The revised structure, total synthesis, and absolute configuration of streptophenazine A

A total synthesis of both diastereomers of the originally proposed structure for streptophenazine A (1) has been achieved. However, both synthetic compounds are different from the natural product. Re-examination of NMR data reported for streptophenazine A and a concise total synthesis of both diastereomers of 17 (17a and 17b) led to the structural revision of streptophenazine A to 17b. Asymmetric synthesis of (-)-streptophenazine A was also conducted, and its absolute configuration was determined to be 1'S,2'R.     

Oxo- and oxoperoxo-molybdenum(VI) complexes with aryl hydroxamates: synthesis, structure, and catalytic uses in highly efficient, selective, and ecologically benign peroxidic epoxidation of olefins

A solution obtained by dissolving MoO3 in H2O2 reacts separately with secondary hydroxamic acids (viz., N-benzoyl N-phenyl hydroxamic acid (BPHAH), N-benzoyl N-ortho-, -meta-, -para-tolyl hydroxamic acids, (BOTHAH, BMTHAH, and BPTHAH, respectively), and N-cinnamoyl N-phenyl hydroxamic acid (CPHAH) affording [MoO(O2)(BPHA)2] (1), [MoO(O2)(BOTHA)2] (2), [MoO(O2)(BMTHA)2] (3), [MoO(O2)(BPTHA)2] (4), and [Mo(O)2(CPHA)2](5), respectively. The O and O2 are situated cis to each other in 2-4, but in each case, they are disordered and distributed over four sites. This disorder does not exist in the 6-coordinate cis dioxo complex 5, to which crude MoO(O2)(CPHA)2 (5') was converted during recrystallization. An aqueous molybdate solution readily reacts with all those hydroxamic acids producing [Mo(O)2(hydroxamate)2] (6). While 2, 3, and 4 possess a very distorted pentagonal bipyramidal structure, 5 has a distorted octahedral geometry. In the solid state, as well as in solution, 5 exists as two apparently enantiomerically related molecules differing in the orientation of the pendant phenyl rings. To emphasize that the formation and structural uniqueness of 5 compared to 1-4 is caused by the influence of the cinnamoyl residue, one compound of the 6 series, namely, [Mo(O)2(BPHA)2] (6A), was structurally characterized to prove directly that the special stereochemical properties of 5 rely on the special electronic structure of CPHA- ligand. Complexes 1-5, as well as 6, show high potential and selectivity as catalysts in the epoxidation of olefins at room temperature in the presence of NaHCO3 as a promoter and H2O2 as a terminal oxidant. A comparative epoxidation study has been performed to determine the relative efficiency of the catalysts. To make the epoxidation method cost effective, a study to optimize the use of H2O2 has also been performed. To obtain evidence in favor of our suggested mechanism to this homogeneous olefin --> epoxide conversion, it was necessary to synthesize a peroxo-rich compound, namely, [MoO(O2)2BMTHA]- (7), but the attempted synthesis culminated in the isolation of [MoO(O2)2(C6H5COO)]- (8), obviously, via the hydrolysis of coordinated BMTHA.     

N‐[(Diphenoxyphosphoryl)oxy]‐2‐phenyl‐1H‐benzimidazole as a versatile reagent for synthesis O‐alkylhydroxamic acids

Highly efficient reagent, N‐[(diphenoxyphosphoryl)oxy]‐2‐phenyl‐1H‐benzimidazole was synthesized and its applicability was demonstrated for the synthesis of O‐alkyl hydroxamic acids. The efficiency of the reagent was evaluated through the synthesis of range of O‐alkyl hydroxamic acids from aromatic carboxylic acids as well as N‐protected amino acids. The enatiomeric purity of synthesized compounds was measured using chiral HPLC and the degree of racemization that occurred was found to be negligible.     

O-(α-D-Glucopyranosyl)trichloroacetimidate as a Glucosyl Donor

Model reactions of 0-(α-D-glucopyranosyl)trichloroacetimidate 2α with methanol and choTesterol under various conditions demon-strated that stereocontrolled glucosyl transfer with inversion of configuration at the anomeric center is best carried out in di-chloromethane at low temperatures with boron trifluoride-ether as a catalyst. Under these conditions β-glucoside 4β and β-disaccha-rides 5β- 9β were obtained in good to excellent yields.

