Bromoporphyrins as versatile synthons for modular construction of chiral porphyrins: cobalt-catalyzed highly enantioselective and diastereoselective cyclopropanation

5,10-Bis(2',6'-dibromophenyl)porphyrins bearing various substituents at the 10 and 20 positions were demonstrated to be versatile synthons for modular construction of chiral porphyrins via palladium-catalyzed amidation reactions with chiral amides. The quadruple carbon-nitrogen bond formation reactions were accomplished in high yields with different chiral amide building blocks under mild conditions, forming a family of D2-symmetric chiral porphyrins. Cobalt(II) complexes of these chiral porphyrins were prepared in high yields and shown to be active catalysts for highly enantioselective and diastereoselective cyclopropanation under a practical one-pot protocol (alkenes as limiting reagents and no slow addition of diazo reagents).     

Stereoselective synthesis of functionalized pyrrolidines by ruthenium porphyrin-catalyzed decomposition of alpha-diazo esters and cascade azomethine ylide formation/1,3-dipolar cycloaddition reactions

[reaction: see text] Ruthenium porphyrins catalyze three-component coupling reaction of alpha-diazo esters with a series of N-benzylidene imines and alkenes to form functionalized pyrrolidines in excellent diastereoselectivities. The reaction proceeds via a reactive ruthenium-carbene intermediate and its subsequent reaction with imine to generate azomethine ylide, which reacts with alkenes via 1,3-diploar cycloaddition.     

Synthesis of sterically encumbered porphyrins as catalysts for shape‐selective oxidations

A general method is described for the synthesis of sterically encumbered porphyrins whose shielding superstructure can take on the enzymatic role of substrate discrimination. This method is based on an improved synthesis of pyrroles substituted with a 2,6‐dibromophenyl group, followed by a Suzuki cross‐coupling to replace the Br with aryl groups. Porphyrins assembled from such pyrrole units have a barrel shape with the metal center completely fenced by four β‐substituted terphenyl shielding wings. The Fe and Mn porphyrins prove to be excellent catalysts for regioselective epoxidation of alkenes.     

Synthesis of poly(ethylene glycol)-supported manganese porphyrins: efficient,recoverable and recyclable catalysts for epoxidation of alkenes

Two new poly(ethylene glycol) supported manganese porphyrins have been prepared and their catalytic activity and recyclability were investigated for the epoxidation of alkenes using H2O2 and PhIO as stoichiometric oxidants.     

[Co(TPP)]-Catalyzed Formation of Substituted Piperidines

Radical cyclization via cobalt(III)-carbene radical intermediates is a powerful method for the synthesis of (hetero)cyclic structures. Building on the recently reported synthesis of five-membered N-heterocyclic pyrrolidines catalyzed by Co^II porphyrins, the [Co(TPP)]-catalyzed formation of useful six-membered N-heterocyclic piperidines directly from linear aldehydes is presented herein. The piperidines were obtained in overall high yields, with linear alkenes being formed as side products in small amounts. A DFT study was performed to gain a deeper mechanistic understanding of the cobalt(II)-porphyrin-catalyzed formation of pyrrolidines, piperidines, and linear alkenes. The calculations showed that the alkenes are unlikely to be formed through an expected 1,2-hydrogen-atom transfer to the carbene carbon. Instead, the calculations were consistent with a pathway involving benzyl-radical formation followed by radical-rebound ring closure to form the piperidines. Competitive 1,5-hydrogen-atom transfer from the β-position to the benzyl radical explained the formation of linear alkenes as side products.     

Inhibitory effect of 2,6-di-<Emphasis Type="Italic">tert</Emphasis>-butylphenol groups in iron and manganese porphyrins on the catalytic activity in the oxidation of hydrocarbons by hydrogen peroxide

Iron and manganese porphyrins containing 2,6-di-tert-butylphenyl groups (R₄PFeCl and R₄PMnCl) have been synthesized to be further immobilized on silica gels via various spacers. The activity of these porphyrins in the oxidation of alkanes and alkenes by hydrogen peroxide has been studied. 2,6-Di-tert-butylphenol groups decrease the catalytic activity of porphyrins in oxidation processes.     

