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64 results on '"Amination"'

1. Electrophilic Activation of [1.1.1]Propellane for the Synthesis of Nitrogen‐Substituted Bicyclo[1.1.1]pentanes

Author

Livesley, Sarah, Sterling, Alistair J, Robertson, Craig M, Goundry, William RF, Morris, James A, Duarte, Fernanda, and Aïssa, Christophe

Subjects
[1, 1, 1]propellane, amination, bicyclo[1, 1]pentane, bioisostere, halogen bond, [1.1.1]propellane, bicyclo[1.1.1]pentane, Chemical Sciences, Organic Chemistry
Abstract

Strategies commonly used for the synthesis of functionalised bicyclo[1.1.1]pentanes (BCP) rely on the reaction of [1.1.1]propellane with anionic or radical intermediates. In contrast, electrophilic activation has remained a considerable challenge due to the facile decomposition of BCP cations, which has severely limited the applications of this strategy. Herein, we report the electrophilic activation of [1.1.1]propellane in a halogen bond complex, which enables its reaction with electron-neutral nucleophiles such as anilines and azoles to give nitrogen-substituted BCPs that are prominent motifs in drug discovery. A detailed computational analysis indicates that the key halogen bonding interaction promotes nucleophilic attack without sacrificing cage stabilisation. Overall, our work rehabilitates electrophilic activation of [1.1.1]propellane as a valuable strategy for accessing functionalised BCPs.

Published
2022

2. Ruthenium-Catalyzed Hydroamination of Unactivated Terminal Alkenes with Stoichiometric Amounts of Alkene and an Ammonia Surrogate by Sequential Oxidation and Reduction

Author

Ma, Senjie, Hill, Christopher K, Olen, Casey L, and Hartwig, John F

Subjects
Alkenes, Amination, Aminopyridines, Catalysis, Coordination Complexes, Density Functional Theory, Models, Chemical, Oxidation-Reduction, Ruthenium, Chemical Sciences, General Chemistry
Abstract

Hydroamination of alkenes catalyzed by transition-metal complexes is an atom-economical method for the synthesis of amines, but reactions of unactivated alkenes remain inefficient. Additions of N-H bonds to such alkenes catalyzed by iridium, gold, and lanthanide catalysts are known, but they have required a large excess of the alkene. New mechanisms for such processes involving metals rarely used previously for hydroamination could enable these reactions to occur with greater efficiency. We report ruthenium-catalyzed intermolecular hydroaminations of a variety of unactivated terminal alkenes without the need for an excess of alkene and with 2-aminopyridine as an ammonia surrogate to give the Markovnikov addition product. Ruthenium complexes have rarely been used for hydroaminations and have not previously catalyzed such reactions with unactivated alkenes. Identification of the catalyst resting state, kinetic measurements, deuterium labeling studies, and DFT computations were conducted and, together, strongly suggest that this process occurs by a new mechanism for hydroamination occurring by oxidative amination in concert with reduction of the resulting imine.

Published
2021

3. Cross‐Coupling between Hydrazine and Aryl Halides with Hydroxide Base at Low Loadings of Palladium by Rate‐Determining Deprotonation of Bound Hydrazine

Author

Wang, Justin Y, Choi, Kyoungmin, Zuend, Stephan J, Borate, Kailaskumar, Shinde, Harish, Goetz, Roland, and Hartwig, John F

Subjects
Inorganic Chemistry, Organic Chemistry, Chemical Sciences, Catalysis, Humans, Hydrazines, Hydroxides, Molecular Structure, Palladium, amination, cross-coupling, palladium, reaction mechanisms, synthetic methods, Chemical sciences
Abstract

Reported here is the Pd-catalyzed C-N coupling of hydrazine with (hetero)aryl chlorides and bromides to form aryl hydrazines with catalyst loadings as low as 100 ppm of Pd and KOH as base. Mechanistic studies revealed two catalyst resting states: an arylpalladium(II) hydroxide and arylpalladium(II) chloride. These compounds are present in two interconnected catalytic cycles and react with hydrazine and base or hydrazine alone to give the product. The selectivity of the hydroxide complex with hydrazine to form aryl over diaryl hydrazine was lower than that of the chloride complex, as well as the catalytic reaction. In contrast, the selectivity of the chloride complex closely matched that of the catalytic reaction, indicating that the aryl hydrazine is derived from this complex. Kinetic studies showed that the coupling process occurs by rate-limiting deprotonation of a hydrazine-bound arylpalladium(II) chloride complex to give an arylpalladium(II) hydrazido complex.

Published
2021

4. Catalytic asymmetric addition of an amine N–H bond across internal alkenes

Author

Xi, Yumeng, Ma, Senjie, and Hartwig, John F

Subjects
Inorganic Chemistry, Organic Chemistry, Chemical Sciences, Alkenes, Amination, Amines, Aminopyridines, Ammonia, Catalysis, Chemistry Techniques, Synthetic, Hydrogen, Indicators and Reagents, Iridium, Ligands, Nitrogen, Phosphines, General Science & Technology
Abstract

Hydroamination of alkenes, the addition of the N-H bond of an amine across an alkene, is a fundamental, yet challenging, organic transformation that creates an alkylamine from two abundant chemical feedstocks, alkenes and amines, with full atom economy1-3. The reaction is particularly important because amines, especially chiral amines, are prevalent substructures in a wide range of natural products and drugs. Although extensive efforts have been dedicated to developing catalysts for hydroamination, the vast majority of alkenes that undergo intermolecular hydroamination have been limited to conjugated, strained, or terminal alkenes2-4; only a few examples occur by the direct addition of the N-H bond of amines across unactivated internal alkenes5-7, including photocatalytic hydroamination8,9, and no asymmetric intermolecular additions to such alkenes are known. In fact, current examples of direct, enantioselective intermolecular hydroamination of any type of unactivated alkene lacking a directing group occur with only moderate enantioselectivity10-13. Here we report a cationic iridium system that catalyses intermolecular hydroamination of a range of unactivated, internal alkenes, including those in both acyclic and cyclic alkenes, to afford chiral amines with high enantioselectivity. The catalyst contains a phosphine ligand bearing trimethylsilyl-substituted aryl groups and a triflimide counteranion, and the reaction design includes 2-amino-6-methylpyridine as the amine to enhance the rates of multiple steps within the catalytic cycle while serving as an ammonia surrogate. These design principles point the way to the addition of N-H bonds of other reagents, as well as O-H and C-H bonds, across unactivated internal alkenes to streamline the synthesis of functional molecules from basic feedstocks.

Published
2020

5. Structure and Function of NzeB, a Versatile C–C and C–N Bond-Forming Diketopiperazine Dimerase

Author

Shende, Vikram V, Khatri, Yogan, Newmister, Sean A, Sanders, Jacob N, Lindovska, Petra, Yu, Fengan, Doyon, Tyler J, Kim, Justin, Houk, KN, Movassaghi, Mohammad, and Sherman, David H

Subjects
Organic Chemistry, Chemical Sciences, Bioengineering, Generic health relevance, Alkaloids, Amination, Biocatalysis, Biological Products, Carbon, Cytochrome P-450 Enzyme System, Diketopiperazines, Dimerization, Models, Molecular, Molecular Conformation, Mutagenesis, Site-Directed, Nitrogen, Streptomyces, Substrate Specificity, General Chemistry, Chemical sciences, Engineering
Abstract

The dimeric diketopiperazine (DKPs) alkaloids are a diverse family of natural products (NPs) whose unique structural architectures and biological activities have inspired the development of new synthetic methodologies to access these molecules. However, catalyst-controlled methods that enable the selective formation of constitutional and stereoisomeric dimers from a single monomer are lacking. To resolve this long-standing synthetic challenge, we sought to characterize the biosynthetic enzymes that assemble these NPs for application in biocatalytic syntheses. Genome mining enabled identification of the cytochrome P450, NzeB (Streptomyces sp. NRRL F-5053), which catalyzes both intermolecular carbon-carbon (C-C) and carbon-nitrogen (C-N) bond formation. To identify the molecular basis for the flexible site-selectivity, stereoselectivity, and chemoselectivity of NzeB, we obtained high-resolution crystal structures (1.5 Å) of the protein in complex with native and non-native substrates. This, to our knowledge, represents the first crystal structure of an oxidase catalyzing direct, intermolecular C-H amination. Site-directed mutagenesis was utilized to assess the role individual active-site residues play in guiding selective DKP dimerization. Finally, computational approaches were employed to evaluate plausible mechanisms regarding NzeB function and its ability to catalyze both C-C and C-N bond formation. These results provide a structural and computational rationale for the catalytic versatility of NzeB, as well as new insights into variables that control selectivity of CYP450 diketopiperazine dimerases.

