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因报告的中枢神经系统症状而停用依非韦伦的药物遗传学似乎因种族而异。

Pharmacogenetics of efavirenz discontinuation for reported central nervous system symptoms appears to differ by race.

作者信息

Leger Paul, Chirwa Sanika, Turner Megan, Richardson Danielle M, Baker Paxton, Leonard Michael, Erdem Husamettin, Olson Lana, Haas David W

机构信息

aDepartment of Medicine bVanderbilt Technologies for Advanced Genomics Analysis and Research Design (VANGARD) cVanderbilt Technologies for Advanced Genomics (VANTAGE), Vanderbilt University Medical Center dDepartment of Medicine, Pharmacology, Pathology, Microbiology & Immunology, Vanderbilt University School of Medicine eDepartment of Neuroscience & Pharmacology, Meharry Medical College, Nashville, Tennessee, USA.

出版信息

Pharmacogenet Genomics. 2016 Oct;26(10):473-80. doi: 10.1097/FPC.0000000000000238.

DOI:10.1097/FPC.0000000000000238
PMID:27509478
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5014672/
Abstract

BACKGROUND

Efavirenz frequently causes central nervous system (CNS) symptoms. We evaluated genetic associations with efavirenz discontinuation for CNS symptoms within 12 months of treatment initiation.

METHODS

Patients had initiated efavirenz-containing regimens at an HIV primary care clinic in the Southeastern United States and had at least 12 months of follow-up data. Polymorphisms in CYP2B6 and CYP2A6 defined efavirenz metabolizer categories. Genome-wide genotyping enabled adjustment for population stratification.

RESULTS

Among 563 evaluable patients, 99 (17.5%) discontinued efavirenz within 12 months, 29 (5.1%) for CNS symptoms. The hazard ratio (HR) for efavirenz discontinuation for CNS symptoms in slow versus extensive metabolizers was 4.9 [95% confidence interval (CI): 1.9-12.4; P=0.001]. This HR in Whites was 6.5 (95% CI: 2.3-18.8; P=0.001) and 2.6 in Blacks (95% CI: 0.5-14.1; P=0.27). Considering only slow metabolizers, the HR in Whites versus Blacks was 3.1 (95% CI: 0.9-11.0; P=0.081). The positive predictive value of slow metabolizer genotypes for efavirenz discontinuation was 27% in Whites and 11% in Blacks.

CONCLUSION

Slow metabolizer genotypes were associated significantly with efavirenz discontinuation for reported CNS symptoms. This association was considerably stronger in Whites than in Blacks.

摘要

背景

依非韦伦常引起中枢神经系统(CNS)症状。我们评估了治疗开始后12个月内因CNS症状停用依非韦伦的基因关联。

方法

患者在美国东南部一家HIV初级保健诊所开始含依非韦伦的治疗方案,并至少有12个月的随访数据。CYP2B6和CYP2A6的多态性定义了依非韦伦代谢者类别。全基因组基因分型可对人群分层进行调整。

结果

在563例可评估患者中,99例(17.5%)在12个月内停用依非韦伦,29例(5.1%)因CNS症状停用。慢代谢者与快代谢者相比,因CNS症状停用依非韦伦的风险比(HR)为4.9[95%置信区间(CI):1.9 - 12.4;P = 0.001]。白人中的这一HR为6.5(95% CI:2.3 - 18.8;P = 0.001),黑人中为2.6(95% CI:0.5 - 14.1;P = 0.27)。仅考虑慢代谢者,白人相对于黑人的HR为3.1(95% CI:0.9 - 11.0;P = 0.081)。慢代谢者基因型对依非韦伦停用的阳性预测值在白人中为27%,在黑人中为11%。

结论

慢代谢者基因型与因报告的CNS症状停用依非韦伦显著相关。这种关联在白人中比在黑人中强得多。

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