important organic reactions, including C–C and C–X bond formation reactions.109-121 One of the most attractive features is the tunability (Chapter 2.5) of the ligand as the metal center can be controlled by both the nature of the E-donor and the various substituents on the pincer-ligand (Figure 11). The catalytic activity of pincer-complexes has for example been studied in the aldol reaction126,135,182186 and in transformations involving allyl metal compounds (Chapter 2-3).30,34,123,127129,131,134,135,187 In these catalytic transformations, exclusively symmetrical aryl ECEpincer-metal catalysts (Figure 11a) were applied, due to the stability, modularity and relatively simple availability of these species. It is well documented that the σ-donor/πacceptor properties of the hetero-atoms in the pincer-complexes influence the catalytic activity.129,188,189 For example, the allylation of aldehydes and imines are readily catalyzed by PCP-pincer palladium complexes, whereas complexes with σ-donating hetero-atoms (NCN and SeCSe) displayed lower (if any) catalytic activity.32,128,129,187 Interestingly, formation of allyl metal species proceeds smoothly using NCN, SCS and SeCSe complexes, however PCP complexes display a very low activity.30,33-35,127,129,131 These observations prompted us to synthesize and explore the catalytic activity of a novel class of pincer palladium catalysts by combining the σ-donor/π-acceptor effects of the pincer-ligands. A possible way to accomplish this goal is to use the unsymmetrical ECE’pincer-complexes shown in Figure 11b. Z Z a) b) E Pd E E L E = NR2, PR2, AsR 2, OR, SeR or SR Pd E' L E = NR2, or SR E' = PR2 Figure 11. General formula for a) symmetrical and b) unsymmetrical pincer-complexes. The first unsymmetrical PCN-pincer palladium complexes were reported by Dupont and co-workers115,190 These complexes, generated by chloropalladation of hetero-substituted alkynes, proved to be highly reactive catalyst precursors in coupling of arylboronic acids with aryl chlorides. Aryl based, unsymmetrical (PCN) pincer-metal (i.e., rhodium) complexes have been reported by Milstein and co-workers,191,192 and very recently, an excellent method for synthesis of PCN-pincer palladium complexes was reported by Song and co-workers.193 32 In order to study the composite effects of electron-withdrawing and -donating side arms in palladium-catalyzed aldol reactions and transformations involving allyl metal compounds, we have designed a new aryl-based pincer-complex catalyst. Considering the synthetic aspects of obtaining such a complex (see below), we chose phosphorous as πacceptor hetero-atom and sulfur as the σ-donor, obtaining a PCS- pincer-complex. (Figure 11b, E = SPh, E’ = PPh2) We used the corresponding palladium complex as catalyst in aldol condensation of methyl isocyanoacetate with benzaldehyde as well as in tandem catalytic transformation of allyl chloride or vinyloxirane substrates with aldehyde and sulfonimine reagents. The major focus of this study is on the mechanistic aspects of having two electronically different donor atoms (phosphorous and sulfur) present in the pincer-ligand. Moreover, it was of interest to see whether the PCS-pincer palladium complex would combine the different activities and selectivities of the PCP- and SCSpincer palladium complexes in the respective C-Sn and C-C coupling reactions discussed and could thus lead to a catalytic tandem reaction. This latter aspect is particularly interesting since previous attempts to perform tandem catalytic reactions with a single, symmetrical ECE-pincer-complex failed, and synthetically useful procedures could only be performed by the simultaneous use of two different (NCN and PCP) complexes.129 In the reference reactions, we employed symmetrical SCS- and in some cases PCP-catalysts under the same reaction conditions as the PCS-pincer palladium catalyst. The catalytic performance of the SCS-complexes have previously been unexplored in synthesis and transformations of organometallic compounds. In this study, we were able to present some new interesting applications with this type of catalysts. 