Synthesis and Antimicrobial Activity of New 2,5‐Disubstituted 1,3,4‐Oxadiazoles and 1,2,4‐Triazoles and Their Sugar Derivatives

A series of new 2,5‐disubstituted‐1,3,4‐oxadiazole and 1,2,4‐triazole derivatives were synthesized by heterocyclization of acid hydrazide 1 and thiosemicarbazide derivative 2 . Furthermore, the acyclic C‐nucleoside analogs were prepared by cyclization of their corresponding sugar hydrazones by reaction with acetic anhydride. The antimicrobial activity of the prepared compounds was evaluated and some of the synthesized compounds revealed good activities against fungi.     

Synthesis,Structure and Reactivity of some 2,6‐Disubstituted Dimethylsilylbenzenes

Syntheses are described of a number of 2,6‐difunctionalized dimethylsilylbenzenes, namely, 1‐(HMe₂Si)‐2,6‐Cl₂C₆H₃ ( 13 ), 1‐(HMe₂Si)‐2,6‐Br₂C₆H₃ ( 14 ), 1,2,3‐(HMe₂Si)₃C₆H₃ ( 15 ), 1,2‐(HMe₂Si)₂‐6‐ClC₆H₃ ( 16 ), 1,2‐(HMe₂Si)₂‐6‐BrC₆H₃ ( 17 ), 1‐(HMe₂Si)‐2‐(Ph₂P)‐6‐BrC₆H₃ ( 18 ), diphenyl(1,1,3,3‐tetramethyl‐1,3‐dihydrobenzo[c][1,2,5]oxadisilol‐4‐yl)phosphine oxide ( 19 ) and 8‐Brom‐1,1,3,3‐tetramethyl‐2,2,2,2,‐tetracarbonyl‐1,3‐dihydro‐benzo[d][2,1,3]ferra disilol ( 20 ). Compounds 13 – 20 were characterized by multinuclear NMR spectroscopy and in case of 18 – 20 also by single crystal X‐ray diffraction.     

Design,Synthesis, and Biological Evaluation of 3,5‐Disubstituted 2‐Pyrazineamide Derivatives as Antitubercular Agents

A novel series of 3,5‐disubstituted‐2‐pyrazineamide derivatives ( 5a–5o ) were synthesized and studied for their potential as antitubercular agents. Among them, the compounds 5a , 5g , and 5m showed the good minimal inhibitory concentration of 20, 25, and 25 μg/mL, respectively. The compound 5a displayed excellent minimum inhibitory concentration of 10 μg/mL and is four times more potent compared with the standard drug, rifampicin concentration. In silico docking studies revealed that the compounds 5a and 5c can bind strongly in the active site of 2FUM enzyme and prevent enzyme–substrate interactions. In addition, in silico docking studies were calculated, and based on the data obtained, compound 5a displayed excellent drug‐like properties.     

新型2,6-二取代嘌呤衍生物的合成及其抗肿瘤活性

以2,6-二氯嘌呤为原料,对其2-位和6-位进行结构修饰,合成了8个新型2,6-二胺嘌呤类衍生物(3a~3h),其结构经¹H NMR, IR和MS（ESI）表征。采用MTT法研究了3a~3h对人胃癌SGC-7901细胞的体外抗肿瘤活性。结果表明: 3a, 3b, 3c, 3g具有良好的抗肿瘤活性,其中3c（IC₅₀ 65.01 μmol·L^-1）对人胃癌细胞SGC-7901的抑制作用最强。     

Synthesis of Fluorescent 2,6‐Dicyano‐3,5‐Disubstituted Anilines Using Cellulose Sulfuric Acid in Aqueous Media

The synthesis of some fluorescent 2,6‐dicyano‐3,5‐disubstituted anilines using cellulose sulfuric acid (Cellulose‐SA) as an environmentally benign catalyst in H₂O is described. The one‐pot reaction of 1,3‐diketone and three equiv. of malononitrile was carried out in the presence of one equiv. of a secondary amine, Cellulose‐SA as catalyst, and H₂O as solvent. The photophysical properties (λ_Abs., λ_Flu.) of the synthesized compounds in CH₂Cl₂, MeCN, and MeOH have been measured. The emission spectra of the new compounds in the solid state are also reported.     

