Synthesis,molecular docking,and inhibitory activity of a Ni Schiff-base complex against urease

A Ni(II) Schiff-base complex, Ni(C₁₄H₁₀NOBr₂)₂, was synthesized and structurally characterized by single-crystal X-ray analysis. Its inhibitory activity against Helicobacter pylori urease was evaluated in vitro and showed strong inhibitory activity against H. pylori urease compared with acetohydroxamic acid (IC₅₀ = 42.12 µmol L^?1), which is a positive reference. A docking analysis using the autodock 4.0 program could explain the inhibitory activity of the complex against urease.     

Synthesis,stereochemistry, and spectroscopic characterization of [Rh(η4-cod){(R)-2-(X-benzaldimine)-2-phenylethanol-κ 2 N,O}](acetate) (X = H; 2,4-dimethoxy)

Condensation of X-benzaldehyde with (R)-2-amino-2-phenylethanol gives the enantiopure Schiff bases (R)-2-(X-benzaldimine)-2-phenylethanol (X?=?H, HL1; 2,4-dimethoxy, HL2). The Schiff bases coordinate with dinuclear [Rh(η⁴-cod)(µ-O₂CCH₃)]₂ to afford the cationic complexes [Rh(η⁴-cod){(R)-2-(benzaldimine)-2-phenylethanol-κ ² N,O}](acetate), [Rh(η⁴-cod)(HL1)](ac) (1) and [Rh(η⁴-cod){(R)-2-(2,4-dimethoxy-benzaldimine)-2-phenylethanol-κ ² N,O}](acetate), [Rh(η⁴-cod)(HL2)](ac) (2), respectively. The Schiff bases and complexes are isolated as solids in good yields and characterized by elemental analysis, IR, UV-Vis, ¹H/¹³C-NMR, mass spectroscopy, and polarimetry.     

Metal chelates of ampicillin versus amoxicillin: synthesis,structural investigation,and biological studies

Solid chelates derived from some alkaline earth and transition metal complexes with ampicillin (Hamp, a) and amoxicillin (Hamox, b) were synthesized and characterized using elemental analysis, molar conductivity, IR, magnetic susceptibility, and thermogravimetric studies. Both drugs behave as tetradentate ligands coordinating to metal through amino, imino, and carboxylate as well as through β-lactamic carbonyl. All chelates have octahedral geometry except Cu(II) complexes which have square planar structure and uranium has pentagonal bipyramidal coordination. ¹H- and ¹³C-NMR of the Zn(II) and UO₂(VI) chelates are compared with the free ligands. The antimicrobial activity of the prepared chelates was determined.     

SYNTHESIS AND SPECTROSCOPIC STUDIES OF SOME FUNGITOXIC ORGANOLEAD(IV) COMPLEXES OF SULFUR AND NITROGEN DONOR LIGANDS

Abstract

Some organolead(IV) complexes derived from biologically active sulfur and nitrogen donor ligands have been synthesized and characterized by elemental analyses, molecular weight determinations and conductivity measurements. The trigonal bipyramidal and octahedral geometries for these complexes have been proposed on the basis of electronic, infrared and NMR (¹H and ¹³C) spectral evidences. The antifungal activity of some of the ligands and their complexes have also been evaluated against Fursarium oxysporum SCW. ex Frics f. sp. Ciceri (Pedwick) subram.     

Fading of a novel colorimetric receptor after recognizing H2PO4−

A novel selective and sensitive colorimetric receptor 1 (1, 10-phenanthroline-2, 9-dialdehyde bis-(-p-nitrophenylureasemicarbo-hydrazone)) based on urea showing distinctive color fading phenomenon towards H₂PO₄^? ion was reported. Fancifully, the recognition process of receptor 1 to H₂PO₄^? was not interfered by the existence of others anions. We have probed the binding mechanism of 1-H₂PO₄^? that H₂PO₄^? ion induced competitive hydrogen binding process via intramolecular hydrogen-bond by UV–vis, fluorescence, ¹H NMR titrations and ESI-MS experiments.     