4.1 Synthesis of the Unsymmetrical PC(H)S-pincer Pro-ligand and the PCS-Complexes The synthesis of symmetrical pincer arene ligands typically starts from α,α’-dibromometa-xylene (25a) by nucleophilic displacement of the benzylic bromines (Chapter 2). By applying of excess of NR2-, PR2- SR- or other nucleophiles, the corresponding symmetrical ECE-pincer-ligand can be obtained in usually excellent yields.109-121 As the two bromines in 25a are symmetrically equivalent, synthesis of unsymmetrical ECE’pincer-ligands requires selective and sequential nucleophilic substitution of the benzylic leaving groups, which is obviously a more challenging task. Pro-ligand 43 was prepared in three steps from commercially available α,α’-dibromo-meta-xylene (25a). Reaction of 25a with one equivalent of in situ prepared Li–PPh2(BH3) yielded a mixture containing monophosphine 41 (63%), diphosphine [C6H4[CH2P(BH3)Ph2]2-1,3] (12%) together with unreacted 25a (25%). This mixture of compounds was used without further purification. Full conversion of the benzylic bromides into thioethers was achieved by treatment of the mixture with an excess of thiophenol in the presence of K2CO3. Separation of the resulting borane-protected PC(H)S pro-ligand 42 from the symmetrical SC(H)S- and PC(H)P-pincer arenes was carried out by column chromatography. Subsequent deprotection of the diphenylphosphino-BH3 moiety in 42 with HBF4·OEt2, followed by a basic work-up, gave the PC(H)S-pincer arene 43 as an air- and moisture sensitive white solid (Scheme 19). 33 Br Br BH3 PPh2 Br LiPPh2 . BH3 + THF –78 oC to rt + PPh2 BH3 PPh2 BH3 41 25a Br THF rt Br PhSH, K2CO3 18-Crown-6 BH3 PPh2 SPh + SPh + PPh2 BH3 PPh2 BH3 SPh 42 yield 51 % CH2Cl2 rt 1) HBF4 . Et2O 2) aq. NaHCO3 SPh PPh2 43 yield 74% Scheme 19. Synthesis of the PC(H)S-pincer arene 43. The cationic PCS-Pd(II) complex 16c was prepared via electrophilic C-H activation upon treatment of 43 with [Pd(NCMe)4](BF4)2.194 Complex 16c was readily converted into the neutral complex 16i by treatment with excess NaCl in an acetonitrile/water mixture. Both complexes were isolated as air-stable, yellow solids, which can be stored without change for months in air at ambient temperature (Scheme 20). SPh SPh [Pd(NCMe)4](BF4)2 PPh 2 43 MeCN RT Pd NCMe PPh 2 16c yield 70% BF4 SPh NaCl MeCN/H2O RT Pd PPh2 16i yield 95% Scheme 20. Synthesis of ionic 16c and neutral 16i palladium pincer-complexes. 34 Cl 4.2 Catalytic Performance of Sulfur- and Phosphorous-based Pincer-Complexes as Pre-catalyst in an Aldol Condensation The catalytic activities of the new PCS-pincer-complex 16i, and those of the known SCSand PCP-pincer-complexes 16j195,196 and 16k,197 were compared as Lewis acid precatalysts in the aldol condensation reaction of methyl isocyanoacetate (44) with benzaldehyde 2b (Scheme 21). The data reported in Scheme 21 show that PCS complex 16i is the fastest catalyst (entry 1), with a trans/cis ratio of the product 45 comparable to that obtained when the reaction is carried out with SCS-pincer palladium complex 16j (entry 2). In contrast with these results, the PCP-catalyst 16k is the slowest, also giving a different cis-trans-ratio of the products 45a/b (Scheme 21). Ph2P Pd Cl 16i SPh O OMe H + CN Ph O 44 2b PhS Pd Cl 16j SPh Ph2P [Pd]cat / i Pr2EtN Ph CH2Cl2 RT H entry [Pd]cat 1 2 16i 16j 16k 3 H Pd Cl 16k O PPh2 Ph H + O N N CO2Me MeO2C H trans cis TOF 57% 59% 45b 43% 