Synthesis of a diastereomeric mixture of deuterium-labeled lovastatin and its acid ammonium salt

In this communication, a facile synthesis for (2S/2R)-[²H₃]lovastatin and (2S/2R)-[²H₃]lovastatin acid ammonium salt was described. The stable isotope-labeled (2S/2R)-lovastatin and its acid ammonium salt were prepared from butyric acid via several reaction steps with 11.1 and 6.3 % overall yield, respectively.     

Unique Isle Anion [Cu6Cl10]4- in π-Complex of Cu(I) Chloride with 1-(2-Pyridyl)-4-allyl-piperazinium. Synthesis and crystal structure of [(C5H4NH)NC4H8NH(C3H5]2+[Cu3Cl5]2-

Single crystals of [(C₅H₄NH)NC₄H₈NH(C₃H₅)]²⁺[Cu₃Cl₅]^2? are obtained by ac synthesis in ethanol from 1-(2-pyridyl)-4-allyl-piperazinium and Cu(II) dichlorides and their structure is studied by X-ray diffraction analysis (space group P-1, a = 7.246(7) Å, b = 8.54(1) Å, c = 16.41(1) Å, α = 70.76(8)°, β = 77.24(8)°, λ = 80.42(9)°, V = 30(4) ų, Z = 2, R(F) = 0.0686. In the structure of this π-complex, the Cu and Cl atoms form unusual centrosymmetrical Cu₆Cl₁₀ fragments, each fragment being bonded to two 1-(2-pyridyl)-4-allyl-piper-azinium cations via π-interaction Cu-(C=C). A three-dimensional structure is formed by means of N-H…Cl hydrogen bonds. The trigonal-pyramidal surrounding of the Cu(1) atom includes three Cl atoms and the C=C bond, while the tetrahedral surrounding of Cu(2) and the trigonal surrounding of Cu(3) involve the Cl atoms only.     

Cumulative author index: Vol. 126(1977)–150(1978)

The synthesis of μ-[phenyl(dicyclohexylphosphonio)ethenidyl]-μ-(diphenylphosphido)hexacarbonyldiiron, Fe₂(CO)₆[CC(PCy₂H)Ph](PPh₂) via nucleophilic attack by dicyclohexylphosphine at the β-carbon atom of the σπ-acetylide in Fe₂(CO)₆(CCPh)(PPh₂) is described. This complex, which contains a one-carbon 3-electron bridging ligand has been characterised by microanalysis, infrared, mass, Mössbauer and ³¹P NMR spectroscopy and by a single crystal X-ray structure determination. Crystals are monoclinic, space group P2₁/c with a 10.932(3), b 8.983(2), c 38.644(6) Å, β 94.48(2)°. With four molecules per unit cell and a formula weight of 764.4, the calculated density of 1.342 g cm^?3 agrees with the measured value of 1.34 g cm^?3. The structure was solved by heavy atom methods and refined by least squares techniques with iron and phosphorus atoms having anisotropic thermal parameters, to R and R_w values of 0.068 and 0.075 respectively. In the binuclear molecule an ironiron bond of length 2.550(2) Å is bridged by a diphenylphosphido group and the carbon atom of an unusual dipolar ligand Cy₂(H)P⁺C(Ph)C^?. In the bridging one-carbon-3-electron ligand the coordinated carbon atom is trigonal and the atoms P(1), C(8), C(31), C(7) are virtually coplanar. Structural parameters are compared with those of other complexes containing bridging one-carbon, 3-electron and two-carbon, 3-electron ligands. Nucleophilic attack by phosphorus and nitrogen nucleophiles on σπ-acetylides appears to be a general route to these ligands.     

Stereoselective synthesis of (1′S,3R,4R)-4-acetoxy-3-(2′-fluoro-1′-trimethylsilyloxyethyl)-2-azetidinone

A stereoselective synthesis of (1′S,3R,4R)-4-acetoxy-3-(2′-fluoro-1′-trimethylsilyloxyethyl)-2-azetidinone as a new fluorine-containing intermediate towards β-lactams, is described. The synthetic key step relies upon the dynamic kinetic resolution (DKR) of ethyl 2-benzamidomethyl-4-fluoro-3-oxo-butanoate via asymmetric transfer hydrogenation catalyzed by [Ru(η⁶-arene)(S,S)-R₂NSO₂DPEN].     

