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Characterization of Pt- Pd-spermine complexes for their effect on polyamine pathway and cisplatin resistance in A2780 ovarian carcinoma cells

机译：PtPd-精胺复合物对A2780卵巢癌细胞中多胺途径和顺铂耐药性的影响

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We have previously showed that platinum drugs up-regulate SSAT and SMO and down-regulate ODC and SAMDC in the polyamine pathway. Several studies including our own established that platinum drugs combined with polyamine analog DENSPM produces synergistic increase in SSAT activity with polyamine depletion. Since polyamine pathway is an important therapeutic target, we investigated whether agents containing both platinum and polyamines have similar effects on the polyamine pathway. Two complexes i) Pt-spermine with two cisplatin molecules linked to a spermine in the center and ii) Pd-spermine with similar structure i, but Pd (II) substituted for Pt (II) were analyzed with respect to their effect on the expression of genes in polyamine pathway, SSAT and SMO protein expression, SSAT activity and polyamine pools. Pt-, Pd-spermine complexes induced significant down-regulation of SMO, arginase 2 and NRF-2, with no change in SSAT, while cisplatin as a single agent or in combination with DENSPM induced significant up-regulation of SSAT and SMO. The SSAT activity was not induced by either Pt- or Pd-spermine in A2780 cells; SMO protein levels were significantly elevated compared to the no-drug control and to a similar extent as cisplatin/DENSPM. The Pd-spm treatment induced a fall in putrescine levels to 33%, spermidine to 62% and spermine to 72% while Pt-spm did not induce such a decline. Comparative cytotoxicity studies in A2780 cells indicated the potency to be cisplatin> Pd-Spm>Pt-Spm. Although both complexes exhibit a lower potency, the degree of resistance itself is much lower for Pt-spermine and Pd-spermine in that order (2.5 and 7.5, respectively) compared to cisplatin (~12) as tested in cisplatin resistant A2780/CP cells. These studies suggest that Pd (II)-polyamine complexes may constitute a promising group of inorganic compounds for further studies in the development of novel chemotherapy/adjuvant chemotherapy strategies.

机译：先前我们已经表明，铂类药物在多胺途径中上调SSAT和SMO并下调ODC和SAMDC。包括我们自己在内的数项研究证实，铂类药物与多胺类似物DENSPM结合可在多胺耗尽的情况下协同提高SSAT活性。由于多胺途径是重要的治疗靶点，我们研究了同时含有铂和多胺的药物是否对多胺途径具有相似的作用。两种配合物：i）Pt-精胺，其两个顺铂分子与中心的一个精胺相连； ii）Pd-精胺，具有相似的结构i，但分析了Pd（II）取代了Pt（II）对表达的影响多胺途径中的基因，SSAT和SMO蛋白表达，SSAT活性和多胺库的信息。 Pt-，Pd-精胺复合物诱导SMO，精氨酸酶2和NRF-2显着下调，而SSAT无变化，而顺铂作为单一药物或与DENSPM组合则诱导SSAT和SMO显着上调。 PSAT或Pd精胺在A2780细胞中均未诱导SSAT活性；与无药对照相比，SMO蛋白水平显着升高，并与顺铂/ DENSPM相似。 Pd-spm处理可导致腐胺水平下降至33％，亚精胺下降至62％，精胺下降至72％，而Pt-spm则不会引起这种下降。在A2780细胞中进行的比较细胞毒性研究表明，其效力为顺铂> Pd-Spm> Pt-Spm。尽管两种复合物均显示出较低的效价，但与顺铂耐药的A2780 / CP细胞中测试的顺铂（〜12）相比，对Pt-精胺和Pd-精胺的抵抗程度本身要低得多（分别为2.5和7.5）。。这些研究表明，Pd（II）-多胺复合物可能构成一组有希望的无机化合物，用于进一步研究新型化学疗法/辅助化学疗法的策略。