Published
2020

6. An enzymatic platform for the asymmetric amination of primary, secondary and tertiary C(sp3)–H bonds

Author

Yang, Yang, Cho, Inha, Qi, Xiaotian, Liu, Peng, and Arnold, Frances H

Subjects
Inorganic Chemistry, Organic Chemistry, Chemical Sciences, Amination, Biocatalysis, Cytochrome P-450 Enzyme System, Escherichia coli, Models, Molecular, Molecular Structure, Stereoisomerism, Chemical sciences
Abstract

The ability to selectively functionalize ubiquitous C-H bonds streamlines the construction of complex molecular architectures from easily available precursors. Here we report enzyme catalysts derived from a cytochrome P450 that use a nitrene transfer mechanism for the enantioselective amination of primary, secondary and tertiary C(sp3)-H bonds. These fully genetically encoded enzymes are produced and function in bacteria, where they can be optimized by directed evolution for a broad spectrum of enantioselective C(sp3)-H amination reactions. These catalysts can aminate a variety of benzylic, allylic and aliphatic C-H bonds in excellent enantioselectivity with access to either antipode of product. Enantioselective amination of primary C(sp3)-H bonds in substrates that bear geminal dimethyl substituents furnished chiral amines that feature a quaternary stereocentre. Moreover, these enzymes enabled the enantioconvergent transformation of racemic substrates that possess a tertiary C(sp3)-H bond to afford products that bear a tetrasubstituted stereocentre, a process that has eluded small-molecule catalysts. Further engineering allowed for the enantioselective construction of methyl-ethyl stereocentres, which is notoriously challenging in asymmetric catalysis.

Published
2019

7. A Multicatalytic Approach to the Hydroaminomethylation of α‐Olefins

Author

Hanna, Steven, Holder, Jeffrey C, and Hartwig, John F

Subjects
Organic Chemistry, Chemical Sciences, Alkenes, Amination, Amines, Catalysis, Coordination Complexes, Formates, Hydrogenation, Iridium, Methylation, Molecular Structure, Rhodium, Sulfonamides, hydroaminomethylation, hydroformylation, multicatalytic, reductive amination, transfer hydrogenation, Chemical sciences
Abstract

We report an approach to conducting the hydroaminomethylation of diverse α-olefins with a wide range of alkyl, aryl, and heteroarylamines at relatively low temperatures (70-80 °C) and pressures (1.0-3.4 bar) of synthesis gas. This approach is based on simultaneously using two distinct catalysts that are mutually compatible. The hydroformylation step is catalyzed by a rhodium diphosphine complex, and the reductive amination step, which is conducted as a transfer hydrogenation with aqueous, buffered sodium formate as the reducing agent, is catalyzed by a cyclometallated iridium complex. By adjusting the ratio of CO to H2 , we conducted the reaction at one atmosphere of gas with little change in yield. A diverse array of olefins and amines, including hetreroarylamines that do not react under more conventional conditions with a single catalyst, underwent hydroaminomethylation with this new system, and the pharmaceutical ibutilide was prepared in higher yield and under milder conditions than with a single catalyst.

Published
2019

8. A Multicatalytic Approach to the Hydroaminomethylation of α-Olefins.

Author

Hanna, Steven, Holder, Jeffrey C, and Hartwig, John F

Subjects
Iridium, Rhodium, Sulfonamides, Amines, Formates, Alkenes, Molecular Structure, Methylation, Amination, Hydrogenation, Catalysis, Coordination Complexes, hydroaminomethylation, hydroformylation, multicatalytic, reductive amination, transfer hydrogenation, Chemical Sciences, Organic Chemistry
Abstract

We report an approach to conducting the hydroaminomethylation of diverse α-olefins with a wide range of alkyl, aryl, and heteroarylamines at relatively low temperatures (70-80 °C) and pressures (1.0-3.4 bar) of synthesis gas. This approach is based on simultaneously using two distinct catalysts that are mutually compatible. The hydroformylation step is catalyzed by a rhodium diphosphine complex, and the reductive amination step, which is conducted as a transfer hydrogenation with aqueous, buffered sodium formate as the reducing agent, is catalyzed by a cyclometallated iridium complex. By adjusting the ratio of CO to H2 , we conducted the reaction at one atmosphere of gas with little change in yield. A diverse array of olefins and amines, including hetreroarylamines that do not react under more conventional conditions with a single catalyst, underwent hydroaminomethylation with this new system, and the pharmaceutical ibutilide was prepared in higher yield and under milder conditions than with a single catalyst.

Published
2019

9. Design, synthesis, and biological activity of substituted 2-amino-5-oxo-5H-chromeno[2,3-b]pyridine-3-carboxylic acid derivatives as inhibitors of the inflammatory kinases TBK1 and IKKε for the treatment of obesity

Author

Beyett, Tyler S, Gan, Xinmin, Reilly, Shannon M, Gomez, Andrew V, Chang, Louise, Tesmer, John JG, Saltiel, Alan R, and Showalter, Hollis D

Subjects
Medicinal and Biomolecular Chemistry, Chemical Sciences, Nutrition, Diabetes, Obesity, Metabolic and endocrine, Affordable and Clean Energy, 3T3-L1 Cells, Amination, Animals, Anti-Obesity Agents, Chromans, Crystallography, X-Ray, Drug Design, Humans, I-kappa B Kinase, Mice, Molecular Docking Simulation, Protein Kinase Inhibitors, Protein Serine-Threonine Kinases, Pyridines, Amlexanox, TANK-binding kinase 1, Inhibitor of nuclear factor kappa-B kinase, subunit epsilon, TBK1 center dot amlexanox co-crystal, SAR, Inhibitor of nuclear factor kappa-B kinase subunit epsilon, TBK1·amlexanox co-crystal, Organic Chemistry, Pharmacology and Pharmaceutical Sciences, Medicinal & Biomolecular Chemistry, Biochemistry and cell biology, Medicinal and biomolecular chemistry, Organic chemistry
Abstract

The non-canonical IκB kinases TANK-binding kinase 1 (TBK1) and inhibitor of nuclear factor kappa-B kinase ε (IKKε) play a key role in insulin-independent pathways that promote energy storage and block adaptive energy expenditure during obesity. Utilizing docking calculations and the x-ray structure of TBK1 bound to amlexanox, an inhibitor of these kinases with modest potency, a series of analogues was synthesized to develop a structure activity relationship (SAR) around the A- and C-rings of the core scaffold. A strategy was developed wherein R7 and R8 A-ring substituents were incorporated late in the synthetic sequence by utilizing palladium-catalyzed cross-coupling reactions on appropriate bromo precursors. Analogues display IC50 values as low as 210 nM and reveal A-ring substituents that enhance selectivity toward either kinase. In cell assays, selected analogues display enhanced phosphorylation of p38 or TBK1 and elicited IL-6 secretion in 3T3-L1 adipocytes better than amlexanox. An analogue bearing a R7 cyclohexyl modification demonstrated robust IL-6 production in 3T3-L1 cells as well as a phosphorylation marker of efficacy and was tested in obese mice where it promoted serum IL-6 response, weight loss, and insulin sensitizing effects comparable to amlexanox. These studies provide impetus to expand the SAR around the amlexanox core toward uncovering analogues with development potential.

Published
2018

10. Direct Amination of Alcohols Catalyzed by Aluminum Triflate: An Experimental and Computational Study

Author

Payard, Pierre‐Adrien, Gu, Qingyi, Guo, Wenping, Wang, Qianran, Corbet, Matthieu, Michel, Carine, Sautet, Philippe, Grimaud, Laurence, Wischert, Raphael, and Pera‐Titus, Marc

Subjects
alcohols, amination, density functional calculations, homogeneous catalysis, nucleophilic substitution, Chemical Sciences, General Chemistry
Abstract

Among the best-performing homogeneous catalysts for the direct amination of activated secondary alcohols with electron-poor amine derivatives, metal triflates, such as aluminum triflate, Al(OTf)3 , stand out. Herein we report the extension of this reaction to electron-rich amines and activated primary alcohols. We provide detailed insight into the structure and reactivity of the catalyst under working conditions in both nitromethane and toluene solvent, through experiment (cyclic voltammetry, conductimetry, NMR spectroscopy), and density functional theory (DFT) simulations. Competition between aniline and benzyl alcohol for Al in the two solvents explains the different reactivities. The catalyst structures predicted from the DFT calculations were validated by the experiments. Whereas a SN 1-type mechanism was found to be active in nitromethane, we propose a SN 2 mechanism in toluene to rationalize the much higher selectivity observed when using this solvent. Also, unlike what is commonly assumed in homogeneous catalysis, we show that different active species may be active instead of only one.

