Study on isohexenylnaphthazarins polymerization in alkaline media

The chiral pair alkannin and shikonin (A/S) and their isohexenylnaphthazarin (IHN) esters, which are naturally occurring hydroxynaphthoquinones (HNQ), are potent pharmaceutical substances with a wide spectrum of biological activity. The stability of A/S and their derivatives during process and storage is crucial to their use as drugs, cosmetics and food additives. The influence of alkaline media and of IHN esters hydrolysis was experimentally investigated on IHN polymerization by size exclusion chromatography (SEC). It was proved that during IHN esters hydrolysis, polymeric A/S and IHN are formed. An optimization of the hydrolysis conditions of IHN esters was also approached in terms of polymerization. Hydrolysis of IHN from a pure mixture of pigments proved preferable to that of preliminary root extracts by means of IHN polymerization, even for analytical determination; non-polar solvents are proposed for the extraction of IHN from roots, followed by hydrolysis, aiming to minimize the polymeric IHN and A/S formed. It was also proved that polymerization of IHN in alkaline media and during hydrolysis of IHN esters proceeds through the intermediate formation of semiquinones; after acidification, coupling of semiquinones with phenoxyl radicals results in polymeric IHN structures.     

Encapsulation of isohexenylnaphthazarins in cyclodextrins

Naturally occurring isohexenylnaphthazarins (IHN), such as Alkannin, Shikonin (A/S) and their derivatives, are potent pharmaceutical substances with a wide spectrum of biological activity. In the present study, inclusion complexes of alkannin and shikonin commercial samples and IHN derivatives in the form of an oily extract of Alkanna tinctoria roots were formed with beta-cyclodextrin (CD) and beta-HPCD. These complexes were investigated to evaluate the effect of complexation on their aqueous solubility, decoloration, and also the percentage of polymeric A/S and IHN derivatives enclosed in the CDs cavity, since these decrease the active monomeric IHN. Both beta-CD and beta-HPCD increased the aqueous solubility of A/S and IHN derivatives and thus inclusion complexes can be used as drug delivery systems for A/S in both internal (capsules, tablets) and external hydrophilic pharmaceutical and cosmetic preparations (creams, gels, sprays) with enhanced bioavailability. The inclusion complexes formed had a pale purple colour, contributing to the partial decoloration of the A/S and thus of the fi nal pharmaceutical preparations. Finally, CDs selectively included more monomeric and less polymeric IHN, compared with the initial each time sample that is encapsulated; thus inclusion complexes may present enhanced biological activity.     

Solid-phase extraction for purification of alkannin/shikonin samples and isolation of monomeric and dimeric fractions

Isohexenylnaphthazarins (IHN), commonly known as alkannins and shikonins (A/S), are potent pharmaceutical substances with a wide spectrum of wound healing, antimicrobial, anti-inflammatory, and antitumor activity. Purification of A/S is crucial for their use in pharmaceuticals and for biological experimentation. Dimeric and oligomeric A/S derivatives co-exist with the active monomeric ones in most of the samples produced either by (semi)-synthesis or biotechnologically or isolated from natural products. Oligomeric A/S derivatives have not been studied for biological activity hitherto and a method to isolate them is essential.     

Determination of naturally occurring hydroxynaphthoquinone polymers by size-exclusion chromatography

Summary Polymerization of alkannin, shikonin, and their derivatives, potent pharmaceutical substances, crucially affects their use in pharmaceuticals, cosmetics, and as food colorants, because it leads to loss of their antimicrobial activity, reduction of the lustre of their red coloration, and a decrease in their solubility. In this study size-exclusion chromatography (SEC) has been used for the first time for qualitative and quantitative analysis of monomeric and polymeric hydroxynaphthoquinone alkannin and shikonin derivatives. The purity and degree of polymerization has been determined to evaluate severalAlkanna tinctoria root samples from different geographical sources, and commercial samples of alkannin and shikonin, as pharmaceutical raw materials. Conditions for extraction of hydroxynaphthoquinones fromAlkanna tinctoria roots with olive oil were optimized in terms of polimerization, aiming to improve the biological activity of the final pharmaceutical product, Helixderm.     

