Palladium(II)-Catalyzed Synthesis of 2-(Biphenyl-2-yloxy)pyridines and N-Pyridylcarbazoles via Carbon-Hydrogen Bond Activation

Lin, Pi-shan

06 July 2011

This thesis is composed of two parts. The palladium-catalysted synthesis of 2-arylphenols and carbazoles via carbon-hydrogen (C-H) bond activation is described. Treatment of 2-phenoxypyridines with two and a half equivalents of potassium aryltrifluoroborate and 10 mol % of Pd(OAc)2 in the presence of two equivalents of Ag2CO3, one equivalent of p-benzoquinone (BQ), and four equivalents of DMSO with (or without) H2O at 130-140 oC for 48 h in dried CH2Cl2 gave the ortho-arylated 2-phenoxypyridines in modest to excellent yields. The investigation of kinetic isotope effect (kH/kD) is determined to be 5.25, which indicates that C-H bond cleavage occurs in the rate-determining step. 2-(Biphenyl-2-yloxy)pyridines was treated with methyl trifluoromethanesulfonate and subsequently sodium methoxide to give the 2-arylphenols to demonstrate the pyridine is a removable directing group. On the other hand, a novel one-pot synthesis for N-pyridylcarbazoles by the reaction of N-phenylpyridin-2-amines with potassium aryltrifluoroborates using Pd(OAc)2 as the catalyst is presented. For instance, reaction of N-phenylpyridin-2-amines with four equivalents of potassium aryltrifluoroborate under the optimal reaction condition gave N-pyridylcarbazoles in 67% yield along with N-(biphenyl-2-yl)pyridin-2-amine in 13% yield. The investigation of kinetic isotope effect (kH/kD) for first C-H bond activation/C-C bond formation step is determined to be 2.14, and that of the second C-H bond activation/C-N bond formation steps is 1.18. On the basis of KIE analysis, it might indicate that first C-H activation undergo direct C-H bond cleacage, and second step should be via electrophilic aromatic substitution.

C-H bond activation

N-Pyridylcarbazole

2-(biphenyl-2-yloxy)pyridines

Palladium (II)-Catalyzed Ortho Arylation of 9-(Pyridin-2-yl)-9H-carbazoles via C-H Bond Activation And Mechanistic Investigation

Wu, Chung-chiu

09 July 2012

A one-pot synthesis of ortho-arylated 9-(pyridin-2-yl)-9H-carbazoles via C-H bond activation, in which palladium(II)-catalyzed cross-coupling of 9-(pyridin-2-yl)-9H-carbazoles with potassium aryltrifluoroborates is presented. Silver nitrate and tert-butanol were proved to be the best oxidant and solvent for the process, respectively. The product yields fluctuated from modest to excellent, and the reaction showed sufficient functional group tolerance. p-Benzoquinone served as an important ligand for the transmetalation and reductive elimination steps in the catalytic process. The key intermediate of the reaction, 9-(pyridin-2-yl)-9H-carbazole palladacycle was isolated and confirmed by X-ray crystallography. The kinetic isotope effect (kH/kD) for the C-H bond activation step was measured as 0.87. In addition, Hammett experiment gave a negative rho value, -2.14 with a reasonable correlation (R2 = 0.90). The directing group, pyridyl was demonstrated as a removable functional group. Finally, a rational catalytic mechanism is presented based on all experimental evidence.