Synthesis and Glycosidase Inhibitory Activity of 7‐Deoxycasuarine

Reaction of 1,4‐anhydro‐2,3,5‐tri‐O‐benzyl‐1‐deoxy‐1‐imino‐D ‐arabinitol N‐oxide ( 8 ) with allyl alcohol produced a 3.6 : 1 mixture of the two pyrrolo[1,2‐b]isoxazole derivatives 13 and 14 . The major adduct 13 was converted to 7‐deoxycasuarine ( 7 ), a potent, specific, and competitive inhibitor of amyloglucosidase from Rhizopus mold (see Table).     

Synthesis and Antimicrobial Activity of Some 1,3‐Disubstituted Indeno[1,2‐c]pyrazoles

Synthesis of new 3‐alkyl indeno[1,2‐c]pyrazoles, possessing 4‐substituted thiazole moiety at position‐1 derived from 2‐acyl indane‐1,3‐diones, has been described. These compounds and their precursor were screened for their antibacterial (Staphylococcus aureus, Bacillus subtilis, Escherichia coli) and antifungal (Aspergillus niger, Candida albicans) activities.     

Synthesis and Antibacterial Activity of Novel Substituted Purine Derivatives

A series of novel N‐substituted‐2‐(6‐morpholino‐9H‐purin‐9‐yl)acetamide and 4‐(9‐((5‐substituted‐1,3,4‐oxadiazole/thiadiazole‐2‐yl)methyl)‐9H‐purin‐6‐yl)‐morpholine derivatives were synthesized and evaluated their antibacterial activities against rice bacterial leaf blight and tobacco bacterial wilt caused by Xanthomonas oryzae pv. oryzae (Xoo) and Ralstonia solanacearum (R. solanacearum) via the turbidimeter test in vitro. Antibacterial bioassay indicated that most compounds demonstrated good inhibitory effect against Xoo and R. solanacearum. Especially, compound 6a demonstrated the best inhibitory effect against Xoo with half‐maximal effective concentration (EC₅₀) value of 8.39 μg/mL, which was even better than those of commercial agents Bismerthiazol and Thiodiazole copper. The synthesized purine derivatives containing amide and 1,3,4‐oxadiazole/thiadiazole moieties exhibited excellent antibacterial activities against Xanthomonas oryzae pv. oryzae and R. solanacearum in vitro.     

Synthesis and Antimicrobial Activity of Some New 3,4‐Disubstituted Pyrroles and Pyrazoles

A variety of 3,4‐disubstituted pyrroles and pyrazoles were synthesized by the treatment of 1,3‐dipolar reagents viz., tosylmethyl isocyanide, and diazomethane to heteroaryl chalcones and evaluated for their antimicrobial activity. Among all the tested compounds, 14b and 15b displayed promising antimicrobial activity when compared with the standards particularly against Bacillus subtilis and Aspergillus niger.     

Chemoenzymatic Synthesis of All Four Diastereomers of 2,6‐Disubstituted Piperidines through Stereoselective Monoamination of 1,5‐Diketones

The regioselectivity of various enantiocomplementary ω‐transaminases was evaluated for the stereoselective monoamination of designated 1,5‐diketones; excellent conversions, enantio‐ and regioselectivities were observed. The resulting amino‐ketones underwent spontaneous intramolecular ring closure to afford Δ1‐piperideines, which served as precursors for the cis‐ and anti‐piperidine scaffold as demonstrated for the synthesis of the alkaloids dihydropinidine and epi‐dihydropinidine. Key to the success of accessing the trans‐piperidines was a Lewis acid mediated conformational change of the Δ1‐piperideines in the reduction step. Thus, all four diastereomers of 2,6‐disubstituted piperidines could successfully be prepared.     

The Biomimetic Synthesis and First Characterization of the (+)‐ and (−)‐Isocentrolobines, 2,6‐cis‐ and 2,6‐trans‐Disubstituted Tetrahydro‐2H‐pyrans

The four stereoisomers of the novel title compounds were prepared by oxidative cyclization of their enantiomerically pure diarylheptanoid precursors by means of the straightforward biomimetic approach presented in the preceding article. The isocentrolobines are the methoxy regioisomers of the natural (+)‐ and (−)‐centrolobines and were characterized for the first time. The synthetic procedure established the absolute configurations and the unambiguous correlation with the chiroptical data. The spectroscopic and the chiroptical data of the isocentrolobines are highly similar to those of the natural products. The single diagnostic parameter that would allow a immediate assignment in the presence of only one of the isomers is the higher melting point (ca. 50°) of the cis‐configured isocentrolobines.     