Simultaneous determination of monomeric and oligomeric alkannins and shikonins by high-performance liquid chromatography-diode array detection-mass spectrometry

Alkannin and shikonin (A/S) derivatives have been found in the roots of several Boraginaceous species and are produced through plant tissue cultures. The chiral compounds alkannins and shikonins are potent pharmaceutical substances with a wide spectrum of pharmacological activities such as wound healing, antimicrobial, anti-inflammatory, anticancer and antioxidant. Although oligomeric A/S derivatives have been detected in root extracts and commercial samples their detection and determination through high-performance liquid chromatography has not been reported. Therefore, in the present study a rapid, simple high-performance liquid chromatography-diode array detection-mass spectrometry (HPLC-DAD-MS) method was developed to detect, separate and determine monomeric and oligomeric/polymeric derivatives of alkannin/shikonin simultaneously for the first time. An optimization of HPLC-DAD parameters was performed. Both atmospheric pressure chemical ionization (APCI) and electrospray ionization (ESI) modes were applied, in order to compare detection of monomeric and oligomeric A/S. Additionally, oligomeric A/S constituents in several samples were identified and the mode of A/S polymerization was proposed.     

Analysis of alkannin derivatives from Alkanna species by high-performance liquid chromatography/photodiode array/mass spectrometry

Alkannin, shikonin (A/S) and their derivatives are enantiomeric hydroxynaphthoquinone red pigments found in the roots of almost 150 species of the Boraginaceae family. A/S have been shown to exhibit strong wound healing, antimicrobial, anti-inflammatory and antioxidant activities and recent extensive research has well established their antitumor properties. A/S and their derivatives comprise the active ingredients of several pharmaceutical and cosmetic preparations. Although A/S have been efficiently synthesized and have been produced by cell tissue cultures in high yield, most of the pharmaceutical preparations worldwide contain A/S extracted from the roots of Boraginaceous species, found in nature. In the present study, a high-performance liquid chromatography/photodiode array/mass spectrometry (HPLC/PDA/MS) method was established to identify monomeric hydroxynaphthoquinones of the alkannin series and other metabolites from Boraginaceous root extracts. This method can be applied for the identification of alkannin derivatives and other metabolites from Boraginaceous cell cultures, and also to determine active ingredients in pharmaceutical preparations containing A/S derivatives. A phytochemical investigation of the Alkanna genus grown in Greece was also performed. Fifty-three root samples belonging to 10 species of the genus Alkanna (A. calliensis, A. corcyrensis, A. graeca, A. methanaea, A. orientalis, A. pindicola, A. primuliflora, A. sieberi, A. stribrnyi and A. tinctoria) were collected from several regions of the Greek flora and analyzed for their constituent hydroxynaphthoquinones and other metabolites. In most of the above Alkanna samples tested, the main hydroxynaphthoquinones were determined to be beta,beta-dimethylacrylalkannin, isovalerylalkannin + alpha-methyl-n-butylalkannin and acetylalkannin. The hydroxynaphthoquinone constituents and their proportions were found to vary among Alkanna species. Unknown metabolites (not monomeric hydroxynaphthoquinones) were detected by HPLC-PDA-MS, while in several Alkanna species hydroxynaphthoquinones were detected for the first time.     

