2H-Indazolo[2,1-b]phthalazine-trione derivatives: Inhibition on some metabolic enzymes and molecular docking studies

In this study, substituted 2H-indazolo[2,1-b]phthalazine-1,6,11-trione compounds ( 4a–d ) obtained via one-pot three-component condensation reaction of aromatic aldehydes, cyclic 1,3-dione, and phthalhydrazide in ethanol catalyzed by Y(OTf)₃ showed satisfactory inhibitory effects against some important enzymes. Also, these molecules had K_i values in the row of 185.92 ± 36.03-294.82 ± 50.76 nM vs carbonic anhydrase I (CA I), 204.93 ± 46.90-374.10 ± 83.63 nM against human CA II, 937.16 ± 205.82-1021.83 ± 193.66 nM against α-glycosidase (α-Gly), respectively. For cholinesterase enzymes, the K_i values were found in the range of 47.26 ± 9.62-72.05 ± 19.47 nM against acetylcholinesterase (AChE) and 65.03 ± 9.88-102.83 ± 25.04 nM against butyrylcholinesterase (BChE), respectively. The inhibition effects of these compounds against enzymes whose name are AChE, BChE, α-Gly, hCA I, and hCA II, were compared with control molecules like tacrine, acarbose, and acetazolamide.     

Experimental and computational investigations on the high binding-selectivity of pyrimidine derivatives by a pillar[5]arene

The binding selectivity of an adenine-monofunctionalized pillar[5]arene (H) with a series of pyrimidine derivatives were investigated through ¹H NMR experiments and density functional theory (DFT) study. High binding-selectivity was demonstrated. Typically, H displayed very strong binding strength with 6-(2,4-dioxo-3, 4-dihydropyrimidin-1 (2H)-yl)hexanenitrile (G1) [K_a >10⁵ M^?1], up to about 3000-fold as compared with 1-hexylpyrimidine-2,4(1H, 3H)-dione (G5) [K_a = 31 M^?1]. The strong binding ability of H with G1 was due to the cooperative multiple hydrogen bond, dipole-dipole, C-H···π and π···π interactions. The high binding-selectivity was also verified by calculation results. The calculated interaction energy (ΔE_i) of G1?H was ?12.92 Kcal·mol^?1 while that of G5?H was ?2.85 Kcal·mol^?1.     

Synthesis and inhibition profiles of N-benzyl- and N-allyl aniline derivatives against carbonic anhydrase and acetylcholinesterase – A molecular docking study

The alkyl and aryl derivatives of aniline are important starting materials in fine organic synthesis. Allyl bromide and benzyl chloride were taken as substrates for the alkylation reaction and as a halide ion scavenger. Triethylamine was utilized at reflux condition of N,N-dimethylacetamide (DMA). Novel synthesized N-benzyl and N-allyl aniline derivatives (1a-f) were evaluated to be highly potent inhibitors for acetylcholinesterase (AChE) and carbonic anhydrases (hCAs). The half maximal inhibitory concentration (IC₅₀) of N-benzyl- and N-allyl aniline derivatives were calculated between 243.11 and 633.54 nM for hCA I, 296.32–518.37 nM for hCA II and 182.45–520.21 nM for AChE enzymes. On the other hand, K_i values are in the range of 149.24 ± 15.59 to 519.59 ± 102.27 nM for AChE, 202.12 ± 16.21 to 635.31 ± 45.33 nM for hCA I and 298.57 ± 94.13 to 511.18 ± 115.98 nM for hCA II isoenzyme. Additionally, in silico molecular docking computations were performed with Autodock Vina program to support the experimental in vitro studies for both hCAs and AChE inhibitors. The in silico molecular docking results demonstrated that the scores are in good agreement with the experimental results.     

