Über Juliprosin,ein weiteres Alkaloid aus Prosopis julifloraA.DC. 180. Mitteilung über organische Naturstoffe

Juliprosine, a Further Alkaloid Isolated from Prosopis juliflora A .DC . By catalytic hydrogenation of the second base juliprosine ( 2 ) isolated from Prosopis juliflora (Leguminosae) the hexahydroderivative 5 was formed. The same product was obtained also by catalytic hydrogenation of juliprosopine ( 1 ) of known structure. The absolute configuration of 2 was deduced by comparison of [M]_D values of Prosopis alkaloids of known absolute configuration.     

Macrocyclische Spermidinalkaloide aus Pleurostylia africana LOES. 9. Mitteilung über Celastraceen-Inhaltsstoffe

Macrocyclic Spermidine Alcaloids from Pleurostylia africana LOES . The structure of pleurostyline, a new macrocyclic spermidine alkaloid from Pleurostylia africana (Celastraceae), has been elucidated mainly by ¹H- and ¹³C-NMR.-spectroscopy. Pleurostyline represents a new structure type in which spermidine is incorporated in a 13-membered lactam ring to which an additional cinnamoyl residue is fused to yield a 7-membered ring. The same plant contains also the spermidine alkaloids celacinnine and cellallocinnine of which ¹³C- and high field ¹H-NMR.-measurements have been carried out for the first time. Both alkaloids are interconvertible by UV.-irradiation. In addition the existence of rotational isomerism of one amide group of these alkaloids has been demonstrated by NMR.-spectroscopy.     

高效液相色谱化学发光法检测牛奶中残留四环素类化合物的研究

基于四环素类抗生素药物中的四环素(TC)、土霉素(OTC)、金霉素(CTC)和多西环素(DC)能够强烈增敏通过恒电流电解方法在线电生BrO^－和鲁米诺之间产生的化学发光, 提出了一种高效液相色谱(HPLC)化学发光(CL)法检测4种四环素类抗生素药物的新方法. 以Nucleosil RP-C₁₈ (250 mm×4.6 mm, i.d., 5 μm, pore size, 100 Å)为色谱柱, 0.05 mol• L^－1磷酸二氢钾(pH 2.5)-乙腈(30∶70, V∶V)为流动相, 流速1.2 mL/min, 柱温25 ℃, 同时分离检测四种抗生素的总时间为11 min. 研究并优化了流动相、电生试剂化学发光检测的条件. 四种抗生素的检出限为0.002～0.008 μg•mL^－1 (3σ), 对0.01 μg•mL^－1的四种抗生素测定的相对标准偏差为2.0%～3.6% (n＝11). 该方法已成功应用于牛奶中残留四环素类抗生素含量的分析.     

1,2‐, 1,7‐ and 1,12‐Dicarba‐closo‐dodecaborane(12) Derivatives Revisited by 13C NMR Spectroscopy and DFT Calculations. First Observation of Isotope‐Induced Chemical Shifts 1Δ10/11B(13C), and the Signs and Magnitudes of Coupling Constants 1J(13C,13C) and 1J(13C,11B)

The origin of broadening of ¹³C(carborane) NMR signals of 1,2‐, 1,7‐ and 1,12‐dicarba‐closo‐dodecaboranes(12) and several diphenylsilyl derivatives has been examined in detail and could be traced only partially to unresolved ¹³C–¹¹B spin‐spin coupling. Other contributions to the line widths arise from ¹³C–¹H dipole‐dipole interactions and, in particular, from isotope‐induced chemical shifts ¹Δ^10/11B(¹³C), observed here for carboranes for the first time. In the case of 1‐diphenylsilyl‐1,2‐dicarba‐closo‐dodecaborane(12), the coupling constant ¹J(¹³C,¹³C) = 9.3 Hz was measured in natural abundance of ¹³C. The small value of this coupling constant and its negative sign is predicted by calculations based on optimised structures [B3LYP/6‐311+G(d,p) level of theory] of the parent carboranes and 1‐silyl‐1,2‐dicarba‐closo‐dodecaborane(12) as a model compound [calcd. ¹J(¹³C,¹³C) = –10.5 Hz]. Calculated coupling constants ¹J(¹³C,¹¹B) are small (<7 Hz), in contrast to published assumptions, and of either sign, whereas ¹J(¹¹B,¹¹B) are all positive and range up to 15 Hz.     

