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首页> 外文期刊>Journal of the National Cancer Institute >Cisplatin and oxaliplatin toxicity: importance of cochlear kinetics as a determinant for ototoxicity.
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Cisplatin and oxaliplatin toxicity: importance of cochlear kinetics as a determinant for ototoxicity.

机译:顺铂和奥沙利铂毒性:耳蜗动力学作为耳毒性决定因素的重要性。

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BACKGROUND: Cisplatin is a cornerstone anticancer drug with pronounced ototoxicity, whereas oxaliplatin, a platinum derivative with a different clinical profile, is rarely ototoxic. This difference has not been explained. METHODS: In HCT-116 cells, cisplatin (20 microM)-induced apoptosis was reduced by a calcium chelator from 9.9-fold induction (95% confidence interval [CI] = 8.1- to 11.7-fold), to 3.1-fold induction (95% CI = 2.0- to 4.2-fold) and by superoxide scavenging from 9.3-fold (95% CI = 8.8- to 9.8-fold), to 5.1-fold (95% CI = 4.4- to 5.8-fold). A guinea pig model (n = 23) was used to examine pharmacokinetics. Drug concentrations were determined by liquid chromatography with post-column derivatization. The total platinum concentration in cochlear tissue was determined by inductively coupled plasma mass spectrometry. Drug pharmacokinetics was assessed by determining the area under the concentration-time curve (AUC). Statistical tests were two-sided. RESULTS: In HCT-116 cells, cisplatin (20 microM)-induced apoptosis was reduced by a calcium chelator from 9.9-fold induction (95% confidence interval [CI] = 8.1- to 11.7-fold to 3.1-fold induction) (95% CI = 2.0- to 4.2-fold) and by superoxide scavenging (from 9.3-fold, 95% CI = 8.8- to 9.8-fold, to 5.1-fold, 95% CI = 4.4- to 5.8-fold). Oxaliplatin (20 microM)-induced apoptosis was unaffected by calcium chelation (from 7.1- to 6.2-fold induction) and by superoxide scavenging (from 5.9- to 5.6-fold induction). In guinea pig cochlea, total platinum concentration (0.12 vs 0.63 microg/kg, respectively, P = .008) and perilymphatic drug concentrations (238 vs 515 microM x minute, respectively, P < .001) were lower after intravenous oxaliplatin treatment (16.6 mg/kg) than after equimolar cisplatin treatment (12.5 mg/kg). However, after a non-ototoxic cisplatin dose (5 mg/kg) or the same oxaliplatin dose (16.6 mg/kg), the AUC for perilymphatic concentrations was similar, indicating that the two drugs have different cochlear pharmacokinetics. CONCLUSION: Cisplatin- but not oxaliplatin-induced apoptosis involved superoxide-related pathways. Lower cochlear uptake of oxaliplatin than cisplatin appears to be a major explanation for its lower ototoxicity.
机译:背景:顺铂是具有明显耳毒性的基石抗癌药,而奥沙利铂(一种具有不同临床特征的铂衍生物)很少具有耳毒性。这种差异尚未得到解释。方法:在HCT-116细胞中,钙螯合剂将顺铂(20 microM)诱导的凋亡从9.9倍诱导(95%置信区间[CI] = 8.1-降至11.7倍)降低到3.1倍诱导( 95%CI = 2.0-至4.2倍)和超氧化物清除率从9.3倍(95%CI = 8.8至9.8倍)增至5.1倍(95%CI = 4.4至5.8倍)。使用豚鼠模型(n = 23)检查药代动力学。通过柱后衍生化液相色谱法测定药物浓度。通过感应耦合等离子体质谱法测定耳蜗组织中的总铂浓度。通过确定浓度-时间曲线(AUC)下的面积来评估药物药代动力学。统计检验是双面的。结果:在HCT-116细胞中,钙螯合剂将顺铂(20 microM)诱导的凋亡从9.9倍诱导(95%置信区间[CI] = 8.1-诱导13.1倍至3.1倍诱导)降低(95) %CI = 2.0-至4.2-倍)和通过超氧化物清除(从9.3倍,95%CI = 8.8-至9.8-倍,至5.1倍,95%CI = 4.4-至5.8-倍)。奥沙利铂(20 microM)诱导的细胞凋亡不受钙螯合(从7.1到6.2倍的诱导)和超氧化物清除(从5.9到5.6倍的诱导)的影响。在豚鼠耳蜗中,静脉注射奥沙利铂治疗后的总铂浓度(分别为0.12和0.63 microg / kg,P = .008)和淋巴管药物浓度(分别为238和515 microM x分钟,P <.001)较低(16.6毫克/公斤),然后再按等摩尔顺铂处理(12.5毫克/公斤)。但是,在无耳毒性的顺铂剂量(5 mg / kg)或相同的奥沙利铂剂量(16.6 mg / kg)之后,周淋巴浓度的AUC相似,表明两种药物的耳蜗药代动力学不同。结论:顺铂而不是奥沙利铂诱导的细胞凋亡涉及与超氧化物有关的途径。奥沙利铂的耳蜗摄取量低于顺铂,这似乎是其耳毒性较低的主要原因。

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