1H-NMR studies on substance P hexapeptide analogs

¹H-nmr studies of [pGlu⁶]SP_6–11, [gpGlu⁶,mPhe⁷]SP_6–11, and [pGlu⁶,N-CH₃Phe⁷]SP_6–11 in DMSO-d₆ reveal characteristic chemical shifts, ³J_NH-αCH, temperature dependence, as well as deuterium exchange half-times. Marked similarities are revealed for the two first analogs, whereas the N-methylated analog is clearly different. Possible conformations are considered.     

Organic derivatives of aluminium. Part I. Reactions of alkanolamines with aluminium isopropoxide

Reactions of alkanolamines [R₁R₂NXOH; R₁ = H, CH₃, C₂H₅; R₂ = H, CH₃, C₂H₅ and X = -CH₂CH₂-, -CH₂CH₂CH₂-, -CH₂CHCH₃, -C₆H₄CH₂CH₂-] with aluminium isopropoxide in different molar ratios (1 to 3) yield compounds of the type Al(OPrⁱ)_3?n(OXNR₁R₂)_n, where ‘n’ can be 1, 2 and 3. Most of the derivatives are distillable liquids, soluble in common organic solvents and susceptible to hydrolysis even by atmospheric moisture. The new derivatives are characterized by elemental analysis, IR and ¹H NMR spectra. Molecular weight measurements of Al(OPrⁱ)_3?n(OXNR₁R₂)_n reveal them to be tetrameric in nature.     

Chiral Metal Complexes. 27. Stereoselectivity in the synthesis and reaction of coordinated aminomalonic acid derivatives

The synthesis is reported of a series of ternary cationic complexes of general form [Co(R,Rpicchxn)(ARMA)⁺ (where picchxn is the N₄ tetradentate N,N′-di(2-picolyl)-1,2-diaminocyclohexane and ARMA is a bidentate α-substituted-α-aminomalonate dianion). The aminomalonic acid (NH₂· C(COOH)₂·R) derivatives investigated have R = -CH₃ (AMMAH₂), -CH₂·CH₃ (AEMAH₂), -CH₂· CH₂·CH₃ (APMAH₂), -CH₂·(CH₂)₂·CH₃ (ABuTMAH₂, -CH₂·C₆H₅ (ABMAH₂), -CH₂·(p-C₆H₄)· C(CH₃)₃ (ABuBMAH₂) and -CH₂·C₁₀H₇ (ANMAH₂). The isomeric species in the complex products have been separated using cation exchange chromatography and each isomer has been characterized using NMR and circular dichroism techniques. In each synthesis the major isomeric product obtained has a Λ-β₁ topology. However, where ARMAH₂ possesses a lengthy alkyl sidechain trace amounts of Δ-α-[Co(R,R-picchxn)(ARMA)]⁺ isomers have been observed during the synthetic reactions. This unusual isomeric form readily undergoes inversion of its absolute configuration in DMSO solution to yield the more thermodynamically stable Λ-β₁-[Co(R,R-picchxn()R-ARMA)]⁺ species stereospecifically.In the case of Λ-β₁-[Co(R,R,-pichxn)(S-APMA)]ClO₄·2NaClO₄·5H₂O the crystal structure has been determined. The compound crystallises in the orthorhombic space group P2₁2₁2₁, with a = 10.056(3),b = 16.475(7),c = 23.370(7)Å and Z = 4. The structure was refined to R = 0.079 for 4460 non-zero reflexions, and confirms the absolute configuration of each chiral centre to be consistent with the NMR and circular dichroism interpretations.The decar☐ylation of these chelate ARMAH₂ derivatives under acid conditions leads to corresponding complexes containing mixtures of coordinated R-andS-α-aminoacids in various ratios. This ratio has been determined in each case, and factors which may influence the degree of chiral induction observed are discussed.     

Syntheses of Jasmonic Acid Related Compounds and Their Structure-Activity Relationships on the Growth of Rice Seedings

Jasmonic acid (JA)-related compounds were synthesized, and their inhibitory activities on rice seedling growth were investigated. Three functions (C-1 CH₂COOH or CH₂COOCH₃, C-2 (Z)-2′-pentenyl or n-pentyl and C-3 ketone or hydroxyl) were essential for exhibiting inhibitory activity in this series of compounds. A dihydro-JA-related compound, 4-acetyl-nonanoic acid, also showed inhibitory activity similar to JA.     

