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谷胱甘肽S-转移酶基因多态性与个体对顺铂耳毒性作用的敏感性

Glutathione S-transferase genetic polymorphisms and individual sensitivity to the ototoxic effect of cisplatin.

作者信息

Peters U, Preisler-Adams S, Hebeisen A, Hahn M, Seifert E, Lanvers C, Heinecke A, Horst J, Jürgens H, Lamprecht-Dinnesen A

机构信息

Institute for Human Genetics, University of Münster, Germany.

出版信息

Anticancer Drugs. 2000 Sep;11(8):639-43. doi: 10.1097/00001813-200009000-00007.

Abstract

One of the side effects of cisplatin therapy in malignant neoplasms is ototoxicity. This effect shows a wide inter-individual range which is more variable than the pharmacokinetic parameters. Oxidative stress has been implicated in cisplatin ototoxicity. The glutathione S-transferase (GST) supergene family encodes isoenzymes that appear to be critical in protection against oxidative stress. Certain GST loci are polymorphic, demonstrating alleles that are null (GSTM1 and GSTT1), encode low-activity variants (GSTP1) or are associated with variable inducibility (GSTM3). The aim of our study was to investigate genetic risk factors involved in the ototoxicity of cisplatin and to determine whether the polymorphisms in five GST genes affect the individual risk of ototoxicity by cisplatin. Two groups of patients were analyzed in this study: group H, 20 patients early and highly sensitive to the ototoxicity of cisplatin; and group N, 19 patients with no hearing impairment under comparable doses of the drug. We found a protective effect for the GSTM3*B allele with a frequency of 0.18 in the group with normal hearing after therapy versus 0.025 in the group with hearing impairment. (chi2=5.37; p=0.02).

摘要

顺铂治疗恶性肿瘤的副作用之一是耳毒性。这种效应在个体间差异很大,比药代动力学参数的变化更大。氧化应激与顺铂耳毒性有关。谷胱甘肽S-转移酶(GST)超基因家族编码的同工酶似乎在抵抗氧化应激中起关键作用。某些GST基因座是多态性的,表现出无效等位基因(GSTM1和GSTT1)、编码低活性变体的等位基因(GSTP1)或与可变诱导性相关的等位基因(GSTM3)。我们研究的目的是调查顺铂耳毒性相关的遗传风险因素,并确定五个GST基因的多态性是否会影响个体对顺铂耳毒性的易感性。本研究分析了两组患者:H组,20例对顺铂耳毒性早期且高度敏感的患者;N组,19例在相同剂量药物下无听力损害的患者。我们发现,治疗后听力正常组中GSTM3*B等位基因频率为0.18,而听力受损组为0.025,具有保护作用(χ2 = 5.37;p = 0.02)。

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