Novel Mannich bases with strong carbonic anhydrases and acetylcholinesterase inhibition effects: 3-(aminomethyl)-6-{3-[4-(trifluoromethyl)phenyl]acryloyl}-2(3H)-benzoxazolones

In this study, a new series of Mannich bases, 3-(aminomethyl)-6-{3-[4-(trifluoromethyl)phenyl]acryloyl}-2( 3H )-benzoxazolones ( 1a–g ), were synthesized by the Mannich reaction. Inhibitory effects of the newly synthesized compounds towards carbonic anhydrases (CAs) and acetylcholinesterase (AChE) enzymes were evaluated to find out new potential drug candidate compounds. According to the inhibitory activity results, K_i values of the compounds 1 and 1a–g were in the range of 12.3 ± 1.2 to 154.0 ± 9.3 nM against hCA I, and they were in the range of 8.6 ± 1.9 to 41.0 ± 5.5 nM against hCA II. Ki values of acetazolamide (AZA) that was used as a reference compound were 84.4 ± 8.4 nM towards hCA I and 59.2 ± 4.8 nM towards hCA II. K_i values of the compounds 1 and 1a–g were in the range of 35.2 ± 2.0 to 158.9 ± 33.5 nM towards AChE. K_i value of Tacrine (TAC), the reference compound, was 68.6 ± 3.8 nM towards AChE. Furthermore, docking studies were done with the most potent compounds 1d , 1g , and 1f (in terms of hCA I, hCA II, and AChE inhibition effects, respectively) to determine the binding profiles of the series with these enzymes. Additionally, the prediction of ADME profiles of the compounds pointed out that the newly synthesized compounds had desirable physicochemical properties as lead compounds for further studies.     

Novel silver(I)N-heterocyclic carbene complexes bearing 2-(4-hydroxyphenyl)ethyl group: Synthesis,characterization, and enzyme inhibition properties

Herein, novel silver-based N-heterocyclic carbene (NHC) complexes bearing 2-(4-hydroxyphenyl)ethyl group were synthesized. Novel Ag(I)NHC complexes were synthesized from the 2-(4-hydroxyphenyl)ethyl-substituted benzimidazolium salts and silver oxide via in situ deprotonation method. The successful formation of all Ag(I)NHC complexes was proved by using ¹H NMR, ¹³C NMR, FTIR spectroscopy, and elemental analysis techniques. In addition, their inhibitory effects have been investigated of these substances on acetylcholinesterase (AChE), α-glycosidase (α-Gly), human carbonic anhydrase I (hCA I), and human carbonic anhydrase II (hCA II) enzymes. It has been seen that all compounds have a better ability to inhibit compared with existing tried inhibitors. Among these, the best inhibitor against AChE enzyme is 1g (K_i : 9.54 ± 0.98 μM and IC₅₀ : 17.40), and against α-Gly, 1c showed the highest effect (K_i 3.09 ± 0.36 μM and IC₅₀ 7.91). The best inhibitor against hCA I and hCA II enzymes are 1c and 1g compounds. For hCA I and hCA II, IC₅₀ values were calculated as 17.85 and 9.06 μM and K_i values were measured as 5.45 ± 2.02 and 8.99 ± 2.02 μM, respectively.     

Synthesis,EGFR-TK inhibition and anticancer activity of new quinoxaline derivatives

Abstract

Ethyl 4-substituted-3-oxo-quinoxaline-2-carboxylates 3–5 were obtained via alkylation of ethyl 3-oxo-3,4-dihydroquinoxaline-2-carboxylate (1). Compound 1 was heterocyclized using hydrazines, ethylenediamine, and ethanolamine to give pyrazoloquinoxalines 6, 7, diazepinoquinoxaline 8, and oxazepinoquinoxaline 10. The quinoxaline-2-carboxamides 9, 11, 12 were prepared via condensation of compound 1 with different amines. Compound 1 was thiated using Lawesson’s reagent affording quinoxaline-3-thione 13, in fair yield. In addition, the reaction of 4-methyl-3-oxoquinoxaline 3 with some binucleophiles led to a series of new oxoquinoxaline derivatives 14–18. The molecular structure of compounds 1, 3, and 9 was confirmed by X-ray crystallography.

