阿片和阿片受体在神经轴的不同水平上介导抗感觉。

Physiologia Bohemoslovaca Pub Date : 1990-01-01
A Herz, M J Millan
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引用次数: 0

摘要

目前实验疼痛研究的核心问题之一是确定各种阿片样物质(阿片肽和生物碱)和多种阿片样物质受体在调节伤害性过程中的身份、位置和作用机制。在大脑层面,采用几种实验方法的研究指出-内啡肽在镇痛中的重要作用,由中脑导水管周围灰质的电刺激引起。耐受性和交叉耐受性研究表明,多阿片受体介导了这种作用。delta-,特别是chi-阿片受体在脑疼痛调节中的重要性文献记载较少。在脊髓水平,痛觉在脊髓背角中传递,那里有丰富的阿片肽和所有类型的阿片受体。阿片受体介导的抗感觉过程似乎在这一区域最重要,但三角洲阿片受体也可能参与其中。此外,在一定条件下可以证明chi-阿片受体的作用。最近的实验表明,阿片类药物也可能调节外周的伤害感觉,特别是在炎症组织中。阿片受体及其内源性配体——阿片肽的鉴定标志着疼痛研究进入了一个新时代。几种类型阿片受体的分化和随后一系列阿片肽的表征说明了阿片系统的惊人复杂性。这种多样性对一般神经生物学的影响,特别是对疼痛机制的理解,目前还没有完全理解。在本报告中,阿片能疼痛控制的一些方面在神经轴的不同水平将被讨论。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Opioids and opioid receptors mediating antinociception at various levels of the neuraxis.

One of the central issues in present experimental pain research is to establish the identity, location, and mechanism of action of various opioids (opioid peptides and alkaloids) and multiple opioid receptors in the modulation of nociceptive processes. At the cerebral level, studies employing several experimental approaches point to an essential role of beta-endorphin in analgesia, induced by electrical stimulation of the periaqueductal grey of the midbrain. Tolerance and cross-tolerance studies suggest that mu-opioid receptors mediate this effect. The significance of delta- and, in particular, chi-opioid receptors in cerebral pain modulation is less well documented. At the spinal level, nociception is relayed in the dorsal horn, where opioid peptides as well as all types of opioid receptors are abundant. mu-opioid receptor-mediated antinociceptive processes appear to be most important in this region, but delta-opioid receptors may also be involved. In addition, a role of chi-opioid receptors can be demonstrated under certain conditions. Recent experiments indicate that opioids may also modulate nociception in the periphery, in particular in inflamed tissue. The identification of opioid receptors and their endogenous ligands, the opioid peptides, marked the beginning of a new era in pain research. The differentiation of several types of opioid receptors and the subsequent characterization of a series of opioid peptides illustrate the striking complexity of opioid systems. The implications of this multiplicity for neurobiology in general and for the understanding of pain mechanisms in particular are presently not fully understood. In this presentation some aspects of opioidergic pain control at various levels of the neuraxis will be discussed.

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