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中国临床药理学与治疗学 ›› 2018, Vol. 23 ›› Issue (2): 154-158.doi: 10.12092/j.issn.1009-2501.2018.02.007

• 临床药理学 • 上一篇    下一篇

OCT2、MDR1基因多态性与婴幼儿万古霉素血药浓度及临床疗效的相关性研究

陈曜曜1,史道华1,刘光华2,牛培广1,刘柏晨1   

  1. 1 福建医科大学附属福建省妇幼保健院药剂科,2 儿科,福州 350001,福建
  • 收稿日期:2017-08-03 修回日期:2017-09-07 出版日期:2018-02-26 发布日期:2018-03-02
  • 通讯作者: 史道华,男,博士,主任药师,教授,硕士生导师,研究方向:临床药学。 Tel: 13600818237 E-mail: shidh@yeah.net
  • 作者简介:陈曜曜,女,本科,主管药师,研究方向:临床药学。 Tel: 13960797427 E-mail: fjfycyy@163.com
  • 基金资助:

    福建省妇幼保健院科研课题(妇保院研15-15)

Effects of OCT2 and MDR1 gene polymorphisms on vancomycin concentration and clinical efficacy in infants

CHEN Yaoyao1,SHI Daohua1,LIU Guanghua2,NIU Peiguang1,LIU Baichen1   

  1. 1 Department of Pharmacy, 2 Department of Pediatrics,Fujian Provincial Maternity and Children's Hospital, Affiliated Hospital of Fujian Medical University, Fuzhou 350001, Fujian, China
  • Received:2017-08-03 Revised:2017-09-07 Online:2018-02-26 Published:2018-03-02

摘要:

目的: 考察有机阳离子转运体2(OCT2)和多药耐药基因1(MDR1)的基因多态性与婴幼儿万古霉素稳态谷浓度及临床疗效的相关性。方法: 收集91例万古霉素治疗的婴幼儿患者血样,酶免疫放大分析法测定万古霉素血药浓度,聚合酶链式反应(PCR)和DNA测序技术检测基因分型。比较OCT2 G808T(rs316019)和MDR1 C3435T(rs1045642)不同基因型对万古霉素谷浓度及临床疗效的影响。结果: 91例患者中,谷浓度达到10~20 μg/mL的比例为16.5%;5~<10 μg/mL和10~20 μg/mL浓度范围万古霉素的临床有效率(88%,93.3%)显著高于5 μg/mL以下浓度(44%)(P<0.05),同时5~<10 μg/mL和10~20 μg/mL浓度范围万古霉素的临床有效率相近。OCT2 G808T纯合突变型(TT)患者万古霉素谷浓度(10.15±2.35) μg/mL和谷浓度/剂量比(0.98±0.27) μg·mL-1·mg-1·kg均显著高于野生型(GG)患者(6.92±2.83) μg/mL和(0.59±0.22) μg·mL-1·mg-1·kg(P<0.05);同时,TT型患者临床有效率(100%)明显高于GG型(73.2%)(P<0.05);而MDR1 C3435T突变型和野生型患者的万古霉素谷浓度、谷浓度/剂量比及临床疗效相近(P>0.05)。结论: OCT2 G808T基因突变可能与婴幼儿患者万古霉素的稳态谷浓度及临床疗效相关。

关键词: 万古霉素, 药物转运体, 基因多态性, 血药浓度, 婴幼儿

Abstract:

AIM: To study the effects of organic cation transporter 2 (OCT2) and multidrug resistance gene 1 (MDR1) gene polymorphisms on plasma concentration and clinical efficacy of vancomycin in infants. METHODS: Ninety-one infants that treated with vancomycin were recruited. The plasma concentrations of vancomycin were measured by enzyme multiplied immunoassay technique. The genotypes of OCT2 G808T (rs316019) and MDR1 C3435T (rs1045642) were determined by polymerase chain reaction followed with direct sequencing. The association between different genotypes and the concentrations and clinical efficacy of vancomycin were analyzed. RESULTS: There were 16.5% patients which the concentration reached 10-20 μg/mL. The curative effect of 5-<10 μg/mL (88%) and 10-20 μg/mL (93.3%) were significant higher than that of <5 μg/mL (44%) (P<0.05); and the curative effect of 5-<10 μg/mL and 10-20 μg/mL were similar. The plasma concentration (10.15±2.35) μg/mL and concentration/dose values (0.98±0.27) μg·mL-1·mg-1·kg of vancomycin in infants with OCT2 TT genotype were significantly increased than that of OCT2 GG genotypes (6.92±2.83) μg/mL, (0.59±0.22) μg·mL-1·mg-1·kg (P<0.05). Meanwhile, the clinical efficacy of vancomycin in TT genotype (100%) was higher than that in GG genotype (73.2%) (P<0.05). However, the concentration and clinical efficacy of vancomycin in the infants with mutant type and wild type of MDR1 C3435T were similar (P>0.05). CONCLUSION: OCT2 G808T polymorphism is associated with the plasma concentrations and clinical efficacy of vancomycin in infants.

Key words: vancomycin, drug transporter, polymorphisms, plasma concentration, infant

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