41% 82% 18% 17 45a 75 46 Scheme 21. Aldol condensation of benzaldehyde and methyl isocyanoacetate. The turn over frequency (TOF) is given as mol of product per mol of catalyst in the first hour Previous studies126,189 have shown that 16k is the real catalyst for this reaction, whereas the SCS-pincer palladium complex 16j is in fact a pre-catalyst.126 This is indicated by the fact that complex 16j126 as well as the PCS-complex 16i (but not 16k) can be converted by the methyl isocyanoacetate substrate 44 into the corresponding 1:1 isocyanide insertion products 46a and 46b (Scheme 22). E E E' O OMe MeO N OMe Pd Cl + 2 CN O CH2Cl2 RT 44 16i E = SPh E' = PPh2 16j E = SPh E' = SPh CN Pd E' Cl 46a E = SPh E' = PPh 2 46b E = SPh E' = SPh Scheme 22. Insertion of 44 into the Pd-C bond of 16i and 16j126. 35 O Insertion of an isocyanide into the M–C bond of a cyclometallated compound has been extensively studied126,188,189 and has also been documented for ECE-pincer palladium-d8 complexes (NCN188,189 and SCS126,195,196). The fact that PCP-pincer-complex 16k appears to be stable towards insertion189 has been ascribed to the stronger P-Pd coordination of the two ortho-(diphenylphosphino)methyl substituents relative to the Pd–N and Pd–S bonding in the corresponding NCN- and SCS-pincer palladium(II) complexes. Recently, it was shown126,188,189 that a likely reaction mechanism for this insertion reaction involves coordination of the isocyanide as a ligand cis to the aryl C-atom in the symmetrical ECEpincer palladium complex (E = NMe2 or SPh), which may only occur through prior decoordination of one or both of the ortho-ligands. These findings prompted us to also study the reactivity of PCS complex 16i towards alkyl isocyanide 44 in CH2Cl2. It was found that PCS complex 16i readily reacted with isocyanide 44 to afford quantitatively complex 46a (Scheme 22), incorporating two isocyanoacetate molecules. One of the isocyanoacetates has inserted into the Pd–C bond, whereas the second one is η1-Ccoordinated to the palladium centre. Complex 46a was characterized by elemental analysis and by IR- and NMR spectroscopy. The rapid insertion of 44 into the Pd–C bond of complex 16i contrasts with the stability of 16k towards this reagent and has been ascribed to the more labile coordination of the Pd-S bond in 16j compared to that of the Pd-P one. As a consequence, in 46a it is the S-donor ligand that is the non-coordinated one. With regard to the mechanistic details of the aldol reaction catalyzed by 16i it seems likely that prior Pd-S bond cleavage occurs with η1-coordination of the incoming methyl isocyanoacetate (44). This is followed by insertion of the isocyanide into the Pd–C bond, which is followed by η1-coordination of the second molecule of 44 to give 46a (cf. reaction in Scheme 22). Subsequently, it is the η1-coordinated isocyanoacetate (44) molecule that then undergoes the aldol reaction. Consequently, the resulting isocyanoacetate (44) insertion compounds (46a-b) are the active catalysts in the aldol reaction in cases of PCS (16i) and SCS (16j) which in fact are true pre-catalysts. In contrast, the PCP-pincer-complex 16k follows a different reaction coordinate, involving halide displacement and η1-C coordination of a methyl isocyanoacetate (44).189 The catalytic results obtained with complexes 16i, 16j, and 16k in this aldol condensation show how changes in the nature of the pincer-ligand donor arms can affect the reactivity of the corresponding metal complexes. In this specific case, changing the arms from symmetrical sulfur hetero-atoms (16j) to symmetrical phosphorous hetero-atoms (16k) alters the direct interaction/reaction of these complexes with 44, and as a result alters the mechanism of the catalyzed reaction, resulting in different activities (TOFs and product selectivities). 