Microwave‐Assisted Synthesis of Novel 2,4‐Dihydro‐5‐[4‐(trifluoromethyl)phenyl]‐3H‐1,2,4‐triazol‐3‐ones and Potentiometric Determination of Their pKa in Nonaqueous Solvents

The novel 4‐amino‐ or 4‐aryl‐substituted 2,4‐dihydro‐5‐[(4‐trifluoromethyl)phenyl]‐3H‐1,2,4‐triazol‐3‐ones 3a – 3g were synthesized by reaction of N‐(ethoxycarbonyl)‐4‐(trifluoromethyl)benzenehydrazonic acid ethyl ester ( 2 ) and primary amines or hydrazine by microwave irradiation. Compounds 3a – 3g were potentiometrically titrated with tetrabutylammonium hydroxide (Bu₄NOH) in four nonaqueous solvents, i.e., ⁱPrOH, ^tBuOH, MeCN, and N,N‐dimethylformamide (DMF). Also half‐neutralization potential values and the corresponding pK_a values were determined in all cases.     

Intrinsic Acid–Base Properties of a Hexa‐2′‐deoxynucleoside Pentaphosphate,d(ApGpGpCpCpT): Neighboring Effects and Isomeric Equilibria

The intrinsic acid‐base properties of the hexa‐2′‐deoxynucleoside pentaphosphate, d(ApGpGpCpCpT) [=(A1?G2?G3?C4?C5?T6)=(HNPP)^5?] have been determined by ¹H NMR shift experiments. The pK_a values of the individual sites of the adenosine (A), guanosine (G), cytidine (C), and thymidine (T) residues were measured in water under single‐strand conditions (i.e., 10 % D₂O, 47 °C, I=0.1 M , NaClO₄). These results quantify the release of H⁺ from the two (N7)H⁺ (G?G), the two (N3)H⁺ (C?C), and the (N1)H⁺ (A) units, as well as from the two (N1)H (G?G) and the (N3)H (T) sites. Based on measurements with 2′‐deoxynucleosides at 25 °C and 47 °C, they were transferred to pK_a values valid in water at 25 °C and I=0.1 M . Intramolecular stacks between the nucleobases A1 and G2 as well as most likely also between G2 and G3 are formed. For HNPP three pK_a clusters occur, that is those encompassing the pK_a values of 2.44, 2.97, and 3.71 of G2(N7)H⁺, G3(N7)H⁺, and A1(N1)H⁺, respectively, with overlapping buffer regions. The tautomer populations were estimated, giving for the release of a single proton from five‐fold protonated H₅(HNPP)^±, the tautomers (G2)N7, (G3)N7, and (A1)N1 with formation degrees of about 74, 22, and 4 %, respectively. Tautomer distributions reveal pathways for proton‐donating as well as for proton‐accepting reactions both being expected to be fast and to occur practically at no “cost”. The eight pK_a values for H₅(HNPP)^± are compared with data for nucleosides and nucleotides, revealing that the nucleoside residues are in part affected very differently by their neighbors. In addition, the intrinsic acidity constants for the RNA derivative r(A1?G2?G3? C4?C5?U6), where U=uridine, were calculated. Finally, the effect of metal ions on the pK_a values of nucleobase sites is briefly discussed because in this way deprotonation reactions can easily be shifted to the physiological pH range.     

Amido‐3‐hydroxypyridin‐4‐ones as Iron(III) Ligands

The synthesis and physicochemical properties of a range of 2‐ and 6‐amido‐3‐hydroxypyridin‐4‐ones are described. All the amido‐substituted 3‐hydroxypyridin‐4‐ones have lower pK_a values than 1,2‐dimethyl‐3‐hydroxypyridin‐4‐one (deferiprone). This is due to the inductive effect of the amido group. Furthermore, the pK_a values of the 3‐hydroxy group in 1‐nonsubstituted pyridinones are dramatically lower than those of the corresponding 1‐alkyl analogues, indicating that a strong hydrogen bond exists between the 2‐amido function and the 3‐oxygen anion, which stabilises the anion. As a result of the decreased competition with protons, the pFe³⁺ values of this group of molecules are higher than that of deferiprone. The distribution coefficients of these molecules are also increased despite the lack of a hydrophobic 1‐alkyl substituent and this is ascribed to the intramolecular hydrogen bond. X‐ray diffraction studies confirm the existence of the intramolecular hydrogen bond.     