potassium aryltrifluoroborate

palladium catalysis

C-H bond activation

carbazole

Suzuki-Miyaura coupling reaction

Understanding mechanisms for C-H bond activation

Vastine, Benjamin Alan

15 May 2009

The results from density functional theory (DFT) studies into C–H bond activation, hydrogen transfer, and alkyne–to–vinylidene isomerization are presented in this work. The reaction mechanism for the reductive elimination (RE) of methane from [ κ3- TpPtIV(CH3)2H (1)] (Tp = hydridotris(pyrazolyl)borate) by oxidative addition (OA) of benzene to form [ κ3-TpPtIV(Ph)2H] (19) was investigated through DFT calculations. For 31 density functionals, the calculated values for the barriers to methane formation (Ba1) and release (Ba2) from 1 were benchmarked against the experimentally reported values of 26 (Ba1) and 35 (Ba2) kcal•mol-1, respectively. The values for Ba1 and Ba2, calculated at the B3LYP/DZP level of theory, are 24.6 and 34.3 kcal•mol-1, respectively. The best performing functional was BPW91 where the m.a.e. for the calculated values of the two barriers is 0.68 kcal•mol-1. Classic and newly proposed mechanisms for metal-mediated hydrogen transfer (HT) were analyzed with density functional theory (DFT) and Bader's "Atoms In Molecules" (AIM) analysis. Seven sets of bonding patterns that characterize theconnectivity in metal-mediate HT were found from the analysis of representative models for σ-bond metathesis ( σBM), oxidative addition / reductive elimination (OA/RE), and alternative mechanisms. The mechanism for the formation of the alkynyl, vinylidene complex, [(PiPr3)2Rh(CCPh)(CC(H)(Ph))] (2), by the addition of two equivalents of phenylacetylene (PA) to [( η3-C3H5)Rh(PiPr3)2] (1) was studied through DFT calculations. Two experimentally observed intermediates on the reaction coordinate are the η2-PA, alkynyl complex, [(PiPr3)2Rh( η2-HCCPh)(CCPh)] (Ia) and the fivecoordinate, pseudo square-pyramidal, RhIII–H complex, [(PiPr3)2Rh(H)(CCPh)2] (Ib), and were found to be in equilibrium. The relative energies of Ia, Ib, and 2 (relative to 1 + 2PA) depend on the phosphine that was used in the calculation; the predicted product is 2 with PiPr3 and PEt3 but Ia with PMe3, PMe2Ph, PMePh2, PPh3, and PH3. The equilibrium between Ia and Ib was calculated with PEt3 and one conformation of PiPr3. We investigated the mechanism for the formation of 2 from Ia, and a lower energy pathway where the π-bound PA of Ia slips to bind through the σ-C–H bond prior to the formation of 2 through hydrogen migration was found.

Density functional theory

C-H bond activation

hydrogen transfer

Bader's analysis

Ruthenium-Catalyzed Synthesis of Biaryls through C–H Bond Functionalizations

Diers, Emelyne

14 October 2013

No description available.

540

catalysis

C–H bond functionalization

ruthenium

sustainable chemistry

biaryls

Valsartan

Chemie  (PPN62138352X)

3d metal complexes with the perfluoro-tert-butoxide and perfluoropinacolate ligands: dioxygen reduction and intermolecular substrate oxidation

Brazeau, Sarah Elizabeth

24 April 2020

A CuI fully fluorinated O-donor monodentate alkoxide complex, K[Cu(OC4F9)2] (1), was previously shown to form a trinuclear copper–dioxygen species with a {Cu3(3-O)2} core, TOC4F9, upon reactivity with O2 at low temperature. A significantly expanded kinetic and mechanistic study of TOC4F9 formation is reported using stopped-flow spectroscopy. The TOC4F9 complex performed catalytic oxidase conversion of para-hydroquinone (H2Q) to para-benzoquinone (BQ) and hydroxylation of 2,4-di-tert-butylphenolate (DBP) to catecholate, making TOC4F9 the first tri-copper species to perform tyrosinase (both monooxygenase and oxidase) chemistry. As opposed to 1, when K+ is fully encapsulated in {K(18C6)}[Cu(OC4F9)2] (4), O2 was not reduced under identical conditions. To study the effects of both alkali cation and the degree of encapsulation on reduction of O2, derivative complexes were synthesized with Na+ (16), {Na(DME)}+ (17), {Na(15C5)}+ (18), {K(15C5)}+ (19), {K(15C5)2}+ (20), Cs+ (21), {Cs(18C6)}+ (22), and {Cs(18C6)2}+ (23). Reduction of O2 was found to be encapsulation-dependent, and cation size was also determined to affect the chromophore observed. These results suggest that cation…F/O interactions between the CuI complexes assemble aggregates that are required to form reactive {Cun−O2} species. However, catalytic oxidation of H2Q to BQ and sub-stoichiometric oxidation of DBP to catecholate occurred regardless of whether a {Cun−O2} intermediate was detected, suggesting that a reactive species may self-assemble in the presence of substrate in all complex derivatives unable to reduce O2. A series of heteroleptic mixed phosphine/alkoxide 3d complexes was designed to evaluate PPh3 as a protecting group. Complexes of the form [(Ph3P)2M(OC4F9)2] (M= Fe (24), Co (25), Ni (26), Zn (27)) and [(Ph3P)2M(pinF)] (M= Co (31), Ni (32), Zn (33)) were prepared and characterized, along with related complexes with non-reactive L-donors for comparison, [(DME)Fe(OC4F9)2] (28) and [(Ph3PO)2M(OC4F9)2] (M= Fe (29), Ni (30)). Dimeric [Fe2(-O)(OPPh3)2(OC4F9)4] (36) was isolated after O2 reactivity with 24, and 28 and 29 were able to generate intermediate species capable of both oxidation of H2Q to BQ and oxygen atom transfer of thioanisole to methyl phenyl sulfoxide. The choice of fluorinated ligand influences O2 reactivity with CoII (25, 31), but not for NiII (26, 32). Related dimeric compounds [Co2(pinF)2(THF)4)] (34) and [Zn2(pinF)2(THF)2)] (35) were also isolated.