Cross-linked poly (4-vinylpyridine) supported azide ion as a versatile and recyclable polymeric reagent for synthesis of 1-substituted-1H-1,2,3,4-tetrazoles

Cross-linked poly (4-vinylpyridine) supported azide ion, [P₄-VP]N₃, is easily prepared and used as an efficient polymeric reagent for synthesis of 1-substituted-1H-1,2,3,4-tetrazoles via condensation reaction of azide ion, primary aromatic amines, and triethyl orthoformate in glacial acetic acid. After optimization of the reaction conditions, a wide variety of primary aromatic amines were also subjected to preparation of the corresponding 1-aryl-1 H-1,2,3,4- tetrazoles using [P₄-VP]N₃ under heterogeneous conditions. In this method, the reaction times were very short and the isolated yields were excellent (90–98 %). 1-Aryl-1H-1,2,3,4- tetrazole products were characterized by Fourier transform infrared (FT-IR) and some of them were also characterized by proton nuclear magnetic resonance (¹H NMR) spectroscopy, and physical properties were compared with the literature values of known compounds. The spent polymeric reagent were regenerated quantitatively and reused for several cycles without significant loss of their activity.     

Preparation of l-serine and l-cystine stereospecifically labeled with deuterium at the β-position

The synthesis of l-serine and l-cystine stereospecifically labeled with deuterium at the β-position is described. The carboxyl group of d-serine was transformed into chirally deuterium-labeled alcohol via asymmetric reduction of 1-deuterio aldehyde, while the original hydroxymethyl group was converted into a carboxyl functionality to afford (2S,3R)-[3-²H]serine. Functional group interconversions of the hydroxyl group in the obtained deuterium-labeled l-serine gave (2R,2′R,3S,3′S)-[3,3′-²H₂]cystine.     

The preparation of multimetallic complexes using sterically bulky N-centred tripodal dialkyl phosphino ligands

Sterically bulky monodentate and bidentate phosphines have been widely used as ligands for metal complexation and catalyst formation. Bulky tridentate phosphine ligands are however much rarer and have not been widely investigated even though they may be considered attractive ligands for coordination chemistry studies and catalysis. Here we report the synthesis of two new N-centred tripodal phosphine ligands bearing bulky cyclohexyl and tert-butyl groups. The coordination chemistry of the cyclohexyl triphosphine ligand N(CH₂PCy₂)₃ (4) was investigated and found to react with Mo and W hexacarbonyls preferentially forming bidentate metal tetracarbonyl complexes [Mo(CO)₄{N(CH₂PCy₂)₃-κ²P}] (6) and [W(CO)₄{N(CH₂PCy₂)₃-κ²P}] (7) over the expected facial capping tridentate complexes. The steric bulk of the cyclohexyl groups on the phosphorus atoms is sufficient to prevent the third arm of the ligand from coordinating and adopting the required geometry for facial coordination. This ‘steric control’ at the metal centre results in the third arm remaining freely available for further metal coordination. The coordination chemistry of this free phosphine arm on complexes 6 and 7 was investigated further and used to prepare a series of gold, platinum and silver multimetallic complexes. The X-ray crystal structures of the resulting mixed bi and trimetallic complexes [W(CO)₄{N(CH₂PCy₂)₃-κ²P}AuCl] (8), [[Mo(CO)₄{N(CH₂PCy₂)₃-κ²P}]₂(μ-PtCl₂)] (9) and [[W(CO)₄{N(CH₂PCy₂)₃-κ²P}]₂(μ-Ag)]ClO₄ (11) are reported.     