Synthesis,spectroscopic properties,and antimicrobial activity of some new 5-phenylazo-6-aminouracil-vanadyl complexes

Six complexes, [VO(L¹-H)₂]?·?5H₂O (1), [VO(OH)(L^2,3?H)(H₂O)]?·?H₂O (2,3), [VO(OH)(L^4,5?H)(H₂O)]?·?H₂O (4,5), [VO(OH)(L⁶?H)(H₂O)]?·?H₂O (6), were prepared by reacting different derivatives of 5-phenylazo-6-aminouracil ligands with VOSO₄?·?5H₂O. The infrared and ¹H NMR spectra of the complexes have been assigned. Thermogravimetric analyses (TG, DTG) were also carried out. The data agree quite well with the proposed structures and show that the complexes were finally decomposed to the corresponding divanadium pentoxide. The ligands and their vanadyl complexes were screened for antimicrobial activities by the agar-well diffusion technique using DMSO as solvent. The minimum inhibitory concentration (MIC) values for 1–4 and 6 were calculated at 30°C for 24–48?h. The activity data show that the complexes are more potent antimicrobials than the parent ligands.     

The Reaction Activity of Aromatic Carbonyl Compounds with Diphenylphosphine Oxide Studied by 31P NMR

Abstract

A series of α-hydroxyphosphine oxides were prepared by the reactions of diphenylphosphine oxide and aromatic carbonyl compounds and characterized by ¹H NMR, ¹³C NMR, ³¹P NMR, FT-IR, ESI-MS, and HR-MS spectra. The reaction rates and experimental conditions of aromatic aldehydes and aromatic ketones were obviously different due to the activity of their carbonyls. The different substituents of the aromatic aldehydes affected the reaction rate too, and the quantitative reactivity of their substituent conformed to the Hammett equation. The results were confirmed by ³¹P NMR spectroscopy.     

Excellent Ag+ selective receptors: Syntheses and complexation properties of novel biscalix[4]arene with benzalazine groups

By reacting mono-substituted or 1,3-bi-substituted [2-(p-formylphenyloxy)ethyloxy]-p-tert-butylcalix[4]arene (3 or 4) with hydrazine hydrate in ‘1+2’ or ‘2+2’ condensation mode, novel benzalazine-bridging biscalix[4]arenes 5 and 7 were conveniently obtained in the yields of 76 and 81%, respectively. Condensation of compound 4 and salicylide hydrazone gave a novel calix[4]arene benzalazine derivative 6 in the yield of 85%. The structures and conformations of all new compounds were characterised by elemental analyses, ESI-MS, ¹H NMR and ¹H–¹H COSY techniques. Biscalix[4]arene 7 adopts a symmetrical cone conformation with tube cavity. The liquid–liquid extraction experiment showed that all new hosts possessed excellent complexation abilities towards soft metal cations. Compound 7 exhibited high complexation selectivity towards Ag⁺. The Ag⁺/Na⁺ and Ag⁺/Hg²⁺ extraction percentages of host 7 were as high as 73.1 and 54.9, respectively. The UV–vis spectra complexation experiments revealed that the complexation constant of receptor 7 with Ag⁺ was 1.9 × 10⁵ M^? 1 and the 1:1 stoichiometry of receptor 7–Ag⁺ complex was formed. The ¹H NMR spectra complexation experiments suggested that Ag⁺ was bound in a cavity composed of two benzalazine groups on bridging chains.     

Natural products as sources of new fungicides (II): antiphytopathogenic activity of 2,4-dihydroxyphenyl ethanone derivatives

A series of 17 simple 1-(2,4-dihydroxyphenyl) ethanones were synthesised, and their structures characterised by ¹H, ¹³C NMR and ESI-MS. Their in vitro antifungal activities were evaluated against five phytopathogenic fungi including Glomerella cingulate, Botrytis cirerea, Fusarium graminearum, Curvularia lunata and Fusarium oxysporum f. sp. vasinfectum by the mycelial growth inhibition assay. Compounds 2g and 2h exhibited broad-spectrum inhibitory activity against the mycelial growth of the tested pathogens with IC₅₀ values in the range of 16–36 μg/mL, and in particular being more active to G. cingulate, with IC₅₀ values of 16.50 and 19.25 μg/mL, respectively, than the other pathogens. Preliminary SAR indicated that an α,β-unsaturated ketone unit of the alkyl chain of the compounds is the structure requirement for fungicidal action. The results suggested that 2g and 2h may be promising leads in the development of new antifungal agents.     

