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Clinical Trials and Observations: A PAI-1 (SERPINE1) polymorphism predicts osteonecrosis in children with acute lymphoblastic leukemia: a report from the Childrens Oncology Group

机译:临床试验和观察:PAI-1(SERPINE1)多态性预测急性淋巴细胞白血病患儿的骨坏死:儿童肿瘤学组的一份报告

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摘要

As glucocorticoid use increased in acute lymphoblastic leukemia, osteonecrosis became an increasingly frequent complication. Besides increased age, host risk factors are poorly defined. We tested whether 12 polymorphisms were associated with osteonecrosis among patients 10 years and older treated on the CCG1882 protocol. Candidate genes (TYMS, MTHFR, ABCB1, BGLAP, ACP5, LRP5, ESR1, PAI-1, VDR, PTH, and PTHR) were chosen based on putative mechanisms underlying osteonecrosis risk. All children received dexamethasone, with doses varying by treatment arm. A PAI-1 polymorphism (rs6092) was associated with risk of osteonecrosis in univariate (P = .002; odds ratio = 2.79) and multivariate (P = .002; odds ratio = 2.89) analyses (adjusting for gender, age, and treatment arm). Overall, 21 of 78 (26.9%) children with PAI-1 GA/AA genotypes, versus 25 of 214 (11.7%) children with GG genotype, developed osteonecrosis. PAI-1 polymorphisms and PAI-1 serum levels have previously been associated with thrombosis. We conclude that PAI-1 genetic variation may contribute to risk of osteonecrosis.
机译:随着在急性淋巴细胞白血病中糖皮质激素的使用增加,骨坏死成为越来越常见的并发症。除了年龄增长外,宿主风险因素的定义还不明确。我们测试了CCG1882方案治疗的10岁及10岁以上患者中是否有12种多态性与骨坏死相关。根据潜在的骨坏死风险机制选择候选基因(TYMS,MTHFR,ABCB1,BGLAP,ACP5,LRP5,ESR1,PAI-1,VDR,PTH和PTHR)。所有儿童均接受地塞米松,剂量因治疗组而异。 PAI-1多态性(rs6092)与单因素(P = 0.002;比值比= 2.79)和多变量(P = 0.002;比值比= 2.89)的骨坏死风险相关(针对性别,年龄和治疗进行调整)臂)。总体而言,PAI-1 GA / AA基因型的78名儿童中有21名(26.9%),而GG基因型的214名儿童中有25名(11.7%)发生了骨坏死。 PAI-1多态性和PAI-1血清水平以前与血栓形成有关。我们得出的结论是,PAI-1基因变异可能会导致骨坏死的风险。

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