Intramolecular phenylborane complexes with monobasic bidentate Schiff bases

A series of intramolecular complexes with Schiff base ligands having N∩S and N∩O donor systems were synthesized in an open vessel under microwave irradiation (MWI) using a domestic microwave oven. The reaction time has been brought down from hours to seconds with improved yield as compared with the conventional heating. The complexes have been characterized on the basis of elemental analysis, conductance measurements and spectroscopic analysis. Based on the IR, ¹H NMR, ¹¹B NMR and ¹³C NMR spectroscopic studies, a tetrahedral geometry has been proposed for the resulting complexes. The compounds have been screened in vitro against bacteria and fungi to test their antimicrobial property and in vivo in male albino rats to test their antifertility property. The testicular sperm density, motility and density of cauda epididymal spermatozoa along with biochemical parameters of reproductive organs have been examined and discussed. Copyright © 2007 John Wiley & Sons, Ltd.     

A 13C-NMR. Study of cis-trans isomeric vitamins A, carotenoids and related compounds.

The ¹H-decoupled ¹³C-NMR. spectra of 35 all-trans, 17 mono-cis vitamin A compounds (acetates, alcohols, aldehydes, acids and esters) and of one 11, 13-di-cis compound (11, 13-di-cis retinol) are reported. Included in this investigation are desmethyl-, desmethylethyl, and aryl-vitamin A analogues and others as well as 30 reference compounds of smaller molecular weight. Furthermore, the ¹³C-NMR. spectra of 23 β-apo- and other carotenoids were studied. A complete assignment of the signals of all 106 compounds to the specific carbon atoms was achieved by extensive application of lanthanide shift reagents, mainly Yb(dpm)₃, by CW-offset and selective ¹H-decoupling experiments, by comparison of the shifts of related compounds, and in three cases by utilization of specifically deuteriated compounds (11, 12-D₂-retinol and retinyl acetate, 15, 15′-D₂-β-carotene). The chemical shift differences between the cis- and trans-vitamin A compounds and the applicability of the shift reagents for the assignment of the ¹³C-NMR. spectra are discussed.     

1,2,3-thiadiazoles. I. Synthesis of sodium (or potassium) 1,2,3-thiadiazole-4-thiolates via thiocarbazonate esters and N-acylthiohydrazonate esters

A general synthesis of 1,2,3-thiadiazole-4-thiolates 1 and their derivatives 2–3 by an extension of the Hurd-Mori 1,2,3-thiadiazole synthesis is described. Treatment of methyl (or ethyl) [1-(alkylthio)alkylidene]hydrazinocarboxylates 11 (thiocarbazonate esters) or other N-acylthiohydrazonate esters [Y = ureido ( 12 ) or arenesulfonyl ( 13 )] with thionyl chloride affords 2–3 efficiently. Intermediates 11–13 are readily obtained from the N²-thioacylcarbazates 8 , N³-thioacylsemicarbazides 9 , or N²-thioacyl-N¹-(p-toluenesulfonyl)hydrazides 10 , respectively, by S-alkylation. Physicochemical properties of the 1,2,3-thiadiazoles 1–3 and N-acylthiohydrazonate esters 11–13 are also described.     

1H-NMR.-, 13C-NMR.-, UV.- und CD.-Daten von synthetischem (3S, 3′S)-Astaxanthin,seinem 15-cis-Isomeren und einigen analogen Verbindungen

¹H-NMR., ¹³C-NMR., UV. and CD. spectral data of synthetic (3S, 3′S)-astaxanthin, its 15-cis isomer, and some related compounds ¹H-NMR., ¹³C-NMR., UV. and CD. spectra are reported for synthetic (3S, 3′S)-astaxanthin ( 1 ), its 15-cis isomer ( 2 ), its diacetate ( 3 ), and the 15, 15′-didehydro compound ( 5 ). These data prove the identity of the synthetic and the naturally occuring compound 1 . A full interpretation of the ¹H- and ¹³C-NMR. spectra is given and confirms the configuration of all the double bonds. The conformation of the cyclohexene end group of all the compounds is shown to be identical. The signs of the different CD. maxima of 15-cis-astaxanthin are found to be opposite to those of the all-trans compound.     