Published
2018

11. Direct Amination of Alcohols Catalyzed by Aluminum Triflate: An Experimental and Computational Study.

Author

Payard, Pierre-Adrien, Gu, Qingyi, Guo, Wenping, Wang, Qianran, Corbet, Matthieu, Michel, Carine, Sautet, Philippe, Grimaud, Laurence, Wischert, Raphael, and Pera-Titus, Marc

Subjects
alcohols, amination, density functional calculations, homogeneous catalysis, nucleophilic substitution, General Chemistry, Chemical Sciences
Abstract

Among the best-performing homogeneous catalysts for the direct amination of activated secondary alcohols with electron-poor amine derivatives, metal triflates, such as aluminum triflate, Al(OTf)3 , stand out. Herein we report the extension of this reaction to electron-rich amines and activated primary alcohols. We provide detailed insight into the structure and reactivity of the catalyst under working conditions in both nitromethane and toluene solvent, through experiment (cyclic voltammetry, conductimetry, NMR spectroscopy), and density functional theory (DFT) simulations. Competition between aniline and benzyl alcohol for Al in the two solvents explains the different reactivities. The catalyst structures predicted from the DFT calculations were validated by the experiments. Whereas a SN 1-type mechanism was found to be active in nitromethane, we propose a SN 2 mechanism in toluene to rationalize the much higher selectivity observed when using this solvent. Also, unlike what is commonly assumed in homogeneous catalysis, we show that different active species may be active instead of only one.

Published
2018

12. Catalytic Hydrothiolation: Regio- and Enantioselective Coupling of Thiols and Dienes

Author

Yang, Xiao-Hui, Davison, Ryan T, and Dong, Vy M

Subjects
Alkynes, Allyl Compounds, Amination, Catalysis, Ligands, Rhodium, Stereoisomerism, Sulfhydryl Compounds, Sulfides, Chemical Sciences, General Chemistry
Abstract

We report a Rh-catalyzed hydrothiolation of 1,3-dienes, including petroleum feedstocks. Either secondary or tertiary allylic sulfides can be generated from the selective addition of a thiol to the more substituted double bond of a diene. The catalyst tolerates a wide range of functional groups, and the loading can be as low as 0.1 mol %.

Published
2018

13. Solvation-Guided Design of Fluorescent Probes for Discrimination of Amyloids.

Author

Cao, Kevin J, Elbel, Kristyna M, Cifelli, Jessica L, Cirera, Jordi, Sigurdson, Christina J, Paesani, Francesco, Theodorakis, Emmanuel A, and Yang, Jerry

Subjects
Brain, Humans, Alzheimer Disease, Cyanoacrylates, Amyloid, Peptide Fragments, Fluorescent Dyes, Acylation, Amination, Amyloid beta-Peptides, Optical Imaging, Protein Aggregation, Pathological, Protein Aggregation, Pathological, Neurosciences, Neurodegenerative, Dementia, Aging, Brain Disorders, Alzheimer's Disease, Acquired Cognitive Impairment, Alzheimer's Disease including Alzheimer's Disease Related Dementias, Neurological, Biochemistry and Cell Biology, Other Physical Sciences
Abstract

The deposition of insoluble protein aggregates in the brain is a hallmark of many neurodegenerative diseases. While their exact role in neurodegeneration remains unclear, the presence of these amyloid deposits often precedes clinical symptoms. As a result, recent progress in imaging methods that utilize amyloid-specific small molecule probes have become a promising avenue for antemortem disease diagnosis. Here, we present a series of amino-aryl cyanoacrylate (AACA) fluorophores that show a turn-on fluorescence signal upon binding to amyloids in solution and in tissue. Using a theoretical model for environmental sensitivity of fluorescence together with ab initio computational modeling of the effects of polar environment on electron density distribution and conformational dynamics, we designed, synthesized, and evaluated a set of fluorophores that (1) bind to aggregated forms of Alzheimer's-related β-amyloid peptides with low micromolar to high nanomolar affinities and (2) have the capability to fluorescently discriminate different amyloids based on differences in amino acid composition within the binding pocket through exploitation of their solvatochromic properties. These studies showcase the rational design of a family of amyloid-binding imaging agents that could be integrated with new optical approaches for the clinical diagnosis of amyloidoses, where accurate identification of the specific neurodegenerative disease could aid in the selection of a proper course for treatment.

Published
2018

14. Solvation-Guided Design of Fluorescent Probes for Discrimination of Amyloids.

Author

Cao, Kevin J, Elbel, Kristyna M, Cifelli, Jessica L, Cirera, Jordi, Sigurdson, Christina J, Paesani, Francesco, Theodorakis, Emmanuel A, and Yang, Jerry

Subjects
Brain, Humans, Alzheimer Disease, Cyanoacrylates, Amyloid, Peptide Fragments, Fluorescent Dyes, Acylation, Amination, Amyloid beta-Peptides, Optical Imaging, Protein Aggregation, Pathological, Alzheimer's Disease, Dementia, Neurodegenerative, Neurosciences, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Acquired Cognitive Impairment, Brain Disorders, Aging, Neurological
Abstract

The deposition of insoluble protein aggregates in the brain is a hallmark of many neurodegenerative diseases. While their exact role in neurodegeneration remains unclear, the presence of these amyloid deposits often precedes clinical symptoms. As a result, recent progress in imaging methods that utilize amyloid-specific small molecule probes have become a promising avenue for antemortem disease diagnosis. Here, we present a series of amino-aryl cyanoacrylate (AACA) fluorophores that show a turn-on fluorescence signal upon binding to amyloids in solution and in tissue. Using a theoretical model for environmental sensitivity of fluorescence together with ab initio computational modeling of the effects of polar environment on electron density distribution and conformational dynamics, we designed, synthesized, and evaluated a set of fluorophores that (1) bind to aggregated forms of Alzheimer's-related β-amyloid peptides with low micromolar to high nanomolar affinities and (2) have the capability to fluorescently discriminate different amyloids based on differences in amino acid composition within the binding pocket through exploitation of their solvatochromic properties. These studies showcase the rational design of a family of amyloid-binding imaging agents that could be integrated with new optical approaches for the clinical diagnosis of amyloidoses, where accurate identification of the specific neurodegenerative disease could aid in the selection of a proper course for treatment.

Published
2018

15. Transition‐Metal‐Catalyzed Selective Functionalization of C(sp3)−H Bonds in Natural Products

Author

Karimov, Rashad R and Hartwig, John F

Subjects
Inorganic Chemistry, Organic Chemistry, Chemical Sciences, Biological Products, Catalysis, Molecular Conformation, Transition Elements, amination, catalysis, C-H bond functionalization, oxidation, regioselectivity, C−H bond functionalization, Chemical sciences
Abstract

Direct functionalization of natural products is important for studying the structure-activity and structure-property relationships of these molecules. Recent advances in the transition-metal-catalyzed functionalization of C(sp3 )-H bonds, the most abundant yet inert bonds in natural products, have allowed natural product derivatives to be created selectively. Strategies to achieve such transformation are reviewed.

Published
2018

16. Enantioselective Synthesis of Spliceostatin G and Evaluation of Bioactivity of Spliceostatin G and Its Methyl Ester

Author

Ghosh, Arun K, Reddy, Guddeti Chandrashekar, MacRae, Andrew J, and Jurica, Melissa S

Subjects
Organic Chemistry, Chemical Sciences, Amination, Esters, Molecular Structure, RNA Splicing, Spiro Compounds, Stereoisomerism, Chemical sciences
Abstract

An enantioselective total synthesis of spliceostatin G has been accomplished. The synthesis involved a Suzuki cross-coupling reaction as a key step. The functionalized tetrahydropyran ring was constructed from commercially available optically active tri-O-acetyl-d-glucal. Other key reactions include a highly stereoselective Claisen rearrangement, a Cu(I)-mediated 1,4 addition of MeLi to install the C8 methyl group, and a reductive amination to incorporate the C10 amine functionality of spliceostatin G. Biological evaluation of synthetic spliceostatin G and its methyl ester revealed that it does not inhibit splicing in vitro.

