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Associations between genetic variants in folate and drug metabolizing pathways and relapse risk in pediatric acute lymphoid leukemia on CCG-1952

机译:叶酸和药物代谢途径的遗传变异与小儿急性淋巴性白血病CCG-1952复发风险之间的关联

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Genetic variation in drug detoxification pathways may influence outcomes in pediatric acute lymphoblastic leukemia (ALL). We evaluated relapse risk and 24 variants in 17 genes in 714 patients in CCG-1961. Three TPMT and 1 MTR variant were associated with increased risks of relapse (rs4712327, OR 3.3, 95%CI 1.2–8.6; rs2842947, OR 2.7, 95%CI 1.1–6.8; rs2842935, OR 2.5, 95%CI 1.1–5.0; rs10925235, OR 4.9, 95%CI 1.1–25.1). One variant in SLC19A1 showed a protective effect (rs4819128, OR 0.5, 95%CI 0.3–0.9). Our study provides data that relapse risk in pediatric ALL is associated with germline variations in TPMT , MTR and SLC19A1. Highlights ? Genetic variants in the folate pathway may influence ALL outcome. ? We evaluated 24 SNPs in 17 genes on relapse risk in pediatric ALL. ? Three TPMT variants were associated with an increased risk of relapse. ? One MTR variant was positively associated with risk of relapse. ? One variant in SLC19A1 showed a protective effect on relapse. ? TPMT, MTR and SLC19A1 are associated with relapse risk in pediatric ALL.
机译:药物排毒途径的遗传变异可能会影响小儿急性淋巴细胞白血病(ALL)的预后。我们在CCG-1961中评估了714例患者中17个基因的复发风险和24个变异。 3种TPMT和1种MTR变异与复发风险增加相关(rs4712327,OR 3.3,95%CI 1.2-8.6; rs2842947,OR 2.7,95%CI 1.1-6.8; rs2842935,OR 2.5,95%CI 1.1-5.0; rs10925235,或4.9,95%CI 1.1–25.1)。 SLC19A1的一个变体显示出保护作用(rs4819128,OR 0.5,95%CI 0.3-0.9)。我们的研究提供的数据表明,小儿ALL的复发风险与TPMT,MTR和SLC19A1的种系变异有关。强调 ?叶酸途径的遗传变异可能影响所有结果。 ?我们评估了小儿ALL复发风险中17个基因中的24个SNP。 ?三种TPMT变异与复发风险增加相关。 ?一种MTR变异与复发风险呈正相关。 ? SLC19A1中的一种变体显示出对复发的保护作用。 ? TPMT,MTR和SLC19A1与小儿ALL的复发风险相关。

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