Synthesis and Evaluation of Thymol-Based Synthetic Derivatives as Dual-Action Inhibitors against Different Strains of H. pylori and AGS Cell Line

Following a similar approach on carvacrol-based derivatives, we investigated the synthesis and the microbiological screening against eight strains of H. pylori, and the cytotoxic activity against human gastric adenocarcinoma (AGS) cells of a new series of ether compounds based on the structure of thymol. Structural analysis comprehended elemental analysis and ¹H/¹³C/¹⁹F NMR spectra. The analysis of structure–activity relationships within this molecular library of 38 structurally-related compounds reported that some chemical modifications of the OH group of thymol led to broad-spectrum growth inhibition on all isolates. Preferred substitutions were benzyl groups compared to alkyl chains, and the specific presence of functional groups at para position of the benzyl moiety such as 4-CN and 4-Ph endowed the most anti-H. pylori activity toward all the strains with minimum inhibitory concentration (MIC) values up to 4 µg/mL. Poly-substitution on the benzyl ring was not essential. Moreover, several compounds characterized by the lowest minimum inhibitory concentration/minimum bactericidal concentration (MIC/MBC) values against H. pylori were also tested in order to verify a cytotoxic effect against AGS cells with respect to 5-fluorouracil and carvacrol. Three derivatives can be considered as new lead compounds alternative to current therapy to manage H. pylori infection, preventing the occurrence of severe gastric diseases. The present work confirms the possibility to use natural compounds as templates for the medicinal semi-synthesis.     

Synthesis,antimicrobial activity and QSAR studies of 2,5-disubstituted benzoxazoles

In this study, a new series of 2,5-disubstituted benzoxazoles was synthesized and their structures were elucidated by elemental analysis, MASS, ¹H-NMR, ¹³C-NMR and IR spectral data. Newly and previously synthesized 2,5-disubstituted benzoxazole derivatives were evaluated for antibacterial and antifungal activity against standard strains and their drug-resistant isolates. Microbiological results showed that the compounds presented a large spectrum of activity having MIC values of 250–7.8 µg mL^?1 against the tested microorganisms. Among the newly synthesized derivatives 3–22, compound 11 was the most active against Candida krusei out of all; however, it was one dilution less potent than standard drug fluconazole. In addition, all the new and previous compounds were more active than standard drugs ampicillin trihydrate and rifampicin against Pseudomonas aeruginosa and its gentamicin-resistant isolate. The 2D-QSAR (Quantitative Structure–Activity Relationship) analysis of a set of newly and previously synthesized benzoxazoles tested for growth inhibitory activity against methicillin-resistant Staphylococcus aureus (MRSA) was also performed by using multivariable regression analysis. The activity contributions for substituent effects of these compounds were determined from the correlation equation for predictions of the lead optimization.     

Computer-assisted structure elucidation of organic compounds III: Automatic fragment generation from13C-NMR spectra

The interpretation of carbon-NMR spectra is mainly based on the comparison with suitable reference data taken from literature. The whole information contents of¹³C-NMR spectra cannot be utilized by manual interpretation. Therefore a network of interactive computer programs has been developed, which simulates the strategy of the spectroscopist in generating structural fragments from the spectral data. The most important knowledge source for this process is a carbon-NMR data base containing some 17,500 spectra. Structural fragments are generated automatically from this data file and assembled by a model builder to complete chemical structures using constraints derived from the spectral data. A comparison of the experimental carbon-NMR spectrum with the estimated ones allows the generation of a sorted hitlist.For part II see: H. Kalchhauser, W. Robien,J. Chem. Inf. Comput. Sci. 1985,25, 103.     

(1iR,1iiR,2iR,2iiR)-Ni,Nii-(1,3-亚苯基双(亚甲基))环己烷-1,2-二胺作为配体的双核铂配合物的合成及其抗癌活性

以(1ⁱR,1ⁱⁱR,2ⁱR,2ⁱⁱR)-Nⁱ,Nⁱⁱ-(1,3-亚苯基双(亚甲基))环己烷-1,2-二胺(HL)作为配体,设计并合成了7种双核铂配合物,并利用IR,¹H NMR,¹³C NMR,ESI-MS和元素分析等进行了表征。通过MTT法测定目标双核铂配合物对人类HepG-2,A549,HCT-116和MCF-7四种癌细胞系的细胞毒性。结果表明,所有的化合物对HepG-2,A549和HCT-116细胞系均表现了良好的细胞毒活性,但对MCF-7细胞系均无活性。其中,以3-羟基环丁烷-1,1-二羧酸为离去基团的配合物P7对HepG-2和A549细胞系的活性优于卡铂,对HCT-116细胞系的活性接近于奥沙利铂。     

13C, 15N and 113Cd NMR and Molecular Orbital Studies of Novel Bile Acid N-(2-aminoethyl)amides and Their Cd2+-complexes

