新型2-溴苯酰胺类小分子CCR5拮抗剂的合成及其GTPγS结合性

以2-羟基-5-溴苯甲醛为起始原料,经取代,还原和NBS溴化反应制得5-溴-2-(4-氯苯甲氧基)溴甲苯(3);以4-哌啶酮盐酸盐为原料,经保护,还原和缩合反应制得N-烯丙基-2-溴-N-哌啶基苯酰胺(7);3和7经取代反应合成了一个新型的非肽类小分子CCR5拮抗剂——N-烯丙基-2-溴-N-{N-[2-(4-氯苯甲氧基)-5-溴苄基]-4-哌啶基}苯酰胺(8),总产率32.5%,其结构经1H NMR,13C NMR,IR和ESI-MS表征。用GTPγS法测试了8的生物结合性。结果表明:8的生物结合性与TD0232接近,其IC50为(8.12±0.3)nmol·L-1。     

新型六[间-(β-噻吩基)苯基]苯衍生物的合成

3,3’-二溴二苯乙炔与β-噻吩频哪醇硼酸酯发生Suzuki偶联反应制得3,3’-二(2,5-二十二烷基-3-噻吩)二苯乙炔(7);Co2(CO)8催化7自身环三聚合成了新型六[间-(β-噻吩基)苯基]苯衍生物——六{3-[2’,5’-二(十二烷基)-3-噻吩]苯基}苯,产率86%,其结构经1H NMR和MS表征。     

波生坦的合成工艺改进

以4,6-二氯-5-(2-甲氧基苯氧基)-2,2'-双嘧啶和4-叔丁基苯磺酰胺为原料,经缩合反应制得中间体N-{6-氯-5-(2-甲氧基-苯氧基)[2,2'-嘧啶]-4-基}-4-(叔丁基苯基)-磺酰胺(3);3与乙二醇经缩合反应合成了波生坦(1),总收率81.4%。3经水解反应合成了N-{6-羟基-5-(2-甲氧基-苯氧基)[2,2'-嘧啶]-4-基}-4-(叔丁基苯基)-磺酰胺(4);4与1,2-二溴乙烷经缩合反应合成了1,2-双{[5-(2-甲氧基苯氧基)-2-(2-嘧啶-2-基-嘧啶-4-基]-4-叔丁基苯磺酰胺}-乙二醇(5),其结构经1H NMR,13C NMR和MS确证。4和5为波生坦中可能存在的杂质。     

新型两亲性氮杂六芳基苯的合成

以5-溴-2-十二烷基嘧啶为原料,经Sonogashira偶联等反应制得1,2-双(2-十二烷基嘧啶-5-基)乙炔(4); 1-溴-4-(2-(2-(2-甲氧基乙氧基)乙氧基)乙氧基)苯(5)与双频哪醇合二硼反应制得化合物(6); 4,4′-二溴苯偶酰与1,3-二苯基丙酮经羟醛缩合反应制得四芳基环戊二烯酮衍生物(7); 化合物4与7经Diels-Alder反应制得化合物8; 8与6〖STBZ〗通过Suzuki-Miyaura偶联反应合成新型两亲性氮杂六芳基苯(9),化合物6~9为新化合物,其结构经¹H NMR, ¹³C NMR和HR-MS(MALDI-TOF)表征。     

新型CCR5拮抗剂——N-【1-{5-溴-2-[(4-氯苄基)氧基]苄基}-4-哌啶基】-N-乙基吡啶甲酰胺的合成

以5-溴水杨醛和4-氯苄氯为原料,通过消去、还原及溴化反应制得中间体4-溴-2-溴甲基-1-[(4-溴苄基)氧]苯(3);哌啶-4-酮经Boc保护、还原等4步反应制得中间体N-乙基-N-(4-哌啶基)吡啶甲酰胺(7);3与7通过消去反应合成了一种新型CCR5拮抗剂——N-【1-{5-溴-2-[(4-氯苄基)氧基]苄基}-4-哌啶基】-N-乙基吡啶甲酰胺,其结构经1H NMR,13C NMR和ESI-MS表征。     