Reactions of N-cyanomethyl groups attached to a tetraaza macrocyclic copper(II) complex leading to the formation of various hetero-functionalized macrocyclic complexes

New hetero-functionalized macrocyclic complexes [CuL²](ClO₄)₂ (I) and [CuL³](ClO₄)₂ (II) bearing one N-CH₂CONH₂ or one N-CH₂C(NH)NH(CH₂)₂CH₃ pendant arm as well as one N-CH₂CN group have been prepared by the selective reaction of water or n-propylamine with one of the two N-CH₂CN groups in [CuL¹](ClO₄)₂ (L¹ = 2,13-bis(cyanomethyl)-5,16-dimethyl-2,6,13,17-tetraazatricyclo[16.4.0.^1.180^7.12]docosane). The complex [CuL⁴](ClO₄)₂ (III) bearing both N-CH₂CONH₂ and N-CH₂C(NH)NH(CH₂)₂CH₃ pendant arms can be prepared by either the reaction of I with n-propylamine or the hydrolysis of II. The N-CH₂CONH₂ and/or N-CH₂C(NH)NH(CH₂)₂CH₃ groups of I, II, and III are coordinated to the metal ion. The crystal structure of II shows that the complex has distorted square-pyramidal coordination polyhedron with a considerably strong apical Cu-N (N-CH₂C(NH)NH(CH₂)₂CH₃) bond (2.101(6) Å). The addition of HClO₄ (?0.01 M) to an acetonitrile (or DMSO) solution of II or III produces [Cu(HL³)](ClO₄)₃ (IIa) or [Cu(HL⁴)](ClO₄)₃ (IIIa), showing that the N-CH₂C(NH)NH(CH₂)₂CH₃ pendant arm of each complex is readily protonated in the non-aqueous solvent; the resulting N-CH₂C()NH(CH₂)₂CH₃ group of IIa or IIIa is not involved in coordination. However, the N-CH₂C(NH)NH(CH₂)₂CH₃ group of II is not protonated even in ?1.0 M HClO₄ aqueous solution. In the case of III, most of the complex exists as the protonated form [Cu(HL⁴)]³⁺ in ?0.1 M HClO₄ aqueous solutions.     

Reactions of Low Valent Transition Metal Complexes with Hydrogen Peroxide. Are they “Fenton-Like” or not? 4. The Case of Fe(II)L,L = Edta; Hedta and Tcma

The question whether hydroxyl free radicals are formed in the reactions of divalent iron complexes Fe(II)L; L = edta; hedta; tcma (tcma = l-acetato-l,4,7-triazacyclononane) with hydrogen peroxide in neutral and slightly acidic solutions was studied by using the β elimination reaction as an assay for the formation of hydroxyl free radicals, OH. The results show that at pH<5.5 the iron(II)peroxide intermediate complex decomposes rapidly to yield free hydroxyl radicals for L=edta and hedta. This is in contrast to the mechanism of the corresponding Fe(II)nta peroxide complex, which probably decomposes to form Fe(IV)nta which then reacts with organic substrates to yield aliphatic free radicals. Thus, the non-participating ligand L has an appreciable effect on the mechanism of reaction of the metal center with hydrogen peroxide. Blank experiments using ionizing radiation as the source of CH₂CR(CH₃)OH, R = H or CH₃ radicals indicate that when L = tcma intermediates of the type LFe^III-CH₂CR(CH₃)OH_aq are formed, but their major mode of decomposition is not the β elimination reaction. Thus, the present assay for the formation of hydroxyl free radicals by the Fenton Reaction does not fit the latter system.     