With Brtosnsted acids, fast glucosyl transfer to the acid anion was mainly observed and required no further acidic catalysis. With strong acids formation of the thermodynamically more stable product dominated. However, with the weaker carboxylic acids highly diastereoselective inversion of configuration at the anomeric center led, for instance, to β-1-O-acyl derivatives 11β - 18β, revealing a convenient method for the synthesis of O-glycosyl-carb-oxylates. This method was also applied to resolution of racemic carboxylic acids.

Similar results were obtained with N-nucleophiles. Hydrazoic acid gave exclusively α-azide 19a. Nitrogen heterocycles gave with boron trifluoride-ether catalysis mainly β-nucleosides 20β - 23β. Reaction of trichloroacetimidate 2α with O-nucleophiles in aceto-nitrile as solvent led to different products due to competition     

Synthesis,Characterization and in vitro Antitumour Activity of the Di—n—butyltin（IV） Complexes of Some Arylhydroxamates

Fourteen new di-n-butyltin(IV)complexes of hydroxamic acids of the formula Bu2SnL2(HL-hydroxamic acids)were synthesized by the reaction of Bu2SnO and hydroxamic acids in dry toluene and ethanol media.The compounds were characterized by elemental analyses,molecular weight,IR and 1H NMR spectoscopy.The results indicate that n-Bu2SnL2 have distorted trans-octahedral structure.The antitumor activity in vitro against human A-549 tumor cells and P388 leukemia was presented,and their structure-activity relationship was discussed.     

Total synthesis, revised structure, and biological evaluation of biyouyanagin A and analogues thereof

Isolated from Hypericum species H. chinese L. var. salicifolium, biyouyanagin A was assigned structure 1a or 1b on the basis of NMR spectroscopic analysis. This novel natural product exhibited significant anti-HIV properties and inhibition of lipopolysaccharide-induced cytokine production. Described herein are the total syntheses of biyouyanagin A and several analogues (3-11), structural revision of biyouyanagin A to 2b, and the biological properties of all synthesized compounds. The total synthesis proceeded through cascade sequences that efficiently produced enantiomerically pure key building blocks 15b (ent-zingiberene) and 18 (hyperolactone C) and featured a novel [2 + 2] photoinduced cycloaddition reaction which occurred with complete regio- and stereoselectivity. Biological investigations with the synthesized biyouyangagins A (2-11) and hyperolactones C (12-16) revealed that the activity of biyouyanagin A most likely resides in its hyperolactone C structural domain.     

九子参苷A的结构

从石竹科植物九子参(Silene rubicunda Franch.)根中得到一个糖链上带双乙酰基的新三萜八糖苷──九子参苷A(rubicunoside A, 1)。以化学降解反应、酶解和波谱分析, 得到15个衍生物, 其结构最后确定为皂树酸-3-O-β-D-吡喃半乳糖-(1→2)-[β-D-吡喃木糖-(1→3)]-β-D-吡喃葡萄糖醛酸-28-O-β-D-吡喃木糖-(1→3)-β-D-吡喃木糖-(1→4)-α-L-吡喃鼠李糖-(1→4)-[2'-O-乙酰基-β-D-吡喃鸡纳糖-(1→2)]-[3'-O-乙酰基]-β-D-吡喃夫糖苷{3-O-β-D-galactopyranosyl-(1→2)-[→β-D-xylopyranosyl-(1→3)]-β-D-glucuronopyranosyl quillaic acid 28-O-β-D-xylopyranosyl-(1→3)-β-D-xylopyranosyl-(1→4)-α-L-rhamnopyranosyl-(→4)-[2'-OAc-→β-D-quinovopyranosyl-(1→2)]-[3'-OAc]-β-D-fucopyranoside, 1}。同时发现甘草酸酶的两个新酶解特性。。     

Monohydroxamic acids and bridging dihydroxamic acids as chelators to ruthenium(III) and as nitric oxide donors: syntheses, speciation studies and nitric oxide releasing investigations