Inorganic chemistry

C-H bond

Copper

Dioxygen

Fluorinated alkoxide

Oxidation

Phosphine

Iridium-Catalyzed Carbon-Carbon Bond Formation Reactions via C-H Bond Activation / イリジウム触媒によるC-H結合活性化を経るC-C結合形成反応

Ebe, Yusuke

23 March 2017

京都大学 / 0048 / 新制・課程博士 / 博士(理学) / 甲第20192号 / 理博第4277号 / 新制||理||1615(附属図書館) / 京都大学大学院理学研究科化学専攻 / (主査)教授 依光 英樹, 教授 丸岡 啓二, 講師 西村 貴洋 / 学位規則第4条第1項該当 / Doctor of Science / Kyoto University / DGAM

iridium

C-H bond activation

carbon-carbon bond formation

[3 + 2] annulation

hydroarylation

400

Development of Iridium-Catalyzed Skeletal Transformations of Aryl Ethers through Carbon-Carbon Bond Formation / イリジウム触媒を用いたアリールエーテルの炭素-炭素結合形成を伴う骨格変換反応の開発

Kusaka, Satoshi

25 July 2022

京都大学 / 新制・課程博士 / 博士(工学) / 甲第24148号 / 工博第5035号 / 新制||工||1786(附属図書館) / 京都大学大学院工学研究科合成・生物化学専攻 / (主査)教授 杉野目 道紀, 教授 大江 浩一, 教授 中尾 佳亮 / 学位規則第4条第1項該当 / Doctor of Philosophy (Engineering) / Kyoto University / DGAM

Iridium-Catalyzed Reactions

C–H Bond Activation

Heterocycles

Isomerization

Aryl Ethers

500

INVESTIGATION OF Ir(100) STRUCTURAL AND ELECTRONIC PROPERTIES TOWARDS C-H BOND ACTIVATION IN STEAM ETHANE REFORMING

Ore, Rotimi Mark

01 August 2023

The reaction barrier and heat of formation of the various dehydrogenation reactions involved in the steam reforming of ethane is a critical concern in the applications and understanding of these reactions. Focusing on Ir-based catalyst, we report a comprehensive reaction network of dehydrogenation of ethane on Ir(100) based on extensive density functional theory calculations performed on 10 C-H bond cleavage reactions, utilizing the Vienna Ab Initio Package codes. The geometric and electronic structures of the adsorption of C2Hx species with corresponding transition-state structures is reported. We found that the C-H bond in CH3C required the most energy to activate, due to the most stable four-fold hollow adsorption site configuration. Ethane can easily dissociate to CH3CH and CH2CH2 on Ir(100) and further investigation of surface temperature dependence will contribute to the research effort in this area. By using the degree of dehydrogenation of the reactant species as a variable to correlate the C-H bond cleavage barrier as well as reaction energy. DFT studies reveal that the surface Ir(100) to a great extent promotes ethane dehydrogenation when compared to other surfaces.

C-H bond activation

Ethane dehydrogenation

Heterogeneous catalysis

Ir(100)

Iridium catalyst

Steam reforming

C-H fonctionnalisation de purines : synthèse d’inhibiteurs potentiels de la HSP90 / C-H functionalization of purines : synthesis of potential inhibitors of HSP90

Sahnoun, Sophian

16 February 2011

Les résistances aux traitements actuels contre le cancer incitent à trouver de nouvelles cibles thérapeutiques. Une de ces cibles, la hsp90 (heat shock protein 90), impliquée dans la maturation de protéines clientes oncogènes, se révèle très prometteuse car son inhibition induit la dégradation de ces protéines par la voie du protéasome.PU3 et PU24S sont des inhibiteurs de la hsp90 de type purine fonctionnalisés en position 8. Dans le but d’identifier des composés encore plus actifs et/ou de nouvelles familles d’inhibiteurs, nous avons développé de nouveaux procédés sélectifs métallo-catalysés permettant l’activation de liaisons C-H de divers hétérocycles, et en particulier des purines (adénines, xanthines). Ces nouvelles approches ont permis un accès direct et simple à de nombreuses purines fonctionnalisées en C-8 par des groupements aromatiques, hetéroaromatiques, éthyléniques et benzyliques. / Resistance to current treatments of cancer encourages finding new therapeutical targets. The heat shock protein 90 (hsp90) is a molecular chaperon which regulates the folding of many client proteins associated with all of the six hallmarks of cancer, and helps maintaining their proper conformation. Consequently, the hsp90 has become an exciting new target in cancer drug discovery since the inhibition of its ATPase activity leads to depletion of these client proteins via the proteasomal pathway. PU3 and PU24S are purine-based hsp90 inhibitors functionalized on C-8 position. In the aim to identify more active compounds and/or new subfamilies of inhibitors, we have developed new metal-catalyzed C-H activation processes of various heterocycles including purines and other azoles. These new and simple approaches have allowed the access to numerous C-8 functionalized purines bearing (het)aryl, alkenyl and benzyl moieties.