Preparative isolation and purification of alkannin/shikonin derivatives from natural products by high-speed counter-current chromatography

Alkannin and shikonin (A/S) and their derivatives have been found in the roots of several Boraginaceous species and are also produced through plant tissue cultures. The chiral compounds A/S are potent pharmaceutical substances with a wide spectrum of biological and pharmacological activities like wound healing, antimicrobial, anti-inflammatory, anticancer and antioxidant activity. High-speed counter-current chromatography (HSCCC) was applied for the first time to the separation, preparative isolation and purification of A/S and their esters from extracts of Alkanna tinctoria roots, as well as commercial samples. The constituents of HSCCC fractions and their purity were determined by high-performance liquid chromatography-diode array detection-mass spectrometry (HPLC-DAD-MS), since DAD cannot detect oligomeric A/S derivatives that are present in most of the samples containing the respective monomeric derivatives. The purity of HSCCC fractions was compared with the one of fractions isolated by column chromatography (CC) using as stationary phases silica gel and Sephadex LH-20. As shown, the purity of monomeric alkannin/shikonin was greater by HSCCC than CC separation of commercial A/S samples.     

Ab initio and semiempirical study of structure and electronic spectra of hydroxy substituted naphthoquinones

The geometries of hydroxy derivatives of 1,4-naphthoquinone (NQ), viz., 2-hydroxy-1,4-naphthoquinone (2HNQ), 5-hydroxy-1,4-naphthoquinone (5HNQ), and 5,8-dihydroxy-1,4-naphthoquinone (DHNQ), have been optimized using the semiempirical and ab initio theoretical methods. Semiempirical methods used for the optimization are Austin Model 1 (AM1) and Zerner's Intermediate Neglect of Differential Overlap/1(ZINDO/1). For ab initio calculations the 6-31G* basis set is used. The electronic spectra of 1,4-naphthoquinone and its hydroxy derivatives are calculated using the semiempirical Zerner's Intermediate Neglect of Differential Overlap/Spectroscopy (ZINDO/S) method employing the geometries optimized at AM1, ZINDO/1 and ab initio levels and compared with their electronic absorption spectra measured by us. For hydroxy substituted systems, such calculations for spectral assignments are made for the first time. It is found that though the predictions of the three theoretical methods for the geometries are similar, the predictions of the ZINDO/S method using the ZINDO/1 optimized geometries, are better for the transition wavelengths in the visible region of the hydroxy substituted naphthoquinones, especially for 5HNQ and DHNQ.     

Catalytic Conversion of 2-Naphthol to 2-Hydroxy-1,4-naphthoquinone Under Mild Conditions

Introduction 2-Hydroxy-1,4-naphthoquinone (HNQ), existing in natural plants,1,2 is popularly separated and purified as dye or pigment. Recent research results show that, with the function to prevent the formation of protein coenzyme of HIV-I, HNQ can inhibit HIV virus from copying and propagating,3,4 HNQs derivatives and di-chloroallyl lawsone are also the inhibitor for RNA syn-thesis of cancer.5 It is well known that there is a rela-tionship between the side chain attached to HNQ an…     

Synthesis and molecular docking of some new bis-thiadiazoles as anti-hypertensive α-blocking agents

Abstract

Twelve bis-thiadiazole derivatives were synthesized in high yield via the reaction of 2,2′-terephthaloyl bis(N-phenylhydrazine carbothioamide) with a variety of hydrazonoyl chlorides in ethanol containing catalytic amounts of TEA. All the newly synthesized compounds were characterized by physical and chemical tools (FT-IR, ¹H NMR, ¹³C NMR, and Mass spectrometry). Moreover, all the novel synthesized derivatives were screened for their antihypertensive α-blocking efficacy against to assess their pharmaceutical significance. The encouraging promising results obtained from antihypertensive α-blocking activity studies on the newly synthesized derivatives make the synthesis of a new series of these compounds and studying of their pharmaceutical importance an active area for more and more investigations. The molecular docking of the most active derivative 15?b against the human dopamine D3 receptor was performed by the Molecular Operating Environment (MOE 2014. 0901) program.     