The synthesis and spectroscopic characterisation of novel mononuclear Ru(III)(edta)(hydroxamato) complexes of general formula [Ru(H2edta)(monoha)] (where monoha = 3- or 4-NH2, 2-, 3- or 4-C1 and 3-Me-phenylhydroxamato), as well as the first example of a Ru(III)-N-aryl aromatic hydroxamate, [Ru(H2edta)(N-Me-bha)].H2O (N-Me-bha = N-methylbenzohydroxamato) are reported. Three dinuclear Ru(III) complexes with bridging dihydroxamato ligands of general formula [{Ru(H2edta)}2(mu-diha)] where diha = 2,6-pyridinedihydroxamato and 1,3- or 1,4-benzodihydroxamato, the first of their kind with Ru(III), are also described. The speciation of all of these systems (with the exception of the Ru-1,4-benzodihydroxamic acid and Ru-N-methylbenzohydroxamic systems) in aqueous solution was investigated. We previously proposed that nitrosyl abstraction from hydroxamic acids by Ru(III) involves initial formation of Ru(III)-hydroxamates. Yet, until now, no data on the rate of nitric oxide (NO) release from hydroxamic acids has been published. We now describe a UV-VIS spectroscopic study, where we monitored the decrease in the ligand-to-metal charge-transfer band of a series of Ru(III)-monohydroxamates with time, with a view to gaining an insight into the NO-releasing properties of hydroxamic acids.     

Reaction of Azalactone with Hydroxylamine Synthesis of β -Aminophenylalanine

Treatment of azlactones^1–5 with hydroxylamine under different experimental conditions yields hydroxamic acids (2), disubstituted hydroxamic acids (3), β -hydroxylamino-hydroxamic acids (10) and several other compounds. The acid (10a) upon Catalytic hydrogenation gives M-benzoylamino-β aminophenylalanine amide (15) which gave β -aminophenylalanine (16) on hydrolysis.     

Synthesis，Crystal and Molecular Structure of 1，1＇－Bis（N－phenylhydroxyaminocarbonyl）ferrocene

Ｓｙｎｔｈｅｓｉｓ，ＣｒｙｓｔａｌａｎｄＭｏｌｅｃｕｌａｒＳｔｒｕｃｔｕｒｅｏｆ１，１＇－Ｂｉｓ（Ｎ－ｐｈｅｎｙｌｈｙｄｒｏｘｙａｍｉｎｏｃａｒｂｏｎｙｌ）ｆｅｒｒｏｃｅｎｅ￥ＺｈａｎｇＷｅｎ；ＬｉＦｅｎｇ－Ｚｅ；ＬｉｕＱｉ－Ｗａｎｇ（Ｄｅｐａｒｔｍ...     

Amyloid–β peptides time-dependent structural modifications: AFM and voltammetric characterization

The human amyloid beta (Aβ) peptides, Aβ_1-40 and Aβ_1-42, structural modifications, from soluble monomers to fully formed fibrils through intermediate structures, were investigated, and the results were compared with those obtained for the inverse Aβ_40-1 and Aβ_42-1, mutant Aβ_1-40Phe¹⁰ and Aβ_1-40Nle³⁵, and rat Aβ_1-40Rat peptide sequences. The aggregation was followed at a slow rate, in chloride free media and room temperature, and revealed to be a sequence-structure process, dependent on the physicochemical properties of each Aβ peptide isoforms, and occurring at different rates and by different pathways. The fibrilization process was investigated by atomic force microscopy (AFM), via changes in the adsorption morphology from: (i) initially random coiled structures of ∼0.6 nm height, corresponding to the Aβ peptide monomers in random coil or in α-helix conformations, to (ii) aggregates and protofibrils of 1.5–6.0 nm height and (iii) two types of fibrils, corresponding to the Aβ peptide in a β-sheet configuration. The reactivity of the carbon electrode surface was considered. The hydrophobic surface induced rapid changes of the Aβ peptide conformations, and differences between the adsorbed fibrils, formed at the carbon surface (beaded, thin, <2.0 nm height) or in solution (long, smooth, thick, >2.0 nm height), were detected. Differential pulse voltammetry showed that, according to their primary structure, the Aβ peptides undergo oxidation in one or two steps, the first step corresponding to the tyrosine amino acids oxidation, and the second one to the histidine and methionine amino acids oxidation. The fibrilization process was electrochemically detected via the decrease of the Aβ peptide oxidation peak currents that occurred in a time dependent manner.     

游离氨基酸对Аβ多肽异常聚集作用的影响

阿尔兹海默氏病的主要病因之一,是病人大脑的海马区和皮质区中Аβ多肽异常聚集形成了老年脑斑.本工作通过质谱方法研究游离氨基酸存在下铜离子和Аβ多肽的相互作用,发现由于其侧链极性和强配位能力,天冬氨酸、谷氨酸、亮氨酸、酪氨酸、苏氨酸和组氨酸6种氨基酸能够在较低浓度下明显抑制铜离子和Аβ多肽的结合,由此推测游离氨基酸可能是一种新的与Аβ多肽异常聚集相关的微环境因素.     

