2,2-二甲基-4-(2,5-二氟苯基)-5-[(4-氨基磺酰基)苯基]-3(2H)-呋喃酮的合成

用2,5-二氟苯乙酸与茴香硫醚经傅-克反应、与3-溴-3-甲基-2-氧代丁腈成环及硝酸氧化制得2,2-二甲基-4-(2,5-二氟苯基)-5-[(4-甲磺酰基)苯基]-3(2H)-呋喃酮(7),7与乙酐反应后再经过硫酸氢钾复合盐氧化、氢氧化钠水解得4-[2,2-二甲基-3-氧代-4-(2,5-二氟苯基)-3(2H)-呋喃-5-基]苯磺酸钠(9),最后依次与磺酰氯和氨水反应制得2,2-二甲基-4-(2,5-二氟苯基)-5-[(4-氨基磺酰基)苯基]-3(2H)-呋喃酮,总收率约46％.     

(2R,3S)-2-[(R)-1-[3,5-二(三氟甲基)苯基]乙氧基]-3-(4-氟苯基)吗啉盐酸盐的合成

对甲氧基苯甲醛(3)和2-氨基乙醇进行还原胺化反应得2-(4-甲氧基苄胺基)乙醇(4),4和乙醛酸经成环反应得2-羟基-4-对甲氧基苄基吗啉-3-酮(5),5和三氟乙酐反应得6后与(R)-1-[3,5-二(三氟甲基)苯基]乙醇(7)缩合,再经结晶诱导不对称转化、格氏反应、氢化脱保护及成盐反应制得阿瑞吡坦关键中间体(2R,3S)-2-[(R)-1-[3,5-二(三氟甲基)苯基]乙氧基]-3-(4-氟苯基)吗啉盐酸盐,总收率约18%(以3计)。     

4-(4-氨基苯基)-3-吗啉酮的合成

用两种方法制得抗凝剂利伐沙班的中间体4-(4-氨基苯基)-3-吗啉酮(1):①溴苯相继与乙醇胺、氯乙酰氯反应得4-苯基吗啉酮,再经硝化、还原生成1,总收率约32%;②溴苯先硝化,再与乙醇胺反应得到2-(4-硝基苯胺基)乙醇,再经氯乙酰氯闭环、还原反应制得1,总收率约47%.     

(E)-3-(4-羟基-2-甲氧基苯基)丙烯酸甲酯的合成

4-羟基-2-甲氧基苯甲醛和丙二酸在吡啶和苯胺催化下,经Knoevenagel缩合反应制得(E)-3-(4-羟基-2-甲氧基苯基)丙烯酸,再在1-(3-二甲胺基丙基)-3-乙基碳二亚胺盐酸盐和4-二甲胺基吡啶作用下与甲醇成酯制得(E)-3-(4-羟基-2-甲氧基苯基)丙烯酸甲酯,总收率为58.5％.     

4-(2-溴乙酰基)-3-氟苯硼酸的制备

4-溴-2-氟苯基氰经格氏反应得到4-溴-2-氟苯乙酮,先保护羰基,再经格氏反应和二羟硼基取代、溴代制得4-(2-溴乙酰基)-3-氟苯硼酸,总收率54%.     

叔丁基[2-溴-4-(溴甲基)-6-硝基苯基]氨基甲酸酯的合成

以4-甲基-2-硝基苯胺为起始原料,经过两次溴代反应和氨基保护合成了未见文献报道的化合物叔丁基[2-溴-4-(溴甲基)-6-硝基苯基]氨基甲酸酯,总收率60.64%,其结构经LC/MS和1H NMR确证。     