Flow-injection determination of indole derivatives in pharmaceutical mixtures

The reactions of tryptamine derivatives with 4-chloro-5,7-dinitrobenzofurazan were studied. The composition of the products of analytical reactions was found from the data of elemental analysis, and their structures were confirmed by ¹H NMR spectra. The working conditions were selected for the flow-injection determination of 22 indole derivatives in pharmaceutical mixtures as 5,7-dinitrobenzofurazans with spectrophotometric detection at 490 nm. Optimum results were obtained using acetonitrile-buffer solution (pH 6.8) flows. The analytical range for biologically active substances was between 0.04 and 0.61 μg/mL. The throughput was 25–35 sample/h. The detection limit was 0.01 μg/mL. Serotonin, mexamine, melatonine, sumatryptan, and indolylacetic acid derivatives were determined in pharmaceuticals and in reaction mixtures from the synthesis of biologically active substances.     

Quantum-chemical study of the effect of the association phenomenon on the active sites structure in butadiene polymerization reaction initiated by organolithium compounds

The electronic and geometric structures of monomeric and associated forms of crotyllithium (models for the active sites in the anionic polymerization of butadiene) have been calculated using a CNDO method. It appears that the cisoid configuration of the chain ends is energetically preferred for monomeric and dimeric forms of living macromolecules; in the case of tetramer, the transoid configuration is the more stable. The characteristics of C_α and C_γ atoms of substituted allylic groups undergo a certain bringing together when passing from monomer to dimer. The results are used for interpretation of the dependence of polybutadiene microstructure upon conditions during polymerization.     

Recent synthetic methodologies for pyridopyrazines: An update

Abstract

Among heterocyclic compounds, pyridopyrazines are the scaffolds that have gained considerable attention on academic and industrial level due to their widespread applications as intermediates in the preparation of advanced and biologically potent pharmaceutical materials. Many pyridopyrazine derivatives are available in market to cure various pharmacological disorders. These candidates can be synthesized via a number of synthetic routes using various reagents like cyclocondensation of diaminopyridines with carbonyl compounds or their derivatives etc. In the present review, we have elaborated all these protocols along with different factors and reaction conditions such as use of metal catalyst, solvent-free and microwave irradiation, one-pot synthesis etc. that have resulted in high regioselectivity and yields. The review focuses on the synthetic methodologies developed in the last decade for different pyridopyrazine derivatives.     

2-羟基-1,4-萘醌的合成及铁卟啉-氧催化中间体形成平衡常数的测定

铁卟啉催化剂;羟基萘醌;2-羟基-1;4-萘醌的合成及铁卟啉-氧催化中间体形成平衡常数的测定     

New Trimethoxybenzamides and Trimethoxyphenylureas Derived from Dimethylcarbazole as Cytotoxic Agents. Part I

A convenient synthesis of novel functionalized 1,4‐dimethylcarbazole derivatives containing 3,4,5‐trimethoxybenzamido‐ureido or N‐(3,4,5‐trimethoxyphenyl)ureido group starting from their corresponding indole derivatives is reported. Three derivatives prepared ( 5g , 6c , and 6g ) were active against leukemia cell lines HL60. Both 5g and 6g showed potent antiproliferative activity against KB cell lines, likely associated with the inhibition of tubulin polymerization.     

New Perspectives in Living/Controlled Anionic Polymerization

Summary: Control of the reactivity and selectivity of active species remains a major challenge in the course of living/controlled polymerizations of vinyl and heterocyclic monomers. We have found that alkyl metal derivatives such as dialkylmagnesium or trialkylaluminum derivatives or the corresponding alkoxyakyl metal derivatives, when added to conventional anionic polymerization systems, are very effective mediators for the controlled anionic polymerization of both styrenic and oxirane monomers. When used as additives to alkali metal alkyl initiators (alkyl lithium, alkyl sodium) for the styrene anionic polymerizations, they strongly retard the reactivity of the propagating species and allow controlling the polymerization in very unusual conditions (bulk, very high temperature). On the contrary, when used in combination to the same alkali metal based initiators for the anionic polymerization of ethylene oxide or propylene oxide, these additives can drastically enhance the reactivity and the selectivity of the propagating species allowing a fast living-like polymerization to proceed already at low temperature in hydrocarbon media.     

