Synthesis and bioactivity of novel 3-(1-hydroxyethylidene)-5-substituted-pyrrolidine-2,4-dione derivatives

Ten novel 5-substituted derivatives of 3-(l-hydroxyethylidene)pyrrolidine-2,4-dione were synthesized.The compounds were confirmed by IR,:H NMR,MS and elemental analysis.The bioassay indicated that these compounds showed noticeable herbicidal activities,and compounds 6f and 6j exhibited excellent inhibitory activities against the stalk of Echinochloa crusgalli,with EC50 values of 94.4 and 72.7 mg/L,respectively.     

Ferrocenylethynyl derivatives of nucleoside triphosphates: synthesis, incorporation, electrochemistry, and bioanalytical applications

Modified dATP (2'-deoxyadenosine-5'-triphosphate) and dUTP (2'-deoxyuridine-5'-triphosphate) bearing ferrocene (Fc) labels linked via a conjugate acetylene spacer were prepared by single-step aqueous-phase cross-coupling reactions of 7-iodo-7-deaza-dATP or 5-iodo-dUTP with ethynylferrocene. The Fc-labeled dNTPs were good substrates for DNA polymerases and were efficiently incorporated to DNA by primer extension (PEX). Electrochemical analysis of the 2'-deoxyribonucleoside triphosphates (dNTPs) and PEX products revealed significant differences in redox potentials of the Fc label bound either to U or to 7-deazaA and between isolated dNTPs and conjugates incorporated to DNA. Prospective bioanalytical applications are outlined.     

Decomposition of zinc (1-hydroxyethylidene)diphosphonate induced by aliphatic amines and ammonia. Molecular structures of ammonium (1-hydroxyethylidene)diphosphonates

A suspension of sparingly soluble zinc (1-hydroxyethylidene)diphosphonate ZnH₂L?2H₂O (H₄L = MeC(OH)[P(O)(OH)₂]₂) is rapidly transformed into an aqueous solution when treated with ammonia or aliphatic amines (hexamethylenediamine, triethylamine, tert-butylamine, di-n-butylamine) containing no hydrophilic groups ?OH and ?(OCH₂CH₂)_n?. The dissolution effect is due to the decomposition of the coordination polymer giving ammonium derivatives. Dehydrated dry powders of the corresponding ammonium compounds based on triethylamine, tert-butylamine, or di-n-butylamine rapidly dissolve in water to form transparent colorless solutions, whereas hexamethylenediamine and ammonia derivatives are poorly soluble. (1-Hydroxyethylidene)diphosphonic acid forms ammonium salts with hexamethylenediamine, triethylamine, and tert-butylamine. The molecular structures of these compounds are considered.

     

Oligonucleotides and nucleotidylpeptides. XXXII. Synthesis and hydrolytic stability of amino acid derivatives of adenosine 5′-di(tri)phosphates

The synthesis has been effected of the ethyl esters of adenosine-5′-diphospho-(P_β→N)-and adenosine-5′-triphospho(P_γ→N)-alanine. It has been shown that under the conditions of synthesis the serine analogues of ATP and ADP decompose. An investigation of the hydrolytic stability of the compounds synthesized has shown that they are unstable in acid and alkaline media. In an acid medium the phosphoramide bond is cleaved more rapidly than the phosphoric anhydride bond (in the case of the ADP analogue), while in an alkaline medium the ester bond is saponified and the phosphoric anhydride bond is cleaved. The ATP analogue is more labile both in acid and in alkaline media.     

Alkylsulfanylphenyl derivatives of cytosine and 7-deazaadenine nucleosides, nucleotides and nucleoside triphosphates: synthesis, polymerase incorporation to DNA and electrochemical study

Aqueous Suzuki–Miyaura cross‐coupling reactions of halogenated nucleosides, nucleotides and nucleoside triphosphates derived from 5‐iodocytosine and 7‐iodo‐7‐deazaadenine with methyl‐, benzyl‐ and tritylsufanylphenylboronic acids gave the corresponding alkylsulfanylphenyl derivatives of nucleosides and nucleotides. The modified nucleoside triphosphates were incorporated into DNA by primer extension by using Vent(exo‐) polymerase. The electrochemical behaviour of the alkylsulfanylphenyl nucleosides indicated formation of compact layers on the electrode. Modified nucleotides and DNA with incorporated benzyl‐ or tritylsulfanylphenyl moieties produced signals in [Co(NH₃)₆]³⁺ ammonium buffer, attributed to the Brdi?ka catalytic response, depending on the negative potential applied. Repeated constant current chronopotentiometric scans in this medium showed increased Brdi?ka catalytic response, which suggests the deprotection of the alkylsulfanyl derivatives to free thiols under the conditions.     

