首页> 外文期刊>Pain. >In vitro opioid induced proliferation of peripheral blood immune cells correlates with in vivo cold pressor pain tolerance in humans: a biological marker of pain tolerance.
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In vitro opioid induced proliferation of peripheral blood immune cells correlates with in vivo cold pressor pain tolerance in humans: a biological marker of pain tolerance.

机译:阿片样物质诱导的外周血免疫细胞增殖与人类体内的冷压痛耐受性相关:这是疼痛耐受性的生物学标志。

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摘要

There is substantial evidence for bidirectional communication between the immune system and the central nervous system, as the cells and signalling molecules of the immune system influence many central nervous system functions, for instance nociception. Opioids, such as morphine, produce analgesia and numerous other central and peripheral effects including sedation and euphoria, while their effects on the immune system are wide-ranging. There is considerable interindividual variability in basal nociception and response to opioids, however, the physiological and biological mechanisms underlying this are unclear. Therefore, we investigated the relationship between the immune system and basal nociceptive thresholds, using the proliferative response of isolated peripheral blood mononuclear cells and cold pressor pain tolerance. Here we show that the percent increase in proliferation of peripheral immune cells from 13 healthy subjects incubated with morphine ex vivo is highly correlated with the subjects' tolerance to noxious cold stimuli (Pearson r = 0.92, P < 0.0001). These pilot data provide evidence of a novel objective biological marker of pain tolerance in humans, which also links the immune and opioid systems with basal pain tolerance.
机译:免疫系统和中枢神经系统之间存在双向通讯的大量证据,因为免疫系统的细胞和信号分子会影响许多中枢神经系统功能,例如伤害感受。阿片类药物(例如吗啡)会产生镇痛作用以及许多其他中枢和外周效应,包括镇静和欣快感,而它们对免疫系统的作用范围很广。基底伤害感受和对阿片样物质的反应之间存在很大的个体差异,但是尚不清楚其基础的生理和生物学机制。因此,我们使用离体外周血单个核细胞的增殖反应和冷压痛耐受性,研究了免疫系统与基础伤害阈值之间的关系。在这里,我们显示了13名健康受试者体内吗啡离体培养的外周免疫细胞的增殖百分率与受试者对有害冷刺激的耐受性高度相关(Pearson r = 0.92,P <0.0001)。这些初步数据提供了人类疼痛耐受性的新型客观生物学标志物的证据,该标志物还将免疫和阿片类药物系统与基础疼痛耐受性联系起来。

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