Published
2018

18. Enantioselective Synthesis of Spliceostatin G and Evaluation of Bioactivity of Spliceostatin G and Its Methyl Ester.

Author

Ghosh, Arun K, Reddy, Guddeti Chandrashekar, MacRae, Andrew J, and Jurica, Melissa S

Subjects
Esters, Spiro Compounds, RNA Splicing, Molecular Structure, Amination, Stereoisomerism, Organic Chemistry, Chemical Sciences
Abstract

An enantioselective total synthesis of spliceostatin G has been accomplished. The synthesis involved a Suzuki cross-coupling reaction as a key step. The functionalized tetrahydropyran ring was constructed from commercially available optically active tri-O-acetyl-d-glucal. Other key reactions include a highly stereoselective Claisen rearrangement, a Cu(I)-mediated 1,4 addition of MeLi to install the C8 methyl group, and a reductive amination to incorporate the C10 amine functionality of spliceostatin G. Biological evaluation of synthetic spliceostatin G and its methyl ester revealed that it does not inhibit splicing in vitro.

Published
2018

20. Site-selective oxidation, amination and epimerization reactions of complex polyols enabled by transfer hydrogenation

Author

Hill, Christopher K and Hartwig, John F

Subjects
Inorganic Chemistry, Organic Chemistry, Chemical Sciences, Substance Misuse, Alcoholism, Alcohol Use and Health, Amination, Amines, Catalysis, Hydrogenation, Molecular Structure, Oxidation-Reduction, Polymers, Ruthenium, Chemical sciences
Abstract

Polyoxygenated hydrocarbons that bear one or more hydroxyl groups comprise a large set of natural and synthetic compounds, often with potent biological activity. In synthetic chemistry, alcohols are important precursors to carbonyl groups, which then can be converted into a wide range of oxygen- or nitrogen-based functionality. Therefore, the selective conversion of a single hydroxyl group in natural products into a ketone would enable the selective introduction of unnatural functionality. However, the methods known to convert a simple alcohol, or even an alcohol in a molecule that contains multiple protected functional groups, are not suitable for selective reactions of complex polyol structures. We present a new ruthenium catalyst with a unique efficacy for the selective oxidation of a single hydroxyl group among many in unprotected polyol natural products. This oxidation enables the introduction of nitrogen-based functional groups into such structures that lack nitrogen atoms and enables a selective alcohol epimerization by stepwise or reversible oxidation and reduction.

Published
2017

21. Ligand–Substrate Dispersion Facilitates the Copper-Catalyzed Hydroamination of Unactivated Olefins

Author

Lu, Gang, Liu, Richard Y, Yang, Yang, Fang, Cheng, Lambrecht, Daniel S, Buchwald, Stephen L, and Liu, Peng

Subjects
Inorganic Chemistry, Organic Chemistry, Chemical Sciences, Alkenes, Amination, Catalysis, Copper, Kinetics, Ligands, General Chemistry, Chemical sciences, Engineering
Abstract

The current understanding of ligand effects in transition metal catalysis is mostly based on the analysis of catalyst-substrate through-bond and through-space interactions, with the latter commonly considered to be repulsive in nature. The dispersion interaction between the ligand and the substrate, a ubiquitous type of attractive noncovalent interaction, is seldom accounted for in the context of transition-metal-catalyzed transformations. Herein we report a computational model to quantitatively analyze the effects of different types of catalyst-substrate interactions on reactivity. Using this model, we show that in the copper(I) hydride (CuH)-catalyzed hydroamination of unactivated olefins, the substantially enhanced reactivity of copper catalysts based on bulky bidentate phosphine ligands originates from the attractive ligand-substrate dispersion interaction. These computational findings are validated by kinetic studies across a range of hydroamination reactions using structurally diverse phosphine ligands, revealing the critical role of bulky P-aryl groups in facilitating this process.

Published
2017

22. Multidimensional Correlations in Asymmetric Catalysis through Parameterization of Uncatalyzed Transition States

Author

Orlandi, Manuel, Toste, F Dean, and Sigman, Matthew S

Subjects
Amination, Catalysis, Hydrogen Bonding, Oxidation-Reduction, Stereoisomerism, Tetrahydroisoquinolines, asymmetric catalysis, chiral-anion phase-transfer catalysis, free-energy relationships, molecular parameterization, multidimensional correlation analysis, Chemical Sciences, Organic Chemistry
Abstract

The study of the oxidative amination of tetrahydroisoquinolines under chiral-anion phase-transfer (CAPT) catalysis by multidimensional correlation analysis (MCA) is revisited. The parameterization of the transition states (TSs) for the uncatalyzed reaction, the introduction of conformational descriptors, and the use of computed interaction energies and distances as parameters allowed access to a considerably simplified mathematical correlation of substrate and catalyst structure to enantioselectivity. The equation obtained is suggestive of key interactions occurring at the TS. Specifically, the CAPT catalyst is proposed to coordinate the intermediate iminium cation by P=O⋅⋅⋅H-O hydrogen-bonding and N⋅⋅⋅H-C electrostatic interactions. The conformational freedom of the benzyl substituent of the substrate was also found to be important in providing an efficient mode of molecular recognition.

Published
2017

23. Multidimensional Correlations in Asymmetric Catalysis through Parameterization of Uncatalyzed Transition States.

Author

Orlandi, Manuel, Toste, F Dean, and Sigman, Matthew S

Subjects
Tetrahydroisoquinolines, Amination, Oxidation-Reduction, Catalysis, Stereoisomerism, Hydrogen Bonding, asymmetric catalysis, chiral-anion phase-transfer catalysis, free-energy relationships, molecular parameterization, multidimensional correlation analysis, Organic Chemistry, Chemical Sciences
Abstract

The study of the oxidative amination of tetrahydroisoquinolines under chiral-anion phase-transfer (CAPT) catalysis by multidimensional correlation analysis (MCA) is revisited. The parameterization of the transition states (TSs) for the uncatalyzed reaction, the introduction of conformational descriptors, and the use of computed interaction energies and distances as parameters allowed access to a considerably simplified mathematical correlation of substrate and catalyst structure to enantioselectivity. The equation obtained is suggestive of key interactions occurring at the TS. Specifically, the CAPT catalyst is proposed to coordinate the intermediate iminium cation by P=O⋅⋅⋅H-O hydrogen-bonding and N⋅⋅⋅H-C electrostatic interactions. The conformational freedom of the benzyl substituent of the substrate was also found to be important in providing an efficient mode of molecular recognition.

Published
2017

24. Intermolecular Hydroamination of 1,3-Dienes To Generate Homoallylic Amines

Author

Yang, Xiao-Hui, Lu, Alexander, and Dong, Vy M

Subjects
Alkenes, Allyl Compounds, Amination, Amines, Catalysis, Ligands, Mandelic Acids, Naphthalenes, Rhodium, Chemical Sciences, General Chemistry
Abstract

We report a Rh-catalyzed hydroamination of 1,3-dienes to generate homoallylic amines. Our work showcases the first case of anti-Markovnikov selectivity in the intermolecular coupling of amines and 1,3-dienes. By tuning the ligand properties and Brønsted acid additive, we find that a combination of rac-BINAP and mandelic acid is critical for achieving anti-Markovnikov selectivity.

Published
2017

25. Well-defined Ti 4 pre-catalysts for the ring-opening polymerisation of lactide

Author

Cols, Jean-Marie EP, Taylor, Cameron E, Gagnon, Kevin J, Teat, Simon J, and McIntosh, Ruaraidh D

Subjects
Inorganic Chemistry, Chemical Sciences, Amination, Catalysis, Coordination Complexes, Crystallography, X-Ray, Dioxanes, Ligands, Models, Molecular, Phenols, Polymerization, Titanium, Theoretical and Computational Chemistry, Other Chemical Sciences, Inorganic & Nuclear Chemistry, Inorganic chemistry
Abstract

The synthesis and full characterisation of four discrete tetrametallic titanium complexes is reported. These well-defined compounds are isostructural in the solid state and share the same general formula: Ti4(μ-O)2L4 (L = 1, 2, 3 or 4). Using a combination of NMR techniques the complexes are found to be stable in solution, even at elevated temperatures. Further studies show that the carboxylate moieties of the supporting amine bis(phenolate) ligands can be displaced by a more strongly coordinating solvent. This reversible process causes the coordinatively saturated Ti4(μ-O)2L4 complexes to separate into two Ti2(μ-O)L2 subunits which we envisaged would be catalytically active. Proof-of-concept experiments establish that all four of these complexes display catalytic activity in the ring-opening polymerisation of rac-lactide. These aggregates can therefore be viewed as air and moisture stable pre-catalysts for a range of reactions.

