Park H-J, Shinn H K, Ryu S H, Lee H-S, Park C-S, Kang J-H
Department of Anesthesiology, Inha University Hospital, Inha University, Incheon, South Korea.
Clin Pharmacol Ther. 2007 Apr;81(4):539-46. doi: 10.1038/sj.clpt.6100046. Epub 2006 Dec 27.
P-glycoprotein (PGP) is a polymorphic transporter encoded by the ABCB1 gene that contributes to the access of xenobiotics into the brain. There is no report on associations between genetic polymorphisms in ABCB1 and the clinical effects of fentanyl, although fentanyl may be a substrate of PGP. One hundred and twenty-six (126) unrelated Korean patients under spinal anesthesia with intravenous fentanyl (2.5 microg/kg) were recruited. Clinical effects (bispectral index, respiration rate, and need for oxygen supplementation) were monitored and these were compared between genotypes for three single nucleotide polymorphisms in ABCB1 (1236C>T, 2677G>T/A, and 3435C>T). The allele and genotype frequencies were similar to previous data from Asians; the three major haplotypes, TTT (30%), TGC (24%), and CGC (24%) were expected among nine known haplotypes. During the initial 10 min, there were differences in suppression of respiration rate by fentanyl among the three genotypes (P=0.0933 for 1236C>T; P=0.0941 for 2677G>A/T; P=0.0013 for 3435C>T, repeated-measures analysis of variance), but the differences in bispectral index among genotypes were not observed. Furthermore, patients carrying the linked 3435T and 2677T alleles showed a significant difference in the level of respiratory suppression (P=0.0056); those with genotypes susceptible to fentanyl (1236TT, 2677TT, and 3435TT) showed early (2-3 min) and profound suppression of respiration (65-73% of initial respiration rate) compared with other resistant genotypes (83-85% of initial respiration rate in 1236CC, 2677GG, and 3435CC). Although the need to supply oxygen was not significantly different between genotypes, there was a trend for increased demand by patients carrying both 1236T and 3435T alleles (P=0.0847). In conclusion, our results confirm ABCB1 genotype data for Koreans and suggest that analysis of ABCB1 polymorphisms may have clinical relevance to prevent respiratory suppression by intravenous fentanyl or to anticipate its clinical effects.
P-糖蛋白(PGP)是一种由ABCB1基因编码的多态性转运蛋白,它影响外源性物质进入大脑。虽然芬太尼可能是PGP的底物,但尚无关于ABCB1基因多态性与芬太尼临床效应之间关联的报道。招募了126名接受脊髓麻醉并静脉注射芬太尼(2.5微克/千克)的无血缘关系的韩国患者。监测临床效应(脑电双频指数、呼吸频率和吸氧需求)并比较ABCB1基因中三个单核苷酸多态性(1236C>T, 2677G>T/A, 和3435C>T)的不同基因型之间的差异。等位基因和基因型频率与之前亚洲人的数据相似;在9种已知单倍型中,三种主要单倍型TTT(30%)、TGC(24%)和CGC(24%)出现频率较高。在最初10分钟内,三种基因型之间芬太尼对呼吸频率的抑制存在差异(1236C>T,P=0.0933;2677G>A/T,P=0.0941;3435C>T,P=0.0013,重复测量方差分析),但未观察到基因型之间脑电双频指数的差异。此外,携带连锁的3435T和2677T等位基因的患者在呼吸抑制水平上存在显著差异(P=0.0056);与其他耐药基因型(1236CC、2677GG和3435CC患者为初始呼吸频率的83 - 85%)相比,芬太尼敏感基因型(1236TT、2677TT和3435TT)的患者出现早期(2 - 3分钟)且深度的呼吸抑制(初始呼吸频率的65 - 73%)。虽然各基因型之间吸氧需求无显著差异,但携带1236T和3435T等位基因的患者有吸氧需求增加的趋势(P=0.0847)。总之,我们的结果证实了韩国人的ABCB1基因型数据,并表明分析ABCB1基因多态性可能对预防静脉注射芬太尼引起的呼吸抑制或预测其临床效应具有临床意义。
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