Oxo-bridged metal carbene complexes. Synthesis,structure and reactivities of [[Os(Por)(CPh2)]2]O (Por = porphyrinato dianion)

Dinuclear mu-oxo osmium porphyrins containing terminal Os=CPh2 bonds with a linear C=Os-O-Os=C moiety were prepared, which are reactive toward pyridine to form [Os(Por)(CPh2)(py)] and are active catalysts for inter- and intra-molecular cyclopropanation of alkenes and for carbene insertion into saturated C-H bonds.     

Sterically crowded cyclopropanation catalysts. Syn-selectivity using rhodium(III)porphyrins

Rhodium(III)porphyrins catalyze the decomposition of ethyl diazoacetate and the transfer of ethoxy-carbonylcarbene to alkenes to form cyclopropanes in moderate to high yields. When compared with other catalysts a large syn-selectivity was observed on reaction with cis-alkenes. This selectivity increased with the size of the substituents, and suggested a preferential direction of approach of the alkene towards a rhodium—carbene complex.     

Stereo- and enantioselective alkene epoxidations: a comparative study of D4- and D2-symmetric homochiral trans-dioxoruthenium(VI) porphyrins

The mechanism of stoichiometric enantioselective alkene epoxidations by the D4- and D2-symmetric homochiral trans-dioxoruthenium(VI) porphyrins, [RuVI(D4-Por*)O2] (1) and [RuVI(D2-Por*)O2] (2a), in the presence of pyrazole (Hpz) was studied by UV/Vis spectrophotometry and analysis of the organic products. The enantioselectivity of styrene oxidations is more susceptible to steric effects than to substituent electronic effects. Up to 72% ee was achieved for epoxidation of 3-substituted and cis-disubstituted styrenes by employing 1 as the oxidant, whereas entantioselectivities of only 20-40% were obtained in the reactions with 2-substituted and trans-disubstituted styrenes. Complex 2a oxidized 2-substituted styrenes to their epoxides in up to 88% ee. Its reactions with trans-alkenes are more enantioselective (67% ee) than with the cis-alkenes (40% ee). Based on a two-dimensional NOESY NMR study, 2a was found to adopt a more open conformation in benzene than in dichloromethane, which explains the observed solvent-dependent enantioselectivity of its reactions with alkenes. The oxidation of aromatic alkenes by the chiral dioxoruthenium(VI) porphyrins proceeds through the rate-limiting formation of a benzylic radical intermediate; the observed enantioselectivity (eeobs) depends on both the facial selectivity of the first C-O bond formation step and the diastereoselectivity of the subsequent epoxide ring closure. To account for the observed facial selection, "side-on" and "top-on" approach transition state models are examined (see: B. D. Brandes, E. N. Jacobsen, Tetrahedron Lett. 1995, 36, 5123).     

Proline‐Modified Porphyrin Catalysts for Enantioselective Epoxidations: Design,Synthesis, and Reactivity

The syntheses of various strapped and ‘picket‐fence’ chiral porphyrins are described, and their reactivities towards the enantioselective epoxidation of alkenes are reported. Four L ‐proline residues provide the chirality for the various meso‐substituted catalysts, which differ by either the spatial arrangement of the stereogenic centers or the nature and length of the straps. The resulting bridged structures possess four amide linkages in each strap, leading to highly rigid molecules with well‐defined geometries whereas the strapped Fe catalysts gave rise to only moderate enantioselectivities, the C₂‐symmetrical ones being superior to the D₂‐symmetrical compounds. The D₂‐symmetrical ‘picket‐fence’ porphyrins were as selective as their strapped counterparts.     