Thermally initiated disproportionation of manganese(II) bis(1-hydroxyethylidene)diphosphonate. Formation and properties of the lepidoid structure of manganese(II) (1-hydroxyethylidene)diphosphonate-2-hydroxyethaneaminium whiskers. Agronomical efficiency of the manganese(II) complex with (1-hydroxyethylidene)diphosphonic acid

Russian Chemical Bulletin - The reaction of poorly soluble manganese(II) bis(1-hydroxyethylidene)diphosphonate tetrahydrate (Mn(H3L)2?4H2O) with 2-aminoethanol (H2NCH2CH2OH) in an aqueous...     

Thermal and hydrolytic decomposition of derivatives of N-(1-Piperidinoanthra-quinon-2-yl)oxaziridine

On being heated in toluene or treated with alcoholic alkalies, 3-phenyl- and 3-methyl-2-(1-piperidinoanthraquinon-2-yl) oxaziridines undergo both isomerization into 1-piperidino-2-acylaminoanthraquinones and also conversion into 8, 13-dioxo-1, 2, 3, 4, 8,13-hexahydropyridyl [1,2-a]-anthra [2,1-d]imidazole.     

Kinetic analysis of hydrolytic reaction of homo- and heterochiral adenylyl(3'-5')adenosine isomers: breaking homochirality reduces hydrolytic stability of RNA

The hydrolytic stability of the diastereomeric isomers of ApA was compared and the results show that heterochiral ApAs are more rapidly hydrolyzed than homochiral ApAs at low temperatures, suggesting that hydrolytic selection in cold environments in conjunction with selective polymerization may have been effective in enriching the homochirality of RNA.     

Synthesis, characterization and hydrolytic stability of poly (amic acid) ammonium salt

A series of new poly (amic acid) ammonium salt (PAAS) precursors were prepared by incorporating different amounts of triethylamine (TEA) into terpolymer polyamic acid (PAA), which was synthesized by pyromellitic dianhydride (PMDA), 4,4’-oxydianiline (ODA) and p-phenylenediamine (PDA) in dimethylacetamide (DMAc). Then, the PAAS films were made by casting their solutions onto glass plates followed by the evaporation of the solvent. The chemical structure of PAAS films was confirmed by ¹H NMR and FTIR spectroscopy. Mechanical properties, intrinsic viscosities and solubility of PAAS precursors were examined, respectively. It was found that the intrinsic viscosity of PAA solution obviously decreased with storage time during 30 days, while no distinct changes were observed in the intrinsic viscosity of the PAAS (the mole ratio of TEA/repeating unit of PAA = 2/1) solution after 90 days. The results suggested that hydrolytic stability of the PAAS films was significantly improved as compared with that of PAA film due to the polyelectrolyte structure of PAAS. Moreover, the thermal and mechanical properties of polyimide (PI) films prepared from PAAS precursors were also investigated, respectively.     

Reactions of diiron(III) tris[(1-hydroxyethylidene)diphosphonate] tetrahydrate and iron(III) tris[(1-hydroxyethylidene)diphosphonate] tetrahydrate with <Emphasis Type="Italic">p</Emphasis>-aminobenzoic acid. Molecular structure of bis(4-carboxyphenylaminium) (1-hydroxyethylidene)diphosphonate

Diiron(III) tris[(1-hydroxyethylidene)diphosphonate] tetrahydrate and iron(III) tris[(1-hydroxyethylidene) diphosphonate] tetrahydrate react with p-aminobenzoic acid in water to form diiron(III) pentakis(4-carboxyphenylaminium) tris(1-hydroxyethylidene)diphosphonate dihydrate and iron(III) hexakis(4-carboxyphenylaminium) tris(1-hydroxyethylidene)diphosphonate dihydrate. The crystal structure of bis(4-carboxyphenylaminium) (1-hydroxyethylidene)diphosphonate obtained by the reaction of (1-hydroxyethylidene)diphosphonic acid with p-aminobenzoic acid in methanol was established.     