前列腺癌显像剂~(18)F-8-乙氧基-2-(4-氟苯基)-3-硝基-2H-色烯的合成

目的制备前列腺癌显像剂~(18)F-8-乙氧基-2-(4-氟苯基)-3-硝基-2H-色烯的前体8-乙氧基-2-(4-N,N,N-三甲基氨基苯基)-3-硝基-2H-色烯季胺三氟甲磺酸盐;用前体和放射性核素~(18)F合成~(18)F-8-乙氧基-2-(4-氟苯基)-3-硝基-2H-色烯。方法以2-羟基-1-乙氧基-3-醛基苯为起始原料,经烯化、环化、磺化、成盐反应得到标记前体8-乙氧基-2-(4-N,N,N-三甲基氨基苯基)-3-硝基-2H-色烯季胺三氟甲磺酸盐;然后与放射性核素~(18)F经亲核氟代反应,得到~(18)F-8-乙氧基-2-(4-氟苯基)-3-硝基-2H-色烯。标记前体8-乙氧基-2-(4-N,N,N-三甲基氨基苯基)-3-硝基-2H-色烯季胺三氟甲磺酸盐及各步反应中间体的结构均经核磁共振谱和质谱确证。结果与结论成功合成前列腺癌诊断显影剂~(18)F-8-乙氧基-2-(4-氟苯基)-3-硝基-2H-色烯,标记率为(25.8±2.6)%(n=5,未经衰减校正),TLC测定其放化纯度(RCP)为97.5%,为进一步临床研究奠定了基础。     

2-(5-甲基-2-苯基-4-(口恶)唑)-乙醇的合成

以丙酰乙酸乙酯为起始原料,先溴化得到4-溴丙酰乙酸乙酯,再在甲苯中与苯甲酰胺回流环合得到2-(5-甲基-2-苯基-4-(口恶)唑)-乙酸乙酯,最后经氢化铝锂还原,得到目标杂环中间体2-(5-甲基-2-苯基-4-(口恶)唑)-乙醇.该合成方法反应步骤少,原料便宜,目标物的总收率为67.3%.     

2-(3,4,5-三氯苯基)-1,2,4-三嗪-3,5(2H,4H)-二酮的合成

2,6-二氯-4-硝基苯胺经重氮化、氯代及还原得到3,4,5-三氯苯胺,再以N,N′-二(乙氧羰基)丙二酰胺为环合剂,经重氮化、偶联、闭环、水解及脱羧反应制得具有抗球虫活性的2-(3,4,5-三氯苯基)-1,2,4-三嗪-3,5(2H,4H) -二酮,总收率约39％(以2,6-二氯4硝基苯胺计).     

(R)-1-(4-苄氧基-3-硝基苯基)-2-溴乙醇的合成

4-羟基-3-硝基苯乙酮经O-苄基化、溴化、还原制得1-(4-苄氧基-3-硝基苯基)-2-溴乙醇,然后酶促拆分得(R,R)-型福莫特罗的关键中间体(R)-1-(4-苄氧基-3-硝基苯基)-2-溴乙醇,总收率约25%.     

实例(4)

某作者采用青霉素与双黄连对小儿呼吸道感染进行治疗效果观察 ,作者用一年的时间 ,收集到小儿呼吸道感染患者 1 54例 ,将全部病例分为两组。治疗组 80例 ,男 49例 ,女 31例。急性扁桃体炎 36例 ,急性咽炎 2 5例 ,支气管炎 1 3例 ,肺炎 6例。对照组 74例 ,男 40例 ,女 34例。急性扁桃体炎 34例 ,急性咽炎 2 4例 ,支气管炎 1 1例 ,肺炎 5例。治疗组采用青霉素与双黄连治疗 ;对照组只用青霉素治疗。两组病例中上呼吸道感染疗程 3～ 5天 ,下呼吸道感染疗程 5～ 7天。治疗结果 ,对照组显效 32例 ,有效 30例 ,总有效率83.6% ;治疗组显效 45例 …     

Idarubicin (4-demethoxydaunorubicin)

4-Demethoxydaunorubicin (4-DMDR, IMI 30, Idarubicin, NSC 256439) is a new analog of daunorubicin (DNR) with antileukemic activity in experimental systems that is superior to that of daunorubicin (DNR) or doxorubicin (DX). The drug is more potent than DNR and DX and is active by both the intravenous and the oral routes of administration. After i.v. and oral administration in humans, Idarubicin is rapidly metabolized to its 13-dihydroderivative (Idarubicinol) and the plasma levels of this metabolite are consistently higher than those of the unchanged drug. Idarubicinol has been shown to be an active metabolite in experimental models, being as potent and as active as the parent compound. Phase II clinical trials of Idarubicin have indicated that: By I.V. route Idarubicin is a potent antileukemic agent active in relapsed or refractory, ANLL, ALL (adult and pediatric) either as single agent or in combination with Ara-C at doses of 8-12 mg/m2 by i.v. day 1, 2 and 3 or 7-8 mg/m2 i.v. daily X 5 days (adults). There is evidence of lack of cross-resistance with parent drugs and other antileukemic agents. Phase III studies in previously untreated acute leukemias have been initiated. By oral route Idarubicin has antitumor activity in breast cancer at the doses of 35-45 mg/m2 q 3-4 weeks or 15 mg/m2 daily X 3 days q 3-4 weeks. Idarubicin has activity as a single agent in adult leukemias at the doses of 20-30 mg/m2/day X 3 days. The safety of administration (no risk of extravasation), the good tolerability and the reduced potential for cardiac toxicity, make oral Idarubicin particular attractive for further clinical development. Whether Idarubicin proves to be more effective and/or less cardiotoxic in clinical therapy than DNR or DX remains to be seen through prospective randomized studies which have been already initiated both in leukemias and solid tumors.     