Published
2016

26. Well-defined Ti4 pre-catalysts for the ring-opening polymerisation of lactide.

Author

Cols, Jean-Marie EP, Taylor, Cameron E, Gagnon, Kevin J, Teat, Simon J, and McIntosh, Ruaraidh D

Subjects
Titanium, Phenols, Dioxanes, Ligands, Crystallography, X-Ray, Amination, Catalysis, Models, Molecular, Coordination Complexes, Polymerization, Crystallography, X-Ray, Models, Molecular, Inorganic & Nuclear Chemistry, Inorganic Chemistry, Other Chemical Sciences, Theoretical and Computational Chemistry
Abstract

The synthesis and full characterisation of four discrete tetrametallic titanium complexes is reported. These well-defined compounds are isostructural in the solid state and share the same general formula: Ti4(μ-O)2L4 (L = 1, 2, 3 or 4). Using a combination of NMR techniques the complexes are found to be stable in solution, even at elevated temperatures. Further studies show that the carboxylate moieties of the supporting amine bis(phenolate) ligands can be displaced by a more strongly coordinating solvent. This reversible process causes the coordinatively saturated Ti4(μ-O)2L4 complexes to separate into two Ti2(μ-O)L2 subunits which we envisaged would be catalytically active. Proof-of-concept experiments establish that all four of these complexes display catalytic activity in the ring-opening polymerisation of rac-lactide. These aggregates can therefore be viewed as air and moisture stable pre-catalysts for a range of reactions.

Published
2016

27. Copper-Mediated C–N Coupling of Arylsilanes with Nitrogen Nucleophiles

Author

Morstein, Johannes, Kalkman, Eric D, Bold, Christian, Cheng, Chen, and Hartwig, John F

Subjects
Amination, Amines, Catalysis, Copper, Organometallic Compounds, Silanes, Sodium Fluoride, Chemical Sciences, Organic Chemistry
Abstract

A method for the oxidative coupling of arylsilanes with nitrogen nucleophiles is reported. This method occurs with a broad range of heptamethyltrisiloxylarenes and nitrogen nucleophiles, proceeds with the arylsilane as limiting reagent, and does not require a fluoride activator with electron-poor arylsilanes. The combination of this method with C-H silylation generates arylamines from unactivated arenes with site selectivity controlled by steric effects. This combination of steps gives direct access to many compounds that cannot be accessed via alternative C-H functionalization methods, including direct C-H amination or the combination of C-H borylation and amination.

Published
2016

28. Asymmetric Electrophilic α‑Amination of Silyl Enol Ether Derivatives via the Nitrosocarbonyl Hetero-ene Reaction

Author

Sandoval, David, Samoshin, Andrey V, and de Alaniz, Javier Read

Subjects
Alcohols, Amination, Catalysis, Copper, Ethers, Molecular Structure, Nitroso Compounds, Organosilicon Compounds, Stereoisomerism, Chemical Sciences, Organic Chemistry
Abstract

The first example of a general asymmetric nitrosocarbonyl hetero-ene reaction is described. The procedure uses a copper-catalyzed aerobic oxidation of a commercially available chiral nitrosocarbonyl precursor (EleNOr) and is operationally simple. The transformation is both high yielding and highly diastereoselective for a range of silyl enol ether derivatives. A variety of synthetically useful postfunctionalization reactions are presented along with a mechanistic rationale that can be used as a predictive model for future asymmetric reactions with nitrosocarbonyl intermediates.

Published
2015

29. Asymmetric Electrophilic α-Amination of Silyl Enol Ether Derivatives via the Nitrosocarbonyl Hetero-ene Reaction.

Author

Sandoval, David, Samoshin, Andrey V, and Read de Alaniz, Javier

Subjects
Copper, Alcohols, Ethers, Nitroso Compounds, Organosilicon Compounds, Molecular Structure, Amination, Catalysis, Stereoisomerism, Organic Chemistry, Chemical Sciences
Abstract

The first example of a general asymmetric nitrosocarbonyl hetero-ene reaction is described. The procedure uses a copper-catalyzed aerobic oxidation of a commercially available chiral nitrosocarbonyl precursor (EleNOr) and is operationally simple. The transformation is both high yielding and highly diastereoselective for a range of silyl enol ether derivatives. A variety of synthetically useful postfunctionalization reactions are presented along with a mechanistic rationale that can be used as a predictive model for future asymmetric reactions with nitrosocarbonyl intermediates.

Published
2015

30. 18F-Fluorodeoxyglucamines: Reductive amination of hydrophilic 18F-fluoro-2-deoxyglucose with lipophilic amines for the development of potential PET imaging agents

Author

Baranwal, Aparna and Mukherjee, Jogeshwar

Subjects
Medicinal and Biomolecular Chemistry, Organic Chemistry, Chemical Sciences, Biomedical Imaging, Neurosciences, Amination, Amines, Animals, Brain, Fluorodeoxyglucose F18, Humans, Oxidation-Reduction, Positron-Emission Tomography, Radiopharmaceuticals, Rats, Receptors, Dopamine D1, Dopamine D1 receptor, PET, Imaging, F-18-FDG, F-18-Fluorodeoxyglucamine, (18)F-FDG, (18)F-Fluorodeoxyglucamine, Pharmacology and Pharmaceutical Sciences, Medicinal & Biomolecular Chemistry, Medicinal and biomolecular chemistry, Organic chemistry
Abstract

Maillard reaction of (18)F-FDG with biological amines results in the formation of (18)F-fluorodeoxyglycosylamines ((18)F-FDGly) as pseudo-Amadori products. To increase in vivo stability, we report the reductive amination of FDGly to provide reduced fluorodeoxyglucamines (FDGlu). (18)F-Fluorodeoxyglucamines ((18)F-FDGlu), resulting from linking (18)F-FDG (hydrophilic) to lipophilic molecules containing amine group may be useful as positron emission tomography (PET) imaging agents. Two amine derivatives, 7-chloro-8-hydroxy-3-methyl-l-(3'-aminophenyl)-2,3,4,5-tetrahydro-lH-3-benzazepine (SCH 38548 for dopamine D1 receptors) and BTA-0 (for Aβ amyloid) were reacted with FDG under reductive amination conditions to yield stable products, FDGluSCH and FDGluBTA. FDGluSCH had high binding affinity to rat brain dopamine D1 receptors with a Ki of 19.5 nM while FDGluBTA had micromolar affinity for human frontal cortex Aβ plaques. (18)F-FDGluSCH was prepared in low to modest radiochemical yields and preliminary results showed binding to the rat striatum in brain slices. In vivo stability of(18)F-FDGluSCH needs to be determined. Our results suggest that (18)F-FDG is a useful 'radioactive synthon' for PET radiotracer development. Its usefulness will have to be determined on the basis of the structure-activity relationship of the target molecule.

Published
2015

31. Mechanism and Dynamics of Intramolecular C–H Insertion Reactions of 1‑Aza-2-azoniaallene Salts

Author

Hong, Xin, Bercovici, Daniel A, Yang, Zhongyue, Al-Bataineh, Nezar, Srinivasan, Ramya, Dhakal, Ram C, Houk, KN, and Brewer, Matthias

Subjects
Inorganic Chemistry, Organic Chemistry, Chemical Sciences, Theoretical and Computational Chemistry, Alkadienes, Amination, Aza Compounds, Benzyl Compounds, Models, Molecular, Pyrazoles, Salts, Stereoisomerism, General Chemistry, Chemical sciences, Engineering
Abstract

The 1-aza-2-azoniaallene salts, generated from α-chloroazo compounds by treatment with halophilic Lewis acids, undergo intramolecular C-H amination reactions to form pyrazolines in good to excellent yields. This intramolecular amination occurs readily at both benzylic and tertiary aliphatic positions and proceeds at an enantioenriched chiral center with retention of stereochemistry. Competition experiments show that insertion occurs more readily at an electron-rich benzylic position than it does at an electron-deficient one. The C-H amination reaction occurs only with certain tethers connecting the heteroallene cation and the pendant aryl groups. With a longer tether or when the reaction is intermolecular, electrophilic aromatic substitution occurs instead of C-H amination. The mechanism and origins of stereospecificity and chemoselectivity were explored with density functional theory (B3LYP and M06-2X). The 1-aza-2-azoniaallene cation undergoes C-H amination through a hydride transfer transition state to form the N-H bond, and the subsequent C-N bond formation occurs spontaneously to generate the heterocyclic product. This concerted two-stage mechanism was shown by IRC and quasi-classical molecular dynamics trajectory studies.

