Genetic polymorphisms have been shown to affect opioid requirement for pain relief. However, true genetic effect is often difficult to assess due to underlying pain conditions and placebo effects. The goal of this study was to understand how common polymorphisms affect opioid effects while controlling for these factors. A randomized, double-blind, placebo-controlled study was implemented to assess how opioid effects are modulated by COMT (rs6269, rs4633, rs4848, rs4680), OPRM1 (A118G), and OPRK1 (rs1051660, rs702764, rs16918875). One hundred and eight healthy subjects underwent experimental pain testing before and after morphine, butorphanol, and placebo (saline). Association analysis was performed between polymorphisms/haplotypes and opioid response, while correcting for race, gender, placebo effects, and multiple comparisons. Pressure pain was significantly associated with rs6269 and rs4633 following butorphanol. The AA genotype of rs4680 or A_T_C_A/ A_T_C_A (rs6269_rs4633_ rs4818_rs4680) diplotype of COMT, combined with the AG genotype of OPRM1 A118G, showed significantly increased pressure pain threshold from butorphanol. Opioid effects on pressure, ischemic, heat pain, and side effects were nominally associated with several SNPs and haplotypes. Effects were often present in one opioid but not the other. This indicates that these polymorphisms affect pain relief from opioids, and that their effects are opioid and pain modality specific.

译文

:遗传多态性已显示会影响阿片类药物缓解疼痛的需求。但是,由于潜在的疼痛状况和安慰剂作用,通常很难评估真正的遗传作用。这项研究的目的是了解常见的多态性如何在控制这些因素的同时影响阿片类药物的作用。已实施一项随机,双盲,安慰剂对照的研究,以评估COMT(rs6269,rs4633,rs4848,rs4680),OPRM1(A118G)和OPRK1(rs1051660,rs702764,rs16918875)如何调节阿片类药物的作用。 108名健康受试者在吗啡,布托啡诺和安慰剂(盐水)之前和之后进行了实验性疼痛测试。在校正种族,性别,安慰剂效应和多重比较的同时,在多态性/单倍型与阿片样物质反应之间进行了关联分析。布托啡诺后rs6269和rs4633与压力疼痛显着相关。 rs4680或A_T_C_A / A_T_C_A(rs6269_rs4633_ rs4818_rs4680)双倍体的AA基因型与OPRM1 A118G的AG基因型相结合,显示了丁烷酚的压力疼痛阈值明显增加。阿片类药物对压力,局部缺血,热痛和副作用的影响名义上与几种SNP和单倍型有关。一种阿片类药物常有作用,而另一种则无作用。这表明这些多态性影响阿片类药物的镇痛作用,并且其作用是阿片类药物和特定疼痛方式的结果。

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