Synthese von Humaninsulin. II. Aufbau des cyclischen Fragments A(1–13)

Synthesis of human insulin. II. Preparation of the A(1–13) fragment. The present report gives a detailed account of the synthesis of the protected tridecapeptide A(1–13), Boc? Gly? Ile? Val? Glu(OBu^t)? Gln Ser(Bu^t)? Leu? OH ( 20 ), an essential intermediate in the recently published total synthesis of human insulin [1]. The main feature in the synthesis of 20 was the specific formation of a disulfide bond between A6 and A11 in the presence of an additional cysteine residue (A7). The selective ring closure was accomplished with the segment A(6–13), H? Cys(Trt)? Cys(Acm)? Thr(Bu^t)? Ser(Bu^t)? Ile? Cys(Trt)? Ser(Bu^t)? Leu? OH ( 18 ), which was obtained by way of conventional synthesis routes. Treatment of 18 with iodine in trifluoroethanol formed the desired disulfide bridge from the two S-trityl-cysteine residues without affecting the S-acetamidomethyl-protected cysteine A7. A final azide coupling with the N-terminal derivative A(1–5) ( 3 ) provided the tridecapeptide fragment 20 as a crystalline compound.     

Borchelate und Bormetallchelate, 4. Mitt.

The i.r., u. v.,¹H n.m.r.,¹³C n.m.r., and¹¹B n.m.r. spectra of several substituted diphenylboron chelates derived from salicylaldehyde azomethines were compared with respect to the influence of the amine substituentR. O–B–N-6-ring constitution of the chelates29–32 [R=OH, NH₂, NHC₆H₅, N(CH₃)₂] can be deduced from the spectra.

Als 3. Mitt. gilt:F. Umland undE. Hohaus mit Beiträgen vonW. Riepe, K. Brodte, C. Schleyerbach undD. Szonn. Untersuchungen über borhaltige Ringsysteme vom Chelattyp. Forschungsbericht des Landes Nordrhein-Westfalen Nr. 2538. Opladen: Westdeutscher Verlag. 1976.     

Hydrogen‐bonding characteristics and unique ring‐opening polymerization behavior of Ortho‐methylol functional benzoxazine

Monofunctional benzoxazine with ortho‐methylol functionality has been synthesized and highly purified. The chemical structure of the synthesized monomer has been confirmed by ¹H and ¹³C nuclear magnetic resonance spectroscopy (NMR), Fourier transform infrared spectroscopy (FT‐IR) and elemental analysis. One‐dimensional (1D) ¹H NMR is used with respect to varied concentration of benzoxazines to study the specific nature of hydrogen bonding in both ortho‐methylol functional benzoxazine and its para counterpart. The polymerization behavior of benzoxazine monomer has been also studied by in situ FT‐IR and differential scanning calorimetry, experimentally supporting the polymerization mechanism of ortho‐methylol functional benzoxazine we proposed before. © 2016 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2016 , 54, 3635–3642     

Stereoselektive Hydrid-Reduktion von Tetronsäurederivaten. Synthese verzweigtkettiger Tetrofuranosen

Stereoselective Hydride Reduction of Tetronic Acid Derivatives, Synthesis of Branched-Chain Tetrofuranoses The 3-methoxymethyl derivatives of 2-methyl-D , L -threofuranose ( 10a ) and 2-deoxy-2-methyl-D ,L -erythrofuranose ( 11a ) are prepared starting from 2-methyl-tetronic acid ( 1 ). The key step is the stereoselective reduction of the 3-oxo-function of 2-chloro-2-methyl-3-oxo-γ-butyrolacton ( 2 ) by sodiumborohydride, which proceeds predominantly anti with respect to the C,Cl-bond. The configuration of the reduction products has been established by ¹H- and ¹³C-NMR.-spectroscopy.     

