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首页> 外文期刊>Cancer chemotherapy and pharmacology. >A novel method for quantification of gemcitabine and its metabolites 2',2'-difluorodeoxyuridine and gemcitabine triphosphate in tumour tissue by LC-MS/MS: comparison with (19)F NMR spectroscopy.
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A novel method for quantification of gemcitabine and its metabolites 2',2'-difluorodeoxyuridine and gemcitabine triphosphate in tumour tissue by LC-MS/MS: comparison with (19)F NMR spectroscopy.

机译:通过LC-MS / MS定量测定肿瘤组织中吉西他滨及其代谢物2',2'-二氟脱氧尿苷和吉西他滨三磷酸的新方法:与(19)F NMR光谱比较。

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PURPOSE: To develop a sensitive analytical method to quantify gemcitabine (2',2'-difluorodeoxycytidine, dFdC) and its metabolites 2',2'-difluorodeoxyuridine (dFdU) and 2',2'-difluorodeoxycytidine-5'-triphosphate (dFdCTP) simultaneously from tumour tissue. METHODS: Pancreatic ductal adenocarcinoma tumour tissue from genetically engineered mouse models of pancreatic cancer (KP ( FL/FL ) C and KP ( R172H/+) C) was collected after dosing the mice with gemcitabine. (19)F NMR spectroscopy and LC-MS/MS protocols were optimised to detect gemcitabine and its metabolites in homogenates of the tumour tissue. RESULTS: A (19)F NMR protocol was developed, which was capable of distinguishing the three analytes in tumour homogenates. However, it required at least 100 mg of the tissue in question and a long acquisition time per sample, making it impractical for use in large PK/PD studies or clinical trials. The LC-MS/MS protocol was developed using porous graphitic carbon to separate the analytes, enabling simultaneous detection of all three analytes from as little as 10 mg of tissue, with a sensitivity for dFdCTP of 0.2 ng/mg tissue. Multiple pieces of tissue from single tumours were analysed, showing little intra-tumour variation in the concentrations of dFdC or dFdU (both intra- and extra-cellular). Intra-tumoural variation was observed in the concentration of dFdCTP, an intra-cellular metabolite, which may reflect regions of different cellularity within a tumour. CONCLUSION: We have developed a sensitive LC-MS/MS method capable of quantifying gemcitabine, dFdU and dFdCTP in pancreatic tumour tissue. The requirement for only 10 mg of tissue enables this protocol to be used to analyse multiple areas from a single tumour and to spare tissue for additional pharmacodynamic assays.
机译:目的:建立灵敏的分析方法来定量吉西他滨(2',2'-二氟脱氧胞苷,dFdC)及其代谢物2',2'-二氟脱氧尿苷(dFdU)和2',2'-二氟脱氧胞苷-5'-三磷酸(dFdCTP )同时从肿瘤组织中取出。方法:吉西他滨给药后,从基因工程胰腺癌小鼠模型(KP(FL / FL)C和KP(R172H / +)C)中收集胰腺导管腺癌肿瘤组织。 (19)F NMR光谱法和LC-MS / MS方案进行了优化,以检测肿瘤组织匀浆中的吉西他滨及其代谢产物。结果:开发了一种(19)F NMR方案,该方案能够区分肿瘤匀浆中的三种分析物。但是,它需要至少100 mg的相关组织,每个样品需要很长的采集时间,因此不适用于大型PK / PD研究或临床试验。 LC-MS / MS方案是使用多孔石墨碳分离出分析物而开发的,能够从低至10 mg的组织中同时检测所有三种分析物,dFdCTP的灵敏度为0.2 ng / mg。分析了单个肿瘤的多块组织,显示肿瘤内dFdC或dFdU浓度(细胞内和细胞外)几乎没有变化。在细胞内代谢产物dFdCTP的浓度中观察到肿瘤内变化,这可能反映了肿瘤内不同细胞结构的区域。结论:我们已经开发了一种灵敏的LC-MS / MS方法,该方法能够定量胰腺肿瘤组织中的吉西他滨,dFdU和dFdCTP。仅需10 mg组织的要求就可以将该协议用于分析单个肿瘤的多个区域,并为其他药物动力学测定节省组织空间。

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