Donor–acceptor perylenediimide–ferrocene conjugates: synthesis,photophysical, and electrochemical properties

Donor–acceptor, perylenediimide–ferrocene conjugates have been synthesized by Suzuki, and Sonogashira coupling reactions. The photophysical and electrochemical properties of these conjugates are discussed. It has been shown that fluorescence as well as the electron affinity of the perylenediimide can be tuned by attaching the appropriate ferrocenyl derivatives.     

Ru(II)–DMSO complexes containing aromatic and heterocyclic acid hydrazides: Structure,electrochemistry and biological activity

The reaction of cis-[RuCl₂(DMSO)₄] with a family of aromatic and heterocyclic acid hydrazides yielded new complexes of the general formula trans-[RuCl₂(DMSO)₂(hydrazide)] · nH₂O (n = 0; 1–6; n = 1; 7). The new complexes have been characterized by IR, UV–Vis and ¹H NMR spectroscopic methods. In addition, the structure of one of the complexes, [RuCl₂(DMSO)₂(tcah)] · H₂O (tcah = thiophene-2-carboxylic acid hydrazide), has been determined by single crystal X-ray diffraction. All the studies reveal the neutral bidentate coordination of the hydrazide ligands through the acyl oxygen and amine nitrogen atoms. The electron transfer properties of the complexes were studied by cyclic voltammetry and all the complexes except one show an irreversible/quasi-reversible reduction wave (Ru^II/Ru^I) and an uncoupled oxidation peak (Ru^III/ Ru^II). The preliminary DNA-binding ability of the complexes, studied with herring sperm DNA, shows the binding of the complexes with DNA with a lesser affinity than classical intercalators. The complexes have also been screened for their antibacterial activity against five pathogenic bacteria.     

Structure–activity relationship of polyamine conjugates for uptake via polyamine transport system

Structural Chemistry - High toxicity of anticancer drugs led to development of targeted drug delivery directly to the specific organs. Polyamine transport system (PTS) of mammalian cells is one of...     

Synthesis,characterization and antimalarial activity of new iridium–chloroquine complexes

Chloroquine base (CQ) reacts with [Ir(COD)Cl]₂ and IrCl₃ · 3H₂O to yield of Ir(CQ)Cl(COD) (1) and Ir₂Cl₆(CQ) · 3H₂O (2), respectively. Reaction of [Ir(COD)Cl]₂ with CQ in the presence of NH₄PF₆ leaded to [Ir(CQ)(Solv)₂]PF₆ (3). The three new iridium–CQ complexes were characterized by a combination of elemental analysis, IR and NMR spectroscopies and evaluated in vitro against Plasmodium beghei. Comparison of the IC₅₀ values obtained with the experimental compounds with that determined for chloroquine diphosphate indicated a higher activity for complex 2, while complexes 1 and 3 showed a similar and lower activity, respectively.     

Synthesis,antiproliferative evaluation,and structure–activity relationships of novel triazole–isoindoline hybrids bearing 3,4,5-trimethoxyphenyl moiety

As an aspect of our ongoing research on developing novel antiproliferative agents, 31 new triazole–isoindoline hybrids bearing 3,4,5-trimethoxyphenyl moiety were synthesized and evaluated for their antiproliferative activity against four cancer cell lines (HepG2, HeLa, PC-3, and HCT116). Some compounds showed excellent potency, and compared to fluorouracil, the most promising compound 6s exhibited 5.8-, 4.3-, and 1.3- fold increase in activities against HeLa, HepG2, and PC-3 cell lines with IC₅₀ values of 9.7, 10.7, and 16.8 μM, respectively. Moreover, structure–activity relationship studies indicated that a much shorter amide linkage and electron-withdrawing groups at phenyl ring of the acetamide fragment contribute to the antitumour activity.     

Synthesis and α-amylase inhibitory activity of glucose-deoxynojirimycin conjugates

Inhibitors of α-amylase have attracted attention for their putative effects against diabetes mellitus. Although numerous studies have explored natural small molecule inhibitors, acarbose is currently the only compound with sufficient inhibitory potency and drug-like characteristics to be considered as a potential therapeutic agent. We have synthesized conjugates of the potent glucosidase inhibitor, 1-deoxynojirimycin, and glucose, with the aim of enhancing inhibitory activity against α-amylase. This synthetic conjugate showed increased inhibition of α-amylase compared to 1-deoxynojirimycin alone, suggesting that similar modifications of existing glucosidase inhibitors may yield more potent α-amylase inhibitors.     