The base-catalyzed isomerization of trans-RCo(H2O)L (L=5,7,7,12,14,14-hexamethyl-1,4,8,11-tetraazacyclotetradeca-4,11-diene)

The sec, rac-CH₃Co(H₂O)L²⁺ (L=5,7,7,12,14,14-hexamethyl-1,4,8,11-tetraazacyclotetradeca-4,11-diene) was prepared successfully via meso-CH₃Co(H₂O)L²⁺ in aqueous solution. The isomerizations from meso-RCo(H₂O)L²⁺ (R=CH₃, C₂H₅ and C₃H₇) and sec, rac-CH₃Co(H₂O)L²⁺ to pri, rac-RCo(H₂O)L²⁺ were both base catalyzed in aqueous solution. The kinetic results showed the reaction to be first order in both organocobalt complex and hydroxide ion with the reactivity order for the alkyl group being C₃H₇ ∼ C₂H₅ ? CH₃. However, the conversion from the most steric hindered isomer form of sec, rac- was slow. The ratio of the isomerization rate constants between meso-CH₃Co(H₂O)L²⁺ and sec, rac-CH₃Co(H₂O)L²⁺ to pri, rac-CH₃Co(H₂O)L²⁺ is almost a factor of 100. The thermodynamic activation parameters for these isomerization reactions were investigated.     

Irreversible Inhibition of Transglutaminases by Sulfonium Methylketones: Optimization of Specificity and Potency with w-Aminoacyl Spacers

Abstract

Sulfonium methylketones, of structure Cbz-Phe-NH(CH₂)_nCOCH₂S ⁺ (CH₃)₂, n < 2, are specific and potent inactivators of transglutaminases. The length of the -(CH₂)_n-spacer moiety, n = 1-5, is a critical determinant for both the specificity and potency of the inactivator. The dipeptidyl analog Cbz-Phe-Gly-(CH₂)_nS ⁺ (CH₃)₂, n = 1, is a more powerful inactivator of the thiol proteinase cathepsin B, k/K < 3 × 10⁵ M^?1 min^?1, than of transglutaminases, k_i(appl/K_i(appl < 1.5 × 10⁴ M^?1 min^?1. In contrast, the γ-aminobutyryl analog, n = 3, is a very potent transglutaminase inactivator with k_i(apP/ K_i(appl = 3.1 < 10⁶M^?1min^?1, but does not inactivate cathepsin B. In cell studies, the y-aminobutyryl and w-aminohexyl analogs inhibited the transglutaminase-mediated process of ionophore-induced cross-linked envelope formation by human malignant keratinocytes and the order of potency was related to that found for enzyme inhibition. The sulfonium methylketones, in equilibrium with the resonance stabilized ylides, are chemically inert towards glutathione under ambient conditions demonstrating the potential utility of this novel class of transglutaminase inhibitors for the study of enzyme inhibition in cellular environments.     

Photolytic CO-substitution reaction of organoiron thiocarboxylate derivatives CpFe(CO)2SCOR (R=alkyl, aryl) with diphosphines (Ph2P(CH2)nPPh2) (n=1-6): X-ray crystal structure of [CpFe(dppm)SCO(3,5-(NO2)2C6H3)]

The photolytic CO-substitution reaction of the organoiron thiocarboxylate complexes CpFe(CO)₂SCOR (R=CH₃, 2-CH₃C₆H₄, 2-NO₂C₆H₄, 4-NO₂C₆H₄, 3,5-(NO₂)₂C₆H₃) with diphosphines (Ph₂P(CH₂)_nPPh₂) [n=1 (dppm), n=2 (dppe), n=3 (dpppr), n=4 (dppb), n=5 (dppp), n=6 (dpph)] at room temperature using 1:2 (metal-ligand) molar ratio afforded exclusively the disubstituted complexes CpFe(Ph₂P(CH₂)_nPPh₂)SCOR when n=1, 2 and 3 and the monosubstituted analogs CpFe(CO)(Ph₂P(CH₂)_nPPh₂)SCOR when n=4, 5 and 6. This reaction was found to be strongly influenced by the backbone length of the diphosphine ligand, the nature of the R group of the thiocarboxylate moiety and the metal-ligand molar ratios. The crystal structure of CpFe(dppm)SCO(3,5-(NO₂)₂C₆H₃) was determined.     