Polymers Containing Lactone Groups

Polymers containing intact lactone groups are a new class of macromolecules with reactive groups, which are relatively easy to obtain by polymerization, polycondensation and polyaddition, as well as by reactions on existing macromolecules. Polymers with β-lactone Groups in particular can enter into numerous addition reactions, which can be used, for example, to obtain macromolecules containing hydroxy acid or amino acid groupings. The reactions proceed under mild conditions, and can even be carried out in aqueous media, frequently giving water-soluble polymers. The polymers can be cross-linked at low temperatures, even from the aqueous phase, by the addition of bifunctional or oligofunctional reagents. Polymers containing β-lactone groups can also be used as a basis for graft co-polymers; polyester or polyether branches can be grafted on, depending on whether monomeric lactones or monomeric epoxides are used.     

Single-site anionic polymerization. Monomeric ester enolaluminate propagator synthesis, molecular structure, and polymerization mechanism

The synthesis and molecular structure of the first examples of monomeric lithium ester enolaluminates that serve as structural models for single-site anionic propagating centers, as well as the mechanism of their polymerization of methacrylates catalyzed by conjugate organoaluminum Lewis acids, are reported. Reactions of isopropyl alpha-lithioisobutyrate (2) with suitable deaggregating and stabilizing organoaluminum compounds such as MeAl(BHT)2 (BHT = 2,6-di-tert-butyl-4-methylphenolate) in hydrocarbons cleanly generate lithium ester enolaluminate complexes such as Li+[Me2C=C(OiPr)OAlMe(BHT)2]- (3). Remarkably, complex 3 is isolable and exists as a monomer in both solid and solution states. Unlike the uncontrolled polymerization of methacrylates by the aggregating enolate 2, the methacrylate polymerization by the monomeric 3 is controlled but exhibits low activity. However, the well controlled and highly active polymerization can be achieved by using the 3/MeAl(BHT)2 propagator/catalyst pair, which is conveniently generated by in situ mixing of 2 with 2 equiv of MeAl(BHT)2. The structure of the added organoaluminum compounds has marked effects on the degree of monomer activation, enolaluminate formation and reactivity, and polymerization control. Kinetics of the polymerization by the 3/MeAl(BHT)2 pair suggest a bimolecular, activated-monomer anionic polymerization mechanism via single-site ester enolaluminate propagating centers. The molecular structures of activated monomer 1, aggregated initiator 2, and monomeric propagator 3 have been determined by X-ray diffraction studies.     

Structure elucidation of benzopyran-2-ol in solution and in solid state following the reduction of coumarin by DIBAL-H

Lactols are compounds of increasing interest in the synthesis of active pharmaceutical derivatives. Nevertheless, the product obtained by the reduction of the carbonyl group of coumarin has been described only twice, and without definition of its precise chemical structure. Since these studies, doubts have been raised about the existence of a monomeric or dimeric form. Our study has led us to conclude definitely that the single dimeric form exists and to precisely define the spectral properties of the two diastereoisomers.     

Photoinitiated Free-Radical Polymerization of 4,5,6,7-Tetrahalogenated Fluoresceins

We demonstrated the photoredox catalytic performances of fluorescein derivatives, bearing heavy halogen atoms (Br or I) on a benzoic acid group, using photoinitiated free-radical polymerization. 4,5,6,7-Tetrabromofluorescein and 4,5,6,7-tetraiodofluorescein were used as visible-light-photoredox catalysts to initiate polymerization of poly(ethylene glycol) diacrylate and N-vinylpyrrolidone in the presence of triethanolamine under aerobic conditions. Their photocatalytic performances were evaluated by the hydrogelation of photopolymerization both on the surface of an agarose film and in a liquid solution. The polymerization degree increased considerably in the following order: tetraiodofluorescein<tetrabromofluorescein<fluorescein. This result was different from fluorescein derivatives containing the heavy halogen atoms on a xanthene core ring. Consequently, the location of the heavy halogen atoms was crucial in the photocatalytic performance of fluorescein derivatives.