4.3 SCS- and PCS-Pincer-Complexes as Catalysts for Tandem Catalysis As shown in Chapter 2 and in several other studies,30,33,34,129 NCN- and SeCSe-pincer palladium complexes are excellent catalysts for preparation of allyl metal species, such as allylstannanes (Scheme 23, 47 → 49a) and allylboronates. However, PCP-pincer palladium complexes are less efficient catalysts in these processes. On the contrary, allylation of aldehydes and imines (Scheme 23, 49a → 4/5) can be performed more efficiently with PCP-catalysts than with the corresponding NCN- or SeCSe-catalysts.129 36 Accordingly, we anticipated that with PCS-pincer palladium catalyst 16c it should be possible to perform both catalytic processes in tandem. Indeed, a tandem catalytic coupling of allyl chlorides (47a and 47b) and vinyloxirane (29c) with aldehyde 2e or sulfonimine 3a reagents could be achieved with hexamethylditin (48) in the presence of catalytic amounts (5 mol%) of 16c or 16l (Scheme 23, Table 6). BF4 BF4 [Pd]cat = R Ph2P Pd SPh NCMe 16c Cl + Me3Sn-SnMe3 47 48 [Pd]cat PhS Pd SPh NCMe 16l R SnMe3 49a [Pd]cat Ar-CH=Z 2e Z = O 3 Z = NSO2Ph ZH R NO2 4 or 5 Scheme 23. Tandem catalytic approach for stannylation of allyl chlorides followed by allylation of aldehydes and imines. These reactions resulted in formation of homoallylic alcohols (4v-x) and homoallylic amines (5a-b) via intermediate formation of allylstannanes (49). These processes could be performed under mild conditions (40°C) as genuine one-pot reactions in a single operational step. Accordingly, all reagents were mixed together at the outset of the reaction, and after the allotted reaction time (16h) the products (4 or 5) were isolated. The reactions with allyl chloride (47a) proceeded cleanly and with relatively high isolated yields of 63-78% (Table 6, entries 1 and 3). When a substituted allyl chloride (such as cinnamyl chloride, 47b) was used, the yields dropped slightly (59-60%), but they still remained respectable, considering that the product is formed in a tandem catalytic process (Table 6, entries 5 and 7). The diastereoselectivity of the reaction is poor in the case of allylation of 4nitrobenzaldehyde (2e, entry 5), but it is rather promising for allylation of sulfonimine 3a (entry 7). The major diastereomer is the anti form in the case of allylation of 2e and the syn form in that of allylation of 3a. Previously, we have studied128,134 the roles of steric and electronic interactions in determining the stereoselectivity in pincer-complexcatalyzed allylation reactions. These studies have clearly shown that the allylation of aldehydes (such as 2e) proceeds with anti selectivity, while the opposite (syn selectivity) occurs for the corresponding process with imine substrates (such as 3a). These previous observations128,134 are in perfect agreement with the stereoselectivity observed in the presented processes catalyzed by 16c and 16l (Table 6). 37 Table 6. Tandem catalytic transformations of allylic substrates.a Entry Substrate Electrophile Cat. Cond.b 16c 40/16 Product OH O Cl 1 2 47a 47a 3 47a 4 5 2e 2e NSO2Ph 3a 3a 47a Ph Cl 2e NO2 16l 40/16 16c 40/16 4v 4v NHSO2Ph NO2 16l 40/16 16c 40/16 5a 5a OH Ph 47b 6 4w 2e 47b 16l 40/16 Yieldc drd 63 - 80 - 78 - 73 - 59 3:1 74 9:1 60 1:5 48 1:4 46 5:3 57 3:1 NO2 NO2 NO2 4w NHSO2Ph 7 47b 3a 16c 40/16 Ph 8 47b O 9[e] 10 [e] a d 29c 29c 3a 16l 40/16 2e 16c 20/16 5b 5b OH HO 2e 16l 20/16 4x 4x NO2 NO2 In a typical reaction, 5 mol% catalyst was used in THF. b Temperature/time [°C]/[h].c Isolated yield Diastereomeric ratio: anti/syn. e LiOAc (10 mol%) and water (2 equiv) were also added to the reaction. As previously reported,110,129 symmetrical PCP-pincer palladium complexes do not catalyze