MDR1 C3435T和GABRG2 C588T基因多态性在癫痫发作中的作用以及MDR1对抗癫痫药物(苯妥英)吸收的影响。
Role of MDR1 C3435T and GABRG2 C588T gene polymorphisms in seizure occurrence and MDR1 effect on anti-epileptic drug (phenytoin) absorption.
作者信息
Ponnala Shivani, Chaudhari Jaydip Ray, Jaleel Momin Abdul, Bhiladvala Dilnawaz, Kaipa Prabhakar Rao, Das Undurti N, Hasan Qurratulain
机构信息
Department of Cancer Biology and Pharmacology, University of Illinois College of Medicine at Peoria, Peoria, Illinois, USA.
出版信息
Genet Test Mol Biomarkers. 2012 Jun;16(6):550-7. doi: 10.1089/gtmb.2011.0225. Epub 2012 Jan 12.
AIMS
To assess the role of MDR1 and gamma-aminobutyric acid receptor-gamma 2 sub unit (GABRG2) gene polymorphism in seizure susceptibility in generalized seizure (GS) and febrile seizure (FS) patients and to evaluate MDR1 C3435T gene polymorphism's role in absorption of the anti-epileptic drug, phenytoin (PHT) in a cohort of patients.
METHODS
One hundred twenty-seven cases of seizure (86 GS and 41 FS) patients were analyzed for MDR1 C3435T and GABRG2 C588T gene polymorphisms using restriction fragment length polymorphism-polymerase chain reaction. Serum PHT levels were analyzed.
RESULTS
The T allele of MDR1 C3435T and GABRG2 C588T gene polymorphism was higher in GS in the Indian population compared with controls. From the data in GS, CT and TT genotype carriers of the MDR1 gene and TT genotype carriers of the GABRG2 gene had more recurrent seizures compared with others. MDR1 T allele carriers in the seizure reoccurrence (SR) group of GS and FS were high compared with the well-controlled seizure group (with no seizures after treatment). TT genotype carriers in SR group were high in FS (with regard to MDR1 gene polymorphism) and GS (with regard to GABRG2 gene polymorphism) compared with a well-controlled seizure group. MDR1 C3435T gene polymorphism affects serum PHT levels (p<0.015). Association of dose PHT ratio and genotype groups of MDR1 C3435T gene polymorphism showed a significant association (p<0.05). MDR1*CC genotype was more common in cases with low serum PHT levels.In addition, it is evident that CT and TT genotype carriers have a high percentage of SR with elevated serum PHT levels.
CONCLUSIONS
Our results show that the MDR1 3435T and GABRG2 588T alleles play a role in seizure occurrence. Moreover, the MDR1 3435T allele also affects PHT absorption. We suggest MDR1 C3435T and GABRG2 C588T genotyping would be of value in order to lower the risk of concentration-dependent drug toxicity and for better patient management.
目的
评估多药耐药基因1(MDR1)和γ-氨基丁酸受体γ2亚基(GABRG2)基因多态性在全身性癫痫(GS)和热性惊厥(FS)患者癫痫易感性中的作用,并在一组患者中评估MDR1 C3435T基因多态性在抗癫痫药物苯妥英钠(PHT)吸收中的作用。
方法
采用限制性片段长度多态性-聚合酶链反应分析127例癫痫患者(86例GS和41例FS)的MDR1 C3435T和GABRG2 C588T基因多态性。分析血清PHT水平。
结果
在印度人群中,与对照组相比,GS患者中MDR1 C3435T和GABRG2 C588T基因多态性的T等位基因频率更高。从GS的数据来看,MDR1基因的CT和TT基因型携带者以及GABRG2基因的TT基因型携带者比其他患者有更多的癫痫复发。与癫痫控制良好组(治疗后无癫痫发作)相比,GS和FS癫痫复发(SR)组中MDR1 T等位基因携带者比例较高。与癫痫控制良好组相比,SR组中FS患者(就MDR1基因多态性而言)和GS患者(就GABRG2基因多态性而言)的TT基因型携带者比例较高。MDR1 C3435T基因多态性影响血清PHT水平(p<0.015)。MDR1 C3435T基因多态性的剂量PHT比值与基因型组之间存在显著关联(p<0.05)。MDR1*CC基因型在血清PHT水平低的患者中更常见。此外,显然CT和TT基因型携带者血清PHT水平升高时癫痫复发率较高。
结论
我们的结果表明,MDR1 3435T和GABRG2 588T等位基因在癫痫发作中起作用。此外,MDR1 3435T等位基因也影响PHT的吸收。我们建议进行MDR1 C3435T和GABRG2 C588T基因分型,以降低浓度依赖性药物毒性风险并实现更好的患者管理。
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