Published
2015

32. A Nucleophilic Strategy for Enantioselective Intermolecular α‑Amination: Access to Enantioenriched α‑Arylamino Ketones

Author

Miles, Dillon H, Guasch, Joan, and Toste, F Dean

Subjects
Organic Chemistry, Chemical Sciences, Alkenes, Amination, Aniline Compounds, Hydrazones, Hydrocarbons, Aromatic, Ketones, Stereoisomerism, General Chemistry, Chemical sciences, Engineering
Abstract

The enantioselective addition of anilines to azoalkenes was accomplished through the use of a chiral phosphoric acid catalyst. The resulting α-arylamino hydrazones were obtained in good yields and excellent enantioselectivities and provide access to enantioenriched α-arylamino ketones. A serendipitous kinetic resolution of racemic α-arylamino hydrazones is also described.

Published
2015

33. Nickel‐Catalyzed Amination of Aryl Chlorides with Ammonia or Ammonium Salts

Author

Green, Rebecca A and Hartwig, John F

Subjects
Amination, Ammonia, Ammonium Compounds, Catalysis, Crystallography, X-Ray, Ligands, Molecular Conformation, Nickel, Nitriles, amination, ammonia, arylation, cross-coupling, nickel, Chemical Sciences, Organic Chemistry
Abstract

The nickel-catalyzed amination of aryl chlorides to form primary arylamines occurs with ammonia or ammonium sulfate and a well-defined single-component nickel(0) precatalyst containing a Josiphos ligand and an η(2)-bound benzonitrile ligand. This system also catalyzes the coupling of aryl chlorides with gaseous amines in the form of their hydrochloride salts.

Published
2015

34. Direct Asymmetric Amination of α‑Branched Cyclic Ketones Catalyzed by a Chiral Phosphoric Acid

Author

Yang, Xiaoyu and Toste, F Dean

Subjects
Organic Chemistry, Chemical Sciences, Amination, Catalysis, Chemistry Techniques, Synthetic, Ketamine, Ketones, Phosphoric Acids, Stereoisomerism, General Chemistry, Chemical sciences, Engineering
Abstract

Here we report the direct asymmetric amination of α-substituted cyclic ketones catalyzed by a chiral phosphoric acid, yielding products with a N-containing quaternary stereocenter in high yields and excellent enantioselectivities. Kinetic resolution of the starting ketone was also found to occur on some of the substrates under milder conditions, providing enantioenriched α-branched ketones, another important building block in organic synthesis. The utility of this methodology was demonstrated in the short synthesis of (S)-ketamine, the more active enantiomer of this versatile pharmaceutical.

Published
2015

35. Metal-catalysed azidation of tertiary C–H bonds suitable for late-stage functionalization

Author

Sharma, Ankit and Hartwig, John F

Subjects
Amination, Azides, Carbon, Catalysis, Electrons, Hydrogen, Indicators and Reagents, Iron, Nitrogen, General Science & Technology
Abstract

Many enzymes oxidize unactivated aliphatic C-H bonds selectively to form alcohols; however, biological systems do not possess enzymes that catalyse the analogous aminations of C-H bonds. The absence of such enzymes limits the discovery of potential medicinal candidates because nitrogen-containing groups are crucial to the biological activity of therapeutic agents and clinically useful natural products. In one prominent example illustrating the importance of incorporating nitrogen-based functionality, the conversion of the ketone of erythromycin to the -N(Me)CH2- group in azithromycin leads to a compound that can be dosed once daily with a shorter treatment time. For such reasons, synthetic chemists have sought catalysts that directly convert C-H bonds to C-N bonds. Most currently used catalysts for C-H bond amination are ill suited to the intermolecular functionalization of complex molecules because they require excess substrate or directing groups, harsh reaction conditions, weak or acidic C-H bonds, or reagents containing specialized groups on the nitrogen atom. Among C-H bond amination reactions, those forming a C-N bond at a tertiary alkyl group would be particularly valuable, because this linkage is difficult to form from ketones or alcohols that might be created in a biosynthetic pathway by oxidation. Here we report a mild, selective, iron-catalysed azidation of tertiary C-H bonds that occurs without excess of the valuable substrate. The reaction tolerates aqueous environments and is suitable for the functionalization of complex structures in the late stages of a multistep synthesis. Moreover, this azidation makes it possible to install a range of nitrogen-based functional groups, including those from Huisgen 'click' cycloadditions and the Staudinger ligation. We anticipate that these reactions will create opportunities to modify natural products, their precursors and their derivatives to produce analogues that contain different polarity and charge as a result of nitrogen-containing groups. It could also be used to help identify targets of biologically active molecules by creating a point of attachment--for example, to fluorescent tags or 'handles' for affinity chromatography--directly on complex molecular structures.

Published
2015

36. Metal-catalysed azidation of tertiary C-H bonds suitable for late-stage functionalization.

Author

Sharma, Ankit and Hartwig, John

Subjects
Amination, Azides, Carbon, Catalysis, Electrons, Hydrogen, Indicators and Reagents, Iron, Nitrogen
Abstract

Many enzymes oxidize unactivated aliphatic C-H bonds selectively to form alcohols; however, biological systems do not possess enzymes that catalyse the analogous aminations of C-H bonds. The absence of such enzymes limits the discovery of potential medicinal candidates because nitrogen-containing groups are crucial to the biological activity of therapeutic agents and clinically useful natural products. In one prominent example illustrating the importance of incorporating nitrogen-based functionality, the conversion of the ketone of erythromycin to the -N(Me)CH2- group in azithromycin leads to a compound that can be dosed once daily with a shorter treatment time. For such reasons, synthetic chemists have sought catalysts that directly convert C-H bonds to C-N bonds. Most currently used catalysts for C-H bond amination are ill suited to the intermolecular functionalization of complex molecules because they require excess substrate or directing groups, harsh reaction conditions, weak or acidic C-H bonds, or reagents containing specialized groups on the nitrogen atom. Among C-H bond amination reactions, those forming a C-N bond at a tertiary alkyl group would be particularly valuable, because this linkage is difficult to form from ketones or alcohols that might be created in a biosynthetic pathway by oxidation. Here we report a mild, selective, iron-catalysed azidation of tertiary C-H bonds that occurs without excess of the valuable substrate. The reaction tolerates aqueous environments and is suitable for the functionalization of complex structures in the late stages of a multistep synthesis. Moreover, this azidation makes it possible to install a range of nitrogen-based functional groups, including those from Huisgen click cycloadditions and the Staudinger ligation. We anticipate that these reactions will create opportunities to modify natural products, their precursors and their derivatives to produce analogues that contain different polarity and charge as a result of nitrogen-containing groups. It could also be used to help identify targets of biologically active molecules by creating a point of attachment--for example, to fluorescent tags or handles for affinity chromatography--directly on complex molecular structures.

Published
2015

37. Vicinal Diamination of Alkenes under Rh-Catalysis

Author

Olson, David E, Su, Justin Y, Roberts, D Allen, and Du Bois, J

Subjects
Inorganic Chemistry, Organic Chemistry, Chemical Sciences, Alkenes, Amination, Catalysis, Diamines, Molecular Structure, Organometallic Compounds, Rhodium, General Chemistry, Chemical sciences, Engineering
Abstract

The synthesis of 1,2-diamines has been achieved through a single-step, tandem sequence involving Rh-catalyzed aziridination followed by NaI-promoted rearrangement to an isomeric cyclic sulfamide. Facile ring opening of these products in hot water and pyridine affords differentially protected vicinal diamines. Demonstration of the utility of this method for the syntheses of (±)-enduracididine and (±)-allo-enduracididine is highlighted.

