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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Population-specific genetic variants important in susceptibility to cytarabine arabinoside cytotoxicity.
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Population-specific genetic variants important in susceptibility to cytarabine arabinoside cytotoxicity.

机译:特定于人群的遗传变异对阿糖胞苷阿糖胞苷的细胞毒性敏感。

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Cytarabine arabinoside (ara-C) is an antimetabolite used to treat hematologic malignancies. Resistance is a common reason for treatment failure with adverse side effects contributing to morbidity and mortality. Identification of genetic factors important in susceptibility to ara-C cytotoxicity may allow for individualization of treatment. We used an unbiased whole-genome approach using lymphoblastoid cell lines derived from persons of European (CEU) or African (YRI) ancestry to identify these genetic factors. We interrogated more than 2 million single nucleotide polymorphisms (SNPs) for association with susceptibility to ara-C and narrowed our focus by concentrating on SNPs that affected gene expression. We identified a unique pharmacogenetic signature consisting of 4 SNPs explaining 51% of the variability in sensitivity to ara-C among the CEU and 5 SNPs explaining 58% of the variation among the YRI. Population-specific signatures were secondary to either (1) polymorphic SNPs in one population but monomorphic in the other, or (2) significant associations of SNPs with cytotoxicity or gene expression in one population but not the other. We validated the gene expression-cytotoxicity relationship for a subset of genes in a separate group of lymphoblastoid cell lines. These unique genetic signatures comprise novel genes that can now be studied further in functional studies.
机译:阿糖胞苷阿糖胞苷(ara-C)是一种抗代谢药物,用于治疗血液系统恶性肿瘤。耐药性是治疗失败的常见原因,其不良副作用导致发病和死亡。鉴定对ara-C细胞毒性易感性重要的遗传因素可以使治疗个体化。我们使用来自欧洲(CEU)或非洲(YRI)血统的人的淋巴母细胞细胞系的无偏全基因组方法来鉴定这些遗传因素。我们询问了超过200万个单核苷酸多态性(SNP)与ara-C的易感性相关,并通过集中研究影响基因表达的SNP来缩小了研究的范围。我们确定了一个独特的药理学特征,其由4个SNP组成,解释了CEU中对ara-C敏感性的51%的变化,而5个SNP解释了YRI之间58%的变化。特定于人群的特征是继发于(1)一个人群中的多态性SNP但在另一个人群中是单态的,或(2)SNP与一个人群中的细胞毒性或基因表达显着相关,而在另一个人群中则没有。我们验证了单独的一组淋巴母细胞系中基因的子集的基因表达-细胞毒性关系。这些独特的遗传特征包括新的基因,现在可以在功能研究中对其进行进一步研究。

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