4-(甲氧基噻吩基)-3-(取代苯甲酰基)-吡咯类化合物的合成与抗肿瘤活性研究

分别以2-甲氧基噻吩、3-甲氧基噻吩、3,4-二溴噻吩和取代苯乙酮为原料,经过溴甲氧基取代反应、VilsmeierHack反应、羟醛缩合和Van Leusen吡咯合成法,设计并合成了33个未见文献报道的4-取代噻吩基吡咯类化合物.其结构均经~1H NMR,~(13)C NMR及HRMS确认,同时采用噻唑蓝(MTT)法测试了目标化合物对CHO、HCT-116、MGC80-3、SGC-7901以及HUVEC细胞增殖抑制活性.结果显示,部分化合对MGC80-3细胞有较强(IC_(50)≤20μml/L)或中等(20μmol/LIC_(50)≤50μmol/L)增殖抑制作用,其中[4-(3,4-二甲氧基噻吩-2-基)-1H-吡咯-3-基](4-苯基苯基)甲酮(4a-2)和[4-(3,4-二甲氧基噻吩-2-基)-1H-吡咯-3-基](3-溴苯基)甲酮(4a-7)的IC_(50)值分别为8.6和8.5μmol/L;化合物4a-7对HCT-116细胞有中等抑制活性;化合物4a-2和4a-7对SGC-7901细胞有中等增殖抑制活性;并且几乎所有化合物对正常人体细胞HUVEC无明显抑制作用.     

盐酸普拉格雷的合成工艺改进

以2-氧代-N-三苯甲基-2,4,5,6,7,7-a-六氢噻吩并[3,2-c]吡啶为原料,经酰化、脱保护反应制得2-乙酰氧基-5,6,7,7-a-四氢噻吩并[3,2-c]吡啶盐酸盐(4); 4与2-溴-2-(2-氟苯基) 1-环丙基乙酮缩合得2-[2-(乙酰氧基)-6,7-二氢噻吩并[3,2-c]吡啶-5(4H)-基]-1-环丙基-2-(2-氟苯基)乙酮(5); 5再经成盐反应得到盐酸普拉格雷,总收率75.0%,其结构经¹H NMR和MS（ESI）确证。     

以二苯甲酮为端基的第一代树状取代酞菁锌的合成

4-甲基二苯甲酮经N-溴代丁二酰亚胺溴代制得4-溴甲基二苯甲酮(1);1与3,5-二羟基苯甲醇反应合成了外围带有二苯甲酮取代基的第一代树枝状分子3,5-二(二苯甲酮-4-甲氧基)苯甲醇(2);2与4-硝基邻苯二甲腈缩合制得外围带有二苯甲酮取代基的第一代树枝状分子4-[3,5-二(二苯甲酮-4-甲氧基)苯甲氧基]邻苯二甲腈(3);3经"液相法"环合生成外围带有二苯甲酮取代基的第一代树枝状分子取代的酞菁锌配合物——四[3,5-二(二苯甲酮-4-甲氧基)苯甲氧基]锌酞菁[ZnPc(C35H27O5)4],其结构经UV,1HNMR,IR和MS表征。     

5-[2-(对苯偶氮苯氧基)丁氧基]苯基-10,15,20-三[(对甲氧基苯基)]卟啉及其金属配合物的合成

以5-[2-(4-溴丁氧基)苯基]-10,15,20-三(对甲氧基苯基)卟啉和对羟基偶氮苯为原料,经取代反应合成新化合物5-[2-(对苯偶氮苯氧基)丁氧基]苯基-10,15,20-三[(对甲氧基苯基)]卟啉(2),2经配位反应合成了金属铜,锌配合物(2a)和(2b),其结构经UV-Vis,1H NMR,IR和元素分析表征。     

新型含吡唑和三唑基联吡啶类化合物的合成及其光学性能

以对-吡唑基苯甲醛(1a)[或对-1,2,4-三唑基苯甲醛(1b)]和苯乙酮经Aldol缩合反应得4-吡唑查尓酮(2a)[或4-三唑查尔酮(2b)];2a或2b与2-乙酰基吡啶(3)经Michael加成反应得1-苯基-5-(2-吡啶基)-3-[4-(1-吡唑基)苯基]-1,5-戊二酮(4a)或1-苯基-5-(2-吡啶基)-3-[4-(1-[1,2,4]-三唑基)苯基]-1,5-戊二酮(4b);4a或4b与AcONH4经关环反应合成了两种新型含吡唑和三唑基的联吡啶衍生物——6-苯基-4-[4-(1H-吡唑基)苯基]-2,2'-联吡啶(5a)或6-苯基-4-[4-(1H-1,2,4-三唑基)苯基]-2,2'-联吡啶(5b),其结构经1H NMR,IR,MS和元素分析表征。UV-Vis和FL研究结果表明:5a和5b的λmax分别位于290 nm和280nm;5a和5b的λem均位于360 nm。     