N1-(2-furoylmethyl) and N1-(5-nitro-2- furoylmethyl) derivatives of uracil and its 5-substituted derivatives

The corresponding N₁-(2-furoylmethyl) and N₁-(5-nitro-2-furoylmethyl) derivatives of uracil and its 5-substituted derivatives were obtained by the reaction of 2-bromo- and 5-nitro-2-bromoacetylfurans with uracil, 5-fluorouracil, and thymine. The structures of these compounds as N₁-substituted uracils were proved by a study of the UV spectra at various pH values. The computational method of expanding the UV spectra into individual bands was used.Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 9, pp. 1268–1270, September, 1971.     

Hydroxy-1-aminoindans and derivatives: preparation, stability, and reactivity

The chemical stability and reactivity of hydroxy-1-aminoindans and their N-propargyl derivatives are strongly affected by the position of the OH group and its orientation relative to that of the amino moiety. Thus, the 4- and 6-OH regioisomers were found to be stable, while the 5-OH analogues were found to be inherently unstable as the free bases. The latter, having a para orientation between the OH and the amino moieties, could be isolated only as their hydrochloride salts. 7-Hydroxy-1-aminoindans and 7-hydroxy-1-propargylaminoindans represent an intermediate case; while sufficiently stable even as free bases, they exhibit, under certain experimental conditions, unexpected reactivity. The instability of the 5- and 7-hydroxy-aminoindans is attributed to their facile conversion to the corresponding, reactive quinone methide (QM) intermediates. The o-QM obtained from 7-hydroxy-aminoindans was successfully trapped with ethyl vinyl ether via a Diels-Alder reaction to give tricyclic acetals 32a,b.     

Structure and stability of oxygen adsorption on Si(n) (n = 5-10) clusters

The structures, binding energies, and electronic properties of one oxygen atom (O) and two oxygen atoms (2O) adsorption on silicon clusters Si(n) with n ranging from 5 to 10 are studied systematically by ab initio calculations. Twelve stable structures are obtained, two of which are in agreement with those reported in previous literature and the others are new structures that have not been proposed before. Further investigations on the fragmentations of Si(n)O and Si(n)O2 (n = 5-10) clusters indicate that the pathways Si(n)O --> Si(n-1) + SiO and Si(n)O2 --> Si(n-2) + Si2O2 are most favorable from thermodynamic viewpoint. Among the studied silicon oxide clusters, Si8O, Si9O, Si5O2 and Si8O2 correspond to large adsorption energies of silicon clusters with respect to O or 2O, while Si8O, with the smallest dissociation energy, has a tendency to separate into Si7 + SiO. Using the recently developed quasi-atomic minimal-basis-orbital method, we have also calculated the unsaturated valences of the neutral Si(n) clusters. Our calculation results show that the Si atoms which have the largest unsaturated valences are more attractive to O atom. Placing O atom right around the Si atoms with the largest unsaturated valences usually leads to stable structures of the silicon oxide clusters.     

(212)Pb@C(60) and its water-soluble derivatives: synthesis, stability, and suitability for radioimmunotherapy

Fullerenes could potentially play a valuable role in radioimmunotherapy by more stably encapsulating radionuclides, especially where conventional chelation chemistry is inadequate due to the physical and/or chemical properties of the radionuclide. One of the therapeutically useful radionuclides that requires improved containment in vivo is 212Pb (tau1/2 = 10.6 h), the beta-emitting parent to alpha-emitting 212Bi (tau1/2 = 60.6 min). Myelotoxicity resulting from the accumulation of 212Pb in the bone marrow has limited the use of this radionuclide despite its favorable decay characteristics. In this work, 212Pb@C60 and its malonic ester derivatives were prepared for the first time by allowing the 212Pb to recoil into C60 following alpha-decay from its parent, 0.15-s 216Po, generated in situ from the decay of 224Ra (tau1/2 = 15 days). Repeated washing of the organic phase containing the 212Pb@C60 malonic esters with challenge solutions containing cold Pb2+ ions demonstrated that some of the 212Pb could not be exchanged and was apparently inside of the fullerenes. Malonic esters of endohedral alpha-emitting 213Bi (tau1/2 = 45 min) fullerenes were prepared by an analogous procedure. Following acidification of the esters, a preliminary biodistribution study in mice was performed with the untargeted water-soluble radiofullerenes. It was found that 212Pb did not accumulate in bone after being administered as an endohedral fullerene, in contrast to results with polyhydroxylated radiofullerenes and conventional polyaminocarboxylate chelators for 212Pb. The results indicate that 212Pb is held more tightly in the fullerene than in other methods and suggest that fullerenes may have an important role in the targeted delivery of 212Pb.     