Reactions of Pyridyl‐Functionalized,Chelating λ3‐Phosphinines in the Coordination Environment of RhIII and IrIII

Rh^III and Ir^III complexes based on the λ³‐P,N hybrid ligand 2‐(2′‐pyridyl)‐4,6‐diphenylphosphinine ( 1 ) react selectively at the P?C double bond to chiral coordination compounds of the type [( 1 H ? OH)Cp*MCl]Cl ( 2 , 3 ), which can be deprotonated with triethylamine to eliminate HCl. By using different bases, the pK_a value of the P? OH group could be estimated. Whereas [( 1 H ? O)Cp*IrCl] ( 4 ) is formed quantitatively upon treatment with NEt₃, the corresponding rhodium compound [( 1 H ? O)Cp*RhCl] ( 5 ) undergoes tautomerization upon formation of the λ⁵σ⁴‐phosphinine rhodium(III) complex [( 1? OH)Cp*RhCl] ( 6 ) as confirmed by single‐crystal X‐ray diffraction. Blocking the acidic P? OH functionality in 3 by introducing a P? OCH₃ substituent leads directly to the λ⁵σ⁴‐phosphinine iridium(III) complex ( 8 ) upon elimination of HCl. These new transformations in the coordination environment of Rh^III and Ir^III provide an easy and general access to new transition‐metal complexes containing λ⁵σ⁴‐phosphinine ligands.     

2‐Chloro‐3‐morpholino‐1,4‐naphtho­quinone

The structure of the title compound, C₁₄H₁₂ClNO₃, (I), comprises essentially planar mol­ecules stacked parallel to the a axis. C—H?O hydrogen‐bonding interactions exist to both naphtho­quinone O atoms and the Cl atom, but not to the morpholine O atom.     

2‐(4‐Bromophenyl)‐1,2‐dihydropyrimido[1,2‐a]benzimidazol‐4(3H)‐one and 4‐(4‐methylphenyl)‐3,4‐dihydropyrimido[1,2‐a]benzimidazol‐2(1H)‐one form hydrogen‐bonded base‐paired dimers

The title compounds, 2‐(4‐bromo­phenyl)‐1,2‐di­hydro­pyrimido­[1,2‐a]­benzimidazol‐4‐(3H)‐one, C₁₆H₁₂Br­N₃O, (IVa), and 4‐(4‐methylphenyl)‐3,4‐dihydropyrimido[1,2‐a]benzimidazol‐2‐(1H)‐one, C₁₇H₁₅N₃O, (Vb), both form R(8) centrosymmetric dimers via N—H?N hydrogen bonds. The N?N distance is 2.943 (3) Å for (IVa) and 2.8481 (16) Å for (Vb), with the corresponding N—H?N angles being 129 and 167°, respectively. However, in other respects, the supra­molecular structures of the two compounds differ. Both compounds contain different C—H?π interactions, in which the C—H?π(centroid) distances are 2.59 and 2.47 Å for (IVa) and (Vb), respectively (the latter being a short distance), with C—H?π(centroid) angles of 158 and 159°, respectively. The supramolecular structures also differ, with a short Br?O distance of 3.117 (2) Å in bromo derivative (IVa), and a C—H?O interaction with a C?O distance of 3.2561 (19) Å and a C—H?O angle of 127° in tolyl system (Vb). The di­hydro­pyrimido part of (Vb) is disordered, with a ratio of the major and minor components of 0.9:0.1. The disorder consists of two non‐interchangeable envelope conformers, each with an equatorial tolyl group and an axial methine H atom.     