the formation of the intermediate allylstannanes (Scheme 23, 47 → 49), and so these complexes alone cannot be used as catalysts for coupling of allyl chlorides and aldehydes in the presence of hexamethylstannane 48. Therefore, reactions with PCP complex 16k as reference catalyst were not performed in this study. On the other hand we also studied the catalytic performance of SCS-pincer-complex 16l. To our delight, this complex showed a high catalytic activity, comparable to that of PCS-pincer-complex 16c (entries 2, 4, 6 and 8). The high activity of SCS complex 16l in the tandem catalytic reactions is surprising, because symmetrical ECE-pincer-complexes with σ-donor heteroatoms (e.g. NCN) usually perform poorly128,134,187 in the allylation step (Scheme 23, 49 → 4/5). The isolated yields obtained with the SCS-pincer-complex 16l are particularly high for allylation of aldehyde 2e, while the stereoselectivity using 47b as allyl substrate is even higher than with the PCS-pincer-complex 16c (entry 6). However, in the allylation reaction of sulfonimine 3a the PCS-pincer-complex 16c clearly outperforms 38 16l. The homoallylic amines 5a and 5b (entries 3-4 and 7-8) are formed in higher yields with PCS-catalyst 16c (78 and 60%) than with the SCS-catalyst 16l (73 and 48%). In particular, when the tandem reaction of 47b and 3a was catalyzed with SCS-catalyst 16l (entry 8), a substantial amount of cinnamyl stannane (49a R = Ph) was present in the crude reaction mixture. This finding indicates that the allylation process (Scheme 23, 49 → 5b) of the imine by cinnamyl stannane proceeds very slowly in the presence of 16l as catalyst. We have also succeeded in performing a tandem catalytic coupling reaction of vinyloxirane (29c) with 2e (entries 9 and 10). This reaction proceeds under reaction conditions similar to those used for the allylation with allyl chlorides, except that catalytic amounts of LiOAc and water were added to the reaction mixture. Without this addition of LiOAc and water, vinyloxirane (29c) is decomposed by the catalysts, probably through opening of the epoxy functionality. The coupling reaction of aldehyde 2e with vinyloxirane (29c) leads to formation of an unprotected homoallylic diol (4x), which is a useful synthetic intermediate. As far as we know, this reaction represents the first example of a palladium-catalyzed coupling of a vinyloxirane with an aldehyde to afford homoallylic alcohol 4x. 4.4 Mechanistic Considerations of the Tandem Coupling Reaction On the basis of the above results and our previous mechanistic and modeling studies128,131,134 it is possible to propose a plausible catalytic cycle for the tandem C-Sn and C-C processes (Scheme 24). The first catalytic process is formation of the allylstannane intermediate 49 from allyl chloride 47 (or vinyloxirane 29c) and hexamethylstannane 48. This catalytic reaction is initiated by transmetallation of catalyst 16m with 47 to afford complex 16n and trimetyltin chloride. Formation of a trimethyltinpalladium pincer-complex under similar reaction conditions has been observed for NCNpincer palladium complexes.131 Complex 16n undergoes a nucleophilic substitution reaction with allyl chloride, furnishing allylstannane 49 and recovering PCS-pincer palladium complex 16m. The regenerated catalyst 16m is able to undergo transmetallation with allylstannane 49 to give η1-allylpalladium complex 16o. Similar transmetallation reactions were previously reported for PCP-pincer-complexes and allylstannanes.128 In those studies it was concluded128,187 that complexes with heteroatoms exhibiting π-accepting properties in the ortho-substituents (such as symmetrical PCP-pincer-complexes) undergo more facile transmetallation than the corresponding analogues with strongly σ-electron