Formation of transmembrane ionic channels of primary amphipathic cell-penetrating peptides. Consequences on the mechanism of cell penetration

The ability of three primary amphipathic Cell-Penetrating Peptides (CPPs) CH₃-CO-GALFLGFLGAAGSTMGAWSQPKKKRKV-NH-CH₂-CH₂-SH, CH₃-CO-GALFLAFLAAALS LMGLWSQPKKKRKV-NH-CH₂-CH₂-SH, and CH₃-CO-KETWWETWWTEWSQPKKKRKV-NH-CH₂-CH₂-SH called Pβ, Pα and Pep-1, respectively, to promote pore formation is examined both in Xenopus oocytes and artificial planar lipid bilayers. A good correlation between pore formation and their structural properties, especially their conformational versatility, was established. This work shows that the cell-penetrating peptides Pβ and Pep-1 are able to induce formation of transmembrane pores in artificial bilayers and that these pores are most likely at the basis of their ability to facilitate intracellular delivery of therapeutics. In addition, their behaviour provides some information concerning the positioning of the peptides with respect to the membrane and confirms the role of the membrane potential in the translocation process.     

Preparation of new tetraaza macrocyclic nickel(II) and copper(II) complexes bearing N-propionic methyl ester groups

A 14-membered tetraaza macrocycle, 2,13-bis(2-carbomethoxyethyl)-5,16-dimethyl-2,6,13,17-tetraazatricyclo[16.4.0.^1.180^7.12]docosane (L²) bearing two N-CH₂CH₂COOMe groups, and its nickel(II) and copper(II) complexes have been prepared and characterized. The nickel(II) and copper(II) complexes of 2-(2-carbomethoxyethyl)-5,16-dimethyl-2,6,13,17-tetraazatricyclo[16.4.0.^1.180^7.12]docosane (L³) containing one N-CH₂CH₂COOMe group have also been prepared. The crystal structure of [NiL²](ClO₄)₂ shows that the complex has a slightly distorted trans-octahedral coordination geometry with two relatively short axial Ni-O (N-CH₂CH₂COOMe group) bonds (2.136(3) Å). In various solvents, however, a considerable proportion of [NiL²]²⁺ exists as a square-planar form, in which the functional pendant arms are not involved in coordination. The proportion of the square-planar isomer varies with solvents in the order of nitromethane ? acetonitrile < H₂O < DMF ? DMSO. In the case of [CuL²](ClO₄)₂, only one N-CH₂CH₂COOMe group is involved in coordination. The N-CH₂CH₂COOMe group of [NiL³](ClO₄)₂ is not directly involved in coordination even in the solid state, though the functional group of [CuL³](ClO₄)₂ is coordinated to the metal ion.     

Towards an explanation of carboxylation/oxygenation bifunctionality in Rubisco. Transition structure for the carboxylation reaction of 2,3,4-pentanetriol

We construct a theoretical model of the transition structure for the carboxylation reaction of ribulose-1,5-biphosphate catalyzed by Rubisco. This is a first-order saddle point on the energy hypersurface for the nucleophilic attack of carbon dioxide on CH₃-(CHOH)₃-CH₃ at the C2 center.Ab initio analytical gradients methods at a 4-31G basis set level are used.The carbon framework and oxygens of the stationary structure superpose with the corresponding atoms of 2-carboxyarabinitol-1,5-biphosphate, which is a transition state analog that has recently been highly refined with X-ray methods. The hydroxyl group in C3 iscis to the C2 oxygen. The C3 center is somewhat pyramidized, the dienol O2-C2-C3-O3 is not planar.The geometry of the transition state allows for simple explanations of both the enolization of Rubisco's substrate ribulose-1,5-biphosphate, O₃PO-CH2-CO-(CHOH)₂-CH₂-OPO₃ and oxygenation reaction. The former is due to the pyramidal deformation at C3 and out of plane of O2-C2-C3-O3 framework: the enoliation is intramolecular and is probably enhanced by proton tunnelling. The latter is related with the fact that a rotation around an ethylene-like bond brings the triplet state down in energy. The reactive skeleton has a stationary geometry in the triplet state not very different from the one obtained in the global transition structure. There, the triplet is only 9 kcal/mol above the singlet. The spin densities at C2 and C3 centers clearly indicate the place where oxygenation will take place.     