Preparation of the β3‐Homoselenocysteine Derivatives Fmoc‐β3hSec(PMB)‐OH and Boc‐β3hSec(PMB)‐OH for Solution and Solid‐Phase‐Peptide Synthesis and Selenoligation

The title compounds, 4 and 7 , have been prepared from the corresponding α‐amino acid derivative selenocystine ( 1 ) by the following sequence of steps: cleavage of the Se? Se bond with NaBH₄, p‐methoxybenzyl (PMB) protection of the SeH group, Fmoc or Boc protection at the N‐atom and Arndt–Eistert homologation (Schemes 1 and 2). A β³‐heptapeptide 8 with an N‐terminal β³‐hSec(PMB) residue was synthesized on Rink amide AM resin and deprotected (‘in air’) to give the corresponding diselenide 9 , which, in turn, was coupled with a β³‐tetrapeptide thiol ester 10 by a seleno‐ligation. The product β³‐undecapeptide was identified as its diselenide and its mixed selenosulfide with thiophenol (Scheme 3). The differences between α‐ and β‐Sec derivatives are discussed.     

Importance of a Fluorine Substituent for the Preparation of meta‐ and para‐Pentafluoro‐λ6‐sulfanyl‐Substituted Pyridines

Although there are ways to synthesize ortho‐pentafluoro‐λ⁶‐sulfanyl (SF₅) pyridines, meta‐ and para‐SF₅‐substituted pyridines are rare. We disclose herein a general route for their synthesis. The fundamental synthetic approach is the same as reported methods for ortho‐SF₅‐substituted pyridines and SF₅‐substituted arenes, that is, oxidative chlorotetrafluorination of the corresponding disulfides to give pyridylsulfur chlorotetrafluorides (SF₄Cl‐pyridines), followed by chloride/fluoride exchange with fluorides. However, the trick in this case is the presence on the pyridine ring of at least one fluorine atom, which is essential for the successful transformation of the disulfides into m‐and p‐SF₅‐pyridines. After enabling the synthesis of an SF₅‐substituted pyridine, ortho‐F groups can be efficiently substituted by C, N, S, and O nucleophiles through an S_NAr pathway. This methodology provides access to a variety of previously unavailable SF₅‐substituted pyridine building blocks.     

Benzyl­triethyl­ammonium 2,2,2,4‐tetra­chloro‐2,5‐di­hydro‐1,2λ5‐oxatellurole

The geometry around the Te atom in the anion in C₁₃H₂₂N⁺·C₃H₃Cl₄OTe^? is distorted pseudo‐octahedral with three Cl atoms and the O atom forming the equatorial plane, and the C atom lying opposite the tellurium lone pair. Distances and angles are: Te—O 2.0120 (18), Te—C 2.072 (2), Te—Cl 2.5239 (7), 2.5283 (7) and 2.5577 (7) Å; O—Te—C 81.61 (9), O—Te—Cl 90.69 (6), 90.99 (6) and 168.13 (5), C—Te—Cl 87.13 (8), 86.64 (8) and 86.59 (8), and Cl—Te—Cl 87.02 (2), 90.00 (3) and 173.24 (3)°. The anions are arranged in an infinite zigzag chain parallel to the a axis through a secondary Te?Cl bond [3.8391 (8) Å].     

Ruthenium Catalyzed C−H Acylmethylation of N‐Arylphthalazine‐1,4‐diones with α‐Carbonyl Sulfoxonium Ylides: Highway to Diversely Functionalized Phthalazino‐fused Cinnolines

A direct ortho‐Csp²‐H acylmethylation of 2‐aryl‐2,3‐dihydrophthalazine‐1,4‐diones with α‐carbonyl sulfoxonium ylides is achieved through a Ru^II‐catalyzed C?H bond activation process. The protocol featured high functional group tolerance on the two substrates, including aryl‐, heteroaryl‐, and alkyl‐substituted α‐carbonyl sulfoxonium ylides. Thereafter, 2‐(ortho‐acylmethylaryl)‐2,3‐dihydrophthalazine‐1,4‐diones were used as potential starting materials for the expeditious synthesis of 6‐arylphthalazino[2,3‐a]cinnoline‐8,13‐diones and 5‐acyl‐5,6‐dihydrophthalazino[2,3‐a]cinnoline‐8,13‐diones under Lawesson's reagent and BF₃?OEt₂ mediated conditions, respectively. Of these, the BF₃?OEt₂‐mediated cyclization proceeded in DMSO as a solvent and a methylene source via dual C?C and C?N bond formations.     