The anti-proliferative activity showed that among all the tested compounds, compounds 3, (IC₅₀ 2.51?±?3.0, 4.22?±?1.6 and 2.27?±?1.9?µM), 11 (IC₅₀ 1.32?±?2.61, 1.41?±?1.23 and 1.18?±?1.91?µM) and 17 (IC₅₀ 1.72?±?1.32, 1.85?±?0.94 and 1.92?±?4.83?µM) showed noteworthy anti-proliferative effects against the three cancer cell lines, HCT116, HePG2 and MCF7, respectively, compared to the reference drugs doxorubicin (IC₅₀ 1.41?±?0.58, 0.90?±?0.62 and 1.01?±?3.02?µM) and erlotinib (IC₅₀ 1.63?±?0.81, 1.57?±?0.62 and 1.49?±?0.54?µM). Compounds 3 (0.899?nM), 11 (0.508?nM) and 17 (0.807) showed strong EGFR inhibitory activity compared to Erlotinib (0.439?nM) and these results are in agreement with the docking study. These results suggest that compounds could probably be promising anticancer agents with EGFR inhibitory activity.     

Synthesis and monoamine oxidase A/B inhibitory evaluation of new benzothiazole-thiazolylhydrazine derivatives

Abstract

In this study, a novel series of benzothiazole-thiazolylhydrazine (3a–3i) was synthesized and their structures were characterized by ¹H-NMR, ¹³C-NMR spectrometry, and mass spectroscopy. These compounds were evaluated as inhibitors of type A and type B monoamine oxidase (MAO) enzymes. The most active compound 3b (2-((2-(2-(4-(4-Nitrophenyl)thiazol-2-yl)hydrazineylidene)-2-phenylethyl)thio)benzothiazole) showed strong inhibitory activity at hMAO-A (IC₅₀ of 0.095?±?0.004?µM). Furthermore, compound 3i (2-((2-(2-(4-(2,4-dichlorophenyl)thiazol-2-yl)hydrazineylidene)-2-phenylethyl)thio)benzothiazole) showed significant inhibition profile on hMAO-A with the IC₅₀ values 0.141?±?0.006?µM.     

Studies on the composition and kinetics of chromium(III)-alanine system

Kinetics of the complex formation of chromium(III) with alanine in aqueous medium has been studied at 45, 50, and 55°C, pH 3.3–4.4, and μ = 1 M (KNO₃). Under pseudo first-order conditions the observed rate constant (k_obs) was found to follow the rate equation: Values of the rate parameters (k_an, k, K_IP, and K) were calculated. Activation parameters for anation rate constants, ΔH^≠(k_an) = 25 ± 1 kJ mol^?1, ΔH^≠(k) = 91 ± 3 kJ mol^?1, and ΔS^≠(k_an) = ?244 ± 3 JK^?1 mol^?1, ΔS^≠(k) = ?30 ± 10 JK^?1 mol^?1 are indicative of an (I_a) mechanism for k_an and (I_d) mechanism for k routes (‥substrate Cr(H₂O) is involved in the k route whereas Cr(H₂O)₅OH²⁺ is involved in k′ route). Thermodynamic parameters for ion-pair formation constants are found to be ΔH°(K_IP) = 12 ± 1 kJ mol^?1, ΔH°(K) = ?13 ± 3 kJ mol^?1 and ΔS°(K_IP) = 47 ± 2 JK^?1 mol^?1, and ΔS°(K) = 20 ± 9 JK^?1 mol^?1.     

Synthesis,characterization and biological evaluation of N-substituted triazinane-2-thiones and theoretical–experimental mechanism of condensation reaction

The synthesis of triazinthions and their reactions with some nucleophilic reagents have been investigated during this scientific study. Thus, thiourea with a single component has been synthesized as a result of concomitant reactions of aldehyde and amines trials. The structure of the synthesized compounds was confirmed by ¹H, ¹³C NMR spectroscopy methods. The inhibitory effects of novel N-substituted triazinane-2-thione derivatives on acetylcholinesterase (AChE) activity were performed according to the spectrophotometric method of Ellman et al. These novel N-substituted triazinane-2-thiones derivatives were effective inhibitors of the α-glycosidase, cytosolic carbonic anhydrase I and II isoforms (hCA I and II), and Acetylcholinesterase (AChE) enzymes with K_i values in the range of 1.01 ± 0.28 to 2.12 ± 0.37 nm for α-glycosidase, 13.44 ± 4.39 to 74.98 ± 6.25 nm for hCA I, 10.41 ± 4.8 to 72.6 ± 17.66 nm for hCA II, 36.82 ± 9.95 to 108.48 ± 1.17 nm for AChE, and 624.62 ± 100.34 to 1124.16 ± 205.14 nm for α-glycosidase, respectively.     

