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Role of delivery and trafficking of delta-opioid peptide receptors in opioid analgesia and tolerance.

机译:传递和贩运的δ阿片肽受体在阿片类镇痛和耐受性中的作用。

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摘要

Changes in the number of receptors on the cell surface lead to modulations of physiological functions and pharmacological responses of neurons. Recent studies show that delta-opioid peptide (DOP) and mu-opioid peptide (MOP) receptors have distinct subcellular localizations in neurons. In nociceptive small neurons in the dorsal root ganglia, DOP receptors are sorted into neuropeptide-containing secretory vesicles, enabling the stimulus-induced cell surface expression of these receptors. MOP receptors are constitutively expressed on the cell surface. The physical interaction between DOP receptors and MOP receptors seems to be an important mechanism for the modulation of receptor functions. Experiments in animals show that MOP-receptor-mediated spinal analgesia is enhanced and morphine tolerance does not develop when DOP receptor functions are pharmacologically or genetically attenuated. Thus, the delivery and trafficking of DOP receptors are crucial processes that modulate opioid analgesia and tolerance.
机译:细胞表面受体数量的变化导致生理功能的调节和神经元的药理反应。最近的研究表明,δ-阿片肽(DOP)和μ阿片肽(MOP)受体在神经元中具有不同的亚细胞定位。在背根神经节的伤害性小神经元中,DOP受体被分类为含有神经肽的分泌囊泡,从而使这些受体能够通过刺激诱导细胞表面表达。 MOP受体在细胞表面组成性表达。 DOP受体和MOP受体之间的物理相互作用似乎是调节受体功能的重要机制。在动物中进行的实验表明,当DOP受体的功能在药理或遗传上减弱时,MOP受体介导的脊髓镇痛作用会增强,而吗啡耐受性不会提高。因此,DOP受体的递送和运输是调节阿片样物质镇痛和耐受性的关键过程。

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