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首页> 外文期刊>Anticancer Research: International Journal of Cancer Research and Treatment >Dicycloplatin, a Novel Platinum Analog in Chemotherapy: Synthesis of Chinese Pre-clinical and Clinical Profile and Emerging Mechanistic Studies
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Dicycloplatin, a Novel Platinum Analog in Chemotherapy: Synthesis of Chinese Pre-clinical and Clinical Profile and Emerging Mechanistic Studies

机译:双环铂,一种新型铂类化学疗法:中国临床前和临床资料的合成以及新兴的机理研究

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Dicycloplatin (DCP) has better solubility and stability than both cisplatin and carboplatin. Pre-clinical and phase 1 studies demonstrated significant antitumor activity and fewer adverse events than carboplatin. Phase II clinical trials in advanced non-small cell lung cancer found efficacy and safety of DCP-plus-paclitaxel comparable to carboplatin-plus-paclitaxel but better tolerability. This article summarizes and reviews pre-clinical and clinical data for dicycloplatin from the Chinese medical literature. We also report on new mechanistic findings in our laboratory in West Virginia, USA. Patient blood samples were collected for DCP-prototype determination by liquid chromatography mass spectrometry (LC-MS/MS). Molecular studies of ovarian cancer cells treated with DCP or cisplatin were carried out for gene-signature profiling using immunoblotting. Pharmacokinetic mass-spectrometry showed different spectrum profiles of DCP and carboplatin in plasma. Plasma concentration of DCP prototype was 17.1 pLglml 2h after administration, with a peak concentration of 26.9 pigI ml at 0.5 h. Immunoblotting showed DCP-induced activation of DNA damage pathways, including double-phosphorylated checkpoint kinase 2 (CHK2) and breast cancer 1 (BRCA1) and triple-phosphorylated p53, compared to controls. Cisplatin produced a similar profile, with increased p53 protein. DCP and cisplatin activate DNA-damage response through similar pathways. DCP may be more soluble and stable, and better-tolerated.
机译:双环铂(DCP)具有比顺铂和卡铂都更好的溶解度和稳定性。临床前和1期研究表明,与卡铂相比,其具有显着的抗肿瘤活性,且不良事件较少。在晚期非小细胞肺癌的II期临床试验中,发现DCP加紫杉醇的疗效和安全性与卡铂加紫杉醇相当,但耐受性更高。本文总结并综述了来自中国医学文献的双环铂的临床前和临床数据。我们还在美国西弗吉尼亚州的实验室报告了新的机理发现。收集患者血液样本,以通过液相色谱质谱法(LC-MS / MS)测定DCP原型。使用免疫印迹法对DCP或顺铂处理的卵巢癌细胞进行了分子研究,以进行基因特征分析。药代动力学质谱显示血浆中DCP和卡铂的光谱特征不同。给药后2小时,DCP原型的血浆浓度为17.1pLgml / ml,在0.5h时的峰值浓度为26.9pg / ml。与对照相比,免疫印迹显示DCP诱导的DNA损伤途径的激活,包括双磷酸化的检查点激酶2(CHK2)和乳腺癌1(BRCA1)和三磷酸化的p53。顺铂产生相似的图谱,但p53蛋白增加。 DCP和顺铂通过相似的途径激活DNA损伤反应。 DCP可能更易溶,更稳定且耐受性更好。

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