Synthesis and Crystal Structure of the Azide K4[Re6Sei8(N3)a6]·4H2O; Luminescence,Redox, and DFT Investigations of the [Re6Sei8(N3)a6]4– Cluster Unit

The reaction of K₄[Re₆Seⁱ₈(OH)^a₆] · 8H₂O with NaN₃ in water results in the formation of [Re₆Seⁱ₈(N₃)^a]^4– units that crystallize with K⁺ and H₂O to form K₄[Re₆Seⁱ₈(N₃)^a₆] · 4H₂O [P2₁/c (N°14), a = 9.0595(3) Å, b = 13.2457(4) Å, c = 13.2040(5) Å, β = 94.472(1)°]. In the solid state, the unit is characterized by N₃ linear groups forming bond angles of roughly 120° with the Re₆ cluster. The positions of the ν_as and ν_sy bands as well as N–N–N deformation modes of the N₃ groups are discussed. Luminescence properties of the [Re₆Seⁱ₈(N₃)^a]^4– unit were measured in the solid state and in an acetonitrile solution. The redox potential of the [Re₆Seⁱ₈(N₃)^a]^4–/[Re₆Seⁱ₈(N₃)^a]^3– system was measured in acetonitrile. Experimental results were analyzed in the light of density functional theory calculations.     

Reactions of the iso-butyl radical during 1,1′-azoisobutane pyrolysis

Quantitative analysis of the products formed in 1,1′-azoisobutane pyrolyses in the temperature range of 553°–602°K has shown that the major reactions of the iso-butyl radical are Analysis of initial rate data gave log₁₀k₄/(k_c)^1/2(cm^?3/2.mol ^1/2.sec^?1/2) = 7.54±0.44 ? (136.5 + 4.8) kJ/mol/2.303RT, the Arrhenius parameters obtained being in good agreement with thermodynamic data for reaction (4). Measured values of k_a/(k_c)^1/2 where k_a is the rate constant of the reaction iC₄H₉ + AIB → iC₄H₁₀ +. AIB were consistent with published parameters determined by photolysis of 1,1′-azoisobutane. Combination of photolysis and pyrolysis data gave log₁₀ k_a/(k_c)^1/2(cm^3/2.mol^?1/22.sec^?1/2) = 3.68 ± 0.15 ? (27.2 ± 1.2) kJ/mol/2.303RT. The crosscombination ratio for methyl and iso-butyl radicals has been found to be 0.25, indicating that the geometric mean rule does not hold for methyl and iso-butyl radicals.     

Synthesis,structure and magnetic properties of Ni2(NO3)4(APTY)4 (APTY=1,5-dimethyl-2-phenyl-4-{[(1 E )-pyridine-4-ylmethylene]amino}-1,2-dihydro-3 H -pyrazol-3-one)

A novel dinuclear nickel(II) complex Ni₂(NO₃)₄(APTY)₄ (1) (APTY?=?1,5-dimethyl-2-phenyl-4-{[(1E)-pyridine-4-ylmethylene]amino}-1,2-dihydro-3H-pyrazol-3-one), was synthesized by solvothermal reaction of Ni(NO₃)₂?·?6H₂O with APTY in methanol at 353?K. The structure consists of centrosymmetric dimers resulting from octahedrally coordinated Ni atoms bridged by APTY ligands. Weak intermolecular interactions (C–H?···?N, C–H?···?O hydrogen bonding, C–H?···?π and π–π stacking interactions) are responsible for a supramolecular assembly of molecules in the lattice. Magnetic measurements over 1.8–300?K show weak antiferromagnetic coupling between Ni(II) ions with J?=?2.969?cm^?1, g?=?2.280, θ?=??5.903.     