Published
2014

38. Vicinal diamination of alkenes under Rh-catalysis.

Author

Olson, David E, Su, Justin Y, Roberts, D Allen, and Du Bois, J

Subjects
Rhodium, Diamines, Alkenes, Organometallic Compounds, Molecular Structure, Amination, Catalysis, General Chemistry, Chemical Sciences
Abstract

The synthesis of 1,2-diamines has been achieved through a single-step, tandem sequence involving Rh-catalyzed aziridination followed by NaI-promoted rearrangement to an isomeric cyclic sulfamide. Facile ring opening of these products in hot water and pyridine affords differentially protected vicinal diamines. Demonstration of the utility of this method for the syntheses of (±)-enduracididine and (±)-allo-enduracididine is highlighted.

Published
2014

39. From Racemic Alcohols to Enantiopure Amines: Ru-Catalyzed Diastereoselective Amination

Author

Oldenhuis, Nathan J, Dong, Vy M, and Guan, Zhibin

Subjects
Alcohols, Amination, Amines, Catalysis, Molecular Structure, Organometallic Compounds, Ruthenium, Stereoisomerism, Chemical Sciences, General Chemistry
Abstract

A commercially available ruthenium(II) PNP-type pincer catalyst (Ru-Macho) promotes the formation of α-chiral tert-butanesulfinylamines from racemic secondary alcohols and Ellman's chiral tert-butanesulfinamide via a hydrogen borrowing strategy. The formation of α-chiral tert-butanesulfinylamines occurs in yields ranging from 31% to 89% with most examples giving >95:5 dr.

Published
2014

40. Palladium-Catalyzed Amination of Aryl Chlorides and Bromides with Ammonium Salts

Author

Green, Rebecca A and Hartwig, John F

Subjects
Amination, Amines, Ammonia, Aniline Compounds, Catalysis, Hydrocarbons, Brominated, Hydrocarbons, Chlorinated, Molecular Structure, Palladium, Salts, Chemical Sciences, Organic Chemistry
Abstract

We report the palladium-catalyzed coupling of aryl halides with ammonia and gaseous amines as their ammonium salts. The coupling of aryl chlorides and ortho-substituted aryl bromides with ammonium sulfate forms anilines with higher selectivity for the primary arylamine over the diarylamine than couplings with ammonia in dioxane. The resting state for the reactions of aryl chlorides is different from the resting state for the reactions of aryl bromides, and this change in resting states is proposed to account for a difference in selectivities for reactions of the two haloarenes.

Published
2014

41. Nickel-Catalyzed Amination of Aryl Chlorides and Sulfamates in 2‑Methyl-THF

Author

Nathel, Noah F Fine, Kim, Junyong, Hie, Liana, Jiang, Xingyu, and Garg, Neil K

Subjects
nickel, catalysis, amination, cross-coupling 2-methyl-THF, green chemistry, 2-methyl-THF, cross-coupling, Inorganic Chemistry, Organic Chemistry, Chemical Engineering
Abstract

The nickel-catalyzed amination of aryl O-sulfamates and chlorides using the green solvent 2-methyl-THF is reported. This methodology employs the commercially available and air-stable precatalyst NiCl2(DME), is broad in scope, and provides access to aryl amines in synthetically useful yields. The utility of this methodology is underscored by examples of gram-scale couplings conducted with catalyst loadings as low as 1 mol % nickel. Moreover, the nickel-catalyzed amination described is tolerant of heterocycles and should prove useful in the synthesis of pharmaceutical candidates and other heteroatom-containing compounds.

Published
2014

42. Nickel-Catalyzed Amination of Aryl Chlorides and Sulfamates in 2-Methyl-THF.

Author

Fine Nathel, Noah F, Kim, Junyong, Hie, Liana, Jiang, Xingyu, and Garg, Neil K

Subjects
2-methyl-THF, amination, catalysis, cross-coupling, green chemistry, nickel, cross-coupling 2-methyl-THF, Inorganic Chemistry, Organic Chemistry, Chemical Engineering
Abstract

The nickel-catalyzed amination of aryl O-sulfamates and chlorides using the green solvent 2-methyl-THF is reported. This methodology employs the commercially available and air-stable precatalyst NiCl2(DME), is broad in scope, and provides access to aryl amines in synthetically useful yields. The utility of this methodology is underscored by examples of gram-scale couplings conducted with catalyst loadings as low as 1 mol % nickel. Moreover, the nickel-catalyzed amination described is tolerant of heterocycles and should prove useful in the synthesis of pharmaceutical candidates and other heteroatom-containing compounds.

Published
2014

43. From racemic alcohols to enantiopure amines: Ru-catalyzed diastereoselective amination.

Author

Oldenhuis, Nathan J, Dong, Vy M, and Guan, Zhibin

Subjects
Ruthenium, Alcohols, Amines, Organometallic Compounds, Molecular Structure, Amination, Catalysis, Stereoisomerism, General Chemistry, Chemical Sciences
Abstract

A commercially available ruthenium(II) PNP-type pincer catalyst (Ru-Macho) promotes the formation of α-chiral tert-butanesulfinylamines from racemic secondary alcohols and Ellman's chiral tert-butanesulfinamide via a hydrogen borrowing strategy. The formation of α-chiral tert-butanesulfinylamines occurs in yields ranging from 31% to 89% with most examples giving >95:5 dr.

Published
2014

44. Palladium-catalyzed amination of aryl chlorides and bromides with ammonium salts.

Author

Green, Rebecca A and Hartwig, John F

Subjects
Palladium, Ammonia, Salts, Amines, Aniline Compounds, Hydrocarbons, Brominated, Hydrocarbons, Chlorinated, Molecular Structure, Amination, Catalysis, Hydrocarbons, Brominated, Chlorinated, Chemical Sciences, Organic Chemistry
Abstract

We report the palladium-catalyzed coupling of aryl halides with ammonia and gaseous amines as their ammonium salts. The coupling of aryl chlorides and ortho-substituted aryl bromides with ammonium sulfate forms anilines with higher selectivity for the primary arylamine over the diarylamine than couplings with ammonia in dioxane. The resting state for the reactions of aryl chlorides is different from the resting state for the reactions of aryl bromides, and this change in resting states is proposed to account for a difference in selectivities for reactions of the two haloarenes.

Published
2014

45. Enzyme inhibition by hydroamination: design and mechanism of a hybrid carmaphycin-syringolin enone proteasome inhibitor.

Author

Trivella, Daniela BB, Pereira, Alban R, Stein, Martin L, Kasai, Yusuke, Byrum, Tara, Valeriote, Frederick A, Tantillo, Dean J, Groll, Michael, Gerwick, William H, and Moore, Bradley S

Subjects
Cell Line, Tumor, HCT116 Cells, Humans, Alkenes, Ketones, Peptides, Cyclic, Proteasome Endopeptidase Complex, Dipeptides, Antineoplastic Agents, Biological Products, Drug Screening Assays, Antitumor, Cell Proliferation, Molecular Conformation, Structure-Activity Relationship, Amination, Cyclization, Dose-Response Relationship, Drug, Quantum Theory, Models, Molecular, Biocatalysis, Proteasome Inhibitors, Cancer, Medicinal and Biomolecular Chemistry, Organic Chemistry, Biochemistry and Cell Biology
Abstract

Hydroamination reactions involving the addition of an amine to an inactivated alkene are entropically prohibited and require strong chemical catalysts. While this synthetic process is efficient at generating substituted amines, there is no equivalent in small molecule-mediated enzyme inhibition. We report an unusual mechanism of proteasome inhibition that involves a hydroamination reaction of alkene derivatives of the epoxyketone natural product carmaphycin. We show that the carmaphycin enone first forms a hemiketal intermediate with the catalytic Thr1 residue of the proteasome before cyclization by an unanticipated intramolecular alkene hydroamination reaction, resulting in a stable six-membered morpholine ring. The carmaphycin enone electrophile, which does not undergo a 1,4-Michael addition as previously observed with vinyl sulfone and α,β-unsaturated amide-based inhibitors, is partially reversible and gives insight into the design of proteasome inhibitors for cancer chemotherapy.