Tuning the Electronic Properties and Acid‐Response Behavior of N‐Heteroacene‐Based π‐Conjugated Liquids by Changing the Number of π‐Conjugated Substituents

We have designed and synthesized two room‐temperature‐fluorescent π‐conjugated liquids based on the N‐heteroacene framework ( 1 and 2 ). These two π‐conjugated liquids, which contained one and two thiophene rings, respectively, exhibited different electronic properties and rheology behaviors. Single‐crystal X‐ray analysis of dithiophene‐appended compound 4 revealed that two thiophene rings hindered the interactions of the imino N atoms with acids through the formation of interactions between the S atoms of the thiophene rings and the imino N atoms of the pyrazine group. On the other hand, monothiophene‐appended molecules 1 and 3 each contained an unhindered imino N atom on the opposite site to the thiophene ring. Upon dissolving various acids with different pK_a values in compounds 1 and 2 , these slight structural differences gave rise to marked differences in their acid‐response behaviors, thereby resulting in the emission of variously colored fluorescence in the liquid state. Furthermore, when acids with lower pK_a values was dissolved in compounds 1 and 2 , phase transition occurred from an isotropic liquid state to a self‐organized liquid‐crystalline phase.     

Radical and cationic polymerizations of 3‐ethyl‐3‐methacryloyloxymethyloxetane

3‐Ethyl‐3‐methacryloyloxymethyloxetane (EMO) was easily polymerized by dimethyl 2,2′‐azobisisobutyrate (MAIB) as the radical initiator through the opening of the vinyl group. The initial polymerization rate (R_p) at 50 °C in benzene was given by R_p = k[MAIB]^0.55 [EMO]^1.2. The overall activation energy of the polymerization was estimated to be 87 kJ/mol. The number‐average molecular weight (M?_n) of the resulting poly(EMO)s was in the range of 1–3.3 × 10⁵. The polymerization system was found to involve electron spin resonance (ESR) observable propagating poly(EMO) radicals under practical polymerization conditions. ESR‐determined rate constants of propagation (k_p) and termination (k_t) at 60 °C are 120 and 2.41 × 10⁵ L/mol s, respectively—much lower than those of the usual methacrylate esters such as methyl methacrylate and glycidyl methacrylate. The radical copolymerization of EMO (M₁) with styrene (M₂) at 60 °C gave the following copolymerization parameters: r₁ = 0.53, r₂ = 0.43, Q₁ = 0.87, and e₁ = +0.42. EMO was also observed to be polymerized by BF₃OEt₂ as the cationic initiator through the opening of the oxetane ring. The M?_n of the resulting polymer was in the range of 650–3100. The cationic polymerization of radically formed poly(EMO) provided a crosslinked polymer showing distinguishably different thermal behaviors from those of the radical and cationic poly(EMO)s. © 2001 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 39: 1269–1279, 2001     

Crystal structure,thermal properties and detonation characterization of bis(5‐amino‐1,2,4‐triazol‐4‐ium‐3‐yl)methane dichloride