Cynaratriol,ein neues Guajanolid aus der Kardone Cynara cardunculusL. und der Artischocke C. scolymusL.(Compositate)

Cynaratriol, a new guajanolide from Cynara cardunculus L. and C. scolymus L. (Compositae) A new guajanolide given the name cynaratriol ( 4 ) was isolated from the leaves of Cynara cardunculus L The structure of 4 and its derivatives 3, 11, 13-triacetylcynaratriol ( 5 ) and 3, 13-dibenzoyl-cynaratriol ( 6 ) was deduced on the basis of IR.-, ¹H-NMR.-, ¹³C-NMR.- and mass spectroscopic data. 4 is also present in C. Scolymus L. as shown by GC./MS. analysis. The same absolute configuration is suggested for 4 as found for all other Cynara sesquiterpenes.     

Variable temperature multinuclear NMR. Investigation of dimethylformamide exchange on the octakis (N,N-dimethylformamide)-thulium(III) ion

The rate of DMF exchange on [Tm (DMF)₈]³⁺ has been determined by ¹H- and ¹³C-NMR. linebroadening techniques. ¹H-NMR. yields the following solvent exchange parameters; ΔH* = 33.2 (±0.5) kJ mol^?1, ΔS* = 9.9 (±2.4) J K^?1 mol^?1and k (200 K) = 2.94 (±0.09)× 10⁴ s^?1, whilst results from ¹³C-NMR. are similar. No evidence, by ³⁵C1-NMR., was found of contact ion-pair formation when the perchlorate salts were used.     

The Structure of the Antibiotic Hedamycin. I. Chemical,Physical and Spectral Properties

Interpretation of the chemical and spectral (IR., UV., ¹H- and ¹³C-NMR.) properties of the antitumor antibiotic hedamycin (C₄₁H₅₀N₂O₁₁) suggests that the molecule contains a methyl substituted 1-hydroxyanthraquinone nucleus, an α, β-unsaturated ketone, two sugar-like tetrahydropyran rings ( 4 and 8 ) and an aliphatic chain 2 , presumably with an epoxy group (see the Scheme).     

Cryptolepinone vs. Hydroxycryptolepine: Resolution of a question of substituent functionality and double bond isomerization

An indolo[3,2-b]quinoline alkaloid bearing an N-methyl substituent at N5, and an oxygen moiety at the 11-position has been variously described as both cryptolepinone and 11-hydroxycryptolepine by independent research groups. The structure of this alkaloid is unequivocally confirmed as the former, cryptolepinone, with substantial changes in double bond isomerization relative to that which would be required if it were indeed the latter. The structure of the alkaloid was confirmed by, total assignment of the ¹H, ¹³C, and ¹⁵N nmr spectra at natural abundance using 3 mm micro inverse nmr probe technology at 400 and 500 MHz.     

Diels-alder adducts of a spirocyclopentenotriazoloazodienophile. Assignment of their 1H and 13C NMR spectra

1-Phenyl-cyclopenteno[1,2-d]-1,2,3-rriazolo-5-spiro-4′-[perhydropyrazolino-3′,5′-dione] (5) afforded in situ, by oxidation with lead tetraacetate, the corresponding cyclopentenotriazolo-spiropyrazolodione 6 , which was trapped with dienes giving the hetero-Diels-Alder adducts 10–12 in good yields. The Diels-Alder reactions were examined on the basis of AM1 MO calculations. Total assignment of the ¹H- and ¹³C-nmr chemical shifts as well as the relative configuration of these adducts was accomplished with the help of 2D (¹H-¹H COSY, ¹H -¹ H NOESY, ¹H-¹³C XHCORR, ¹H-¹³C COLOC) and NOE difference spectroscopy. The structures of compounds 11a and 11b were also examined by molecular modeling.     