7α-甲基-19-羟基-睾丸素-17β-乙酸酯用节杆菌芳构化: 7α-甲基-雌甾酚醇-17β-乙酸酯和7α-甲基-雌甾酚酮的合成

雌甾酚酮(la)和雌甾酚醇(lb)是治疗妇科病的要药。其17位的乙炔衍生物乙炔雌二醇(lc)及其3-甲醚化合物ld是甾体口服避孕药的组分。7α-甲基-雌甾酚酮(le)的生理活性比la大2～3倍,7α-甲基-乙炔雌二醇(lf)的生理活性比lb大20倍。文献报道le或7α-甲基-雌甾酚醇(lg)是由7α-甲基-△~(1,4)-3-酮或7α-甲基-△~4,6-3-酮及其相应的19-失碳甾体化合物经高温或经酸重排等方法制得;也有用节杆菌转化7α-甲基-19-失碳睾丸素而制得。所有这些合成方法不仅步骤多,而且得率往往不佳。本文报道     

(E)-5-styryl-1H-indole and (E)-6-styrylquinoline derivatives serve as probes for β-amyloid plaques

We report the synthesis and biological evaluation of novel (E)-5-styryl-1H-indole and (E)-6-styrylquinoline derivatives as probes for imaging β-amyloid (Aβ) plaques. These derivatives showed binding affinities for Aβ???? aggregates with K(i) values varying from 4.1 to 288.4 nM. (E)-5-(4-iodostyryl)-1H-indole (8) clearly stained Aβ plaques in the brain sections of Alzheimer's disease (AD) model mice (APP/PS1). Furthermore, autoradiography for [12?I]8 displayed intense and specific labeling of Aβ plaques in the brain sections mentioned above with low background. In biodistribution experiments using normal mice [12?I]8 showed high initial brain uptake followed by rapid washout (4.27 and 0.64% ID/g at 2 and 30 min post injection, respectively). These findings suggests that [123I]8 may be a potential SPECT imaging agent for detecting Aβ plaques in AD brain.     

A New Method for the Microdetermination of Molybdenum (VI) in Steel,Biological Materials and Waters

Abstract

A method is presented for the trace analysis of molybdenum (VI) in standard steel sample, plant tissues, animal tissues, and natural waters. The method is based on the extractive separation of molybdenum from complex matrices by chelating it with a new reagent N-p-methoxypheny1-2-furylacrylohydroxamic acid (MFHA) into isoamyl alcohol followed by spectrophotometric determination, Eight other new hydroxamic acids were studied for the same purpose and MFHA was chosen as it was the most sensitive of these as well as the other hydroxamic acids reported previously, The method enables rapid and reliable analysis of molybdenum at ppb lelvels in environmental matrices.     

Engineering encodable lanthanide-binding tags into loop regions of proteins

Lanthanide-binding tags (LBTs) are valuable tools for investigation of protein structure, function, and dynamics by NMR spectroscopy, X-ray crystallography, and luminescence studies. We have inserted LBTs into three different loop positions (denoted L, R, and S) of the model protein interleukin-1β (IL1β) and varied the length of the spacer between the LBT and the protein (denoted 1?3). Luminescence studies demonstrate that all nine constructs bind Tb3+ tightly in the low nanomolar range. No significant change in the fusion protein occurs from insertion of the LBT, as shown by two X-ray crystallographic structures of the IL1β-S1 and IL1β-L3 constructs and for the remaining constructs by comparing the 1H?15N heteronuclear single-quantum coherence NMR spectra with that of the wild-type IL1β. Additionally, binding of LBT-loop IL1β proteins to their native binding partner in vitro remains unaltered. X-ray crystallographic phasing was successful using only the signal from the bound lanthanide. Large residual dipolar couplings (RDCs) could be determined by NMR spectroscopy for all LBT-loop constructs and revealed that the LBT-2 series were rigidly incorporated into the interleukin-1β structure. The paramagnetic NMR spectra of loop-LBT mutant IL1β-R2 were assigned and the Δχ tensor components were calculated on the basis of RDCs and pseudocontact shifts. A structural model of the IL1β-R2 construct was calculated using the paramagnetic restraints. The current data provide support that encodable LBTs serve as versatile biophysical tags when inserted into loop regions of proteins of known structure or predicted via homology modeling.     