Cationic iridium complexes of the Xantphos ligand. Flexible coordination modes and the isolation of the hydride insertion product with an alkene

Reaction of the Ir(I)-Xantphos complex [Ir(κ²-Xantphos)(COD)][BAr^F₄] (Xantphos = 4,5-bis(diphenylphosphino)-9,9-dimethylxanthene, Ar^F = C₆H₃(CF₃)₂) with H₂ in acetone or CH₂Cl₂/MeCN affords the Ir(III)-hydrido complexes [Ir(κ³-Xantphos)(H)₂(L)][BAr^F₄], L = acetone or MeCN, whereas in non-coordinating CH₂Cl₂ solvent dimeric [Ir(κ³-Xantphos)(H)(μ-H)]₂[BAr^F₄]₂ is formed. A common intermediate in these reactions that invokes a (σ, η²-C₈H₁₃) ligand is reported. Addition of excess tert-butylethene (tbe) to [Ir(κ³-Xantphos)(H)₂(MeCN)][BAr^F₄] results in insertion of a hydride into the alkene to form [Ir(κ³-Xantphos)(MeCN)(CH₂CH₂C(CH₃)₃)(H)][BAr^F₄], an Ir(III) alkyl-hydrido-Xantphos complex. This reaction is reversible, and heating (80 °C) results in the reformation of [Ir(κ³-Xantphos)(H)₂(MeCN)][BAr^F₄] and tbe. These complexes have been characterised by NMR spectroscopy, ESI-MS and single-crystal X-ray diffraction. They show variable coordination modes of the Xantphos ligand: cis-κ²-P,P, fac-κ³-P,O,P and mer-κ³-P,O,P with the later coordination mode like that found in related PNP-pincer complexes.     

Stereochemistry of internucleotide bond formation by the H-phosphonate method. 7. Stereoselective formation of ribonucleoside (RP)- and (SP)-3′-H-phosphonothioate monoesters

Ribonucleoside 3′-H-phosphonothioate monoesters exist in the form of (R_P)- and (S_P)-diastereomers. In order to obtain them in good yields and in high stereochemical purity, stereoselective strategies for their preparation were investigated. For the synthesis of the (R_P)-isomer, a stereoselective sulfhydrolysis of an activated nucleoside H-phosphonate was developed, while the monoesters with an (S_P)-configuration were prepared by asymmetric transformation of diastereomeric mixtures of nucleoside 3′-H-phosphonothioates using either a condensation with 9-fluorenemethanol, followed by β-elimination, or via pivaloylation-hydrolysis reaction sequence. A tentative assignment of the absolute configurations of the obtained diastereomers of 3′-H-phosphonothioate esters was carried out via a stereochemical correlation analysis.     

Practical synthesis of d-[1-C]mannose, l-[1-C] and l-[6-C]fucose

The chemical synthesis of ¹³C-labeled mannose and fucose is important for the preparation of molecular probes used in the conformational study of the oligosaccharide portions of glycoproteins. A new method for the synthesis of the title [1-¹³C]-labeled compounds via the corresponding olefin compounds, which are in turn derived from d-mannitol or l-arabinose by efficient introduction of ¹³C, by the Wittig reaction using Ph₃P¹³CH₃I and n-BuLi, is described. The introduction of ¹³CH₃I to produce the [1-¹³C]- and [6-¹³C]-labeled compounds was accomplished in 62%, 56%, and 71% yields, respectively. All mannose and fucose protons, from H-1 to H-6, were observed by the HMQC-TOCSY technique using 1:1 mixtures of [1-¹³C]- and [6-¹³C]-labeled compounds.     