Progress in fluoroalkylation of organic compounds via sulfinatodehalogenation initiation system

The sulfinatodehalogenation reaction represents one of the most important methodologies to incorporate fluorine into organic molecules. Using inexpensive sulfur-containing reactants such as Na(2)S(2)O(4) under mild conditions, per- and polyfluoroalkyl halides (R(F)X, X = Br, I, CCl(3)) can be transformed smoothly into the corresponding sulfinate salts. This method is also used for the perfluoroalkylation of alkenes, dienes, alkynes and aromatics. Notably, after 1998, the sulfinatodehalogenation of perfluoroalkyl chlorides (R(F)Cl) has been realized by using dimethylsulfoxide (DMSO) as a solvent instead of CH(3)CN/H(2)O in the Na(2)S(2)O(4)/NaHCO(3) initiation system. Perfluoroalkyl chlorides, ethyl chlorofluoroacetates and chlorodifluoroacetates, and even nonfluorinated compounds, such as ethyl chloro- or dichloroacetates and chloroform, were either converted into the corresponding sulfinate salts or alkylated alkenes, alkynes and aromatics (including porphyrins). The sulfinatodehalogenation reaction has remarkable advantages. With the increasing demands to utilize the unique properties of fluorine and fluorinated functional groups in medicinal, agricultural and material sciences, we believe that there will continue to be useful developments in sulfinatodehalogenation chemistry and it will be applied more widely in the future.     

Dendritic metalloporphyrins as catalysts for organic transformations

Dendritic manganese, iron, and ruthenium porphyrins with dendritic wedges attached to the periphery of meso-tetraphenylporphyrin (TPP) or meso-triarylporphyrin macrocycle were reported to be active catalysts for epoxidation or cyclopropanation of alkenes or oxidation of sulfides. The dendritic manganese and iron porphyrin catalysts exhibit considerably higher regioselectivity and shape selectivity than the respective parent catalyst [M(TPP)Cl] (M = Mn, Fe). Systematic increase in shape selectivity, diastereoselectivity, epoxide/sulfoxide selectivity, or catalyst stability with increasing generation number of the dendritic wedges is observed for the alkene epoxidation or sulfide oxidation reactions catalyzed by these dendritic manganese, iron, and ruthenium porphyrins. To cite this article: C.-M. Che, C. R. Chimie 6 (2003).     

Structural and oxo-transfer reactivity differences of hexacoordinate and pentacoordinate (nitro)(tetraphenylporphinato)cobalt(III) derivatives

The oxo-transfer catalyst (nitro)(pyridyl)cobalt(III) tetraphenylporphyrin has been reinvestigated by substitution of the distal pyridine ligand with 4-N,N-dimethylaminopyridine and 3,5-dichloropyridine. Differences in their structures and in the reactivity of the compounds toward catalytic secondary oxo transfer were investigated by FT-IR and UV-visible spectroscopy, cyclic voltammetry, X-ray diffraction, semiempirical calculations, and reactions with alkenes in dichloromethane solution. Very modest differences in the hexacoordinate compounds' structures were predicted and observed, but the secondary oxo-transfer reactivity at the nitro ligand varies markedly with the basicity of the pyridine ligand and the position of the coordination equilibrium. Oxo transfer occurs rapidly through the pentacoordinate species (nitro)cobalt(III) tetraphenylporphyrin that is generated by dissociation of the pyridine ligand and therefore is strongly related to the Hammett parameters of these nitrogenous bases. The reactive pentacoordinate species CoTPP(NO(2)) can be generated in solution by addition of lithium perchlorate to (py)CoTPP(NO(2)) by Lewis acid-base interactions or more simply by using the weaker Lewis base Cl(2)py instead of py as the distal ligand. In contrast to pentacoordinate (nitro)iron porphyrins, disproportionation reactions of CoTPP(NO(2)) compound are not evident. This pentacoordinate derivative, CoTPP(NO(2)), is reactive enough to stoichiometrically oxidize allyl bromide in minutes. Preliminary catalytic oxidation reaction studies of alkenes also indicate the involvement of both radical and nonradical oxo-transfer steps in the mechanism, suggesting formation of a peroxynitro intermediate in the reaction of the reduced CoTPP(NO) with O(2).     

