Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, MN, USA.
Leuk Res. 2012 Jan;36(1):59-66. doi: 10.1016/j.leukres.2011.06.020. Epub 2011 Jul 8.
CYP2B6, CYP2C19, ABCC4, and SOD2 have been implicated in adverse drug reactions and survival after cyclophosphamide (CPA) treatment. 110 BMT patients who received high dose CPA treatment were genotyped for variants in these genes and the results were correlated with toxicity and relapse. CYP2B6 genotype significantly influenced overall toxicity suggesting active CYP2B6 alleles led to higher rates of overall toxicity. The p.R487C deficiency allele was significantly associated with a lower rate of overall toxicity and a higher rate of relapse. SOD2 rs4880 V16A polymorphism was associated with significantly less CPA-related overall toxicity and significantly lower relapse rates by Kaplan-Meier analysis although the SOD2 finding regarding relapse was not significant when evaluated by the cumulative incidence function.
CYP2B6、CYP2C19、ABCC4 和 SOD2 与环磷酰胺 (CPA) 治疗后的不良反应和生存有关。110 名接受高剂量 CPA 治疗的 BMT 患者对这些基因的变异进行了基因分型,并将结果与毒性和复发相关联。CYP2B6 基因型显著影响整体毒性,提示活性 CYP2B6 等位基因导致更高的整体毒性发生率。p.R487C 缺陷等位基因与整体毒性发生率较低和复发率较高显著相关。通过 Kaplan-Meier 分析,SOD2 rs4880 V16A 多态性与明显较少的 CPA 相关的整体毒性和明显较低的复发率相关,尽管 SOD2 关于复发的发现通过累积发生率函数评估时并不显著。
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