Facile Synthesis of 7‐epi‐Taxane and Its Derivatives and Preliminary Evaluation of Anticancer Activity

7‐epi‐Taxane has been achieved efficiently in gram scale from natural taxane via inversion of the 7‐hydroxyl group simply using Ag₂O as catalyst and DMF as solvent. The catalyst could be quantitatively recovered by filtration without loss of catalytic activity. This condition is also applicable to the direct epimerization of taxane derivatives (e.g., docetaxel and paclitaxel) to 7‐epi‐taxane derivatives (e.g., 7‐epi‐docetaxel and 7‐epi‐paclitaxel). Furthermore, 33 ester derivatives of 7‐epi‐taxane with different amino acid moieties at the position of C‐13 were successfully synthesized via esterification without protecting C‐7‐OH. Bioassay results revealed that compounds 13 and 18 have good selectivity against prostatic cancer cell line DU145, with IC₅₀ value as low as 15.9 nmol/L for 18 .     

Synthesis,Cytotoxic Activity Evaluation of Novel 1,2,3‐Triazole Linked Quinazoline Derivatives

A series of novel 1,2,3‐triazole‐quinazoline derivatives were synthesized in five steps starting from anthranilamide by conventional methods. All the title compounds 10a — 10r were evaluated for cytotoxic activity against four human cancer cell lines (MGC ‐803, EC ‐109, MCF ‐7 and HGC ‐27) using MTT assay in vitro . Some of the synthesized compounds exhibited moderate to potent activity against tested cancer cell lines. Among them, compounds 10 h and 10q exhibited excellent growth inhibition against HGC ‐27 and compound 10 m also possessed excellent activity against MCF ‐7, with IC₅₀ values less than 1 µmol/L. Especially, compound 10 h was more cytotoxic than 5‐fluorouracil against all tested four human cancer cell lines.     

Synthesis and Characterization of 5,10‐ and 5,15‐Disubstituted Porphodimethenes

The four porphodimethene isomers, 5,10‐ and 5,15‐disubstituted, have been synthesized in a one‐pot reaction by the Lindsey protocol. Three of them have been characterized by X‐ray crystallography. Structures show that two of them are 5,15‐porphodimethenes: one is syn‐equatorial, another is anti‐configuration; the third one is 5,10‐porphodimethene. In the 5,10‐porphodimethene, the tripyrrane subunit remains planar conformation. ¹H NMR and UV‐vis spectra have also been characterized. Both spectra reveal remarkable difference between 5,10‐ and 5,15‐disubstituted isomers.     

Solvent‐free Synthesis of 2,6‐Dihydroxy‐9H‐purin and Pteridine Derivatives

5,6‐Diaminopyrimidin‐2,4‐diol 1 was reacted with 1,4‐d ‐gluconolactone 2 , 6‐chloro‐4‐cyclopropyl‐7‐floro‐1,4‐dihydro‐1‐oxonaphthalen‐2‐carboxilic acid 4 , (3S)‐9,10‐difloro‐3,7‐dihydro‐3‐methyl‐7‐oxo‐2H‐[1,4]oxazino[2,3,4‐ij]quinolin‐6‐carboxylic acid 6 , and dimethylacetylendicarboxylate to afford 1‐(2,6‐dihydroxy‐9H‐purin‐8‐yl)‐sorbitol 3 , 7‐chloro‐1‐cyclopropyl‐6‐flouro‐3‐(2,6‐dihydroxy‐9H‐purin‐8‐yl)quinoline‐4(1H)‐one 5 , 9,10‐difluoro‐2,3‐dihydro‐6‐(2,6‐dihydroxy‐9H‐purin‐8‐yl)‐3‐methyl‐[1,4]oxazine[2,3,4‐ij]quinoline‐7‐one 7 , and (2,4‐dihydroxy‐6‐oxo‐5,8‐dihydro‐6H‐pteridine‐7‐yiliden)‐acetic acid methyl ester 9 , respectively. The synthesized compounds characterized by IR, ¹H‐NMR, ¹³C‐NMR, GC‐mass, and elemental analysis.