Construction of multiporphyrin arrays using ruthenium and rhodium coordination to phosphines

The synthesis of linear multiporphyrin arrays with mono- and bisphosphine-substituted porphyrins as ligand donors and ruthenium(II) or rhodium(III) porphyrins as ligand acceptors is described. With appropriate amounts of the building blocks mixed, linear dimeric and trimeric arrays have been synthesized and analyzed by (1)H NMR and (31)P NMR spectroscopy. The Ru/Rh acceptor porphyrins can be located either at the periphery or in the center of the array. Likewise, the monophosphine porphyrins can be positioned at the periphery, thus allowing a high degree of freedom in the overall composition of the arrays. This way, both donor and acceptor porphyrins can act as chain extenders or terminators. One of the trimeric complexes with two nickel and one ruthenium porphyrin has also been analyzed by X-ray crystallography. Attempts have also been made to synthesize higher order arrays by mixing appropriate amounts of the porphyrins; however, from the NMR data it cannot be concluded if monodisperse five, seven, or nine porphyrin arrays are present or if the solutions are composed of a statistical mixture of smaller and larger arrays.     

Synthesis of meso-arylsulfanyl- and alkylsulfanyl-substituted porphyrins via palladium-mediated C-S bond formation

A family of new meso-arylsulfanyl- and alkylsulfanyl-substituted porphyrins were efficiently synthesized from direct reactions of meso-brominated porphyrins with thiols via palladium-mediated C-S bond formation. The catalytic method can be performed under mild conditions with both mono- and bis-substituted meso-bromoporphyrins as well as their zinc complexes and is suitable for different types of thiols. With the use of selenols, meso-seleno-substituted porphyrins can also be prepared similarly.     

Dendritic ruthenium porphyrins: a new class of highly selective catalysts for alkene epoxidation and cyclopropanation

Attachment of Fréchet-type poly(benzyl ether) dendrons [G-n] to carbonylruthenium(II) meso-tetraphenylporphyrin (5) using covalent etheric bonds forms a series of dendritic ruthenium(II) porphyrins 5-[G-n](m) (m=4, n=1, 2; m=8, n=0-2). The attachment was realized by treating the carbonylruthenium(II) complex of 5,10,15,20- tetrakis(4'-hydroxyphenyl)porphyrin or 5,10,15,20-tetrakis(3',5'-dihydroxyphenyl)porphyrin with [G-n]OSO(2)Me in refluxing dry acetone in the presence of potassium carbonate and [18]crown-6. Complexes 5-[G-n](m) were characterized by UV/Vis, IR, and NMR spectroscopy and mass spectrometry. All of the dendritic ruthenium porphyrins are highly selective catalysts for epoxidation of alkenes with 2,6-dichloropyridine N-oxide (Cl(2)pyNO). The chemo- or diastereoselectivity increases with the generation number of the dendron and the number of dendrons attached to 5, and complex 5-[G-2](8) exhibits remarkable selectivity or turnover number in catalyzing the Cl(2)pyNO epoxidation of a variety of alkene substrates including styrene, trans-/cis-stilbene, 2,2-dimethylchromene, cyclooctene, and unsaturated steroids such as cholesteryl esters and estratetraene derivative. The cyclopropanation of styrene and its para-substituted derivatives with ethyl diazoacetate catalyzed by 5-[G-2](8) is highly trans selective.     