Impact of N-Truncated Aβ Peptides on Cu- and Cu(Aβ)-Generated ROS: CuI Matters!

In vitro Cu(Aβ_1–x)-induced ROS production has been extensively studied. Conversely, the ability of N-truncated isoforms of Aβ to alter the Cu-induced ROS production has been overlooked, even though they are main constituents of amyloid plaques found in the human brain. N-Truncated peptides at the positions 4 and 11 (Aβ_4–x and Aβ_11–x) contain an amino-terminal copper and nickel (ATCUN) binding motif (H₂N-Xxx-Zzz-His) that confer them different coordination sites and higher affinities for Cu^II compared to the Aβ_1–x peptide. It has further been proposed that the role of Aβ_4–x peptide is to quench Cu^II toxicity in the brain. However, the role of Cu^I coordination has not been investigated to date. In contrast to Cu^II, Cu^I coordination is expected to be the same for N-truncated and N-intact peptides. Herein, we report in-depth characterizations and ROS production studies of Cu (Cu^I and Cu^II) complexes of the Aβ_4–16 and Aβ_11–16 N-truncated peptides. Our findings show that the N-truncated peptides do produce ROS when Cu^I is present in the medium, albeit to a lesser extent than the unmodified counterpart. In addition, when used as competitor ligands (i.e., in the presence of Aβ_1–16), the N-truncated peptides are not able to fully preclude Cu(Aβ_1–16)-induced ROS production.     

Synthesis of methyl‐2,4‐bis(cyclohexane)dispiro‐1,2,3,4,4a,5,6,7‐octahydro‐(lH,3H)quinazoline‐8‐carbodithioate derived from cyclohexanone in one step

The new compound Methyl‐2,4‐bis(cyclohexane)dispiro‐1,2,3,4,4a,5,6,7‐octahydro‐(1H,3H)‐quinazo‐line‐8‐carbodithioate has been synthesized from cyclohexanone and carbon disulfide. It has been characterized by uv‐visible, FTTR , mass spectra and a complete structure proposed based on ¹H and ¹³C NMR spectroscopy.     

Some chemical and analytical aspects of polysaccharide modifications. II. A high-yielding,specific method for the chemical derivatization of galactose-containing polysaccharides: Oxidation with galactose oxidase followed by reductive amination

A versatile and high-yielding method was developed for specifically modifying galactose-containing polysaccharides, exemplified here by two representative galactomannans, guar gum 1 and locust bean gum 5 . Oxidation of the primary alcohol functions of 1 and 5 with galactose oxidase produced the corresponding aldehyde derivatives 2 and 6 which were subsequently derivatized in several ways. Reductive amination with sodium cyanoborohydride of 2 and 6 proceeded smoothly (60–90% yields) and led to stable amine derivatives ( 4 , 7–11 ), which included hydroxyalkylamine- ( 8 ), glycine- ( 9 ), and BSA- ( 11 ) derivatives. The cationic primary amine derivative 12 was similarly reductively alkylated with lactose to yield a product 13 with extended carbohydrate side chains. Oxidation of 2 produced the anionic carboxy derivative 14 , whereas reduction of 2 and 6 with sodium borodeuteride yielded the deuterium labeled neutral species 15 and 16 . The undegraded gums and some of their derivatives were studied by high resolution ¹³C-NMR (100.6 MHz) at 30°C, and the proposed chemical shift assignments were in good qualitative agreement with those of earlier studies. ESR spectroscopy was used to follow the chemical reactions and to derive information about the galactose distribution of 1 and 5 . Mean nearest neighbor distances (r?) between nitroxides attached to 1 and 5 were 1.36 nm (±5%) for 4 and 1.75 nm (±5%) for 7 . These r? values agree favorably with the structural models recently proposed elsewhere, excluding earlier suggestions of homogeneous galactose distributions or regularly alternating blocks of branched and unbranched mannose units. The solution properties, such as viscosity and salt- and organic solvent-compatibility, of some of the guar derivatives appear to be unique and interesting. An alternative oxidation procedure of the galactose residues of 1 and 5 with sodium periodate has been evaluated.