Bis(5‐amino‐1,2,4‐triazol‐4‐ium‐3‐yl)methane dichloride (BATZM·Cl₂ or C₅H₁₀N₈²⁺·2Cl^?) was synthesized and crystallized, and the crystal structure was characterized by single‐crystal X‐ray diffraction; it belongs to the space group C2/c (monoclinic) with Z = 4. The structure of BATZM·Cl₂ can be described as a V‐shaped molecule with reasonable chemical geometry and no disorder, and its one‐dimensional structure can be described as a rhombic helix. The specific molar heat capacity (C_p,m) of BATZM·Cl₂ was determined using the continuous C_p mode of a microcalorimeter and theoretical calculations, and the C_p,m value is 276.18 J K^?1 mol^?1 at 298.15 K. The relative deviations between the theoretical and experimental values of C_p,m, H_T – H_298.15K and S_T – S_298.15K of BATZM·Cl₂ are almost equivalent at each temperature. The detonation velocity (D) and detonation pressure (P) of BATZM·Cl₂ were estimated using the nitrogen equivalent equation according to the experimental density; BATZM·Cl₂ has a higher detonation velocity (7143.60 ± 3.66 m s^?1) and detonation pressure (21.49 ± 0.03 GPa) than TNT. The above results for BATZM·Cl₂ are compared with those of bis(5‐amino‐1,2,4‐triazol‐3‐yl)methane (BATZM) and the effect of salt formation on them is discussed.     

Synthesis and Structure of Low‐valent η4‐Cinnamaldehyde Cobalt Complexes

Three η⁴‐(C=C–C=O) coordination cobalt(I) complexes 1 – 3 were synthesized by the reactions of cinnamaldehyde, p‐fluorocinnamaldehyde, and p‐chlorocinnamaldehyde with CoMe(PMe₃)₄. Complex 4 as η²‐(C=C) coordination was prepared by the reaction of chalcone with Co(PMe₃)₄. The structures of complexes 1 – 4 were confirmed by single‐crystal X‐ray diffraction. Although the reactions didn't undergo C–H bond activation and decarbonylation, the formation of complexes 1 – 4 deepens our understanding of the reactions between α,β‐unsaturated aldehyde or ketone with low‐valent central cobalt atom.     

Synthesis and CD Spectra of Fluoro‐ and Hydroxy‐Substituted β‐Peptides

β‐Amino acids 1 – 3 with OH and F substituents in the α‐position have been prepared (Scheme) from the natural (S)‐α‐amino acids alanine, valine, and leucine, and incorporated into β‐hexa‐ and β‐heptapeptides 4 – 12 . The peptide syntheses were performed according to a conventional solution strategy (Boc/Bn protection) with fragment coupling. The new β‐peptides with (series a ) and without (series b ) terminal protection were isolated in HPLC‐pure form and characterized by NMR spectroscopy and MALDI mass spectrometry. The chemical properties as well as the patterns of the CD spectra (Figs. 3–5) depend upon constitution (OH, F, F₂ substitution) and configuration (l or u) of the amino acid residues, upon the total number of OH and F substituents in the peptide chain, and upon the solvent used (H₂O, MeOH, CF₃CH₂OH, (CF₃)₂CHOH). No reliable clues regarding the structures can be obtained from these CD spectra. Only a full NMR analysis will be able to answer the questions: a) with which known secondary structures (Figs. 1 and 2) of β‐peptides are the OH and F derivatives compatible? b) Are new secondary structures enforced by the polar and/or H‐bonding backbone substituents? Furthermore, the β‐peptides described here will enable us to study changes in chemical, enzymatic, and metabolic stability, and in physiological properties caused by the heteroatoms.     

Kinetics and mechanism of promoted hydrolysis of 4‐nitrophenyl acetate by zinc(II)‐tripod: Different roles of mononuclear and trinuclear species

Coordination studies on Zn(II) complexes of 1,3,5‐tri(2,5‐diazahexyl)benzene (L) show that by comparison with the non‐deprotonation of complex ZnL in a 1:1 system, the three‐dimensional complexiaton decreases the pK_a of the Zn‐bound water molecule, that is, pK_a = 7.47 for trinulclear complex Zn₃L in a 3:1 metal–ligand ratio. These two types of zinc(II) complexes have been examined as catalysts for the hydrolysis of 4‐nitrophenyl acetate (NA) in 10% (v/v) CH₃CN at 298 K, I = 0.10 mol dm^?3 KNO₃ at pH range 6.5–8.2 and 8.5–10, respectively. Kinetic studies show that the second‐order rate constants of NA‐hydrolysis catalyzed by complexes ZnL, Zn₃L, and Zn₃LH_?1 are 0.021, 0.0082, and 0.342 mol^?1 dm³ s^?1, respectively. In all the cases, the pH‐dependent observed first‐order rate constant, k_obs, shows sigmoidal pH–rate profile. The 1:1 complex ZnL–H₂O undergoes NA hydrolysis by direct rate‐determining hydrolysis to produce 4‐nitrophenol(ate) (NP^?) and ZnL(OOCCH₃); while in the 3:1 system the oxygen atom of acetic group forms a H‐bond with the Zn(II)‐bound water of the second branch of tripod indicating that the polynuclear centers are associated and bi‐functional. © 2003 Wiley Periodicals, Inc. Int J Chem Kinet 36: 41–48 2004     