donating ortho-ligands (such as NCN). Considering this, the presence of at least one phosphorous atom in 16c probably allows an efficient transmetallation. On the other hand, the relatively low catalytic activity of 16l in the allylation step (entry 8) may be due to a slow transmetallation of the stannane intermediate 49 to the palladium atom, which is attached to an electron-rich SCS-pincerligand. According to our mechanistic and modeling studies128,134 these η1-allylpalladium complexes readily react with aldehyde or imine electrophiles (2e or 3a). Thus electrophilic substitution by complex 16o gives 50, which subsequently undergoes decomplexation to provide the homoallylic alcohol or amine products (4 or 5) and to regenerate catalyst 16m once again. In this way complex 16m performs as an autotandem catalyst4 controlling two bond formation processes: the stannylation (Sn-C bond 39 formation) of the allyl chloride and the electrophilic substitution (C-C bond formation) of the allylstannane intermediate. Our studies show that the stannylation process (47 → 49) using PCS-catalyst 16c is much faster than the catalytic allylation (49 → 4/5). It was found that in the presence of 16c under the applied reaction conditions (entry 1), but in the absence of an electrophile (e.g. 2e), allyl chloride (47a) was converted into allylstannane (49a) in 30 min, while the full reaction time required for coupling of 48a with 2e is 16 h. This indicates that the catalytic generation of the allyl stannane (49) is completed before significant progress in the allylation has taken place (Scheme 24). Ar-CH=Z 2e or 3a Me3SnCl Ph2P Pd SPh Cl R Me3SnCl 47 SnMe3 R 49 16o R Carbon-carbon coupling Ph2P Pd Stannylation SPh Ph2P Pd SPh SnMe3 16n L 16m ZH Ph 2P Me3Sn Pd Z Ar SPh Cl Ar H2O R 4 or 5 (SnMe3)2 + Me3SnOH Me3SnCl 48 R 50 Scheme 24. Proposed catalytic cycle of the auto-tandem reaction. In summary, aryl-based, unsymmetrical PCS-pincer palladium complexes 16c and 16i were prepared in relatively simple four and five step synthesis sequences, respectively (Scheme 20). These PCS-pincer-complexes, as well as SCS-pincer-complex 16j, proved to be efficient catalysts in the aldol reaction between benzaldehyde and methyl isocyanoacetate, but are obviously pre-catalysts because the methyl isocyanoacetate reactant converts the pincer-catalyst into a ketimine-palladium catalyst. In the aldol condensation reaction the PCS complex gave higher turnover numbers than its PCP and SCS counterparts. The combination of a sulfur and a phosphorus hetero-atom in the side arms, such as in complex 16c, results in a synergetic effect. This effect involves two major components: a weak coordination of the sulfur atom allowing insertion of 44, as well as a strong coordination of the phosphorus atom, which increases the rate of the catalytic process. 40 In the auto-tandem catalytic coupling of allyl chlorides or vinyloxirane with aldehyde or sulfonimine substrates, both 16c and 16l are the true catalytic species. Comparative studies using symmetrical PCP- and SCS-pincer palladium complexes show that a strong synergistic effect is also operative in these catalytic reactions. In the tandem catalytic stannylation and allylation process of allyl chlorides (Table 6) the PCS complex performs much better than the PCP analogue.129 Although, the SCS complex has a surprisingly high catalytic activity, the PCS complex is more efficient in allylation of sulfonimines. In these processes, the PCS-catalyst unifies the attractive catalytic features of the symmetrical analogues: firstly, a high catalytic activity in the stannylation reaction, in which symmetrical complexes with electron-donating hetero-atoms and a weaker coordination interaction to the palladium centre (e.g. NCN or SCS) performs well, and secondly, the more efficiently catalyzed allylation of the electrophile by less electron rich pincer-complexes in which the hetero-atom has a stronger interaction with palladium (i.e. as in PCP). 