The synthesis of P-stereogenic MOP analogues and their use in rhodium catalysed asymmetric addition

The synthesis is reported of novel P-stereogenic binaphthyl substituted monophosphines via a short five-step synthesis using a nickel coupling reaction with separation of the borane-protected diastereomeric products. Extensive coordination studies of these ligands with a number of well-known metal precursors were performed to more effectively understand their behaviour during catalysis.These ligands and some previously reported P-stereogenic ligands were tested in the rhodium catalysed asymmetric addition of phenyl boronic acid to napthaldehyde. These studies in asymmetric catalysis were used to compare the chiral induction of ligands that combine both axial and central chirality with ligands lacking P-stereogenicity.     

P1,P1-Bidentate diastereoisomeric bisdiamidophosphites based on N-benzyltartarimide and their applications in asymmetric catalytic processes

Two novel P¹-stereogenic bisdiamidophosphites derived from (3R,4R)-N-benzyltartarimide as a chiral 1,2-diol have been prepared from readily available starting materials. Palladium and rhodium catalytic systems containing these new P¹,P¹-bidentate ligands afforded 96%, 83% and 65% ee in asymmetric allylic substitution, hydrogenation and addition processes, respectively. These diastereomeric diamidophosphites were found to be complementary stereoselectors.     

Asymmetric Diels–Alder cycloaddition of a di-P-stereogenic dienophile with cyclopentadiene

The Diels–Alder cycloaddition of the di-P-stereogenic dienophile (S_P,S_P)-1 leads to novel di-P-stereogenic norbornene derivatives and proceeds with moderate diastereoselectivity in the absence of a catalyst. In the presence of TiCl₄, however, the diastereoselectivity was raised to 9:1. The major diastereoisomer has been characterized crystallographically. The separation of the diastereomeric cycloadducts was possible by fractional crystallization in the presence of (?)-O,O-dibenzoyltartaric acid monohydrate.     

Synthesis of novel P-stereogenic phenylphosphonamides and their application to Lewis base-catalyzed asymmetric allylation of benzaldehyde

The synthesis of novel P-stereogenic phenylphosphonamides 3 and 11 via an intramolecular nucleophilic substitution of P-stereogenic phosphoramide 8 is described. These compounds were used as chiral Lewis basic catalysts for the asymmetric allylation of benzaldehyde, providing the corresponding homoallylic alcohol derivatives in up to 54% ee.     

The PMe3-catalyzed addition of enantiomerically pure (−)-MenthylO(Ph)P(O)H to electron-deficient alkenes: an efficient way for the preparation of P-stereogenic compounds

A variety of P-stereogenic organophosphorus compounds can be readily prepared by stereoretentive addition. The PMe₃-catalyzed addition of optically active (?)MenthylO(Ph)P(O)H compounds to electron deficient alkenes occur stereospecifically, to produce the corresponding P-stereogenic adducts in high yields. By simply removing the volatiles under vacuum, spectroscopically pure products can be obtained. The present method provides a salt-free clean process for the preparation of P-chiral organophosphorus compounds.     

New class of P-stereogenic chiral Brønsted acid catalysts derived from chiral phosphinamides

A new class of NH Brønsted acid organocatalysts that feature P-stereogenic chirality was developed. These catalysts were prepared from P-stereogenic chiral phosphinamides and show similar reactivity to BINOL derived phosphoric acid toward the reduction of quinolines via transfer hydrogenation. It shows that stereoselectivity is induced by the P-chiral environment that is created by the substituents attached to the phosphorous atom, which can be readily tuned and modified.     

Preparation of enantiomerically pure α-hydroxyl phosphinates via hydrophosphorylation of aldehydes with H-phosphinate

The hydrophosphorylation of aldehydes with a P-stereogenic H-phosphinate was realized by heating two compounds in a neat state or catalyzed by a base, to afford P-retention α-hydroxyl phosphinates. The (S_P,S_C) and other diastereomers were isolated, and their structures were confirmed by NMR spectroscopy and crystallography.     

Asymmetric synthesis of SMS-Phos series’ precursor and a naphthalene analogue

An efficient and high-yielding (up to 57% overall yield) asymmetric route to enantiopure P-stereogenic 1,2-bis[(o-hydroxyaryl)(phenyl)phosphino-P-borane]ethanes wherein aryl = phenyl and naphthyl, is presented. The occurring P-stereomutation is confirmed through X-ray crystal structure analysis of key intermediates.     

