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细胞质 5'-核苷酸酶 II 中的遗传变异与 HapMap 细胞系和急性髓系白血病患者中的表达和阿糖胞苷敏感性相关。

Genetic variants in cytosolic 5'-nucleotidase II are associated with its expression and cytarabine sensitivity in HapMap cell lines and in patients with acute myeloid leukemia.

机构信息

Department of Experimental and Clinical Pharmacology, University of Minnesota, Minneapolis, Minnesota 55455, USA.

出版信息

J Pharmacol Exp Ther. 2011 Oct;339(1):9-23. doi: 10.1124/jpet.111.182873. Epub 2011 Jun 28.

Abstract

Cytosolic 5'-nucleotidase II (NT5C2) is involved in the development of 1-β-d-arabinofuranosylcytosine (ara-C) resistance and has been associated with clinical outcome in patients receiving ara-C-based chemotherapy. NT5C2 inactivates ara-C by dephosphorylating ara-C monophosphate to ara-C. In this study, we sequenced NT5C2 in genomic DNA samples from International HapMap project panels with European [Centre d'Etude du Polymorphisme Humain (CEU); n = 90] or African [Yoruba people in Ibadan, Nigeria (YRI); n = 90] ancestry. We identified 41 genetic variants [one insertion-deletion and 40 single nucleotide polymorphisms (SNPs)], including three nonsynonymous SNPs (Y3A, K47R, and Q136R). Twenty-five SNPs were novel and 16 overlapped with the HapMap data. Subjects with African ancestry had NT5C2 mRNA expression levels that was significantly higher than those with European ancestry (p = 0.005). Furthermore, there was a correlation between NT5C2 mRNA expression and ara-C sensitivity in CEU but not in YRI cell lines. None of the nonsynonymous SNPs demonstrated any effect on NT5C2 activity. The genotypes of several SNPs were significantly associated with NT5C2 mRNA expression and/or ara-C sensitivity in CEU cell lines, but very few were significant in YRI cell lines. Of most interest, SNPs (linkage disequilibrium group CEU.12) in the 5'-untranslated region were associated with NT5C2 expression and ara-C sensitivity in HapMap cell lines and with NT5C2 mRNA expression and ara-C sensitivity in diagnostic leukemic blasts from pediatric patients with acute myeloid leukemia. Functional genomics analysis demonstrated that the promoter SNP rs11191612 was associated with altered luciferase activation in reporter assays and altered DNA-protein binding in gel shift assays. These results suggest that genetic variations in NT5C2 influence its expression and, potentially, cellular responses to nucleoside analogs.

摘要

细胞质 5'-核苷酸酶 II(NT5C2)参与 1-β-D-阿拉伯呋喃糖胞苷(ara-C)耐药的发展,并与接受 ara-C 为基础的化疗的患者的临床结果相关。NT5C2 通过将 ara-C 单磷酸去磷酸化为 ara-C 来使 ara-C 失活。在这项研究中,我们对具有欧洲血统(Centre d'Etude du Polymorphisme Humain [CEU];n = 90)或非洲血统(尼日利亚伊巴丹的约鲁巴人 [YRI];n = 90)的国际人类基因组单体型图计划面板的基因组 DNA 样本进行了 NT5C2 测序。我们鉴定了 41 种遗传变异,包括 1 种插入缺失和 40 种单核苷酸多态性(SNP),其中包括 3 种非同义 SNP(Y3A、K47R 和 Q136R)。25 种 SNP 是新的,16 种 SNP 与 HapMap 数据重叠。具有非洲血统的个体的 NT5C2 mRNA 表达水平明显高于具有欧洲血统的个体(p = 0.005)。此外,在 CEU 细胞系中,NT5C2 mRNA 表达与 ara-C 敏感性之间存在相关性,但在 YRI 细胞系中没有相关性。没有非同义 SNP 对 NT5C2 活性有任何影响。在 CEU 细胞系中,几个 SNP 的基因型与 NT5C2 mRNA 表达和/或 ara-C 敏感性显著相关,但在 YRI 细胞系中非常少。最有趣的是,5'非翻译区中的 SNP(连锁不平衡组 CEU.12)与 HapMap 细胞系中的 NT5C2 表达和 ara-C 敏感性以及儿科急性髓系白血病患者的诊断性白血病细胞中的 NT5C2 mRNA 表达和 ara-C 敏感性相关。功能基因组学分析表明,启动子 SNP rs11191612 与报告基因测定中的荧光素酶激活改变和凝胶迁移阻滞测定中的 DNA-蛋白结合改变相关。这些结果表明,NT5C2 中的遗传变异影响其表达,并可能影响细胞对核苷类似物的反应。

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