Dialkyl- and alkylenedithiophosphates of gallium(III)

Gallium(III) tris-dialkyldithiophosphates, Ga[S₂P(OR)₂]₃ (R = C₂H₅, n-C₃H₇, i-C₃H₇, n-C₄H₉ and i-C₄H₉) and gallium(III) tris-alkylenedithiophosphates, Ga(S₂$\text{POGO}$)₃ [G = -CH₂C(C₂H₅)₂CH₂-, -C(CH₃)₂C(CH₃)₂ and -C(CH₃)₂CH₂CH(CH₃)] have been synthesized for the first time by the reactions of gallium(III) chloride with the alkali metal salt of the corresponding ligand in anhydrous benzene in 1:3 molar ratio respectively.These compounds are crystalline solids or viscous liquids and are soluble in common organic solvents, in which they show monomeric behaviour. Based on elemental analyses, molecular weight determinations, IR and NMR (¹H and ³¹P) spectral data, chelate octahedral structures have been proposed for these derivatives.     

On the identification of ionic species of neutral halogen dimers, monomers and pincer type palladacycles in solution by electrospray mass and tandem mass spectrometry

Electrospray (ESI) mass spectra analysis of acetonitrile solutions of a series of neutral chloro dimers, pincer type, and monomeric palladacycles has enabled the detection of several of their derived ionic species. The monometallic cationic complexes Pd[κ¹-C,κ¹-N,κ¹-S-C(CH₃S-2-C₆H₄)C(Cl)CH₂N(CH₃)₂]⁺ (1a) and [Pd[κ¹-C,κ¹-N,κ¹-S-C(CH₃S-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](CH₃CN)]⁺ (1b) and the bimetallic cationic complex [κ¹-C,κ¹-N,κ¹-S-C(CH₃S-2-C₆H₄)C(Cl)CH₂N(CH₃)₂]Pd-Cl-Pd[κ¹-C,κ¹-N,κ¹-S-C(CH₃S-2-C₆H₄)C(Cl)CH₂N(CH₃)₂]⁺ (1c) were detected from an acetonitrile solution of the pincer palladacycles Pd[κ¹-C,κ¹-N,κ¹-S-C(CH₃S-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](Cl) 1. For the dimeric compounds {Pd[κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](μ-Cl)}₂ (2, Y=H and 3, CF₃), highly electronically unsaturated palladacycles [Pd[κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂]⁺ (2d, 3d) and their mono and di-acetonitrile adducts, namely, [Pd[κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](CH₃CN)]⁺ (2e, 3e) and [Pd[κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](CH₃CN)₂]⁺ (2f and 3f) were detected together with the bimetallic complex [Pd[κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂]-Cl-Pd[κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N](CH₃)₂]⁺ (2a, 3a) and its acetonitrile adducts [κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](CH₃CN)Pd-Cl-Pd[ κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂]⁺ (2b, 3b) and [κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](CH₃CN)Pd-Cl-Pd[κ¹-C, κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂(CH₃CN)]⁺ (2c, 3c). The dimeric palladacycle {Pd[κ¹-C,κ¹-N-C(CH₃O-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](μ-Cl)}₂ (4) is unique as it behaves as a pincer type compound with the OCH₃ substituent acting as an intramolecular coordinating group which prevents acetonitrile full coordination, thus forming the cationic complexes [(C₆H₄(o-CH₃O)CC(Cl)CH₂N(CH₃)₂-κO,κC,κN)Pd]⁺ (4b), [(C₆H₄(o-CH₃O)CC(Cl)CH₂N(CH₃)₂- κO,κC,κN)Pd(CH₃CN)]⁺ (4c) and [(C₆H₄ (o-MeO)CC(Cl)CH₂N(CH₃)₂-κO, κC,κN)Pd-Cl-Pd(C₆H₄(o-CH₃O)CC(Cl)CH₂N(CH₃)₂-κO,κC,κN)]⁺ (4a). ESI-MS spectra analysis of acetonitrile solutions of the monomeric palladacycles Pd[κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](Cl)(Py) (5, Y=H and 6, Y=CF₃) allows the detection of some of the same species observed in the spectra of the dimeric palladacycles, i.e., monometallic cationic 2d-3d, 2e-3e and {Pd[κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](Py)}⁺ (5a, 6a) and {Pd[κ¹-C,κ¹-N-C(Y-2-C₆H₄)C(Cl)CH₂N(CH₃)₂](CH₃CN)(Py)}⁺ (5b, 6b) and the bimetallic 2a, 3a, 2b, 3b, 2c and 3c. In all cationic complexes detected by ESI-MS, the cyclometallated moiety was intact indicating the high stability of the four or six electron anionic chelate ligands. The anionic (chloride) or neutral (pyridine) ligands are, however, easily replaced by the acetonitrile solvent.     