Synthesis, docking studies and biological evaluation of benzo[b]thiophen-2-yl-3-(4-arylpiperazin-1-yl)-propan-1-one derivatives on 5-HT1A serotonin receptors

A series of novel benzo[b]thiophen-2-yl-3-(4-arylpiperazin-1-yl)-propan-1-one derivatives 6a-f, 7a-f and their corresponding alcohols 8a-f were synthesized and evaluated for their affinity towards 5-HT(1A) receptors. The influence of arylpiperazine moiety and benzo[b]thiophene ring substitutions on binding affinity was studied. The most promising analogue, 1-(benzo[b]thiophen-2-yl)-3-(4-(pyridin-2-yl)piperazin-1-yl)propan-1-one (7e) displayed micromolar affinity (K(i) = 2.30 μM) toward 5-HT(1A) sites. Docking studies shed light on the relevant electrostatic interactions which could explain the observed affinity for this compound.     

New ‘2-phenylnaphthalene’-mediated synthesis of benzo[b]naphtho[2,3-d]furan-6,11-diones and 6-oxa-benzo[a]anthracene-5,7,12-triones: first total synthesis of 6-oxa-benzo[a]anthracen-5-ones

We describe here a novel synthesis of benzo[b]naphtho[2,3-d]furan-6,11-diones based on the heteroannulation of 2-(2-bromophenyl)-3-hydroxy-1,4-naphthoquinones. The naphthoquinones were prepared from 3-(2-bromophenyl)naphthalen-2-ols, which were obtained by intramolecular aldol condensation of 2-[3-(2-bromophenyl)-2-oxo-propyl]benzaldehydes. Alternatively, benzo[b]naphtho[2,3-d]furan-6,11-diones were obtained more directly and efficiently by cyclization of 3-(2-bromophenyl)naphthalen-2-ols to benzo[b]naphtho[2,3-d]furans and oxidation of the resulting compounds. Furthermore, the first 6-oxabenzo[a]anthracen-5-one described was similarly obtained from 2-[3-(2-formylphenyl)-2-oxopropyl]benzoic acid and oxidized to 6-oxa-benzo[a]anthracene-5,7,12-trione.     

Synthesis of 2-, 4- and 5-(2-alkylcarbamoyl-1-methylvinyl)-7-alkyloxybenzo[b]furans and their leukotriene B4 receptor antagonistic activity

Variable benzo[b]furan derivatives having (E)- and (Z)-2-alkylcarbamoyl-1-methylvinyl groups at the 2-, 4- and 5-positions and a carboxylpropoxy or (1-phenyl)ethoxy group at the 7-position were prepared to find novel and selective leukotriene B4(LTB4) receptor antagonists. (E)-2-(2-diethylcarbamoyl-1-methylvinyl)-7-(1-phenylethoxy)benzo[b]furan (4v) showed selective inhibition to the human BLT2 receptor (hBLT2). On the other hand, (E)-2-acetyl-4-(2-diethylcarbamoyl-1-methylvinyl)-7-(1-phenylethoxy)benzo[b]furan (7v) inhibited both human BLT(1) receptor (hBLT1) and hBLT2. The (E)-2-(2-diethylcarbamoyl-1-methylvinyl) group lay on approximately the same plane as the benzo[b]furan ring, whereas the (E)-4-(2-diethylcarbamoyl-1-methylvinyl) group had the torsion angle (45.7 degree) from the benzo[b]furan ring plane. However, the (Z)-(2-alkylcarbamoyl-1-methylvinyl)benzo[b]furans were inactive. The inhibitory activity depended on the conformation of the 2-diethylcarbamoyl-1-methylvinyl group.     

