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二甲氧嘧啶(硫代)水杨酸类除草化合物的结构活性关系
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作者 刘常林 《新农药》 2001年第1期21-23,共3页
关键词 ()水杨酸 除草化合物 结构活性关系
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二甲氧嘧啶(硫代)水杨酸类除草化合物的结构活性关系(下)
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作者 刘常林 《新农药》 2001年第4期32-36,45,共6页
关键词 ()水杨酸 除草化合物 结构活性关系
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4,6-二甲氧基-2-[甲氧脲基硫代脲基]嘧啶的合成、晶体结构和理论计算 被引量:9
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作者 黄洁 宋纪蓉 +4 位作者 任莹辉 马海霞 王花丽 胡怀明 文振翼 《化学学报》 SCIE CAS CSCD 北大核心 2006年第1期9-16,共8页
利用2-氨基-4,6-二甲氧基嘧啶在干燥条件下与硫氰酸钾、氯甲酸甲酯在乙酸乙酯溶液中反应制得4-(4,6-二甲氧基嘧啶-2-基)-3-硫代脲酸甲酯,在二甲基甲酰胺溶液中培养出单晶,通过X射线单晶结构分析法测定分子结构和晶体结构,晶体属单斜晶系... 利用2-氨基-4,6-二甲氧基嘧啶在干燥条件下与硫氰酸钾、氯甲酸甲酯在乙酸乙酯溶液中反应制得4-(4,6-二甲氧基嘧啶-2-基)-3-硫代脲酸甲酯,在二甲基甲酰胺溶液中培养出单晶,通过X射线单晶结构分析法测定分子结构和晶体结构,晶体属单斜晶系,空间群为C2/m,晶胞参数为:a=1.6672(3)nm,b=0.66383(12)nm,c=1.1617(2)nm,β=109.275(2)°,V=1.2136(4)nm3,Dc=1.490g/cm3,μ=0.281mm-1,F(000)=568,Z=4,R1=0.0341,wR2=0.1042.运用Gaussian03程序,在6-311G的基组水平上,用HF,MP2以及B3LYP三种计算方法对标题化合物进行了几何全优化,并对其成键情况及自然键轨道(NBO)进行了分析. 展开更多
关键词 4 6-基-2-[脲基脲基] 2-氨基-4 6- 晶体结构 量子化学计算 自然键轨道(NBO)
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Enhanced antitumor effect of TM208 in combination with 5-fluorouracil in H_(22) transplanted mice
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作者 贾琳 徐波 +3 位作者 郭维 葛泽梅 李润涛 崔景荣 《Journal of Chinese Pharmaceutical Sciences》 CAS 2011年第6期615-626,共12页
4-Methylpiperazine-l-carbodithioc-acid-3-cyano-3,3-diphenylpropyl ester hydrochloride(TM208),a newly synthesized dithiocarbamate derivative,exhibits antitumor effect in vivo with low toxicity.However,the antitumor e... 4-Methylpiperazine-l-carbodithioc-acid-3-cyano-3,3-diphenylpropyl ester hydrochloride(TM208),a newly synthesized dithiocarbamate derivative,exhibits antitumor effect in vivo with low toxicity.However,the antitumor effect of TM208 in combination with drugs in clinical use for cytotoxic chemotherapy has not been identified.In our study,the antitumor effects and toxicities of TM208 in combination with cisplatin(DDP),cyclophosphamide(CTX) and 5-fluorouracil(5-Fu),respectively,were evaluated in vivo using a transplanted solid-type hepatocarcinoma H_(22) mice model.The results suggested that 5-Fu(5 mg/kg/2d) potentiated the antitumor effect of TM208(100 mg/kg/d) with significantly higher tumor inhibition rates(P0.01) and a slight elevation of toxicity;however,DDP and CTX in combination with TM208 did not exhibit similar enhanced antitumor effect.For further investigation,we found that the TM208 and 5-Fu combination therapy led to G_2/M cell cycle arrest of tumor cells in vivo by downregulating the protein expression of cyclin Bl,cdc2,cdk7,and upregulating the expression of p21 and p53.The protein expression levels of cyclin Dl and cyclin E were also downregulated in tumor cells treated with TM208 and 5-Fu,while those of cdk4 and cdk2 remained unchanged.The change of mRNA expression level of cdc2 was consistent with that of its protein in each group,while the mRNA expression of cyclin B1 remained unchanged among each group.These results demonstrated the dosage regimen of TM208 for combination therapy and could serve as evidence for clinical use of TM208 as an antineoplastic drug. 展开更多
关键词 Combination therapy Hepatocarcinoma H_(22) DITHIOCARBAMATE 5-FLUOROURACIL Cell cycle-related proteins
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