Iridium(III)-vinylidene chemistry: Conversion of an iridacyclopentadiene-chlorido complex and terminal alkynes to iridacyclopentadiene-vinyl complexes

The reactions of [κ²(C¹,C⁴)-CRCRCRCR](PPh₃)₂Ir(Cl) (9, R = CO₂Me) with propargyl alcohol derivatives (2-propyn-1-ol, 2-methyl-3-butyn-2-ol, 1-ethynylcyclopentanol, and 1-ethynylcyclooctanol), in the presence of water leads to the formation of iridium(III)-vinyl complexes bearing the general structure [κ²(C¹,C⁴)-CRCRCRCR](PPh₃)₂Ir(CO)(κ¹-vinyl) where vinyl = -CHCH₂, -(E)-CHCHMe, -CHC(CH₂)₄, or -CHC(CH₂)₇. In these, the CO ligand was derived from the terminal carbon of the starting alkyne and the oxygen atom from water. Under anhydrous conditions, 9 undergoes reaction with 2-propyn-1-ol to give trimethyl 1,3-dihydro-3-oxo-4,5,6-isobenzofurantricarboxylate, the result of a cycloaromatization/transesterification involving the buta-1,3-dien-1,4-diyl ligand in 9 and 2-propyn-1-ol.     

Action of PGI2 analogs on the pulmonary and systemic circulations in the conscious newborn lamb

Previous work (Lock , J. Pharm. Exp. Ther. :156, 1980) has shown that conventional screening procedures for vasoactive PGI₂ analogs have little value in predicting pulmonary vasodilator activity in the newborn lamb. To gain a better insight into the structural requirements for pulmonary vasoactivity and possibly identify useful compounds for the management of neonatal pulmonary hypertensive disorders, we have tested the following PGI₂ analogs in normoxic and hypoxic newborn lambs: 15(S)-9-deoxy-15-methyl1–9α, 6-nitrilo-PGF₁ (analog I); 9-deoxy-9α, 5-nitrilo-PGF₁ (analog II); (6S, 15S)-15-methyl-PG1₁ (analog III); and (6R, 15S)-15-methyl-PGI₁ (analog IV). A prostaglandin analog mimicking PGI₂ (compound BW245C; (±)-5-(6-carboxyhexyl)-1-(3-cyclohexyl-3-hydroxypropyl)hydantoin) was tested as well. Compounds were injected into a branch pulmonary artery and any local pulmonary effect could be assessed from the change in the ratio of blood flow to the injected lung over total flow. None of the analogs tested proved to be a selective pulmonary dilator. BW245C was a potent peripheral vasodilator (threshold around 0.5 μg/kg) and indirectly lowered pulmonary vascular resistance through its systemic effects. Analog I also dilated the systemic circulation, but only at the highest dose tested (100 μg/kg). The latter finding is surprising because it was previously shown that the parent, non-methylated compound is a fairly potent and selective pulmonary vasodilator. Analog II and IV were inactive at a dose up to, respectively, 30 and 20 μg/kg. Analog III, on the other hand, weakly constricted the systemic circulation at a dose of 10 μg/kg. These findings suggest that the neonatal pulmonary vasculature is endowed with specific receptor sites which can discriminative between closely related PGI₂ analogs.     

Synthesis, characterization, and reactivity of (π-allyl)palladium(II) wrap-around complexes with 1,3-dienes