2,3‐Dihydro‐3‐methyl‐2‐nitrimino‐1,3‐thiazole

The title compound {alternatively, 3‐methyl‐2‐[oxido(oxo)hydrazono]‐2,3‐dihydro‐1,3‐thiazole}, C₄H₅N₃O₂S, was obtained by methyl­ation of N‐(2‐thia­zolyl)­nitr­amine. The molecule lies on a mirror plane and the thia­zole ring is planar, regular in shape and aromatic. The S atom participates in the aromatic sextet via an electron pair on the 3p_z orbital. In the crystal, the mol­ecules are arranged in parallel layers, bound to each other by weak C—H?O and C—H?N hydrogen bonds and by S?O dipolar interactions, with an interlayer separation of 3.23 Å.     

A Regioselective Synthesis of Benzopinacolones through Aerobic Dehydrogenative α‐Arylation of the Tertiary sp3 CH Bond of 1,1‐Diphenylketones with Aromatic and Heteroaromatic Compounds

A regioselective synthesis of symmetrical and unsymmetrical benzopinacolones through aerobic dehydrogenative α‐arylation at the tertiary sp³ C?H bond of substituted 1,1‐diphenylketones with aromatic and heteroaromatic compounds, in the presence of K₂S₂O₈ in CF₃COOH at room temperature, is described. The reaction is proposed to go via a carbocation intermediate, which could be generated directly from cleavage of the sp³ C?H bond of 1,1‐diphenylketone. Subsequent α‐arylation was achieved at the methene sp³ carbon atom of the substituted ketone. A variety of substituted aromatic and heteroaromatic compounds were compatible with this reaction. In addition, benzopinacolones were converted into sterically hindered, tetrasubstituted alkenes and polycyclic aromatic compounds.     

Crystallographic report: Fluoro‐bis‐iso‐propyl‐(2,4,6‐tris‐iso‐propylphenyl)‐ silane,i‐Pr2(2,4,6‐i‐Pr3C6H2)SiF

Owing to steric congestion in i‐Pr₂(2,4,6‐i‐Pr₃C₆H₂)SiF, the geometry at the Si atom deviates slightly from ideal tetrahedral geometry with an increased C? Si? C angle of 119.02(9)° and elongated Si? C and Si? F bond distances. Copyright © 2005 John Wiley & Sons, Ltd.     

Imidazoline‐N‐oxyl: A DFT Study of Its Protonation Reaction

Imidazoline‐based nitroxides are developed as pH probes. Their pK_a values vary over a wide range (from 1 to 11), depending on the substituents attached to the five‐membered cyclic nitroxide. Density functional calculations using the PBE1PBE method at the 6‐31+G(d,p) level, combined with natural bond orbital (NBO), frontier molecular orbital (FMO), geometry, Mulliken charge, and thermodynamic analyses, are carried out to disclose the effects involved in the changes in pK_a. The studies show that the decrease of seven pK_a units from pyrrolidine ( 11 ) to imidazoline‐N‐oxyl 8 is due to the inductive electron‐withdrawing capacity of the nitroxyl group. On the other hand, by combining both the inductive and mesomeric electron‐withdrawing capacities of the NO₂ group with delocalization of the lone pair on the amino N atom of the π system of the vinyl linker, the pK_a of 4.5 of 8 was increased by around three units to 7.8 for 1 / 2 .