High field proton NMR investigations of the metabolic profiles of multidrug-sensitive and -resistant leukaemic cell lines: evidence for diminished taurine levels in multidrug-resistant cells.

X R Jiang, M Yang, C J Morris, A C Newland, D P Naughton, D R Blake, Z Zhang, M C Grootveld
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引用次数: 8

Abstract

High field proton (1H) nuclear magnetic resonance (NMR) spectroscopy has for the first time been employed to investigate and compare the metabolic profiles of vinblastine-sensitive and -resistant T-lymphoid leukaemic cell lines (CCRF-CEM and CEM/VLB100 respectively) and evidence is presented for a significantly lower taurine content in the CEM/VLB100 resistant subline when expressed relative to that of its drug-sensitive parental counterpart. These data suggest differences in the nature and relative involvements of taurine biosynthetic pathways between the two cell lines, a phenomenon that may be related to their differing sensitivities towards chemotherapeutic agents such as adriamycin which promote the generation of cytotoxic reactive oxygen species (ROS) in vivo. However, the 1H NMR data obtained provided no evidence for an increased metabolic consumption of hypotaurine (a metabolic precursor of taurine with powerful .OH radical scavenging properties) in CCRF-CEM cells since differences observed in the hypotaurine: taurine concentration ratio between the drug-sensitive and -resistant cell lines were not statistically significant. Furthermore, hypotaurine is unlikely to compete with alternative endogenous .OH radical scavengers present such as lactate since its level in either of the two cell lines investigated (ca. 6.0 x 10(-8) mol./10(8) cells) is insufficient for it to act as an antioxidant in this context. The biochemical and therapeutic significance of these results are discussed.

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多药敏感和耐药白血病细胞系代谢谱的高场质子核磁共振研究:多药耐药细胞中牛磺酸水平降低的证据。
高场质子(1H)核磁共振(NMR)光谱首次被用于研究和比较长春花碱敏感和耐药t淋巴白血病细胞系(分别为CCRF-CEM和CEM/VLB100)的代谢谱,并有证据表明,相对于对药物敏感的亲本,CEM/VLB100耐药亚系的牛磺酸含量显著降低。这些数据表明两种细胞系之间牛磺酸生物合成途径的性质和相对参与的差异,这一现象可能与它们对化疗药物(如阿霉素)的不同敏感性有关,阿霉素可促进体内细胞毒性活性氧(ROS)的产生。然而,所获得的1H NMR数据没有提供证据表明CCRF-CEM细胞中次牛磺酸(牛磺酸的代谢前体,具有强大的。oh自由基清除能力)的代谢消耗增加,因为在药物敏感和耐药细胞系之间观察到的次牛磺酸:牛磺酸浓度比的差异没有统计学意义。此外,次牛磺酸不太可能与其他内源性oh自由基清除剂(如乳酸)竞争,因为在研究的两种细胞系中(约6.0 × 10(-8) mol /10(8)个细胞),次牛磺酸的水平不足以在这种情况下发挥抗氧化剂的作用。讨论了这些结果的生化和治疗意义。
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