Active monomeric nucleotide intermediate in the oligonucleotide synthesis

The interaction of 3′ - O - acetylthymidine - 5′ - phosphate (pT-Ac) and p - nitrophenylphosphate (pPhNO₂) with triisopropylbenzenesulphonyl chloride (TPS) in pyridine was studied by the pulsed NMR spectroscopy on ³¹P nuclei. The esters investigated were shown to convert to the corresponding disubstituted pyrophosphates, trisubstituted tripolyphosphates and compounds showing a singlet displaced 5–8 ppm from the original ester. The latter are the main final products of the interaction of nucleotide and pPhNO₂ with TPS. The investigation of the chemical conversion of a pT-Ac derivative with a 5·1 ppm shift showed that this product is a powerful phosphorylating reagent. It was shown that this active derivative contains one P atom in accordance with the structure of monomeric metaphosphoric acid ester proposed by Todd for these compounds. The reaction of monomeric metaphosphate with 5′-O-tritylthymidine results information of a compound, containing stoichiometric amounts of pT-Ac and 5′ - O - tritylthymidilyl - (3′ → 5′) - 3′ - O - acetylthymidine residues. This compound was identified as a trisubstituted P¹ - 5′ - O - trityl - P¹ - P² -bis -(3′ - O - acetylthymidine) - pyrophosph     

Synthesis and structural characterization of 1′-(diphenylphosphino)ferrocene-1-carboxamide, its corresponding hydrazide, some heterocycles derived from the hydrazide and palladium(II) complexes with these functional phosphinoferrocene ligands

Two polar phosphinoferrocene ligands, 1′-(diphenylphosphino)ferrocene-1-carboxamide (1) and 1′-(diphenylphosphino)ferrocene-1-carbohydrazide (2), were synthesized in good yields from 1′-(diphenylphosphino)ferrocene-1-carboxylic acid (Hdpf) via the reactive benzotriazole derivative, 1-[1′-(diphenylphosphino)ferrocene-1-carbonyl]-1H-1,2,3-benzotriazole (3). Alternatively, the hydrazide was prepared by the conventional reaction of methyl 1′-(diphenylphosphino)ferrocene-1-carboxylate with hydrazine hydrate, and was further converted via standard condensation reactions to three phosphinoferrocene heterocycles, viz 2-[1′-(diphenylphosphino)ferrocen-1-yl]-1,3,4-oxadiazole (4), 1-[1′-(diphenylphosphino)ferrocen-1-carbonyl]-3,5-dimethyl-1,2-pyrazole (5), and 1-[1′-(diphenylphosphino)ferrocene-1-carboxamido]-3,5-dimethylpyrrole (6). Compounds 1 and 2 react with [PdCl₂(cod)] (cod = η²:η²-cycloocta-1,5-diene) to afford the respective bis-phosphine complexes trans-[PdCl₂(L-κP)₂] (7, L = 1; 8, L = 2). The dimeric precursor [(L^NC)PdCl]₂ (L^NC = 2-[(dimethylamino-κN)methyl]phenyl-κC¹) is cleaved with 1 to give the neutral phosphine complex [(L^NC)PdCl(1-κP)] (9), which is readily transformed into a ionic bis-chelate complex [(L^NC)PdCl(1-κ²O,P)][SbF₆] (10) upon removal of the chloride ligand with Ag[SbF₆]. Pyrazole 5 behaves similarly affording the related complexes [(L^NC)PdCl(5-κP)] (12) and [(L^NC)PdCl(5-κ²O,P)][SbF₆] (13), in which the ferrocene ligand coordinates as a simple phosphine and an O,P-chelate respectively, while oxadiazole 4 affords the phosphine complex [(L^NC)PdCl(4-κP)] (11) and a P,N-chelate [(L^NC)PdCl(4-κ²N³,P)][SbF₆] (14) under similar conditions. All compounds were characterized by elemental analysis and spectroscopic methods (multinuclear NMR, IR and MS). The solid-state structures of 1⋅½AcOEt, 2, 7⋅3CH₃CN, 8⋅2CHCl₃, 9⋅½CH₂Cl₂⋅0.375C₆H₁₄, 10, and 14 were determined by single-crystal X-ray crystallography.     

Cluster chemistry XXV *. Synthesis and structure of Ru4(μ4-η2, P-HCCC6H4PPh2)(CO)11·0.5CH2Cl2

The olefinic tertiary phospine complex Ru₃(CO)₁₀(μ-η², P-CH₂CHC₆H₄PPh₂) is converted to the title μ₄-alkyne-Ru₄ cluster at 135°C; the latter is also formed from H₂Ru₃(μ₃-η², P-HCCC₆H₄PPh₂)(CO)₈ and Ru₃(CO)₁₂. Crystals of the Ru₄ complex are monoclinic, space group P2₁, with a 8.700(3), b 17.611(3), c 11.926(2) Å, β 102.720(3)°, with Z = 2; 1702 data (I > 2.5 (σ)I) were refined to R = 0.026, R_w = 0.028. The molecule contains a distorted octahedral Ru₄C₂ core, one carbon of which is attached to an o-C₆H₄PPh₂ moiety coordinated via P to a wing-tip Ru of the Ru₄ butterfly.     