Pseudoasymmetry, stereogenicity, and the RS-nomenclature comprehended by the concepts of holantimers and stereoisograms

The concepts of holantimer and stereoisogram are applied to comprehensive discussions on the term ‘pseudoasymmetry’, where the concept of RS-stereogenicity is used as a more definite concept than usual stereogenicity. Thereby, three relationships contained in each stereoisogram can be definitely specified: an enantiomeric relationship is related to chiral/achiral, an RS-diastereomeric relationship is related to RS-stereogenic/RS-astereogenic, and a holantimeric relationship is related to scleral/ascleral, which is coined to keep the terminology in a balanced fashion. Such stereoisograms are classified into five types (Types I-V) by virtue of the three relationships. Among them, Type I, III, and V are selected as a set of RS-stereogenic units: chiral/ascleral RS-stereogenic unit (or Type I unit), chiral/scleral RS-stereogenic unit (or Type III unit), and achiral/scleral RS-stereogenic unit (or Type V unit). Thereby, the term ‘pseudoasymmetric stereogenic units’ should be replaced by the term ‘achiral/scleral RS-stereogenic units’ (or ‘Type V units’).     

Access to P-chiral sec- and tert-phosphine oxides enabled by Le-Phos-catalyzed asymmetric kinetic resolution

The synthesis of P-stereogenic building blocks is extremely difficult. Herein we report an efficient kinetic resolution of secondary phosphine oxides via a Le-Phos-catalyzed asymmetric allylation reaction with Morita–Baylis–Hillman carbonates. This method provides facile access to enantioenriched secondary and tertiary P-chiral phosphine oxides with broad substrate scope, both of which could serve as P-stereogenic synthons, and can be rapidly incorporated into a given scaffold bearing a P-stereocenter. The highly desirable late stage modifications demonstrate the practicability of our method and can be a critical contribution to obtaining optimal P-chiral catalysts and ligands.

Herein we report an efficient kinetic resolution of secondary phosphine oxides via a Le-Phos-catalyzed asymmetric allylation reaction with Morita–Baylis–Hillman carbonates.     

Asymmetric synthesis of d-fagomine and its diastereoisomers

A divergent strategy for the asymmetric syntheses of d-fagomine and three of its diastereoisomers has been developed. The diastereoselective conjugate addition of an enantiopure lithium amide to an α,β-unsaturated ester was used as the key step to install the correct configuration required for the C(5)-stereogenic centre within the targets. In situ enolate oxidation generated the corresponding anti-α-hydroxy-β-amino ester, which possessed the correct configuration required for the C(4)-stereogenic centre within both d-fagomine and d-3-epi-fagomine. Subsequent epimerisation of this key anti-α-hydroxy-β-amino ester upon oxidation and diastereoselective reduction gave the corresponding syn-α-hydroxy-β-amino ester, which possessed the correct configuration required for the C(4)-stereogenic centre within both d-4-epi-fagomine and d-5-epi-fagomine. Elaboration of both α-hydroxy-β-amino esters upon reduction to the corresponding aldehydes followed by aldol reaction generated the requisite C(3)-stereogenic centres within the target compounds, then cyclisation and deprotection gave the enantiopure iminosugars in good overall yields, as single diastereoisomers (>99:1 dr).     

Study of incidence of DiPAMP ligand modification on the rhodium(I)-catalyzed asymmetric hydrogenation of α-acetamidostyrene

A series of P-stereogenic enantiopure 1,2-bis[(aryl)(phenyl)phosphino]ethane ligands was prepared through an extensive systematic incorporation of various substituents onto the P-o-anisyl rings of Knowles’ DiPAMP (DiPAMP = 1,2-bis[(o-anisyl)(phenyl)phosphino]ethane). The study of incidence of such modification on the Rh(I)-catalyzed hydrogenation of α-acetamidostyrene is reported revealing that substitution on position 3 is detrimental, while it is beneficial on position 5. Namely, a 2.5-fold increased catalyst activity coupled with a higher enantioselectivity (90% ee) was attained with the P-(2-MeO-3-naphthyl)-substituted ligand under mild conditions (1 bar H₂, rt in MeOH).     

Asymmetric synthesis of chiral glutaric acid derivatives via Rh-catalyzed enantioselective hydrogenation

The first Rh-catalyzed enantioselective hydrogenation of dimethyl 2-methyleneglutarate and its derivatives has been reported. For the hydrogenation of dimethyl 2-methyleneglutarate with a chiral ferrocene-based monodentate phosphoramidite ligand (FAPhos), good enantioselectivity (over 90% ee) with full conversions was achieved. In contrast, the hydrogenation of substrates bearing an aryl substituent at a methylene moiety proved to be more difficult, in which the best enantioselectivity of up to 81% ee was obtained by the use of a P-stereogenic BoPhoz-type ligand.     

