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奥沙利铂所致周围神经病变与ERCC1和GSTP1基因多态性之间的关联。

Associations between oxaliplatin-induced peripheral neuropathy and polymorphisms of the ERCC1 and GSTP1 genes.

作者信息

Inada M, Sato M, Morita S, Kitagawa K, Kawada K, Mitsuma A, Sawaki M, Fujita K, Ando Y

机构信息

Department of Clinical Oncology and Chemotherapy, Nagoya University Hospital, Nagoya, Japan.

出版信息

Int J Clin Pharmacol Ther. 2010 Nov;48(11):729-34. doi: 10.5414/cpp48729.

DOI:10.5414/cpp48729
PMID:20979931
Abstract

OBJECTIVE

Oxaliplatin-induced chronic neuropathy is cumulative and dose-limiting; reliable predictors and determination of the mechanism of this toxic effect are needed.

METHODS

We retrospectively studied 51 Japanese adults with colorectal cancer who had received oxaliplatin-based chemotherapy to explore the pharmacogenetic association between oxaliplatin-induced neuropathy and polymorphisms of the excision repair cross-complementation Group 1 (ERCC1) and glutathione-S-transferases pi 1 (GSTP1) genes.

RESULTS

For the ERCC1 C118T polymorphism, Grade 1 chronic neuropathy developed earlier in patients with C/T and T/T genotypes (median number of treatment cycles at onset = 6) than in those with the reference C/C genotype (7 cycles; p = 0.0162 by the generalized Wilcoxon test). For the GSTP1 Ile105Val polymorphism, chronic neuropathy developed earlier in patients with the reference Ile/Ile genotype (6 cycles) than in those with Ile/Val and Val/Val genotypes (9 cycles; p = 0.0321). ERCC1 C118T and GSTP1 Ile105Val polymorphisms were not significantly associated with an increased risk of developing Grade 2 or more severe chronic neuropathy.

CONCLUSIONS

Our results suggest that ERCC1, C118T and GSTP1 Ile105Val polymorphisms are more strongly related to the time until onset of neuropathy than to the grade of neuropathy. Most likely these polymorphisms influence patients' sensitivity to neuropathy.

摘要

目的

奥沙利铂诱导的慢性神经病变具有累积性且限制剂量;需要可靠的预测指标并确定这种毒性作用的机制。

方法

我们回顾性研究了51例接受以奥沙利铂为基础化疗的日本成年结直肠癌患者,以探讨奥沙利铂诱导的神经病变与切除修复交叉互补组1(ERCC1)和谷胱甘肽-S-转移酶pi 1(GSTP1)基因多态性之间的药物遗传学关联。

结果

对于ERCC1 C118T多态性,C/T和T/T基因型患者(发病时治疗周期中位数 = 6)1级慢性神经病变的发生时间早于参考C/C基因型患者(7个周期;广义Wilcoxon检验,p = 0.0162)。对于GSTP1 Ile105Val多态性,参考Ile/Ile基因型患者(6个周期)慢性神经病变的发生时间早于Ile/Val和Val/Val基因型患者(9个周期;p = 0.0321)。ERCC1 C118T和GSTP1 Ile105Val多态性与发生2级或更严重慢性神经病变的风险增加无显著关联。

结论

我们的结果表明,ERCC1 C118T和GSTP1 Ile105Val多态性与神经病变发病时间的相关性比与神经病变严重程度的相关性更强。这些多态性很可能影响患者对神经病变的敏感性。

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