Structure–activity relationships of cannabinoids: A joint CoMFA and pseudoreceptor modelling study

A cannabinoid pseudoreceptor model for the CB1-receptor has been constructed for 31 cannabinoids using the molecular modelling software YAK. Additionally, two CoMFA studies were performed on these ligands, the first of which was conducted prior to the building of the pseudoreceptor. Its pharmacophore is identical with the initial superposition of ligands used for pseudoreceptor construction. In contrast, the ligand alignment for the second CoMFA study was taken directly from the final cannabinoid pseudoreceptor model. This altered alignment gives markedly improved cross-validated r² values as compared to those obtained from the original alignment with values of 0.79 and 0.63, respectively, for five components. However, the pharmacophore alignment has the better predictive ability. Both the CoMFA and pseudoreceptor methods predict the free energy of binding of test ligands well.     

Design,synthesis, and characterization of fullerene–peptide–steroid covalent hybrids

The present study reports the synthesis, spectral characterization, self-assembly properties, and preliminary in vitro study of antioxidant capacity of two triple covalent hybrids consisting of fullerene C₆₀, peptide, and steroidal moiety. Previously synthesized fulleropyrrolidinic acid and pregnenolone were connected by peptide linker using a multistep DCC/DMAP and/or EDC/HOBT esterification/amidation procedure. The hybrids were characterized by comparative analysis of spectroscopic data obtained from FTIR, UV–vis, HRMS, and extensive NMR experiments (¹H, ¹³C, COSY, HSQC, and HMBC). The self-assembling properties and morphology of triads samples prepared by drop-drying method were examined by scanning electron microscopy (SEM). Preliminary in vitro antioxidant activity was studied by Ferrous ion Oxidation-Xylenol orange (FOX) method.     

Bimetallic Co–Cu polyaniline composites: Structure and electrocatalytic activity

Bimetallic Co–Cu polyaniline composites were produced by oxidative polymerization of aniline, with ammonium peroxydisulfate and hydrogen peroxide as oxidizing agents. Co(II) and Cu(II) chlorides were introduced into the polymer by the in situ method. It was found that the phase constitution of the composites is affected by their synthesis conditions and content of both metals in them. The electrocatalytic activity of the composites in the electrohydrogenation of p-nitroaniline in an aqueous-alcoholic-alkaline medium of the catholyte was studied and found to exceed that of composites synthesized with the use of H₂O₂ and evaporation of the solvent.     

Total synthesis of (−)-synrotolide and the evaluation of its antiproliferative activity

The stereoselective synthesis of (−)-synrotolide was achieved in high overall yield from d-(−)-ribose and 3-butyn-1-ol. The pivotal step in this approach is the selective deprotection of the acetonide group in the presence of acetate groups using TiCl₄. Moreover, the biological activity of (−)-synrotolide was evaluated on HeLa, PANC 1, HepG2, and SK-N-SH cancer cell lines. The (−)-synrotolide selectively and potently inhibited the growth of PANC 1 cell line.     

Synthesis,antioxidant and anticancer screenings of berberine–indole conjugates

Research on Chemical Intermediates - A variety of heterocyclic nitrogen cores in the form of indole moieties were linked to the natural isoquinoline alkaloid molecule berberine to achieve...     

Phenanthroline–dipyrromethene conjugates: synthesis,characterization, and spectroscopic investigations

Mono- and tri-topic ligands, based on dipyrromethenes and the 1,10-phenanthroline nucleus, as well as BF₂ complexes derived thereof are described. While BODIPY 12 has been X-ray crystallographically characterized, the structural features of the free ligands 9 and 10 may render them useful as precursors for the elaboration of novel supramolecular architectures.     

Synthesis of new binary porphyrin–cyanine conjugates and their self-aggregation in organic-aqueous media

1. Download high-res image (132KB)
2. Download full-size image

     

Sensitive routine liquid chromatography–tandem mass spectrometry method for serum estradiol and estrone without derivatization