41 5. General Conclusions and Outlook In this thesis, it was demonstrated that palladium pincer-complexes can be used as highly selective catalysts for synthesis and transformations of organometallic reagents. A novel and versatile method for the preparation of functionalized allylboronates starting from allylic alcohols was presented. Because of the mild conditions and reagents used, this procedure could successfully be combined with several one-pot domino transformations. The basis of these protocols is the clean transformations performed by the highly selective palladium pincer-catalysts. We have shown that the in situ generated allylboronates can be isolated as potassium trifluoro(allyl)borates (A), reacted with ketone (B) or aldehyde (C) electrophiles, or in the Petasis Borono-Mannich reaction (D). The one-pot approach of these transformations is an important key to avoid isolation and purification of the reactive allyl metal intermediates. The products of these reactions are stereodefined densely functionalized homoallylic alcohols or amino acid derivatives (Scheme 25). R [Pd]cat. O NHR' O O OH R' OH B OH R D R B2(OR)4 OH R'NH2 + H COOH OH R' C B KHF2 O R' BF3K OH R'' [InI]cat R R A R R' R'' Scheme 25. Overview of the presented reactions. Moreover, a new procedure for the synthesis of novel unsymmetrical pincer-complexes was presented. These complexes were able to perform an auto-tandem catalytic transformation of allyl chlorides via allylstannanes which were used as allylating reagents in the same reaction vessel. We believe that the clean and selective transformations performed by the studied palladium pincer-complexes can be extended further to involve other type of domino and tandem reactions. The possibility to induce chirality in the above presented reactions is a challenge in future projects. In order to develop such processes, an important factor is to gain a higher insight in the mechanism of the reactions. 42 6. Acknowledgements I would like to thank: My research advisor Prof. Kálmán J. Szabó for inspiration and excellent guidance Prof. Jan-Erling Bäckvall for showing interest in this thesis My co-workers Dr. Sara Sebelius, Vilhelm J. Olsson, Juhanes Aydin, Dr. Marcella Gagliardo, Andreas Kipke, Cesar Estay and Helena Larsson My Dutch co-workers Dr. Marcella Gagliardo, Dr. Nilesh C. Mehendale, Prof. Gerard van Koten and Prof. Robertus J. M. Klein Gebbink, Utrecht University, The Netherlands All the past and present members of the Szabó group Vilhelm J. Olsson and Dr. Niclas Solin for proof-reading The TA staff and Kemiska biblioteket All colleagues at the Department of Organic Chemistry For the generous financial support: “The IDECAT Network of Excellence of the European Community” “K & A Wallenbergs Stiftelse” “John Söderbergs Stiftelse”, “Astra Zeneca” “Svenska Kemistsamfundet” “Ångpanneföreningens Forskningsstiftelse” My family and friends for support 43 7. References (1) (2) (3) (4) (5) (6) (7) (8) (9) (10) (11) (12) (13) (14) (15) (16) (17) (18) (19) (20) (21) (22) (23) (24) (25) (26) (27) (28) (29) (30) (31) (32) (33) (34) (35) (36) (37) Zhu, J.; Bienaymé, H. Multicomponent Reactions; Wiley-VCH: Weinheim, 2005. Tietze, L. F. Chem. Rev. 1996, 96, 115. Poli, G.; Giambastini, G. J. Org. Chem. 2002, 67, 9456. Fogg, D. E.; Santos, E. N. d. Coord. Chem. Rev. 2004, 248, 2365. Wasilke, J.-C.; Obrey, S. J.; Baker, R. T.; Bazan, G. C. Chem. Rev. 2005, 105, 1001. Lee, J. M.; Na, Y.; Han, H.; Chang, S. Chem. Soc. Rev. 2004, 33, 302. 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