Hsp90

Fonctionnalisation directe

Chimie aux micro-ondes

Hsp90

Purines

C-H bond activation

Direct functionalization

Microwave chemistry

Fonctionnalisation directe de liaisons C-H et couplages croisés pour la formation de liaisons C-C et C-N : synthèse de purines 6,8,9-trisubstituées / C-H bond direct functionalization and cross-coupling reactions for C-C and C-N bonds formation : synthesis of 6,8,9-trisubstituted purines

Vabre, Roxane

15 October 2013

La grande variété de propriétés biologiques associées au noyau purine en fait une structure privilégiée pour la conception et la synthèse de nouvelles molécules à visée thérapeutique. Cette spécificité est étroitement liée à la grande diversité de substituants pouvant être introduits sur les différentes positions du noyau purine et en particulier sur C2, C6, C8 et N9. Par conséquent, le développement de méthodes de fonctionnalisation rapides de cette famille de composés est d’un grand intérêt synthétique. Nous nous sommes focalisés sur la formation de liaisons C-C et C-N sur les positions 6 et 8 du noyau purine pour pouvoir présenter de nouveaux outils de synthèse permettant d’introduire une plus grande diversité fonctionnelle. D’une part, nous avons étudié la fonctionnalisation directe de liaisons C-H de purines, sujet encore peu exploré. En effet, de nos jours, le traditionnel couplage croisé (Negishi, Suzuki-Miyaura), utilisé pour la création de liaisons C-C, se voit de plus en plus concurrencé par ces réactions puisqu’elles ne nécessitent pas la préparation d’un partenaire organométallique. Ce sont des réactions dites à économie d’atomes. En nous basant sur l’expérience du laboratoire dans le domaine de la fonctionnalisation directe de liaisons C-H, nous avons envisagé l’alcénylation et l’alcynylation directes en position 8 de la purine, les motifs alcényle et alcynyle étant présents dans certaines purines d’intérêt biologique. D’autre part, nous nous sommes intéressés à deux méthodes de couplage croisé pallado-catalysé permettant la formation de liaisons C-N et C-C : le couplage de Buchwald – Hartwig entre une 8-iodopurine et des amides ou des amines aromatiques, et le couplage de Liebeskind – Srogl entre une 6-thioétherpurine et divers acides boroniques. / Purine is the most widely distributed N-heterocycle scaffold in the nature and its derivatives are well known for their biological and fluorescent properties. These characteristics are linked to the diversity of substituents that can be introduced, especially on the C-2, C-6, C-8 and N-9 positions. Therefore, the development of methods for rapid functionalization of this family of compounds represent a valuable asset. We focused on the formation of C-C and C-N bonds at positions 6 and 8 of the purine ring in order to provide new synthesis tools allowing the introduction of functional diversity. On the one hand, we studied the direct functionalization of C-H bonds of purines, subject still little explored. Indeed, nowadays, traditional cross-coupling reactions (Negishi, Suzuki-Miyaura), used for the creation of C-C bonds, are increasingly challenged by these reactions since they do not require the preparation of an organometallic partner. Their advantage lies in step and atom economy. Based on previous experience in our laboratory in the field of direct functionalization of C-H bonds, we envisioned direct alkenylation and alkynylation at position 8 of the purine, knowing that alkenyl and alkynyl patterns are found in purines of biological interest. On the other hand, we were interested in two pallado-catalyzed cross-coupling methods for the formation of C-N and C-C bonds : Buchwald – Hartwig coupling between 8-iodopurine and aromatic amines or amides, and Liebeskind – Srogl coupling between 6-thioétherpurine and a range of boronic acids.

Méthodologie

Purine

Couplages croisés

Methodology

Purine

Direct C-H bond functionalization

Cross-coupling reactions