Lithocholic acid N-(2-aminoethyl)amide (1) and deoxycholic acid N-(2-aminoethyl)amide(2) have been prepared and characterized by¹H, ¹³C and ¹⁵N NMR. The accurate molecular masses of 1 and 2 have been determined by ESI MS. The formation of the Cd²⁺-complexes (1+Cd and 2+Cd) in CD₃OD solution have been detected by ¹H,¹³C, ¹⁵N and ¹¹³Cd NMR. The ¹³C NMR chemical shift assignments of 1 and 2 and their Cd²⁺-complexes are based on DEPT-135 and z-GS ¹H,¹³C HMQC experiments as well as comparison with the assignments of the related structures. The ¹⁵N NMR chemical shiftassignments of the ligands and theirCd²⁺-complexes are based on z-GS¹H,¹⁵N HMBC experiments. ¹³C NMR chemical shift differences between 1and its 1:1 Cd²⁺-complex based on ab initiocalculations at Hartree-Fock SCI-PCM level using3-21G(d) basis set are in agreement with theexperimental shift changes observed onCd²⁺-complexation.     

NMR studies of molecular motion in tetramethylammonium hydroxide pentahydrate

Polycrystalline (CH₃)₄NOH·5 H₂O (I) and (CH₃)₄NOD·5D₂O (II) have been studied by¹H NMR lineshapes, second moments and spin-lattice relaxation times and by²H NMR lineshapes as a function of temperature. From low temperatures the first motion to occur is reorientation of the internally rigid (CH₃)₄N⁺ ion about a uniqueC ₃ axis (E _ta = 8.37 kJ/mol forI,E _a = 9.00 kJ/mole forII), followed closely by pseudo isotropic reorientation of the whole ion (E _a = 18.10 kJ/mol). Motion of the cage molecules (water and hydroxide ion) occurs at higher temperatures with an apparentE _a = 11.30 kJ/mol. There is some evidence of a phase transition inII but notI in the 220–230 K region.²H NMR lineshapes ofII below 220 K indicate static cage molecules. Some of the²H quadrupole coupling constants derived from these spectra correspond to O·O hydrogen-bond distances which are incompatible with the known room temperature structure ofI. Above the possible transition inII the anisotropic²H lineshapes indicate rapid motion of²H among all possible hydrogen-bond sites via transfer along the bonds and molecular reorientation. This motion persists in the high temperature phase but the lineshape becomes isotropic due to the cubic symmetry of this phase. It is possible that¹H or²H tunnelling plays an important part in the motion of the cage molecules and the different phase behaviour ofI andII.Dedicated to Dr D. W. Davidson in honor of his great contributions to the sciences of inclusion phenomena.     

Acetate platinum(II) compound with 5,7-ditertbutyl-1,2,4-triazolo[1,5-a]pyrimidine that overcomes cisplatin resistance: structural characterization,in vitro cytotoxicity,and kinetic studies

The reaction of silver acetate with cis-[PtI₂(dbtp)₂], where dbtp = 5,7-ditertbutyl-1,2,4-triazolo-[1,5-a]pyrimidine, yielded cis-[Pt(OOCCH₃)₂(dbtp)₂]·dmf (1). The complex has been analyzed by multinuclear magnetic resonance (¹H, ¹³C, ¹⁵N), IR, and Raman. The compound formed two rotamers in CDCl₃ and its spatial structures have been optimized using computational calculation. It was found that head-to-tail rotamer (1a) is more stable than its head-to-head counterpart (1b). In vitro antiproliferative activity against four tumor cell lines (A549, T47D, FaDu, and A2780cis) revealed in all cases significant cytotoxicity (IC₅₀ = 0.26–1.80 μM), possessing IC₅₀ values at least fivefold lower than cisplatin, carboplatin, and oxaliplatin (except A2780cis). The remarkable in vitro activity against T47D and A2780cis suggested the ability to overcome cisplatin resistance in these types of tumor cells. In addition, in vitro toxicity was evaluated against BALB/3T3 and has shown that the lipophilic platinum(II) complex (1) inhibits cell proliferation weaker than cisplatin and oxaliplatin. Additionally, cis-[Pt(OOCCH₃)₂(dbtp)₂]·dmf exhibited selective activity, in contrast to cisplatin or oxaliplatin.     

