首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >The melanocortin-1 receptor gene mediates female-specific mechanisms of analgesia in mice and humans.
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The melanocortin-1 receptor gene mediates female-specific mechanisms of analgesia in mice and humans.

机译:melanocortin-1受体基因介导小鼠和人类的女性镇痛机制。

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Sex specificity of neural mechanisms modulating nociceptive information has been demonstrated in rodents, and these qualitative sex differences appear to be relevant to analgesia from kappa-opioid receptor agonists, a drug class reported to be clinically effective only in women. Via quantitative trait locus mapping followed by a candidate gene strategy using both mutant mice and pharmacological tools, we now demonstrate that the melanocortin-1 receptor (Mc1r) gene mediates kappa-opioid analgesia in female mice only. This finding suggested that individuals with variants of the human MC1R gene, associated in our species with red hair and fair skin, might also display altered kappa-opioid analgesia. We found that women with two variant MC1R alleles displayed significantly greater analgesia from the kappa-opioid, pentazocine, than all other groups. This study demonstrates an unexpected role for the MC1R gene, verifies that pain modulation in the two sexes involves neurochemically distinct substrates, and represents an example of a direct translation of a pharmacogenetic finding from mouse to human.
机译:在啮齿动物中已经证明了调节伤害感受信息的神经机制的性别特异性,并且这些定性的性别差异似乎与κ-阿片受体激动剂的镇痛作用有关,据报道这种药物仅对女性有效。通过定量性状基因座图,然后使用突变小鼠和药理学工具进行候选基因策略研究,我们现在证明黑皮质素-1受体(Mc1r)基因仅在雌性小鼠中介导κ阿片类镇痛。这一发现表明,具有人类MC1R基因变异的个体,在我们的物种中与红发和白皙的皮肤有关,也可能表现出改变的kappa类阿片镇痛作用。我们发现具有两个变异MC1R等位基因的妇女比其他所有组表现出的阿片类药物喷他佐辛镇痛效果明显更高。这项研究证明了MC1R基因的出乎意料的作用,验证了两性中的疼痛调节涉及神经化学上不同的底物,并且代表了从小鼠到人类的药理学发现的直接翻译实例。

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