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UGT1A1基因多态性可预测中国癌症患者中伊立替康引起的严重中性粒细胞减少和腹泻。

UGT1A1 Gene Polymorphism Predicts Irinotecan-Induced Severe Neutropenia and Diarrhea in Chinese Cancer Patients.

作者信息

Peng Hongwei, Duan Zhouping, Pan Decheng, Wen Jinhua, Wei Xiaohua

出版信息

Clin Lab. 2017 Sep 1;63(9):1339-1346. doi: 10.7754/Clin.Lab.2017.170105.

DOI:10.7754/Clin.Lab.2017.170105
PMID:28879724
Abstract

BACKGROUND

Irinotecan was widely used in colon cancer and lung cancer, etc., and adverse reactions occur some times. The primary aim of this research is to investigate the association between UGT1A1 gene polymorphisms and irinotecan-related adverse effect in Chinese Han population with a novel kind of gene chip technology.

METHODS

UGT1A1*6/*28 gene polymorphisms were detected by PCR and gene chip as well as sequencing. The correlation between UGT1A1 gene polymorphisms and severe delayed diarrhea or neutropenia and effect on response rate and progression-free survival were analyzed.

RESULTS

A total of 106 patients receiving irinotecan-based regimens and with detected UGT1A1 gene polymorphisms were enrolled in this research. According to our results, no significant differences of severe diarrhea were found in patients with UGT1A1*6 genotypes (p = 0.608). However, the incidence of severe diarrhea in patients with TA7/7 genotype (66.7%, 4/6) was significantly higher than that in patients with TA6/7 (31.5%, 6/19) or TA6/6 (1.28%, 1/78) genotypes (p < 0.001). The incidence of severe hematologic toxicity in patients with AA (100%, 2/2) was significantly higher than that in patients with GA (33.3%, 7/21) or GG genotype (7.23%, 6/83) (p = 0.011).

CONCLUSIONS

In terms of irinotecan-based regimens in cancers, UGT1A16 plays a more vital role in hematologic toxicity (p = 0.011) whereas UGT1A128 get more involved in diarrhea (p < 0.001).

摘要

背景

伊立替康广泛应用于结肠癌、肺癌等疾病的治疗,且有时会出现不良反应。本研究的主要目的是采用一种新型基因芯片技术,调查中国汉族人群中UGT1A1基因多态性与伊立替康相关不良反应之间的关联。

方法

采用聚合酶链反应(PCR)、基因芯片及测序技术检测UGT1A1*6/*28基因多态性。分析UGT1A1基因多态性与严重迟发性腹泻或中性粒细胞减少之间的相关性,以及对缓解率和无进展生存期的影响。

结果

本研究共纳入106例接受含伊立替康方案治疗且检测了UGT1A1基因多态性的患者。根据研究结果,UGT1A1*6基因型患者的严重腹泻发生率无显著差异(p = 0.608)。然而,TA7/7基因型患者的严重腹泻发生率(66.7%,4/6)显著高于TA6/7基因型患者(31.5%,6/19)或TA6/6基因型患者(1.28%,1/78)(p < 0.001)。AA基因型患者的严重血液学毒性发生率(100%,2/2)显著高于GA基因型患者(33.3%,7/21)或GG基因型患者(7.23%,6/83)(p = 0.011)。

结论

在癌症的含伊立替康方案中,UGT1A16在血液学毒性方面起更重要作用(p = 0.011),而UGT1A128在腹泻方面影响更大(p < 0.001)。

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