Equilibrium and Kinetic Studies on Ligand Substitution Reactions of Trans-[COIII(en)2(Me)H2O]2+: A Model for Coenzyme B12

Ligand substitution of trans-[Co^III(en)₂(Me)H₂O]²⁺ was studied for pyrazole, 1,2,4-triazole and N-acetylimidazole as entering nucleophiles. These displace the coordinated H₂O molecule trans to the methyl group to form trans-[Co(en)₂(Me)azole]. Stability constants at 18°C for the substitution of H₂O by pyrazole, 1,2,4-triazole and N-acetylimidazole are 0.7 ± 0.1, 13.8 ± 1.4 and 1.7 ± 0.2 M^?1, respectively. Second order rate constants at the same temperature for the reaction of trans-[Co^III(en)₂(Me)H₂O]²⁺ with pyrazole, 1,2,4-triazole and N-acetylimidazole are 161 ± 12, 212 ± 11 and 12.9 ± 1.6 M^?1 s^?1, respectively. Activation parameters (ΔH^≠, ΔS^≠) are 67 ± 6 kJ mol^?1, + 27 ± 19 J K^?1 mol^?1; 59 ± 2 kJ mol^?1, + 1 ± 6 J K^?1 mol^?1 and 72 ± 4 kJ mol^?1, + 23 ± 14 J K^?1 mol^?1 for reactions with pyrazole, 1,2,4-triazole and N-acetylimidazole, respectively. Substitution of coordinated H₂O by azoles follows an I_d mechanism.     

Synthesis of spirooxindoles promoted by the deep eutectic solvent,ZnCl2+urea via the pseudo four-component reaction: anticancer,antioxidant, and molecular docking studies

Abstract

Various spirooxindoles (7a–c, 8a–c, 9a–c, and 10a–c) were efficiently synthesized using deep eutectic solvent ZnCl₂+urea and well characterized using IR, ¹H NMR, and ¹³C NMR spectroscopic techniques. The biological screening results showed that the compound 9a exhibited potent anticancer activity against MCF7 and HeLa cell lines with IC₅₀ values 6.47?±?0.01 and 9.14?±?0.32?µM, respectively. The compound 7c exhibited potent activity against the HeLa cell line with IC₅₀ value 6.81?±?0.01?µM. The compound 9a exhibited a potent antioxidant activity with IC₅₀ value 7.34?±?0.17?µM. The comparative molecular docking study against the cancer proteins EGFR and HER2 revealed that the EGFR was the best target protein receptor for the target compounds. Among all the compounds, the compound 9a exhibited the least binding energy ?10.72?kcal/mol against the protein EGFR (PDB ID: 4HJO).     

Supramolecular architecture built of Co(II) and a tripodal ligand containing 1-D water tapes with (H2O)16 cluster units

The reaction of Co(NO₃)₂?·?6H₂O with a tripodal ligand leads to a new complex {[Co(L)]?·?2NO₃?·?8H₂O} (1) confirmed by single-crystal X-ray diffraction, infrared spectroscopy, and elemental analysis. The particular interest of 1 is in the formation of a 1-D water tape consisting of (H₂O)₁₆ cluster units, the neighboring water tapes are connected by free nitrate anions via hydrogen bonds into a 2-D guest layer. These guest layers are alternately packed face-to-face with the 2-D host layers along the a-axis to form a 3-D supramolecular architecture. There exist C–H?···?N and C–H?···?O weak hydrogen bonds between the guest layer and host layer. These weak hydrogen bonds and water–nitrate, water–water hydrogen bonds are important for the stability of the overall structure.     

