New modular P-chiral ligands for Rh-catalyzed asymmetric hydrogenation

New modular P-chiral ligands have been prepared from commercially available (S)-α,α-diphenylprolinol. With these new types of ligands, up to 95% ee was achieved in the Rh-catalyzed asymmetric hydrogenation of functionalized olefins.     

Modular chiral bidentate phosphonites: design, synthesis, and application in catalytic asymmetric hydroformylation reactions

A new class of C(2)-symmetric chiral bidentate phosphonite ligands has been synthesized in moderate to good yields from readily available starting materials. Application of these air-stable chiral phosphonites in the Rh(I)-catalyzed asymmetric hydroformylation of styrene derivatives, vinyl acetate, and allyl cyanide afforded the corresponding chiral aldehydes with high regio- and enantioselectivities under mild reaction conditions. The modular nature of the ligands allows fine-tuning of the selectivities through judicious modifications of the substituents on the ligand backbone. X-ray structural analysis of the catalyst precursor suggested that the steric hindrance caused by the protruding remote substituents of the ligands into the vicinity of the metal center might be an important factor for the enantio-control of the reaction, whereas the sense of asymmetric induction can be rationalized on the basis of a trigonal-bipyramidal transition state diagram.     

Rapid in situ synthesis of [C]methyl azide and its application in C click-chemistry

We synthesized [¹¹C]methyl azide ([¹¹C]MeA) by reacting [¹¹C]methyl iodide ([¹¹C]MeI) in situ with an azide-donor and used it in the synthesis of ¹¹C-labeled 1,2,3-triazoles. A one-pot click approach comprised the infusion of gaseous [¹¹C]MeI into a mixture of NaN₃, ethynylbenzene, and CuI in water at a temperature of 100 °C yielding the ¹¹C-triazole in radiochemical yields (RCY) of 25%. In a two-step labeling protocol, we synthesized the [¹¹C]MeA in acetonitrile in advance to the click step. Using the more soluble complex as source of , a much higher trapping efficiency of [¹¹C]MeI in this solvent ensured an almost quantitative conversion of [¹¹C]MeI to [¹¹C]MeA within 5-10 min at room temperature. The [¹¹C]MeA was thereafter reacted with ethynylbenzene at 100 °C yielding 1-[¹¹C]methyl-4-phenyl-1H-1,2,3-triazole in preparative RCY of 60%. As a final proof of applicability, we used ¹¹C-click-chemistry for the labeling of N-terminal 4-ethynylbenzene derivatized d-Glu-d-Tyr-[Cys-Tyr-Trp-Lys-Thr-Cys]-Thr, a cyclic water-soluble Tyr³-octreotate derivative.     

BINAS - synthesis and use of a new ligand for propylene hydroformylation

BINAS is a new, very efficient ligand for propylene hydroformylation. BINAS is made by the sulfonation of NAPHOS. Different synthetic routes to NAPHOS are discussed. A new two step synthesis starting from 2,2′-bis(bromomethyl)-1,1′-binaphthyl is described.     

o-Alkyl-substituted aromatic phosphanes for hydroformylation studies: synthesis, spectroscopic characterization and ab initio investigations

In earlier hydroformylation studies modification of the rhodium catalyst with o-methyl-substituted or o-ethyl-substituted phosphane ligands have increased regioselectivity to branched aldehydes. The promising results achieved created a need for further studies. Hence, a wider group of o-substituted arylphosphane ligands, e.g. (2-cyclohexylphenyl)diphenylphosphane, (2-isopropylphenyl)diphenylphosphane, (2-methylnaphthyl)diphenylphosphane, (2,5-dimethylphenyl)diphenylphosphane and (2-phenylphenyl)diphenylphosphane were synthesized and tested in rhodium-catalyzed hydroformylation to support the previous findings. Characterization of the ligands was made by NMR spectroscopy (¹H, ³¹P{¹H}, ¹³C{¹H}, HSQC, COSY-90 and COLOC). Additional parameters for evaluation of the stereoelectronic properties of the ligands were provided by quantum mechanical calculations and by synthesizing Rh(acac)(CO)(PR₃) complexes. In the rhodium-catalyzed hydroformylation of propene and 1-hexene the ligands increased the formation of branched aldehydes compared to triphenylphosphane. Additionally the increasing size of the o-alkyl-substituent was found to effect favorably to the iso-selectivity.     

One pot,three component 1,3 dipolar cycloaddition: Regio and diastereoselective synthesis of spiropyrrolidinyl indenoquinoxaline derivatives

A competent and highly discriminating one-pot synthesis of highly diversified novel functionalized indenoquinoxalone grafted spiropyrrolidine linked chromene-3-carbonitrile conjugates accumulating three pharmocophoric cores, heterocyclic indenoquinoxalone, pyrrolidines and chromene-3-carbonitrile in a single molecular framework by means of 1,3-dipolar cycloaddition reaction between indenoquinoxalone, proline/benzyl amine and chromene-3-carbonitrile in ethanol under classical and microwave conditions is described. The three component 1,3-dipolar cycloaddition reaction proceeds via in situ generation of azomethine ylides by the decarboxylative condensation of indenoquinoxalone with proline/benzyl amine and their selectivity towards the endo cyclic double bonds of dipolarophile (chromene-3-carbonitrile) leading to the formation of highly functionalised regio- and diastereoselective molecular hybrids. This methodology exemplifies the green chemistry protocol such as mild reaction conditions, high yields, one-pot procedure and operational simplicity.     