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期刊名称 Oncology Reports
作者
RAMAKUMAR TUMMALA; PAULA DIEGELMAN; SONIA M. FIUZA; LUIS A.E. BATISTA DE CARVALHO; MARIA PAULA M. MARQUES; DEBORA L. KRAMER; KIMBERLY CLARK; SLAVOLJUB VUJCIC; CARL W. PORTER; LAKSHMI PENDYALA;
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年(卷),期 -1(24),1
年度 -1
页码 15–24
总页数 20
原文格式 PDF
正文语种
中图分类肿瘤学;
关键词
spermine complexes polyamine cisplatin ovarian carcinoma;

机译：精胺复合物;多胺;顺铂;卵巢癌;

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专利

1. Characterization of Pt-, Pd-spermine complexes for their effect on polyamine pathway and cisplatin resistance in A2780 ovarian carcinoma cells. [J] . Tummala R, Diegelman P, Fiuza SM, Oncology reports . 2010,第1期

机译：Pt-，Pd-精胺复合物对A2780卵巢癌细胞中多胺途径和顺铂耐药性的影响。
2. Dinuclear platinum complexes with N,N'-bis(aminoalkyl)-1,4-diaminoanthraquinones as linking ligands. Part II. Cellular processing in A2780 cisplatin-resistant human ovarian carcinoma cells: new insights into the mechanism of resistance [J] . Ganna V. Kalayda, Bart A. J. Jansen, Chris Molenaar, Journal of biological inorganic chemistry: JBIC: a publication of the Society of Biological Inorganic Chemistry . 2004,第4期

机译：具有N，N′-双（氨基烷基）-1，4-二氨基蒽醌作为连接配体的双核铂配合物。第二部分A2780顺铂耐药人卵巢癌细胞的细胞加工：耐药机制的新见解
3. Combination effects of platinum drugs and N1, N11 diethylnorspermine on spermidine/spermine N1-acetyltransferase, polyamines and growth inhibition in A2780 human ovarian carcinoma cells and their oxaliplatin and cisplatin-resistant variants. [J] . Tummala R, Diegelman P, Hector S, Cancer chemotherapy and pharmacology. . 2011,第2期

机译：铂类药物和N1，N11二乙基去甲精胺对A2780人卵巢癌细胞及其奥沙利铂和顺铂耐药变体中亚精胺/亚精胺N1-乙酰基转移酶，多胺和生长抑制的联合作用。
4. Genistein and Cisplatin, Alone and in Combination, Suppress Growth of Human Ovarian Carcinoma Cell line SKOV3 [C] . Tang Li, Li Yu International Conference on Future Materials Engineering and Industry Application . 2012

机译：单独和组合，抑制人卵巢癌细胞系Skov3的生长，单独和联合铂和顺铂和顺铂。
5. E3 Ligase Identified by Differential Display (EDD) Enhances Cell Survival and Cisplatin Resistance in Epithelial Ovarian Cancer and Oral Squamous Cell Carcinoma. [D] . Bradley, Amber Thompson. 2014

机译：通过差异显示（EDD）鉴定的E3连接酶可增强上皮性卵巢癌和口腔鳞状细胞癌的细胞存活率和顺铂耐药性。
6. Combination effects of platinum drugs and N1 N11 diethylnorspermine on spermidine/spermine N1-acetyltransferase polyamines and growth inhibition in A2780 human ovarian carcinoma cells and their oxaliplatin and cisplatin-resistant variants [O] . Ramakumar Tummala, Paula Diegelman, Suzanne Hector, -1

机译：铂类药物和N1N11二乙基去甲精胺对A2780人卵巢癌细胞及其奥沙利铂和顺铂耐药变体中亚精胺/亚精胺N1-乙酰转移酶多胺和生长抑制的联合作用
7. Characterization of Pt-, Pd-spermine complexes for their effect on polyamine pathway and cisplatin resistance in A2780 ovarian carcinoma cells [O] . Pendyala null 2010

机译：pt，pd-精胺复合物对a2780卵巢癌细胞多胺途径和顺铂耐药性的表征

Characterization of Pt- Pd-spermine complexes for their effect on polyamine pathway and cisplatin resistance in A2780 ovarian carcinoma cells

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