Heterodivalent Linked Macrocyclic β-Sheets with Enhanced Activity against Aβ Aggregation: Two Sites Are Better Than One

This paper reports a series of heterodivalent linked macrocyclic β-sheets 6 that are not only far more active against amyloid-β (Aβ) aggregation than their monovalent components 1a and 1b but also are dramatically more active than their homodivalent counterparts 4 and 5. The macrocyclic β-sheet components 1a and 1b comprise pentapeptides derived from the N- and C-terminal regions of Aβ and molecular template and turn units that enforce a β-sheet structure and block aggregation. Thioflavin T fluorescence assays show that heterodivalent linked macrocyclic β-sheets 6 delay Aβ(1-40) aggregation 6-8-fold at equimolar concentrations and substantially delay aggregation at substoichiometric concentrations, while homodivalent linked macrocyclic β-sheets 4 and 5 and monovalent macrocyclic β-sheets 1a and 1b only exhibit more modest effects at equimolar or greater concentrations. A model to explain these observations is proposed, in which the inhibitors bind to and stabilize the early β-structured Aβ oligomers and thus delay aggregation. In this model, heterodivalent linked macrocyclic β-sheets 6 bind to the β-structured oligomers more strongly, because N-terminal-derived component 1a can bind to the N-terminal-based core of the β-structured oligomers, while the C-terminal-derived component 1b can achieve additional interactions with the C-terminal region of Aβ. The enhanced activity of the heterodivalent compounds suggests that polyvalent inhibitors that can target multiple regions of amyloidogenic peptides and proteins are better than those that only target a single region.     

Synthesis of a d,d- and l,d-heptose-containing hexasaccharide corresponding to a structure from Haemophilus ducreyi lipopolysaccharides

The synthesis of a linear hexasaccharide, 2-(4-trifluoroacetamidophenyl)ethyl (β-d-galactopyranosyl)-(1→4)-(2-acetamido-2-deoxy-β-d-glucopyranosyl)-(1→3)-(β-d-galactopyranosyl)-(1→4)-(d-glycero-α-d-manno-heptopyranosyl)-(1→6)-(β-d-glucopyranosyl)-(1→4)-l-glycero-α-d-manno-heptopyranoside, corresponding to a structure found in Haemophilus ducreyi LPS, is described. A Barbier reaction between benzyloxymethyl chloride and a properly protected 6-aldo-1-thio-mannopyranoside yielded both the d,d- and the l,d-heptopyranoside (2 and 3, ratio 2:3), which were separated and both used in the synthesis. p-Methoxybenzyl and chloroacetyl groups were employed as temporary protecting groups, selectively removed in the presence of the persistent benzyl, acetyl, benzoyl and isopropylidene groups by treatment with DDQ/H₂O and hydrazine dithiocarbonate, respectively. Thioglycosides were utilised as donors throughout using either NIS/TfOH or DMTST as promoters. The introduction of the spacer into thioglycoside 5 was high-yielding (95%) but with low stereoselectivity (α:β 5:3). All other glycosylations are completely stereoselective. The target hexasaccharide is obtained via a 3+3 block approach with the yield in the final NIS/TfOH-promoted coupling between an N,N-diacetyl-trisaccharide thioglycosyl donor 20 and a 4′′-OH trisaccharide acceptor 13 being 75%.     

Organocatalytic Multicomponent Synthesis of α/β-Dipeptide Derivatives

A straightforward multicomponent Knoevenagel-aza-Michael-cyclocondensation reaction involving readily available hydroxamic acid-derived from naturally occurring α-amino acids allows a diversity-oriented synthesis of novel isoxazolidin-5-ones possessing an N-protected α-amino acid pendant with good to high diastereoselectivities thanks to a match effect with a chiral organocatalyst. These diversely substituted heterocycles, easily isolated as a single diastereoisomer, proved to be versatile platforms for the formation of an array of α/β-dipeptide fragments.     

A synthesis of 3′-α-fluoro-2′,3′-dideoxyadenosine via a bromine rearrangement during fluorination with MOST reagent

A facile method for the synthesis of 3′-α-fluoro-2′,3′-dideoxyadenosine 6 has been developed. Fluorination of 5′-O-acetyl-3′-β-bromo-3′-deoxyadenosine 3 with MOST gave 2′-β-bromo-3′-α-fluoro-2′,3′-dideoxyadenosine 4 via a rearrangement of the 3′-β-bromine to the 2′-β position during 3′-α fluorination. The 2′-β bromine was reduced by radical reduction and then the 5′-O-acetyl group was removed to afford 3′-α-fluoro-2′,3′-dideoxyadenosine 6 in good yield. A possible mechanism for the rearrangement is discussed.