Bioaccumulation and toxicity of 4-nonylphenol (4-NP) and 4-(2-dodecyl)-benzene sulfonate (LAS) in Lumbriculus variegatus (Oligochaeta) and Chironomus riparius (Insecta)

The discharge of surfactants, such as 4-nonylphenol (4-NP) and linear alkylbenzene sulfonates (LAS), into water bodies leads to accumulation of the chemicals in the sediments and may thus pose a problem to benthic organisms. To study the bioaccumulation of surfactants, Oligochaeta worm Lumbriculus variegatus was exposed to sediment-spiked, [14C]-labeled 4-NP and 4-(2-dodecyl)-benzene sulfonate (C12-LAS) in three different sediments (S1-S3). The sediments were characterized for organic carbon (OC) content and particle size distribution. The acute toxicity was examined by exposing L. variegatus and three to four instar Chironomus riparius (Insecta) larvae in water-only exposure to 4-NP and LAS at different concentrations. After 48-h exposure, lethal water concentrations (LC50) and lethal body residues (LBR50) were estimated using liquid scintillation counting. Chronic toxicity was evaluated in two different sediments by exposing first instar C. riparius larvae to sediment-spiked chemicals at different concentrations. After 10 days, the sublethal effects of surfactants were observed by measuring wet weight and head capsule length. Finally, another 10-day test was set up in order to measure the LAS body residues associated with sublethal effects in C. riparius in S2 sediment. The bioaccumulation test revealed that the bioaccumulation of both 4-NP and LAS increased as the sediment organic matter content decreased. It is assumed that the chemical binding to organic material decreased chemical bioavailability. The acute toxicity tests showed that L. variegatus was more tolerant of 4-NP, and C. riparius was more tolerant of LAS when based on water exposure concentration. The LBR-estimates revealed, however, that L. variegatus tolerated clearly higher tissue residues of both chemicals compared with C. riparius. Both chemicals had sublethal effects on C. riparius growth in sediment exposure, reducing larvae wet weight and head capsule size. 4-NP, however, showed an irregular dose-response pattern. The characteristics of the exposure media affected the bioaccumulation potential of both chemicals. Thus, exposure concentrations offered no prediction of body residue, and therefore it is proposed that organism body residue offered a more accurate dose-metric for chemical exposure than the chemical concentration of the environment.     

4-(Phenylaminomethylene)isoquinoline-1,3(2H,4H)-diones as potent and selective inhibitors of the cyclin-dependent kinase 4 (CDK4)

The cyclin-dependent kinases (CDKs), as complexes with their respective partners, the cyclins, are critical regulators of cell cycle progression. Because aberrant regulations of CDK4/cyclin D1 lead to uncontrolled cell proliferation, a hallmark of cancer, small-molecule inhibitors of CDK4/cyclin D1 are attractive as prospective antitumor agents. The series of 4-(phenylaminomethylene)isoquinoline-1,3(2H,4H)-dione derivatives reported here represents a novel class of potent inhibitors that selectively inhibit CDK4 over CDK2 and CDK1 activities. In the headpiece of the 4-(phenylaminomethylene)isoquinoline-1,3(2H,4H)-dione, a basic amine substituent is required on the aniline ring for the CDK4 inhibitory activity. The inhibitory activity is further enhanced when an aryl or heteroaryl substituent is introduced at the C-6 position of the isoquinoline-1,3(2H,4H)-dione core. We present here SAR data and a CDK4 mimic model that explains the binding, potency, and selectivity of our CDK4 selective inhibitors.