首页> 外文期刊>The journal of pain: official journal of the American Pain Society >??-opioid receptor gene A118G polymorphism predicts pain recovery after sexual assault
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??-opioid receptor gene A118G polymorphism predicts pain recovery after sexual assault

机译:阿片类鸦片受体基因A118G多态性预测性侵犯后疼痛恢复

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摘要

Pain is common after sexual assault (SA), but etiology of pain symptoms after SA is unknown. Preclinical studies suggest that the release of endogenous opioids during stress produces delayed-onset hyperalgesia. In human studies, individuals with ??1 G allele at the ??-opioid receptor functional single nucleotide polymorphism A118G have been shown to have a reduced response to opioids. We hypothesized that if opioid-mediated hyperalgesia contributes to pain after SA, women SA survivors with 1 or more G alleles at A118G would experience reduced postassault pain. Among 52 European American women SA survivors presenting for care within 48 hours of SA, those with a G allele (12/52, 23%) experienced less severe pain (F[1,39] = 11.55, P = .002) and a reduced extent of pain (F[1,41] = 11.01, P = .002) during the 6 weeks after SA. These associations between the presence of 1 or more G alleles and reduced pain severity and reduced pain extent after SA remained significant in multivariable models controlling for age, income, education, reported pain prior to assault, and pain at the time of initial evaluation. Perspective: These results suggest that endogenous opioid-mediated hyperalgesia may contribute to pain symptoms after sexual assault. Further studies examining mechanisms mediating the development of pain after sexual assault, and the potential influence of opioid-mediated hyperalgesia, are needed. ? 2013 by the American Pain Society.
机译:性攻击(SA)后疼痛很常见,但SA后疼痛症状的病因尚不清楚。临床前研究表明,应激期间内源性阿片样物质的释放会引起迟发性痛觉过敏。在人体研究中,在α-阿片样物质受体功能性单核苷酸多态性A118G处具有β1G等位基因的个体已显示出对阿片样物质的应答降低。我们假设,如果阿片类药物引起的痛觉过敏导致SA后的疼痛,则在A118G处具有1个或多个G等位基因的女性SA幸存者的发作后疼痛会减轻。在52名在SA的48小时内就诊的SA美国女性幸存者中,G等位基因(12/52,23%)的患者痛苦较轻(F [1,39] = 11.55,P = .002)。 SA后6周内疼痛程度减轻(F [1,41] = 11.01,P = .002)。在1个或多个G等位基因的存在与SA后疼痛严重程度降低和疼痛程度减轻之间的这些关联在控制年龄,收入,教育程度,攻击前报告的疼痛以及初次评估时的疼痛的多变量模型中仍然很重要。观点:这些结果表明,内源性阿片类药物介导的痛觉过敏可能会导致性侵犯后的疼痛症状。需要进行进一步研究,以研究介导性侵犯后疼痛发展的机制,以及阿片类药物介导的痛觉过敏的潜在影响。 ? 2013年,美国疼痛学会。

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