首页> 外文期刊>Anesthesiology >A118G single nucleotide polymorphism of human mu-opioid receptor gene influences pain perception and patient-controlled intravenous morphine consumption after intrathecal morphine for postcesarean analgesia.
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A118G single nucleotide polymorphism of human mu-opioid receptor gene influences pain perception and patient-controlled intravenous morphine consumption after intrathecal morphine for postcesarean analgesia.

机译:人mu阿片受体基因的A118G单核苷酸多态性影响鞘内注射吗啡用于剖宫产镇痛后的疼痛知觉和患者控制的静脉内吗啡消耗。

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BACKGROUND: Previous studies have shown that genetic variability at position 118 of the human mu-opioid receptor gene altered patients' response to intravenous morphine. The purpose of this study was to investigate whether this polymorphism contributes to the variability in response to morphine for postcesarean analgesia. METHODS: After investigators obtained informed consent, 588 healthy women received 0.1 mg intrathecal morphine for postcesarean analgesia. Their blood samples were genotyped for the A118G polymorphism-A118 homozygous (AA), heterozygous (AG), or homozygous for the G allele (GG). Pain scores, the severity of nausea and vomiting, the incidence of pruritus, and the total self-administered intravenous morphine were recorded for the first 24 postoperative hours. RESULTS: Two hundred seventy women (46%) were AA, 234 (40%) were AG, and 82 (14%) were GG. The 24-h self-administered intravenous morphine consumption was lowest in the AA group (P = 0.001; mean, 5.9; 95% confidence interval, 5.1-6.8) versus the AG (8.0; 6.9-9.1) and GG groups (9.4; 7.3-11.5). Pain scores were lowest in the AA group and highest in the GG group, with a statistically significant difference detected between AA, AG, and GG (P = 0.049). Total morphine consumption was also influenced by patients' age and paying status. AA group was associated with the highest incidence of nausea (26 of 272 [9.6%]; P = 0.02) versus the other two groups (13 of 234 [5.6%] and 1 of 82 [1.2%] for AG and GG, respectively). CONCLUSION: Genetic variation at position 118 of the mu-opioid receptor is associated with interindividual differences in pain scores, self-administered intravenous morphine, and the incidence of nausea postoperatively.
机译:背景:以前的研究表明,人类阿片类药物受体基因第118位的遗传变异性改变了患者对静脉吗啡的反应。这项研究的目的是调查这种多态性是否有助于剖宫产后镇痛对吗啡的反应变异性。方法:研究人员获得知情同意后,有588名健康女性接受了0.1 mg鞘内注射吗啡进行剖宫产后镇痛。对他们的血样进行A118G多态性基因型分型-A118纯合(AA),杂合(AG)或G等位基因(GG)纯合。在术后的最初24小时内记录疼痛评分,恶心和呕吐的严重程度,瘙痒的发生率以及静脉注射吗啡的总量。结果:270名女性(46%)为AA,234名(40%)为AG,82名(14%)为GG。相对于AG组(8.0; 6.9-9.1)和GG组(9.4; 6.9),AA组的24小时静脉内吗啡消耗量最低(P = 0.001;平均5.9; 95%置信区间5.1-6.8)。 7.3-11.5)。疼痛评分在AA组中最低,在GG组中最高,在AA,AG和GG之间检测到统计学差异(P = 0.049)。吗啡的总消费量还受患者年龄和支付状况的影响。与其他两组相比,AA组与恶心的发生率最高(272例,占26 [9.6%]; P = 0.02),另外两组(AG和GG分别为13例,占234 [5.6%]和82例,占1.2 [1.2%])。 )。结论:阿片类药物受体118位点的遗传变异与个体之间的疼痛评分,静脉内使用吗啡的自主性差异以及术后恶心的发生有关。

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