The need for a routinely applicable assay to measure low estradiol levels in adult men, postmenopausal women, and young adolescents was recently discussed in an Endocrine Society position statement. Our aim was to develop a sensitive liquid chromatography–tandem mass spectrometry method for estradiol and estrone in human serum without the need for derivatization or extended extraction protocols. After protein precipitation of serum with a mixture of methanol/acetonitrile (85/15) (v/v) containing isotopic internal standards (17β-estradiol-16,16,17-d ₃ and estrone-2,3,4-¹³C), we quantified estradiol and estrone by two-dimensional liquid chromatography–tandem mass spectrometry with electrospray ionization in the negative mode monitoring 5?×?271.20→145.00 (17β-estradiol) and 269.20→145.00 (estrone). Sensitivity was increased by using fluoride and summation of 5 identical transitions for estradiol. Our method was analytically validated, compared against direct immunoassays using serum of 25 adult men, and clinically tested by measuring samples of 3 men at baseline and after chemical castration, 30 postmenopausal women and 15 patients receiving aromatase inhibitors. Total imprecision was below 20 % for the low quality controls. Limit of quantification was 1.3 ng/L (4.8 pmol/L) for estradiol and 1.2 ng/L (4.4 pmol/L) for estrone. Estradiol in Certified Reference Material BCR-576 was within specified uncertainty limits. No significant ion suppression or interference was observed. Our method showed modest correlation with direct immunoassay for estradiol (r ²?=?0.64) but no correlation for estrone (r ²?=?0.12). Patient sample results were within expected ranges. In conclusion, we developed a routinely applicable liquid chromatography–tandem mass spectrometry method for estradiol and estrone measurement which is sensitive enough for use in men, postmenopausal women, and young adolescents.

Anticancer activity of new benzofuroxan–imidazolone hybrids

Novel hybrid compounds containing both benzofuroxan and 1H-imidazol-2(3H)-one moieties were synthesized by an S_NAr reaction between 7-chloro-4,6-dinitrobenzofuroxan and imidazol-2-ones, with the only C⁴ regioisomer having been formed. Cytotoxic effects of parent and obtained compounds were estimated on human cancer and normal cells, while two of imidazolones showed higher cytotoxicity in relation to the M-HeLa cancer line compared to the hybrid products. In relation to the normal liver cell line Chang, the tested compounds were found to be non-toxic and can be promising for further development of anticancer agents.     

Study on the structure–activity of dihydromyricetin and its new production

Myricetin (MY) was firstly synthesized from dihydromyricetin (DMY), and its antioxidant activity was analyzed. FTIR, NMR, and TG measurements confirmed that the DMY turned to MY. Scanning electron microscope observation showed that the 2,3-single bond offered great flexibility on the stage of crystallization to form imperfect crystalline regions; hence, DMY tends to form larger columnar crystals than MY. It has been found that the antioxidative efficiency of DMY was superior to MY, based on the measurement of radical scavenging activity by DPPH and the oxidation induction time of PP-antioxidant samples. The 2,3-double bond in MY structure, known as one of the characteristic determinants, was not an important requirement for antioxidant capacity or even negative correlation observed. Such a deduction was further supported by UV–Vis absorption spectra change when the pH was raised to pH 9. It was concluded that the ortho-trihydroxyl group in the B ring provides an antioxidant defense, and the 2,3-single band of C ring provides the structural stability.     

Mössbauer studies on ferrocene complexes: XVI. Structure of triorganostannyl derivatives of dimethylaminomethylferrocene and N,N-dimethylbenzylamine

A series of new stannylated derivatives of dimethylaminomethylferrocene (DMAMF) and N,N-dimethylbenzylamine have been synthesised and their structures investigated by ¹H, ¹³C and ¹¹⁹Sn NMR together with ⁵⁷Fe and ¹¹⁹Sn Mössbauer spectroscopy. Polystannylated derivatives were synthesised from DMAMF and BuLi in the presence of TMED. The methylene protons of the CH₂NMe₂ group were diastereotopic for all the DMAMF derivatives synthesised. The chemical shift differences of these protons is discussed in terms of conformational changes. ¹³C and 119Sn shifts were used to establish the substitution patterns in the polystannylated derivatives. ¹³C shifts for the 2-substituted derivatives of both DMBA and DMAMF were reasonably additive, for both the free amines and the quaternary ammonium salts. The Mössbauer data show no evidence of pentacoordination in any of the derivatives.     

Synthesis, Structure and Electrochemistry of Macrocyclic 1,1＇-Bis（1,3-phenyleneoxyacetylpyrazoyl）ferrocene

1,1＇-Diacetoacetylferrocene 1 reacted with phenylene-1,3-dioxyactyl hydrazine 2 in absolute ethanol to give the macrocyclic ferrocenyl dipyrazole compound in moderate yield. Determined by X-ray structure analysis, it crystallizes in monoclinic system, space group P21/c with a = 13.7509（4）, b = 8.1277（2）, c = 21.7472（6） A, β = 103.1030（10）°, V = 2367.25（11） A^3, Z = 4, Dc = 1.505 g/cm^3, R = 0.0353 and wR = 0.0811. The electrochemical studies reveal that redox of Fe^＋/Fe in ferrocene is a reversible one-electron process.