Cs4P2Se10: A new compound discovered with the application of solid-state and high temperature NMR

The new compound Cs₄P₂Se₁₀ was serendipitously produced in high purity during a high-temperature synthesis done in a nuclear magnetic resonance (NMR) spectrometer. ³¹P magic angle spinning (MAS) NMR of the products of the synthesis revealed that the dominant phosphorus-containing product had a chemical shift of −52.8 ppm that could not be assigned to any known compound. Deep reddish brown well-formed plate-like crystals were isolated from the NMR reaction ampoule and the structure was solved with X-ray diffraction. Cs₄P₂Se₁₀ has the triclinic space group P-1 with a=7.3587(11) Å, b=7.4546(11) Å, c=10.1420(15) Å, α=85.938(2)°, β=88.055(2)°, and γ=85.609(2)° and contains the [P₂Se₁₀]⁴⁻ anion. To our knowledge, this is the first compound containing this anion that is composed of two tetrahedral (PSe₄) units connected by a diselenide linkage. It was also possible to form a glass by quenching the melt in ice water, and Cs₄P₂Se₁₀ was recovered upon annealing. The static ³¹P NMR spectrum at 350 °C contained a single peak with a −35 ppm chemical shift and a ∼7 ppm peak width. This study highlights the potential of solid-state and high-temperature NMR for aiding discovery of new compounds and for probing the species that exist at high temperature.     

Preparation of phosphinoferrocene carboxamides from isocyanates. Synthesis and structural characterisation of palladium(II) and platinum(II) complexes with 1′-(diphenylphosphino)-1-(N-phenylcarbamoyl)ferrocene

The reaction of in situ generated 1′-(diphenylphosphino)-1-lithioferrocene with isocyanates RNCO affords the respective phosphino-carboxamides Ph₂PfcCONHR (fc = ferrocene-1,1′-diyl, R = cyclohexyl (2), and Ph (3)) in moderate yields. The coordination behaviour of 3 chosen as a representative was studied in palladium(II) and platinum(II) complexes. Depending on the metal precursor and the reaction conditions, the following compounds featuring this ligand as a P-monodentate or an O,P-chelating donor were isolated and characterised by spectroscopic methods (IR, multinuclear NMR and electrospray ionisation MS): trans-[PdCl₂(3-κP)₂] (5), trans-[PtCl₂(3-κP)₂] (6), cis-[PtCl₂(3-κP)₂] (7), [SP-4-4]-[(L^NC)PdCl(3-κP)] (8; L^NC = 2-[(dimethylamino-κN)methyl]phenyl-κC¹), and [SP-4-3]-[(L^NC)PdCl(3-κ²O,P)]SbF₆ (9). Besides, the crystal structures of a phosphine oxide resulting by oxidation of 2, viz Ph₂P(O)fcCONHCy (4), and of complexes 5·2Et₂O and 9 have been determined by single-crystal X-ray diffraction analysis.     

Synthesis of Δ-15-deoxy-PG-J1 methyl ester and epi-Δ-15-deoxy-PG-J1

The synthesis of racemic Δ^12,14-15-deoxy-PG-J₁ is readily achieved in six steps employing as the key transformation a one-pot conjugate addition-Peterson olefination sequence using exo-2-trimethylsilyl-3a,4,7,7a-tetrahydro-4,7-methanoinden-1-one. Additionally a Noyori-type three-component coupling approach is employed for the synthesis of enantioenriched epi-Δ¹²-15-deoxy-PG-J₁ from 4(S)-tert-butyldimethylsilyloxycyclopent-2-enone.     