Synthesis,crystal structure,and catalytic performance of two 3-D supramolecular compounds: (C7N2H7)3(C7N2H6) · PMo12O40 · 2H2O and (C7N2H7)3(C7N2H6)2 · AsMo12O40 · 3H2O

Two organic–inorganic compounds based on Keggin building blocks have been synthesized by hydrothermal methods, (C₇N₂H₇)₃(C₇N₂H₆)?·?PMo₁₂O_40?·?2H₂O (1) and (C₇N₂H₇)₃(C₇N₂H₆)_2?·?AsMo₁₂O_40?·?3H₂O (2) (C₇N₂H₆?=?benzimidazole). Single-crystal X-ray analysis revealed that 1 crystallized in the triclinic system, P-1 space group with a?=?9.8980(4)?Å, b?=?11.2893(4)?Å, c?=?25.8933(9)?Å, α?=?93.307(2)°, β?=?90.630(2)°, γ?=?108.330(2)°, V?=?2740.68(18)?ų, Z?=?2, R ₁(F)?=?0.0740, ωR ₂(F ²)?=?0.1511, and S?=?1.037; 2 crystallized in the triclinic system, P-1 space group with a?=?12.3353(4)?Å, b?=?13.2649(4)?Å, c?=?20.2878(6)?Å, α?=?95.6630(10)°, β?=?100.1720(10)°, γ?=?99.3940(10)°, V?=?3195.72(17)?ų, Z?=?2, R ₁(F)?= 0.0329, ωR₂ (F ²)?=?0.1236, and S?=?1.088. The two compounds show a layer framework constructed from Keggin-polyoxoanion clusters and benzimidazole via hydrogen bonds and π–π stacking interactions, resulting in a 3-D supramolecular network. Both have high catalytic activity for oxidation of methanol. When the initial concentration of the methanol is 5.37?g?m^?3 in air and the flow velocity is 4.51?mL?min^?1, methanol is completely eliminated at 150°C for 1 (160°C for 2).     

Synthesis and crystal structure of the first dinuclear zinc complex containing 1,4,7-triazacyclononane and biological properties of the protonated ligand

Abstract

A new binuclear complex, [Zn₂L₂Cl₄]·2H₂O {L?=?N-aldehyde-N-(4-(benzyloxy)benzyl)-1,4,7triazacyclononane}, was synthesized and characterized by X-ray, elemental analysis, infrared and electronic spectroscopy, and mass spectrometry. The central ion is bridged by the L and lies in a tetrahedral configuration with Zn···Zn distance of 6.283 Å. The complex crystallizes in the triclinic space group Pī. ESI-MS of the complex indicates that the protonated ligand HL⁺ is the active species. The interaction of HL⁺ with calf thymus–DNA (CT–DNA) and bovine serum albumin (BSA) was studied by means of various spectroscopic methods, which revealed that HL⁺ could interact with CT–DNA through groove-binding mode and could quench the intrinsic fluorescence of BSA in a static quenching process. DNA–cleavage experiments indicate that HL⁺ exhibits efficient DNA–cleavage activity in the presence of H₂O₂, hydroxyl radical (HO^?) may serve as the major cleavage active species, and the pseudo-Michaelis–Menten kinetic parameters (K_cat, K_M, V_max); 2.47?h^?1, 2.70?×?10^?4 M and 6.68?×?10^?4 Mh^?1.     

Syntheses,crystal structures and fluorescent properties of four one-dimensional lanthanide coordination polymers with 3-cyanobenzoato