5-Aminolaevulinic acid (ALA) induced formation of different fluorescent porphyrins: a study of the biosynthesis of porphyrins by bacteria of the human digestive tract

Aminolaevulinic acid (ALA) induces porphyrin formation in almost all living cells. The fluorescence spectra of porphyrins produced from a variety of 31 bacterial strains from the human oral cavity and other parts of digestive tract have been examined. Many of the bacteria exposed to ALA were able to induce protoporphyrin IX (PpIX) fluorescence, but under aerobic condition some bacteria can also produced different fluorescent porphyrins, in particular water-soluble porphyrins that can arise from an oxidation of the corresponding porphyrinogen precursors. The formation of fluorescent porphyrins can be different from one bacterial strain to another, but also one specific bacterium can form different fluorescent porphyrins. Irradiation of the ALA incubated cultures led to a rapid formation of water-soluble porphyrins exhibiting fluorescence maxima at wavelengths of 618-620 nm. This light induced formation of water-soluble porphyrins could be attributed to a photooxidation of the non-fluorescent (Uro/Copro)-porphyrinogen precursors. Addition of detergents to some of the bacterial cultures led to a strong PpIX fluorescence increase, indicating that some of the PpIX originally produced can be present in a non-fluorescent, probably aggregated, form. The large abundance of bacteria in the oral cavity and other parts of digestive tract, with their capacity to easily produce fluorescent porphyrins, indicates that such bacterial fluorescence should be suppressed during the ALA-based diagnosis of tumours in order to eliminate false positive results.     

The reaction of porphyrins with organolithium reagents

Porphyrins react readily with organolithium reagents, preferentially in the meso positions. The overall reaction is a nucleophilic substitution and proceeds via initial reaction of the organic nucleophile with a meso carbon yielding an anionic species which is hydrolyzed to a porphodimethene (5,15-dihydroporphyrin), formally constituting an addition reaction to two Cm positions. Subsequent oxidation with 2,3-dichloro-5,6-dicyano-1,4-benzoquinone (DDQ) yields meso-substituted porphyrins. The reaction is highly versatile as it is accomplished in high, often quantitative yields with various alkyl or aryl lithium reagents. In addition, LiR can be used for reaction with a variety of metal complexes (best with NiII, but also with ZnII, CuII, and CoII) and most useful with free base porphyrins. Similarly beneficial this reaction can be used in sequence for the introduction of 1, 2, 3, or 4 (different) meso substituents giving for the first time an entry into any desired meso-substituted porphyrin. If meso-substituted porphyrins are used, reaction with LiR can be used for either the preparation of phlorins (already known reaction), porphodimethenes (5,15-dihydroporphyrins, including those with exocyclic double bonds, for example, 5(1),5(2)-didehydroporphyrins) or chlorins (2,3-dihydroporphyrins) depending on the substituent type in the reactant porphyrins. Thus, this reaction presents a generally applicable method for the facile and versatile functionalization of porphyrins.     

N-acylsulfonamide assisted tandem C-H olefination/annulation: synthesis of isoindolinones

A tandem C-H olefination/annulation sequence directed by N-acylsulfonamides affords a variety of isoindolinones. This transformation is compatible with aliphatic alkenes as well as conjugated alkenes. Notably, molecular oxygen can be used as the sole, eco-friendly oxidant.     

Regioselective and Enantioselective Copper-Catalyzed Hydroaminocarbonylation of Unactivated Alkenes and Alkynes

Given the prevalence of amide backbones in marketed pharmaceuticals and their ubiquity as critical binding units in natural peptides and proteins, it remains important to develop novel methods to construct amide bonds. We report here a general method for the anti-Markovnikov hydroaminocarbonylation of unactivated alkenes under mild conditions, using copper catalysis in combination with hydroxylamine electrophile reagents and poly(methylhydrosiloxane) (PMHS) as a cheap and environmentally friendly hydride source. The reaction tolerates a variety of functional groups and efficiently converts unactivated terminal alkenes, 1,1-disubstituted alkenes, and cyclic alkenes to the corresponding amides with exclusive anti-Markovnikov selectivity (and high enantioselectivities/diastereoselectivities). Additionally, with minimal modification of the reaction conditions, alkynes can also undergo tandem hydrogenation-hydroaminocarbonylation to alkyl amides.