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甾体-双膦酸酯化合物的合成及防治骨质疏松作用研究 被引量:3
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作者 郑虎 吴勇 +1 位作者 陈建 翁玲玲 《药学学报》 CAS CSCD 北大核心 1998年第5期339-343,共5页
双膦酸盐有趋骨性并有抗骨质疏松症活性。甾体激素常用于骨质疏松症的防治。本文设计合成了7个甾体双膦酸酯偶合物,希望新化合物既有趋骨性又有协同抗骨质疏松作用,能得到疗效好副作用小的骨靶向化合物的先导物。经骨细胞培养试验... 双膦酸盐有趋骨性并有抗骨质疏松症活性。甾体激素常用于骨质疏松症的防治。本文设计合成了7个甾体双膦酸酯偶合物,希望新化合物既有趋骨性又有协同抗骨质疏松作用,能得到疗效好副作用小的骨靶向化合物的先导物。经骨细胞培养试验表明,化合物有促进骨形成作用。 展开更多
关键词 双膦酸盐 甾体 靶向化合物 促骨形成 骨质疏松
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DNA靶向手性钌(Ⅱ)配合物的合成、表征及其抗肿瘤作用 被引量:3
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作者 王蓓 吴琼 +3 位作者 孙福强 王淇 谢华松 梅文杰 《广东药学院学报》 CAS 2011年第5期459-463,共5页
目的设计合成2个手性钌(Ⅱ)多吡啶配合物Λ-[Ru(bpy)2(p-NPIP)](PF6)2.2H2O(1)和Λ-[Ru(bpy)2(p-tFPIP)](PF6)2.2H2O(2),评价其体外抗肿瘤活性,并对配合物2与DNA分子的识别机制及其光裂解作用进行初步探讨。方法采用MTT方法评价手性钌(... 目的设计合成2个手性钌(Ⅱ)多吡啶配合物Λ-[Ru(bpy)2(p-NPIP)](PF6)2.2H2O(1)和Λ-[Ru(bpy)2(p-tFPIP)](PF6)2.2H2O(2),评价其体外抗肿瘤活性,并对配合物2与DNA分子的识别机制及其光裂解作用进行初步探讨。方法采用MTT方法评价手性钌(Ⅱ)配合物1和2对肿瘤细胞生长的抑制,并采用电子吸收光谱、荧光光谱和黏度试验等方法研究手性钌配合物2与DNA的分子识别机制;采用凝胶电泳试验评价配合物2对DNA分子的光裂解作用。结果手性钌(Ⅱ)配合物2能够抑制肿瘤细胞的生长,特别是对HO8910PM细胞生长的抑制率IC50=47.8μmol.L-1,与同等条件下顺铂的抗肿瘤活性相当;研究结果表明插入配体上取代基的电子效应对其抗肿瘤活性有较大影响;光谱学试验证明钌多吡啶配合物1和2通过插入方式与DNA结合(Kb=2.86×105 L.mol-1)。结论手性钌(Ⅱ)多吡啶配合物具有一定的抗肿瘤活性,其抗肿瘤活性与钌(Ⅱ)配合物的分子结构及其与DNA分子契合能力相关。 展开更多
关键词 手性钌配合物 靶向化合物 分子识别 抗肿瘤
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药物制剂信息文摘
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《辽宁医药》 2005年第1期54-58,共5页
可溶性银杏叶提取物制剂;从植物中提取活性成分;肝细胞靶向化合物;一种头孢菌素的缓控释制剂处方;微观排列药物转运包衣法;生物可降解微囊的制备;
关键词 药物制剂 可溶性银杏叶提取物制剂 活性成分 肝细胞 靶向化合物 头孢菌素
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In Vitro Inhibition of β-Hematin by 2, 4-Diamino-6- Mercaptopyrimidine & 2-Mercaptopyrimidine
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作者 Amneh Aljazzar Qasem Abu-Remeleh +2 位作者 Abd-Alkareem Alsharif Mohammad Abul Haj Mutaz Akkawi 《Journal of Chemistry and Chemical Engineering》 2010年第12期57-61,共5页
Malaria is a disease that has drawn worldwide attention due to the alarming rise of mortality rates particularly in third world countries. During the Plasmodium parasite intraerythrocytic life cycle, metabolic process... Malaria is a disease that has drawn worldwide attention due to the alarming rise of mortality rates particularly in third world countries. During the Plasmodium parasite intraerythrocytic life cycle, metabolic processes include the formation of hemozoin or malaria pigment. This pigment functions in the prevention of oxygen radical-mediated damage to the parasite. Drugs targeting hemozoin formation such as chloroquine and amodaquine are effective and are still used, but recently Plasmodium parasites have become resistant to these drugs, especially against chloroquine. In this study we looked at the potential use of two heterocyclic pyrimidine derivatives as anti-malaria drugs; 2,4-Diamino-6-Mercaptopyrimidine (DAMP) and 2-Mercaptopyrimidine (2-MP). These compounds bear various coordination sites that enable them to react with metal ions to form coordination compounds. We used two methods for testing the inhibition of ferriprotoporphyrin IX (FP) biomineralisation: semi-quantitative microassay used by Deharo, and a quantitative assay used by G. Blaner and M. Akkawi. We report here the finding that (DAMP) has an in vitro inhibitory effect on I%hematin formation at concentrations and magnitude of nearly similar order to that of chloroquine, 2-MP was found to be effective but to a lower degree than DAMP. 展开更多
关键词 2 4-diamino-6-mercaptopyrimidine (DAMP) 2-mercaptopyrimidine (2-MP) [3-hematin Hemozoin Ferriprotopor-phyrin IX (FP) biomineralisation chloroquine diphosphate (CQ).
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Co-delivery of paclitaxel and gemcitabine via folic acid-conjugated polymeric multi-drug nanoparticles (FA-PMDNPs) for the treatment of breast cancer 被引量:2
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作者 Meng Lei Xueyuan Wang +4 位作者 Hang Miao Jia Wang Sijia Sha Jiang Zhu Yongqiang Zhu 《Journal of Chinese Pharmaceutical Sciences》 CAS CSCD 2020年第10期701-710,共10页
Multi-drug delivery focuses on different signaling pathways in cancer cells and has synergistic antiproliferative effects.In this manuscript,we developed folic acid(FA)-conjugated polymeric multi-drug nanoparticles(FA... Multi-drug delivery focuses on different signaling pathways in cancer cells and has synergistic antiproliferative effects.In this manuscript,we developed folic acid(FA)-conjugated polymeric multi-drug nanoparticles(FA-PMDNPs)consisting of poly-L-lysine(PLL)and poly glutamic-conjugated PTX/GEM(PGA-PTX and PGA-GEM)for FA receptor-targeted synergistic breast cancer therapy.The carboxyl-rich structure of PGA provided plenty reaction sites and negative charge for drug loading.Transmission electron microscopy(TEM)results showed that FA-PMDNPs had uniform particle size and spherical morphology.The hemolysis study proved that FA-PMDNPs had good biocompatibility.In vitro cell viability and in vivo studies showed that FA-PMDNPs more effectively inhibited the proliferation of FA receptor(FR)-overexpressing breast cancer cells(4T1)than the pure drugs.Consequently,these results demonstrated that FA-PMDNPs could be effectively targeted at cancer cells compared with free drugs,indicating their strong potential as efficient multi-drug-carrying nano-platforms for cancer treatment. 展开更多
关键词 FA-receptor targeted Polymeric nanoparticles Combined chemotherapy Breast cancer Drug targeted delivery
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