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首页> 外文期刊>Molecular medicine reports >Effect of CYP3A4*18B polymorphisms and interactions with OPRM1 A118G on postoperative fentanyl requirements in patients undergoing radical gastrectomy
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Effect of CYP3A4*18B polymorphisms and interactions with OPRM1 A118G on postoperative fentanyl requirements in patients undergoing radical gastrectomy

机译:CYP3A4 * 18B基因多态性及与OPRM1 A118G的相互作用对胃癌根治术患者术后芬太尼需求的影响

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摘要

The present study aimed to investigate the effect of cytochrome P450 3A4 (CYP3A4)*18B polymorphisms and the interaction of the μ opioid receptor gene (OPRM1) A118G and CYP3A4*18B polymorphisms on postoperative fentanyl analgesia in Chinese Han patients undergoing radical gastrectomy. In total, 97 patients scheduled to undergo radical gastrectomy under general anesthesia were enrolled in this study. Post-operative patient-controlled intravenous analgesia of fentanyl was administered as analgesia up to 48 h following surgery. Venous blood (2 ml) was obtained from each patient to measure the OPRM1 A118G and CYP3A4*18B genotypes. The differences in fentanyl consumption and adverse effects were compared among the genotypes at 24 and 48 h following surgery. In the first 48 h following surgery, patients in the CYP3A4*18B/ *18B group consumed significantly less fentanyl compared with patients in the *1/*1 group (P=0.032). With regards to the joint genetic effect, during the 48 h period, patients with AA and *1*18B polymorphisms received fewer fentanyl doses compared with those with AG and *1 *1 (P=0.049), while patients with AG and *1*18B polymorphisms received significantly fewer fentanyl doses compared with those with AG and *1 *1 (P=0.010), and patients with *18B *18B polymorphisms received significantly fewer fentanyl doses compared with those with AA and *1*1 (P=0.024) or those with AG and *1*1 polymorphisms (P=0.006). No correlation between OPRM1 A118G and CYP3A4*18B and postoperative nausea, vomiting and dizziness was found. Results demonstrated that 48 h following surgery, patients with the CYP3A4*18B/ *18B genotype required less fentanyl than patients with the CYP3A4*1/*1 genotype to control pain. Additionally, the combined genotype of CYP3A4*18B and OPRM1 A118G may affect fentanyl doses administered for pain control, but not postoperative nausea, vomiting and dizziness.
机译:本研究旨在探讨细胞色素P450 3A4(CYP3A4)* 18B多态性与μ阿片受体基因(OPRM1)A118G和CYP3A4 * 18B多态性对中国汉族接受根治性胃切除术后芬太尼镇痛作用的影响。共有97例计划在全身麻醉下接受根治性胃切除术的患者参加了这项研究。术后至48小时,以患者自控的芬太尼静脉镇痛作为镇痛剂。从每位患者获得静脉血(2 ml)以测量OPRM1 A118G和CYP3A4 * 18B基因型。比较了术后24和48小时基因型之间的芬太尼消耗量和不良反应的差异。在手术后的最初48小时中,CYP3A4 * 18B / * 18B组的患者比* 1 / * 1组的患者服用的芬太尼少得多(P = 0.032)。关于联合遗传效应,在48小时内,AA和* 1 * 18B多态性患者接受芬太尼剂量的剂量少于AG和* 1 * 1(P = 0.049),而AG和* 1患者* 18B多态性的芬太尼剂量明显少于AG和* 1 * 1(P = 0.010),* 18B * 18B多态性的芬太尼剂量明显少于AA和* 1 * 1(P = 0.024)或具有AG和* 1 * 1多态性的那些(P = 0.006)。没有发现OPRM1 A118G和CYP3A4 * 18B与术后恶心,呕吐和头晕之间存在相关性。结果表明,在术后48小时,CYP3A4 * 18B / * 18B基因型患者比控制基因的CYP3A4 * 1 / * 1基因型患者需要更少的芬太尼。另外,CYP3A4 * 18B和OPRM1 A118G的组合基因型可能会影响芬太尼用于控制疼痛的剂量,但不会影响术后恶心,呕吐和头晕。

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