Host-guest chemistry. 2. Amine inclusion compounds of 2-[o-(triphenylphosphoranylidenamino)benzyliden]amino-1H-2,3-dihydroindazol-3-one. X-ray structure of its 1∶1∶1 inclusion complex with isopropylamine and water

The crystal and molecular structure is reported for the inclusion compound 2-[o-(triphenylphosphoranylidenamino)benzyliden]amino-1H-2,3-dihydroindazol-3-one/isopropylamine/water3b. The crystal structure consists of discrete dimeric salt-like aggregates joined together by strong N⁺–H...^–O–C hydrogen bonds between pairs of centrosymmetrically-related indazolonate anions and isopropylammonium cations. Six other inclusion compounds have been prepared and characterized by NMR [with propylamine (3a), withtert-butylamine (3c), withsec-butylamine (3d), withtert-pentylamine (3e), with 1-methylbutylamine (3f) and withiso-pentylamine (3g)]. Two different arrangements are found, both with the host being in the anionic form. The guests are either: (i) one protonated amine and one water molecule (3b and3f); or (ii) one protonated amine and the corresponding neutral amine (3a, 3c, 3d, 3e and3g). Supplementary Data relating to this article (structure factors, thermal components, hydrogen parameters and bond distances and angles, and¹³C-NMR shifts) are deposited with the British Library at Boston Spa, Wetherby, West Yorkshire, U.K., as Supplementary Publication No. SUP 82155 (23 pages).For Part 1, see Reference [1].     

Identification of Initiator Fragments in Polyisobutylene by Nmr Spectroscopy

Abstract

Deuterated polyisobutylenes carrying protonated initiator fragments were prepared by the living polymerization technique employing perdeuterated isobutylene [CD₂=C(CD₃)₂] and select protonated initiators (see Scheme 1). The polymers were analyzed by ¹H- and ¹³C-NMR spectroscopy, and the resonances due to the protic initiator fragments were unequivocally assigned. The assignments of ¹³C-NMR signals were affected by the distortionless enhancement by polarization transfer mode of spectra accumulation.     

Synthesis and structure of 2-phenyl-4-aryl-3,4,5,6-tetrahydrobenzo[h]quinazolines

Summary The reaction of 2-arylidene-1-tetralones1 with benzamidine gave 2-phenyl-4-aryl-3,4,5,6-tetrahydrobenzo[h]quinazolines2. Investigations on the tautomeric equilibria of2 by IR,¹H- and¹³C-NMR showed the compounds to exist predominantly in the tautomeric form2A both in the solid state and in solution. Acetylation and oxidation of the heterocyclic ring of2 provided further evidence for the structural assignment of the title compounds.

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Synthese und Struktur von 2-Phenyl-4-aryl-3,4,5,6-tetrahydrobenzo[h]chinazolinen

Zusammenfassung Die Reaktion von 2-Aryliden-1-tetralonen1 mit Benzamidin ergab 2-Phenyl-4-aryl-3,4,5,6-tetrahydrobenzo[h]chinazoline2. Untersuchungen über das tautomere Gleichgewicht von2 mittels IR,¹H-NMR, und¹³C-NMR Spektroskopie zeigten, daß für die Verbindungen das Tautomere2A dominierte (sowohl in fester Phase als auch in Lösung). Acetylierung und Oxidation des heterocyclischen Ringes von2 ergab weitere Beweise für die Struktur der Titelverbindungen.

     

New amides fromSpilanthes oleracea

In addition to the well known affinin [=spilanthol, (2E,6Z,8E)-deca-2,6,8-trienoic acid isobutylamide (1)], the corresponding 2-methyl-butylamide (2), and two new acetylenic alkamides were isolated fromSpilanthes oleracea L. by reversed phase medium pressure chromatography: (Z)-non-2-en-6,8-diynoic acid isobutylamide (3) and (Z)-dec-2-en-6,8-diynoic acid isobutylamide (4). The structures and their stereochemistries were elucidated by¹H-NMR,¹³C-NMR (2 and3), MS, UV, IR, and CD (2). The chemotaxonomic significance of the distribution of alkamides within theCompositae tribeHeliantheae is briefly discussed.

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Neue Amide ausSpilanthes oleracea (Kurze Mitteilung)

Zusammenfassung AusSpilanthes oleracea wurden neben dem seit langem bekannten Affinin [=Spilanthol, (2E,6Z,8E)-Deca-2,6,8-triensäureisobutylamid (1)] durch Umkehrphasen-Mitteldruckchromatographie das entsprechende 2-Methylbutylamid (2) und zwei neue acetylenische Alkamide isoliert: (Z)-Non-2-en-6,8-diinsäure-isobutylamid (3) und (Z)-Dec-2-en-6,8-diinsäure-isobutylamid (4). Die Strukturen und deren Stereochemie wurden mittels¹H-NMR,¹³C-NMR (2 und3), MS, UV, IR und CD (2) aufgeklärt. Die chemotaxonomische Bedeutung der Verbreitung von Alkamiden innerhalb der Compositen-TribusHeliantheae wird kurz diskutiert.