The hydrothermal reactions of Nd(ClO₄)₃·6H₂O, Gd(ClO₄)₃·6H₂O, Dy(ClO₄)₃·6H₂O, Er(ClO₄)₃·6H₂O with 1,3-dicyanobenzene, give rise to four one-dimensional rare earth-based coordination polymers: [M(3-CNC₆H₄COO)₃(H₂O)₂] _n (where M?=?Nd (1), Gd (2), Dy (3), Er (4), 3-CNC₆H₄COO?=?3-cyanobenzoato), respectively. Their solid-state structures have been characterized by X-ray single-crystal diffraction studies. The results show that 1,3-dicyanobenzene hydrolyzed to give 3-cyanobenzoato under hydrothermal condition, and the four complexes are isomorphous. Crystal data for 1: triclinic, space group P-1, a?=?9.4063(19), b?=?11.485(2), c?=?12.616(3)?Å, α?=?66.38(3), β?=?74.01(3), γ?=?86.96(3)°, V?=?1197.9(4)?ų, Z?=?1, D _c?=?1.704?Mg?m^?3; for 2: triclinic, space group P-1, a?=?9.3712(19), b?=?11.446(2), c?=?12.627(3)?Å, α?=?65.86(3), β?=?73.89(3), γ?=?86.84(3)°, V?=?1184.8(4)?ų, Z?=?1, D _c?=?1.759?Mg?m^?3; for 3: triclinic, space group P-1, a?=?9.3425(19), b?=?11.432(2), c?=?12.703(3)?Å, α?=?65.28(3), β?=?73.80(3), γ?=?86.86(3)°, V?=?1180.6(4)?ų, Z?=?1, D _c?=?1.780?Mg?m^?3; for 4: triclinic, space group P-1, a?=?9.3425(19), b?=?11.432(2), c?=?12.703(3)?Å, α?=?65.28(3), β?=?73.80(3), γ?=?86.86(3)°, V?=?1180.6(4)?ų, Z?=?1, D _c?=?1.7794?Mg?m^?3. The fluorescence emission spectra of compounds 1 to 4 are also reported.     

Syntheses and Antimicrobial Activity of Some Novel 6‐Substituted Dibenzo[d,f][1,3,2]dioxaphophepin‐6‐oxides,Sulfides, and Selenides

6‐Substituted‐dibenzo[d, f][1,3,2]dioxaposphepin‐6‐oxides, sulfides, and selenides (5a–i, 6a–d, and 7a–d) were synthesized by reacting 2,2′‐biphenol (1) with phosphorus tribromide in the presence of triethylamine at 0–30°C and subsequent reaction of the monobromide (2) with different Grignard reagents (3) at room temperature. The products (4) were converted to corresponding oxides, sulfides, and selenides (5a–i, 6a–d, and 7a–d) by oxidation with H₂O₂ at room temperature and refluxing with sulfur and selenium respectively. The chemical structures of all the products were confirmed by analytical, IR, NMR (¹H, ¹³C, and ³¹P), and mass spectral data. Most of these compounds exhibited moderate antimicrobial activity.     

Cuprous complexes and dioxygen,VII. Competition between one- and two-electron reduction of O2 in the autoxidation of Cu(1-methyl-2-hydroxymethyl-imidazole)2+

The complexation of 1-methyl-2-hydroxymethyl-imidazole (L) with Cu(I) and Cu(II) has been studied in aqueous acetonitrile (AN). Cu(I) forms three complexes, Cu(AN)L⁺, CuL₂⁺, and Cu(AN)H_?1L, with stability constants logK(Cu(AN)⁺ + L ? Cu(AN)L⁺) = 4.60 ± 0.02, logβ₂ = 11.31 ± 0.04, and logK(Cu(AN)H_?1L+H⁺ ? Cu(AN)L⁺) = 10.43 ± 0.08 in 0.15M AN. The main species for Cu(II) are CuL²⁺, CuH_?1L⁺, CuH_?1L₂⁺, and CuH_?2L₂. The autoxidation of CuL₂⁺ was followed with an oxygen sensor and spectrophotometrically. Competition between the formation of superoxide in a one-electron reduction of O₂ and a path leading to H₂O₂ via binuclear (CuL₂)₂O was inferred from the rate law with k_a = (2.31 ± 0.12) · 10⁴M ^?2S ^?1, k_b = (1.0 ± 0.2) · 10³M ^?1, k_c = (2.85 ± 0.07) · 10²M ^?2S ^?1, k_d = 3.89 ± 0.14M ^?1S ^?1, k_e = 0.112 ± 0.004, k_f = (2.06 ± 0.24) · 10^?10M S ^?1, k_g = (1.35 ± 0.07) · 10^?7 S ^?1, and k_h = (6.8 ± 1.4) · 10^?7M ^?1 S ^?1.