新型Bluco类β-内酰胺酶分子探针的合成

以2-氰基-6-羟基苯并噻唑为原料,与溴乙醛缩二乙醇缩合制得缩醛后再水解合成中间体6-(2-羰乙基)苯并[d]噻唑-2-甲腈(2);7-苯乙酰氨基-3-氯甲基头孢菌烷酸二苯甲酯依次经碘代和Wittig反应得(Z)-3-[3-(2-氰基苯并[d]噻唑-6-氧)丙-1-烯]-8-羰基-7-(2-苯乙酰氨基)-5-噻-1-氮[4.2.0]辛-2-烯-2-甲酸二苯甲酯(5);5经脱保护、缩合和氧化反应合成了3个新的Bluco类似物,其结构经1H NMR,13C NMR和HR-MS(ESI)表征。     

Electrophilic chemistry of thia-PAHs: stable carbocations (NMR and DFT), S-alkylated onium salts, model electrophilic substitutions (nitration and bromination), and mutagenicity assay

First examples of stable carbocations are reported from several classes of thia-PAHs with four fused rings, namely, benzo[b]naphtho[2,1-d]thiophene (1) and its 3-methoxy derivative (2), phenanthro[4,3-b]thiophene (3) and its 7-methoxy (4), 10-methoxy (5), and 9-methoxy (6) derivatives, phenanthro[3,4-b]thiophene (7) and its 7-methoxy (8) and 9-methoxy (9) derivatives, and 3-methoxybenzo[b]naphtha[1,2-d]thiophene (11). In several cases, the resulting carbocations were also studied by GIAO-DFT. Charge delocalization modes in the resulting carbocations were probed. A series of S-alkylated onium tetrafluoroborates, namely, 1Me+, 1Et+, 2Et+, and 7Me+ (from 1, 2, and 7), 10Me+ and 10Et+ (from benzo[b]naphtha[1,2-d]thiophene 10), 12Me+ and 12Et+ (from phenanthro[3,2-b][1]benzothiophene 12), 13Me+ (from 3-methoxyphenanthro[3,2-b]benzothiophene 13), 14Me+ (from phenanthro[4,3-b][1]benzothiophene 14), and 15Me+ (from 3-methoxyphenanthro[4,3-b][1]benzothiophene 15), were synthesized. PAH-sulfonium salts 1Me+, 1Et+, 10Me+, 10Et+, 12Me+, and 14Me+ proved to be efficient akylating agents toward model nitrogen nucleophile receptors (imidazole and azaindole). Facile transalkylation to model nucleophiles (including guanine) is also supported by favorable reaction energies computed by DFT. Ring opening energies in thia-PAH-epoxides from 1, 3, and 7 and charge delocalization modes in the resulting carbocations were also evaluated. The four-ring-fused thia-PAHs 1, 2, 3, 4, 5, 7, 8, and 11 are effectively nitrated under extremely mild conditions. Nitration regioselectivity corresponds closely to protonation under stable ion conditions. Bromination of 4 and 6 is also reported. Comparative mutagenicity assays (Ames test) were performed on 1 versus 1NO2, 5 versus 5NO2, and 11 versus 11NO2. Compound 5NO2 was found to be a potent direct acting mutagen.     

Structural chemistry of polycyclic heteroaromatic compounds. Part XI. Photoelectron spectra and electronic structures of tetracyclic hetarenes of the triphenylene type

The UV photoelectron spectra of several tetracyclic heteroaromatic compounds (2-9) which are pi-isoelectronic with triphenylene (1) have been recorded and analysed making use of semiempirical AM1 and PM3 as well as ab initio/DFT B3LYP calculations. In one series of compounds (2-7), the peripheral benzene rings of 1 are successively substituted by thiophene rings that are either [b]- or [c]-annellated with the central benzene unit. In 2-7 only marginal shifts are found for most of the IPs of electrons. In the benzotrithiophenes 5-7, a systematic variation is displayed by IP(pi7). Compared to 1, the pi electron system of benzo[c]trithiophene (7) is approximately two times as much destabilized as in the isomers 5 and 6 with [b]annellated thiophene rings. The IP[n(S)] values of the thiophene derivatives 2-7 indicate that these orbitals are clearly destabilized relative to thiophene. The same holds for the n(O) orbital of the furane derivative 9 in comparison with that of furane. In 9, only the higher pi MOs (pi7-pi9) are destabilized whereas the lower levels (pi1-pi4) are stabilized, and those in between (pi5-pi6) remain essentially unshifted. In the pyrrole derivative 8, all pi MOs are substantially destabilized by about 0.5-1.6 eV relative to 1.     

