Yampayon Kittika, Sukasem Chonlaphat, Limwongse Chanin, Chinvarun Yotin, Tempark Therdpong, Rerkpattanapipat Ticha, Kijsanayotin Pornpimol
Department of Pharmacology and Physiology, Faculty of Pharmaceutical Sciences, Chulalongkorn University, 254 Phyathai Rd.,Wangmai, Patumwan, Bangkok, 10330, Thailand.
Division of Pharmacogenetics and Personalized Medicine, Department of Pathology, Faculty of Medicine Ramathibodi Hospital, Mahidol University, Bangkok, Thailand.
Eur J Clin Pharmacol. 2017 Jul;73(7):855-865. doi: 10.1007/s00228-017-2250-2. Epub 2017 Apr 8.
The purpose of this study was to investigate the association of genetic factors including variants in HLA-B and CYP2C genes and non-genetic factors with phenotype-specific phenytoin (PHT)-induced severe cutaneous adverse reactions (SCARs) in Thai patients.
Thirty-six PHT-induced SCAR cases (15 Stevens-Johnson syndrome (SJS) and 21 drug rash with eosinophilia and systemic symptoms (DRESS)/drug hypersensitivity syndrome (DHS)) and 100 PHT-tolerant controls were studied. Variants in HLA-B, CYP2C9, and CYP2C19 genes were genotyped. Fisher's exact test and multiple logistic regression analysis were performed to test the association of genetic and non-genetic factors with specific type of SCARs.
Multiple logistic regression models showed that genetic and non-genetic factors associated with PHT-induced SCARs were specified to its phenotype. HLA-B13:01, HLA-B56:02/04, CYP2C193, and omeprazole co-medication were strong risk factors of DRESS/DHS (adjusted OR = 13.29, p = 0.0001; adjusted OR = 56.23, p = 0.0007; adjusted OR = 6.75, p = 0.0414; and adjusted OR = 9.21, p = 0.0020, respectively). While CYP2C93 and having Chinese ancestry were significant risk factors of SJS (adjusted OR = 10.41, p = 0.0042 and adjusted OR = 5.40, p = 0.0097, respectively). Combined genetic and non-genetic risk factors optimized sensitivity and increased specificity for predicting PHT-induced SCARs.
This study showed that distinct genetic markers were associated with phenotype-specific PHT-induced SCARs. Non-genetic factor, omeprazole co-medication, was strongly associated with PHT-induced DRESS/DHS in addition to variants in HLA-B and CYP2C genes. Combined markers may be better predictors for PHT-induced SCARs.
本研究旨在调查包括HLA - B和CYP2C基因变异在内的遗传因素以及非遗传因素与泰国患者中苯妥英(PHT)诱导的特定表型严重皮肤不良反应(SCARs)之间的关联。
对36例PHT诱导的SCAR病例(15例史蒂文斯 - 约翰逊综合征(SJS)和21例伴有嗜酸性粒细胞增多和全身症状的药疹(DRESS)/药物超敏反应综合征(DHS))以及100例PHT耐受对照进行研究。对HLA - B、CYP2C9和CYP2C19基因的变异进行基因分型。采用Fisher精确检验和多元逻辑回归分析来检验遗传和非遗传因素与特定类型SCARs的关联。
多元逻辑回归模型显示,与PHT诱导的SCARs相关的遗传和非遗传因素因其表型而异。HLA - B13:01、HLA - B56:02/04、CYP2C193以及奥美拉唑联合用药是DRESS/DHS的强危险因素(调整后的OR分别为13.29,p = 0.0001;调整后的OR = 56.23,p = 0.0007;调整后的OR = 6.75,p = 0.0414;调整后的OR = 9.21,p = 0.0020)。而CYP2C93和具有中国血统是SJS的显著危险因素(调整后的OR分别为10.41,p = 0.0042和调整后的OR = 5.40,p = 0.0097)。遗传和非遗传危险因素的组合优化了预测PHT诱导的SCARs的敏感性并提高了特异性。
本研究表明,不同的遗传标记与PHT诱导的特定表型的SCARs相关。除了HLA - B和CYP2C基因的变异外,非遗传因素奥美拉唑联合用药与PHT诱导的DRESS/DHS密切相关。联合标记可能是PHT诱导的SCARs的更好预测指标。
Zotero 插件