Various P-chiral phosphite-type ligands: their synthesis, stereochemistry and use in Pd-catalysed allylation

A new family of readily available modular phosphite, phosphoramidite and diamidophosphite ligands with P^∗-stereocentres have been prepared from inexpensive optically active precursors. Using these novel ligands, up to 91% ee was achieved in Pd-catalysed asymmetric allylic amination. The catalytic performance is affected greatly by the structure of the phosphocentre of the ligand.     

Chiral bidentate phosphabenzene-based ligands: synthesis, coordination chemistry, and application in Rh-catalyzed asymmetric hydrogenations

Novel hydroxy-functionalized phosphabenzenes were synthesized, which provide the possibility to prepare chiral phosphabenzene-phosphites. These systems act as bidentate ligands toward rhodium centers and the corresponding metal complexes were applied in the rhodium-catalyzed asymmetric hydrogenation of prochiral substrates.     

Novel functionalised P-ligands: advances and application

Novel endo- and exocyclic phosphine ligands possessing different functionalities obtained by reduction of the PO precursors with desired stereochemistry are discussed. The diastereoselective deoxygenation including the catalytic reduction processes, the factors defining the reactivity and the role of the substituents on the stability of phosphorus atom configuration in a series of 3-aryl-3-phosphabicyclo[3.1.0]hexanes are reported. The complexation features of the ligands with Rh(III) and Pd(II) were examined and Rh(III) complexes were tested in styrene hydroformylation showing the structure-activity dependence.     

α-Fluorinated cyclic amidophosphite ligands. Their synthesis, Rh complexes and catalytic activity in the hydroformylation of styrene

The synthetic approaches to cyclic phosphite and amido(diamido)phosphite ligands bearing the residues of electron withdrawing perfluorinated tails at the β-position to the phosphorus atom have been elaborated. Catalytic systems based on rhodium complexes of these ligands formed in situ using Rh(CO)₂(acac) as a catalytic precursor demonstrate high activity in the hydroformylation of styrene along with good selectivity in respect to branched aldehyde. Quantum-chemical calculations proved that both the rate of the formation of branched alkyl complex, as well as its reactivity are influenced by the steric and electronic parameters in the same manner.     

A convenient hydroiodination of alkynes using I2/PPh3/H2O and its application to the one-pot synthesis of trisubstituted alkenes via iodoalkenes using Pd-catalyzed cross-coupling reactions

A facile hydroiodination of alkynes using readily-available reagents such as I₂, PPh₃, and H₂O has been developed. This is extended to the one-pot synthesis of trisubstituted alkenes from alkynes via iodoalkenes using Pd-catalyzed cross-coupling and related methods such as the Suzuki–Miyaura cross-coupling, Sonogashira cross-coupling reaction, and Mizoroki–Heck reaction.     

Monomeric ruthenium carbonyls containing 2-substituted pyrazines: From synthesis to catalytic activity in 1-hexene hydroformylation

Synthesis and catalytic properties of a series of ruthenium carbonyl complexes with 2-substituted pyrazine ligands (pz–R; R = Cl, OMe, SMe, CN, NH₂) have been studied. Reactions between the [Ru(CO)₃Cl₂]₂ and the pyrazines led mainly to mononuclear compounds of the type [Ru(CO)₃Cl₂(R–pz)]. All of these ruthenium pyrazine compounds showed activity in 1-hexene hydroformylation. With an exception of NH₂, addition of the substituent to the pyrazine ring was found to improve the catalytic activity compared to the unsubstituted pyrazine. The catalytic cycle was studied by computational DFT methods. The results suggest that the key step in the formation of the active species involves release of one of the carbonyl in the cis position with respect to the pyrazine ring.     

Engaging a thiazole-DMAD zwitterion in novel one-pot multicomponent reactions involving chromones. Expeditious synthesis of thiazolo- and chromenothiazolopyridines

The 1,4-dipole derived from 4,5-dimethylthiazole and DMAD has been shown to react readily with chromone-3-carboxaldehydes resulting, after an unusual rearrangement, in the facile synthesis of thiazolo[3,2-a]pyridine derivatives; in some instances tetracyclic chromenothiazolopyridines were formed.     

New ionic phosphite ligands: synthesis and application in asymmetric Rh-catalyzed hydrogenation

A series of chiral ionic phosphite-type ligands bearing pyridinium and imidazolium fragments were prepared. Testing of these ligands in Rh-catalyzed asymmetric hydrogenation of dimethyl itaconate and methyl 2-acetamidoacrylate resulted in 95% ee of the products with 100% conversion of the reactants.     