Condensed Pyridine Bases. Synthesis and Reactions of Benzofuro[2,3-c]indeno[2,1-e]-, Benzothieno[2,3-c]Indeno[2,1-e]-, Benzofuro-[3,2-c]Indeno[2,1-e]- and Thieno[2,3:4′,5′]-thieno[3,2-c]indeno[2,1-e]pyridines

Condensation of hetarene carboxaldehydes with phthalide gave 2-(3-hydroxy-1-oxoinden-2-yl)benzo[b]furan and 2-(3-hydroxy-1-oxoinden-2-yl)-5-ethylthieno[2,3-b]thiophene. Starting from hetaryl acetic acids gave 3-(3-hydroxy-1-oxoinden-2-yl)benzo[b]furan and 3-(3-hydroxy-1-oxoinden-2-yl)benzo[b]thiophene. Acylation of 3-hydroxy-1-oxoinden-2-yl-substituted heterocycles using acetic anhydride in the presence of 70% HClO₄ leads to the formation of pentacyclic pyrilium salts. Pentacyclic indenopyridines are prepared by treating the pyrilium salts with ammonia. The reaction of the carbonyl group in the indenopyridines with hydroxylamine, hydrazine hydrate, and in reduction using NaBH₄ has been studied.__________Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 3, pp. 435–443, March, 2005.     

Bacterial dioxygenase- and monooxygenase-catalysed sulfoxidation of benzo[b]thiophenes

Asymmetric heteroatom oxidation of benzo[b]thiophenes to yield the corresponding sulfoxides was catalysed by toluene dioxygenase (TDO), naphthalene dioxygenase (NDO) and styrene monooxygenase (SMO) enzymes present in P. putida mutant and E. coli recombinant whole cells. TDO-catalysed oxidation yielded the relatively unstable benzo[b]thiophene sulfoxide; its dimerization, followed by dehydrogenation, resulted in the isolation of stable tetracyclic sulfoxides as minor products with cis-dihydrodiols being the dominant metabolites. SMO mainly catalysed the formation of enantioenriched benzo[b]thiophene sulfoxide and 2-methyl benzo[b]thiophene sulfoxides which racemized at ambient temperature. The barriers to pyramidal sulfur inversion of 2- and 3-methyl benzo[b]thiophene sulfoxide metabolites, obtained using TDO and NDO as biocatalysts, were found to be ca.: 25-27 kcal mol(-1). The absolute configurations of the benzo[b]thiophene sulfoxides were determined by ECD spectroscopy, X-ray crystallography and stereochemical correlation. A site-directed mutant E. coli strain containing an engineered form of NDO, was found to change the regioselectivity toward preferential oxidation of the thiophene ring rather than the benzene ring.     

Synthesis and molecular structure of bis(benzo)aza-14-crown-4 ethers with 7-azabicyclo[3.3.1]nonane and homologous fragments

By condensation of cycloalkanes with 2-{2-[2-(2-formylphenoxy)ethoxy]ethoxy}benzaldehyde and ammonium acetate by Petrenko-Kritchenko method first representatives of new heterocyclic systems, bis(benzo)-aza-14-crown-4 ethers containing a 7-aza-bicyclo[3.3.1]nonane or its homologous fragment, were obtained in 6–15% yield. With growing cycle of the initial cycloketone the yield of the azacrownophane considerably grew. By means of XRD analysis the molecular structure was established of four synthesized macrocycles, the relative configuration of asymmetrical atoms was determined, and the size of the internal cavities of the azacrown part was estimated.     

Etudes photochimiques—XIII : Reactions de photoaddition du benzo[b]thiophene avec des amines et avec le pyrrole

The photochemical behavior of benzo[b]thiophene is different from that of thiophene. The former does not undergo photoisomerization and is not converted into an indole when irradiated in the presence of a primary amine; its photochemical behavior resembles that of naphthalene. Thus photoexcited benzo[b]thiophene gives adducts with primary amines (1(H)), secondary amines (2), and pyrrole (3(H)): an exciplex is an intermediate. The existence of the exciplex is supported by the formation of aldehyde 7 when benzo[b]thiophene is irradiated in aqueous propylamine, the finding that photoexcited benzo[b]thiophene does not react with an alcohol and that photoexcited indole benzo[b]furan, 2-methylbenzo[b]thiophene, and 3-methylbenzo[b]thiophene do not react with propylamine or with piperidine. The results are interpreted in terms of spin densities calculated for the anion radicals of the compounds under study.