Oxygen permselective characteristics of a poly(vinylchloride)/liquid crystal/fluorocarbon ternary composite membrane

Poly(vinyl chloride) (PVC)/N-(4-ethoxybenzylidene)-4'-butylaniline (EBBA)/perfluorotributylamine (PFTA) ternary composite membrane was prepared and its oxygen permselectivity was investigated. In this membrane system, PFTA was contained in micelles formed by a surfactant of an ABA-type block copolymer (L44). The oxygen permeability coefficient, P_O2, for the PFTA-containing ternary composite membrane was greater than that for the PFTA-free binary one. The order of P_O2 for the ternary composite membrane was 10^?9 to 10^?8 cm³ (STP)-cm^?1-sec^?1-cmHg^?1, and the magnitude of the separation factor, P_O2/P_N2, about 3.5—4.0 in the temperature range of the nematic or isotropic state of EBBA. An increase in P_O2 caused by adding PFTA suggests that PFTA enhances the solubility of oxygen in the composite membrane surface. The ternary composite membrane showed a unique trend in its P_O2/P_N2—P_O2 relationship, that is, the magnitude of P_O2/P_N2 increased simultaneously with that of P_O2.     

Asymmetric transfer hydrogenation of ketones catalyzed by ruthenium(II) complexes bearing a chiral phosphinoferrocenyloxazoline ligand

The catalytic activity in asymmetric transfer hydrogenation of ketones using octahedral and half-sandwich (η⁵-indenyl and η⁶-arene) ruthenium(II) complexes containing the chiral ligand (4S)-2-[(S_p)-2-(diphenylphosphino)ferrocenyl]-4-(isopropyl)oxazoline (FcPN) has been explored. Catalytic studies with complex fac-[RuCl₂{η²(P,N)-FcPN}(PMe₃)₂] (1) show excellent TOF values (9600 h⁻¹). Experiments in the presence of free FcPN, which lead to an increase in conversion rates and ee values when the catalyst is complex [Ru(η⁵-C₉H₇){κ²(P,N)-FcPN}(PPh₃)][PF₆] (4) have been carried out. The characterization of the new complexes mer-trans-[RuCl₂{P(OMe)₃}₂{κ²(P,N)-FcPN}] and of the water-soluble complexes fac- and mer-trans-[RuCl₂(PTA)₂{κ²(P,N)-FcPN}] is also reported.     

A new reaction of P4S10 and Lawesson's reagent; a new method for the synthesis of dithieno[3,2-b;2,3-d]thiophenes

A new reaction of P₄S₁₀ and Lawesson's reagent for the synthesis of fused thiophenes has been uncovered. It has given easy access to the synthesis of derivatives of the technologically important heterocycle dithieno[3,2-b;2^′,3^′-d]thiophene, DTT. Electrochemical polymerization of one of the derivatives has been demonstrated.     

Synthesis of the dopamine D2/D3 receptor agonist (+)-PHNO via supercritical fluid chromatography: preliminary PET imaging study with [3-C]-(+)PHNO

Carbon-11 labeled (+)-4-[1-¹¹C]propyl-3,4,4a,5,6,10b-hexahydro-2H-naphtho[1,2-b][1,4]oxazin-9-ol ([1-¹¹C]-(+)-PHNO) is a dopamine D₃-preferring agonist radiopharmaceutical used for medical imaging by positron emission tomography (PET). We report the synthesis of (+)-PHNO using supercritical fluid chromatography for enantiomeric resolution of its norpropyl derivative, HNO, followed by propylation. (+)-HNO was used to prepare the radiolabeling precursor, (+)-trans-4-acetyl-9-triisopropylsilyloxy-2,3,4a,5,6,10b-hexahydro-4H-naphth[1,2b][1,4]oxazine, in 12 steps. Modifications to the labeling procedure were made to ensure consistent preparation of [3-¹¹C]-(+)-PHNO via [¹¹C]CH₃I. A preliminary PET imaging study was carried out with this tracer in an attempt to image dopamine receptors in brown adipose tissue (brown fat) in vivo.