Published
2014

46. Chiral Anion Phase Transfer of Aryldiazonium Cations: An Enantioselective Synthesis of C3‐Diazenated Pyrroloindolines

Author

Nelson, Hosea M, Reisberg, Solomon H, Shunatona, Hunter P, Patel, Jigar S, and Toste, F Dean

Subjects
Anions, Catalysis, Cations, Cyclization, Diazonium Compounds, Indoles, Pyrroles, Stereoisomerism, Tryptamines, amination, asymmetric catalysis, cyclization, phase-transfer catalysis, photolysis, Chemical Sciences, Organic Chemistry
Abstract

Herein is reported the first asymmetric utilization of aryldiazonium cations as a source of electrophilic nitrogen. This is achieved through a chiral anion phase-transfer pyrroloindolinization reaction that forms C3-diazenated pyrroloindolines from simple tryptamines and aryldiazonium tetrafluoroborates. The title compounds are obtained in up to 99% yield and 96% ee. The air- and water-tolerant reaction allows electronic and steric diversity of the aryldiazonium electrophile and the tryptamine core.

Published
2014

47. Analyzing Site Selectivity in Rh2(esp)2‑Catalyzed Intermolecular C–H Amination Reactions

Author

Bess, Elizabeth N, DeLuca, Ryan J, Tindall, Daniel J, Oderinde, Martins S, Roizen, Jennifer L, Du Bois, J, and Sigman, Matthew S

Subjects
Inorganic Chemistry, Organic Chemistry, Chemical Sciences, Amination, Carbon, Catalysis, Hydrogen, Models, Chemical, Rhodium, General Chemistry, Chemical sciences, Engineering
Abstract

Predicting site selectivity in C-H bond oxidation reactions involving heteroatom transfer is challenged by the small energetic differences between disparate bond types and the subtle interplay of steric and electronic effects that influence reactivity. Herein, the factors governing selective Rh2(esp)2-catalyzed C-H amination of isoamylbenzene derivatives are investigated, where modification to both the nitrogen source, a sulfamate ester, and substrate are shown to impact isomeric product ratios. Linear regression mathematical modeling is used to define a relationship that equates both IR stretching parameters and Hammett σ(+) values to the differential free energy of benzylic versus tertiary C-H amination. This model has informed the development of a novel sulfamate ester, which affords the highest benzylic-to-tertiary site selectivity (9.5:1) observed for this system.

Published
2014

48. Analyzing site selectivity in Rh2(esp)2-catalyzed intermolecular C-H amination reactions.

Author

Bess, Elizabeth N, DeLuca, Ryan J, Tindall, Daniel J, Oderinde, Martins S, Roizen, Jennifer L, Du Bois, J, and Sigman, Matthew S

Subjects
Carbon, Hydrogen, Rhodium, Amination, Catalysis, Models, Chemical, Models, Chemical, Chemical Sciences, General Chemistry
Abstract

Predicting site selectivity in C-H bond oxidation reactions involving heteroatom transfer is challenged by the small energetic differences between disparate bond types and the subtle interplay of steric and electronic effects that influence reactivity. Herein, the factors governing selective Rh2(esp)2-catalyzed C-H amination of isoamylbenzene derivatives are investigated, where modification to both the nitrogen source, a sulfamate ester, and substrate are shown to impact isomeric product ratios. Linear regression mathematical modeling is used to define a relationship that equates both IR stretching parameters and Hammett σ(+) values to the differential free energy of benzylic versus tertiary C-H amination. This model has informed the development of a novel sulfamate ester, which affords the highest benzylic-to-tertiary site selectivity (9.5:1) observed for this system.

Published
2014

49. Controlling First-Row Catalysts: Amination of Aryl and Heteroaryl Chlorides and Bromides with Primary Aliphatic Amines Catalyzed by a BINAP-Ligated Single-Component Ni(0) Complex

Author

Ge, Shaozhong, Green, Rebecca A, and Hartwig, John F

Subjects
Amination, Amines, Catalysis, Hydrocarbons, Brominated, Hydrocarbons, Chlorinated, Models, Molecular, Molecular Structure, Naphthalenes, Nickel, Organometallic Compounds, Chemical Sciences, General Chemistry
Abstract

First-row metal complexes often undergo undesirable one-electron redox processes during two-electron steps of catalytic cycles. We report the amination of aryl chlorides and bromides with primary aliphatic amines catalyzed by a well-defined, single-component nickel precursor (BINAP)Ni(η(2)-NC-Ph) (BINAP = 2,2'-bis(biphenylphosphino)-1,1'-binaphthalene) that minimizes the formation of Ni(I) species and (BINAP)2Ni. The scope of the reaction encompasses electronically varied aryl chlorides and nitrogen-containing heteroaryl chlorides, including pyridine, quinoline, and isoquinoline derivatives. Mechanistic studies support the catalytic cycle involving a Ni(0)/Ni(II) couple for this nickel-catalyzed amination and are inconsistent with a Ni(I) halide intermediate. Monitoring the reaction mixture by (31)P NMR spectroscopy identified (BINAP)Ni(η(2)-NC-Ph) as the resting state of the catalyst in the amination of both aryl chlorides and bromides. Kinetic studies showed that the amination of aryl chlorides and bromides is first order in both catalyst and aryl halide and zero order in base and amine. The reaction of a representative aryl chloride is inverse first order in PhCN, but the reaction of a representative aryl bromide is zero order in PhCN. This difference in the order of the reaction in PhCN indicates that the aryl chloride reacts with (BINAP)Ni(0), formed by dissociation PhCN from (BINAP)Ni(η(2)-NC-Ph), but the aryl bromide directly reacts with (BINAP)Ni(η(2)-NC-Ph). The overall kinetic behavior is consistent with turnover-limiting oxidative addition of the aryl halide to Ni(0). Several pathways for catalyst decomposition were identified, such as the formation of the catalytically inactive bis(amine)-ligated arylnickel(II) chloride, (BINAP)2Ni(0), and the Ni(I) species [(BINAP)Ni(μ-Cl)]2. By using a well-defined nickel complex as catalyst, the formation of (BINAP)2Ni(0) is avoided and the formation of the Ni(I) species [(BINAP)Ni(μ-Cl)]2 is minimized.

Published
2014

50. Controlling first-row catalysts: amination of aryl and heteroaryl chlorides and bromides with primary aliphatic amines catalyzed by a BINAP-ligated single-component Ni(0) complex.

Author

Ge, Shaozhong, Green, Rebecca A, and Hartwig, John F

Subjects
Nickel, Amines, Hydrocarbons, Brominated, Hydrocarbons, Chlorinated, Organometallic Compounds, Naphthalenes, Molecular Structure, Amination, Catalysis, Models, Molecular, Hydrocarbons, Brominated, Chlorinated, Models, Molecular, Chemical Sciences, General Chemistry
Abstract

First-row metal complexes often undergo undesirable one-electron redox processes during two-electron steps of catalytic cycles. We report the amination of aryl chlorides and bromides with primary aliphatic amines catalyzed by a well-defined, single-component nickel precursor (BINAP)Ni(η(2)-NC-Ph) (BINAP = 2,2'-bis(biphenylphosphino)-1,1'-binaphthalene) that minimizes the formation of Ni(I) species and (BINAP)2Ni. The scope of the reaction encompasses electronically varied aryl chlorides and nitrogen-containing heteroaryl chlorides, including pyridine, quinoline, and isoquinoline derivatives. Mechanistic studies support the catalytic cycle involving a Ni(0)/Ni(II) couple for this nickel-catalyzed amination and are inconsistent with a Ni(I) halide intermediate. Monitoring the reaction mixture by (31)P NMR spectroscopy identified (BINAP)Ni(η(2)-NC-Ph) as the resting state of the catalyst in the amination of both aryl chlorides and bromides. Kinetic studies showed that the amination of aryl chlorides and bromides is first order in both catalyst and aryl halide and zero order in base and amine. The reaction of a representative aryl chloride is inverse first order in PhCN, but the reaction of a representative aryl bromide is zero order in PhCN. This difference in the order of the reaction in PhCN indicates that the aryl chloride reacts with (BINAP)Ni(0), formed by dissociation PhCN from (BINAP)Ni(η(2)-NC-Ph), but the aryl bromide directly reacts with (BINAP)Ni(η(2)-NC-Ph). The overall kinetic behavior is consistent with turnover-limiting oxidative addition of the aryl halide to Ni(0). Several pathways for catalyst decomposition were identified, such as the formation of the catalytically inactive bis(amine)-ligated arylnickel(II) chloride, (BINAP)2Ni(0), and the Ni(I) species [(BINAP)Ni(μ-Cl)]2. By using a well-defined nickel complex as catalyst, the formation of (BINAP)2Ni(0) is avoided and the formation of the Ni(I) species [(BINAP)Ni(μ-Cl)]2 is minimized.

Published
2014

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