Halogen derivatives of 5-(1′ketoacenaphthylidene)thiazolidine

Acenaphthenequinone and its derivatives readily condense with 3-phenyl-, 3-p-tolyl-, 3-(4-methoxyphenyl)-, 3-(2-methoxyphenyl)-, 3-(4-ethoxyphenyl)rhodanines. The UV absorption spectra of these compounds in dioxane lie in the range 363–390 mμ. Replacement of oxygen by sulfur at position 2 in the thiazolidine ring gives rise to a 14 to 41 mμ bathochromic shift.     

Simultaneous LC-MS-MS Analysis of Capecitabine and its Metabolites (5′-deoxy-5-fluorocytidine, 5′-deoxy-5-fluorouridine, 5-fluorouracil) After Off-Line SPE from Human Plasma

A new single extraction procedure was developed to isolate capecitabine and its major metabolites (5′-deoxy-5-fluorocytidine, 5′-deoxy-5-fluorouridine, and 5-fluorouracil) from human plasma. The simultaneous extraction of the four analytes was performed on an Atoll XWP solid phase support. Separation and detection were by liquid chromatography (5 µm Atlantis C₁₈, 150 × 2.1 mm) and Turbospray Mass spectrometry in negative mode. To our knowledge, this report is the first to use these conditions for the simultaneous analysis of capecitabine and its metabolites.     

5-Isoquinolinesulfonamide derivatives. III. Synthesis and vasodilatory activity of 1-(5-isoquinoline-sulfonyl)piperazine derivatives.

On the basis of a hypothesis that cyclization and alkylation of the diamine part in formula 1 may give highly active compounds, a new series of 5-isoquinolinesulfonamide derivatives, shown as formula 2, were prepared from cyclic diamines. Their vasodilatory effects were subsequently evaluated in vivo according to the increase in arterial blood flow after the formulas were injected locally to the femoral and/or vertebral arteries of dogs. Cyclization of the diamine structure in formula 1 gave very potent vasodilators: 6 and 14. Acylation and sulfonylation of terminal amino nitrogen afforded much less potent compounds. In contrast to the hypothesis, alkylation on the ring carbon and the terminal nitrogen of the cyclic amine afforded less active compounds except for compound 11. The most active compounds, 6, 11 and 14, showed more potent vasodilatory effects and more selective activity to the vertebral artery than either trapidil or diltiazem.     

Synthesis and stereochemical stability of new atropisomeric 1-(substituted phenyl)pyrrole derivatives

Addition of organometallic reagents to optically active methyl 1-(2-methoxycarbonyl-6-trifluoromethylphenyl)pyrrole-2-carboxylate provided the corresponding tetrasubstituted diols and/or pyrrolo[1,2-a]benzoxazepines as pure enantiomers or racemates depending on the organometallic reagents used. Rotational energy barriers around the interconnecting C-N bonds were estimated by molecular modeling calculations and NMR measurements with the aim of clarifying the stereochemical stability order of the new atropisomeric compounds. NMR methods for the determination of the enantiomeric purity of the new compounds are proposed.     

Novel bicyclic nucleoside analogue (1S,5S,6S)-6- hydroxy-5-hydroxymethyl-1-(uracil-1-yl)-3,8-dioxabicyclo[3.2.1]octane: synthesis and incorporation into oligodeoxynucleotides

The novel bicyclic nucleoside (1S,5S,6S)-6-hydroxy-5-hydroxymethyl-1-(uracil-1-yl)-3,8-dioxabicyclo[3.2.1]octane [2'-deoxy-1'-C,4'-C-(2-oxapropano)uridine] (15), expected to be restricted into an O4'-endo furanose conformation, was synthesized from the known 1-(3'-deoxy-beta-D-psicofuranosyl)uracil 5. The phosphoramidite derivative of 15 was successfully incorporated into oligodeoxynucleotides using standard methods, and thermal denaturation studies showed moderate decreases in duplex stabilities of -2.1 and -1.5 degrees C per modification toward complementary DNA and RNA, respectively.