Synthesis of a series of cationic “wrap-around” complexes, η³-, η²- (CH₂-CH-CHR-CH₂-CH₂-CHCHX) Pd(II)L⁺ (R = H, CH₃; X = H, Cl, CO₂Me; L = PPh₃, P(C₄H₄N)₃), is described. These chelate complexes were prepared by exposure of π-allyl chloride dimers, (η³-(CH₂-CX-CH₂)PdCl)₂, to either 1,3-butadiene or isoprene to yield π-allyl chloride dimers of the type (η³-CH₂CHCRCH₂CH₂CH = CH(X)PdCl)₂ which result from insertion of the diene into each π-allyl unit. Abstraction of chloride with either AgSbF₆ or NaB(Ar_F)₄ in the presence of L gives the cationic wrap-around complexes in high yields. Single crystal X-ray diffraction studies of 8a (R = -CH₃, X = -Cl, L = PPh₃) and 9a (R = -H, X = -Cl, L = PPh₃) show that Pd(II) adopts essentially a square planar geometry and the chelate arm occupies a syn orientation with respect to the allyl unit. Exposure of these wrap-around complexes to nitriles of differing basicities displaces the chelated alkene to varying extents and allows assessment of the relative strengths of chelation as a function of substituents, X and R. Initial rapid displacement of the chelated alkene yields a syn-π-allyl isomer which equilibrates with the anti-π-allyl isomer which cannot close to form a chelate. Treatment of 8b with 1,3-butadiene gives not polybutadiene but 2-chloro-4-methyl-1,E-4,6-heptatriene and 2-chloro-4-methyl-1,Z-4,6-heptatriene. Formation of these trienes is first-order in butadiene. This reaction serves as a model for chain-transfer in the polymerization of butadiene.     

Synthesis and reactivity of early-late heterobimetallic complexes displaying a η-tantalum-alkylidene to palladium interaction

Tantalaalkylidene compounds, CHRTaCl₃L₂ (R=^tBu or CMe₂Ph, L=THF or 1/2dimethoxyethane) mixed with the cyclopalladated dimer [Pd(2-C₆H₄CH₂NMe₂)(μ-Cl)]₂, 1, afford good yields of heterodimetallic complexes [Pd(2-C₆H₄CH₂NMe₂)(μ-Cl)(μ-CHR=TaCl₃L], 3a, 3b, in which the TaC unit is η²-interacting with the palladium atom, while a chloride ligand is bridging the tantalum and the palladium atoms. These compounds are fairly stable in air in the solid state and also in solution at RT. The interaction of the TaC unit with Pd in these bimetallic compounds is weak as shown by the ready formation of [Pd(2-C₆H₄CH₂NMe₂)PyCl] and CHRTaCl₃Py₂ upon treatement with pyridine. Compounds analogous to 3a, b can also be obtained with 12 electrons tantalum complexes. Thus treating the same cyclopalladated dimer 1 with CHRTa(OAr)₃ (OAr=2,6-diisopropylphenyloxy) led to a much more stable though electron deficient species: [Pd(2-C₆H₄CH₂NMe₂)(μ-Cl)(μ-CH^tBu=Ta(OAr)₃], 3c. Substitution in 3a of one chloride ion by an alkyl group occurred at the tantalum metal via reaction with ZnR₂ (R=CH₂CMe₂Ph) leading to [Pd(2-C₆H₄CH₂NMe₂)(μ-Cl)(μ-CH^tBu=TaCl₃(CH₂CMe₂Ph)], 4 for which there is no free rotation around the new TaC bond and in which one of the methylene protons is strongly interacting with the palladium centre. This compound is believed to mimic an intermediate to the formation of tantalacarbyne derivative, which was obtained earlier via reaction of the uncomplexed tantalacarbene compound with dialkylzinc compounds.     

Comparative properties of fluorous phosphine ligand complexes: W(CO)5L. Crystal structure of W(CO)5P(C6H4-4-CH2CH2(CF2)7CF3)3

The compounds W(CO)₅P(C₆H₄-4-CH₂CH₂(CF₂)₇CF₃)₃ (1) and W(CO)₅P(CH₂CH₂(CF₂)₅CF₃)₃ (2) were synthesized in order to probe the electronic and physical effects of ligation by perfluorocarbon substituted tertiary phosphine ligands in a W(CO)₅L complex. The π-accepting ability of the fluorous phosphines was found to rank with non-fluorous comparators as P(CH₂CH₂(CF₂)₅CF₃)₃ > P(C₆H₄-4-CH₂CH₂(CF₂)₇CF₃)₃ > PPh₃ > P(p-tolyl)₃ > P(n-octyl)₃. The X-ray crystal structure of W(CO)₅P(C₆H₄-4-CH₂CH₂(CF₂)₇CF₃)₃ shows strong intermolecular association of fluorous components but confirms that the para fluorocarbon subtituents have an insignificant effect on the tungsten coordination environment. Partition coefficients (toluene/perfluoromethylcyclohexane) were measured for compounds 1 and 2.