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Association of CTH variant with sinusoidal obstruction syndrome in children receiving intravenous busulfan and cyclophosphamide before hematopoietic stem cell transplantation

机译:造血干细胞移植前接受静脉注射白消安和环磷酰胺的儿童CTH变异与窦性阻塞综合征的关系

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摘要

Sinusoidal obstruction syndrome (SOS) is a severe complication of hematopoietic stem cell transplantation (HSCT) that can be fatal, often attributed to the conditioning regimen prior to HSCT. We evaluated the association of SOS risk with gene variants in cystathionase (CTH), an enzyme involved in glutathione synthesis, in 76 children receiving intravenous busulfan (Bu) before HSCT. Our results indicated an association with CTHc.1364 G>T (ORTT=10.6, 95% confidence interval (CI)=2.16, 51.54) and SOS risk, which was sex dependent (female patients, ORTT=21.82, 95% CI=3.590–132.649). The interaction between CTHc.1364 G>T and another risk variant (GSTA1*B) was explored. A recessive model with the use of GSTA1*B*B and CTH c.1364 TT genotypes proved to be useful at predicting SOS occurrence, indicating the possibility of using these gene variants as markers of SOS occurrence and to further individualize preemptive treatment aimed at reducing SOS incidence.
机译:窦性阻塞综合征(SOS)是造血干细胞移植(HSCT)的严重并发症,可能是致命的,通常归因于HSCT之前的调理方案。我们评估了76名接受HSCT前静脉注射白消安(Bu)的儿童中SOS风险与胱硫醚酶(CTH)基因变异的关联,胱硫醚酶是一种与谷胱甘肽合成有关的酶。我们的结果表明与CTHc.1364 G> T(ORTT = 10.6,95%置信区间(CI)= 2.16,51.54)和SOS风险相关,这与性别有关(女性患者,ORTT = 21.82,95%CI = 3.590) –132.649)。探索了CTHc.1364 G> T与另一种风险变体(GSTA1 * B)之间的相互作用。事实证明,使用GSTA1 * B * B和CTH c.1364 TT基因型的隐性模型可用于预测SOS发生,表明有可能使用这些基因变体作为SOS发生的标志,并进一步个性化旨在降低SOS的抢先治疗SOS发生率。

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