Molekülsruktur und abs. konfiguration von (+)-p-menthadien-(1,8)-on-(2)-rhodium(I)-h5-cyclopentadienid, (+)-(4S-Carvon) RhI(C5H5)

The title compound crystallizes in the orthorhombic space group P2₁2₁2₁ with 4 molecules in the unit cell (cell dimensions: a 9.778(2), b 10.639(2) and c 12.423(4) Å). The structure was solved by means of the heavy atom method. The rhodium atom is linked to both olefinic double bonds. The terpene carbonyl group does not participate in coordination to rhodium. Unlike the endocyclic olefinic group, which is approximately perpendicular to the coordination plane of rhodium, the exocyclic Cz.sbnd;C double bound shows a considerable deviation from this arrangement. The π-complexation of carvone with rhodium proceeds diastereospecifically. The absolute configuration of (+)-carvone is 4S in agreement with the assignment derived by indirect chemical correlation.     

Copper-Catalyzed Dynamic Kinetic Asymmetric P−C Coupling of Secondary Phosphine Oxides and Aryl Iodides

Transition-metal-catalyzed enantioselective P−C cross-coupling of secondary phosphine oxides (SPOs) is an attractive method for synthesizing P-stereogenic phosphorus compounds, but the development of such a dynamic kinetic asymmetric process remains a considerable challenge. Here we report an unprecedented highly enantioselective dynamic kinetic intermolecular P−C coupling of SPOs and aryl iodides catalyzed by copper complexes ligated by a finely modified chiral 1,2-diamine ligand. The reaction tolerates a wide range of SPOs and aryl iodides, affording P-stereogenic tertiary phosphine oxides (TPOs) in high yields and with good enantioselectivity (average 89.2 % ee). The resulting enantioenriched TPOs were transformed into structurally diverse P-chiral scaffolds, which are highly valuable as ligands and catalysts in asymmetric synthesis.     

Hydroformylation activity of multinuclear rhodium complexes coordinated to dendritic iminopyridyl and iminophosphine scaffolds

The synthesis of poly(propyleneimine)-iminopyridyl and iminophosphine rhodium(I) metallodendrimers, with rhodium coordinated to monodentate (N-donor) and chelating, heterobidentate (P,N) moieties respectively located on the periphery, has been accomplished in order to evaluate their potential as hydroformylation catalysts. Related mononuclear complexes were obtained in a similar manner to model the multinuclear complexes. The multinuclear rhodium(I) complexes were found to be effective catalyst precursors in the hydroformylation of 1-octene, achieving higher conversions, faster reaction rates and slightly enhanced catalytic activity when compared with analogous mononuclear rhodium complexes. Hydroformylation reactions using the tetra- and octanuclear rhodium complexes generally show a chemoselective formation of aldehydes, together with a small amount of isomerisation products.     

Efficient oxidative resolution of a P-stereogenic triarylphosphine and asymmetric synthesis of a P-stereogenic atropoisomeric biphenyl diphosphine dioxide

Racemic 3-methoxyphenyl(1-naphthyl)phenylphosphine 1 was effectively resolved via an oxidative resolution procedure utilizing l-menthyl bromoacetate as the resolving agent to give enantiopure 3-methoxyphenyl(1-naphthyl)phenylphosphine oxide (R)-2 in 41% yield. Reduction of the resolved (R)-4 with HSiCl₃/NEt₃ provided the corresponding phosphine (R)-1 in >97% ee. Ortho-iodination of the enantiopure (R)-4 followed by Ullmann coupling of the resulting iodoarylphosphine oxide gave a P-stereogenic and atropoisomeric biphenyl diphosphine dioxide as a single diastereoisomer. The latter transformation constitutes the first example of an effective transfer of a P-centered chirality to an axial chirality of the atropoisomeric biaryl system. The absolute configurations of the resolved phosphine and the atropoisomeric biaryl system have also been established.     

New chiral phosphite ligands bearing sp2-nitrogen: complexation properties and palladium(II)-catalysed enantioselective allylic alkylation

New homochiral P,N-bidentate phosphite-type ligands containing sp²-nitrogen were synthesised and their complexation with Rh(I) and Pd(II) atoms was investigated. The X-ray crystal structure of one of the chelate chlorocarbonyl rhodium complexes was obtained. E.e.s of up to 85% were attained in the Pd-catalysed allylic substitution reaction using the new P,N-ligands.     

Synthesis of 4-aryl-substituted β-lactam enantiomers by enzyme-catalyzed kinetic resolution

Enantiopure 4-phenyl- and 4-(p-tolyl)-2-azetidinones 3a, 3b, 4a and 4b (with e.e.s of ≥96%) were prepared through lipase-catalyzed asymmetric butyrylation of the primary OH group of N-hydroxymethylated β-lactams (±)-5 and (±)-6 at the (R)-stereogenic centre or by lipase-catalyzed asymmetric debutyrylation of O-butyryloxymethyl-2-azetidinones (±)-7 and (±)-8 at the (R)-stereogenic centre. The ring-opening of lactams 5a, 5b, 6b and 8a with HCl/EtOH afforded the corresponding β-amino ester enantiomers 9a, 9b, 10a and 10b with e.e.s of ≥92%.