Platinum complexes of 2-diphenylphosphinobenzaldehyde-derived P-alkene ligands and their application in the hydroformylation of styrene

Neutral complexes of the formula PtCl₂L₂ (where L = diethyl 2-diphenylphosphino-benzylidene-malonate (1), diisopropyl 2-diphenylphosphino-benzylidene-malonate (2), di-tert-butyl 2-diphenylphosphino-benzylidene-malonate (3), methyl E-2-(2′-diphenylphosphinophenyl)-acrylate (4), tert-butyl E-2-(2′-diphenylphosphinophenyl)acrylate (5)) were prepared. These complexes proved to be excellent precursors to active catalysts for the hydroformylation of styrene. The platinum-containing catalytic systems prepared from malonate-based ligands 1 and 2 provided the highest activity. Chemoselectivities of up to 87% were obtained, while the two aldehyde regioisomers were formed in almost equimolar ratio. The in situ studies by using lower ligand to Pt ratios resulted in slight decrease in both regio- and chemoselectivities.³¹P NMR studies on the PtCl₂L₂ complexes revealed that the formation of trans isomers is highly preferred in the case of benzylidene malonate-type ligands with two ester functionalities (1-3) probably due to steric hindrance. A mixture of cis/trans geometrical isomers (on the Pt) with a predominance of the trans isomer was formed when acrylate-type ligands with one ester functionality (4 and 5) were used.     

Groebke-Blackburn-Bienaymé multicomponent reaction in scaffold-modification of adenine, guanine, and cytosine: synthesis of aminoimidazole-condensed nucleobases

A multicomponent method for scaffold-modification of nucleobases (adenine, guanine, and cytosine) was developed. This modification approach, as an alternative to usual synthetic routes involving protection-deprotection or S_NAr of halo (or leaving group-equivalent)-purines, affords in one step therapeutically-relevant substituted aminoimidazole-[i]-condensed adenine, [b]-condensed guanine, [c]-condensed cytosine. These derived nucleobases possess enhanced lipophilicity and solubility and contain the functionalities useful for further chemical manipulations.     

Facile and efficient synthesis of a new class of bis(3′-indolyl)pyridine derivatives via one-pot multicomponent reactions

A series of 4-aryl-3,5-dicyano-2,6-di(3′-indolyl)pyridine derivatives were synthesized via a one-pot multicomponent reaction of aromatic aldehydes, 3-cyanoacetyl indoles, and ammonium acetate under microwave irradiation. Particularly valuable features of this method include high yields of products, broad substrate scope, short reaction time, and straightforward procedure.     

Novel α-fluorinated cyclic phosphite and phosphinite ligands and their Rh-complexes as suitable catalysts in hydroformylation

Asymmetrical cyclic phosphite and phosphinite ligands of a novel type bearing either trifluoromethyl or pentafluorophenyl group were synthesized using >PCl or >PN< species and racemic fluorinated alcohols. The P-ligands were converted to complexes of Rh^III(L)(Cp^∗)Cl₂ type (where L = phosphite or phosphinite) and, in two instances, their stereostructures were evaluated by X-ray analysis. These complexes along with in situ systems, formed from Rh(CO)₂(acac) precursor and the corresponding ligand, were tested in the hydroformylation of styrene. Both systems provided excellent hydroformylation activities at 100 °C. Using the Rh^I in situ systems, moderate and high regioselectivities towards the branched aldehyde (2-phenyl-propanal) were obtained at 100 and 40 °C, respectively.     

Novel C1-symmetric dibenzophosphole ligands: application in hydroformylation reactions

A new family of non-symmetrical disubstituted dibenzophospholes possessing different steric and electronic effects have been synthesized and characterized. Their preliminary evaluation in rhodium-catalyzed hydroformylation reactions is presented.     

Platinum complexes of malonate-derived monodentate phosphines and their application in the highly chemo- and regioselective hydroformylation of styrene

Neutral complexes of the formula PtCl₂L₂ (where L = diethyl 2-diphenylphosphino-malonate (1), diethyl 2-methyl-2-diphenylphosphinomalonate (2), dibenzyl 2-diphenylphosphinomalonate (3), 1,3-dihydroxy-2-methyl-2-diphenylphosphinopropane (4)) were prepared. These proved to be precursors to active catalysts for the hydroformylation of styrene. The platinum-containing catalytic systems prepared from ligand 4 provided the highest activity, while the platinum compounds prepared from other ligands all showed similar levels of reactivity to each other. The matching of high chemo- and regioselectivities were observed in most cases. Surprisingly, the complexes were practically inactive in imidazolium-type ionic liquids. ³¹P NMR studies on the PtCl₂L₂ complexes revealed that the stereoselectivity of the cis/trans geometrical isomers is strongly dependent on the structure of the ligand.