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吗啡耐受和戒断对细胞免疫功能的影响。

Effects of morphine tolerance and abstinence on cellular immune function.

作者信息

Bhargava H N, Thomas P T, Thorat S, House R V

机构信息

Department of Pharmacodynamics (M/C 865), University of Illinois at Chicago 60612.

出版信息

Brain Res. 1994 Apr 11;642(1-2):1-10. doi: 10.1016/0006-8993(94)90899-0.

DOI:10.1016/0006-8993(94)90899-0
PMID:8032870
Abstract

Female B6C3F1 mice were rendered tolerant-dependent on morphine by a combination of injections and pellet implantation. Mice were injected with morphine sulfate (20 mg/kg, s.c.) twice a day on day 1. On day 2, they were implanted s.c. with a 75 mg morphine pellet for 3 days. On day 5, the pellets were either left intact (tolerant) or removed 8 h prior (abstinent) to carrying out the immune function tests. A high degree of tolerance to the analgesic and hypothermic effect of morphine developed as a result of this procedure. Similarly, physical dependence also developed as evidenced by the signs of the abrupt and naltrexone-precipitated abstinence syndrome. Implantation with morphine pellets resulted in a profound, statistically significant reduction in spleen and thymus weight and cellularities, with the greatest degree of reduction noted in abstinent animals. Morphine tolerance was associated with suppressed B-cell proliferation following in vitro stimulation, as well as interleukin-2 (IL-2) and interleukin-4 production by T-cells. NK cell activity was significantly reduced in morphine-tolerant, but not in morphine-abstinent, mice following a 24 h incubation in the presence or absence of IL-2. In comparison, the in vitro induction of cytotoxic T-cells was significantly depressed in morphine-abstinent, but not morphine-tolerant, animals. Exposure to morphine apparently had limited effect on macrophage function as assessed by production of tumor necrosis factor. These studies demonstrate a differential effect on immune effector and regulatory mechanisms in morphine tolerance and abstinence processes.

摘要

通过注射和植入药粒相结合的方式,使雌性B6C3F1小鼠对吗啡产生耐受性依赖。在第1天,小鼠每天皮下注射硫酸吗啡(20毫克/千克)两次。在第2天,给它们皮下植入一粒75毫克的吗啡药粒,持续3天。在第5天,在进行免疫功能测试前,要么让药粒保持完整(耐受组),要么提前8小时取出(戒断组)。由于这个过程,小鼠对吗啡的镇痛和降温作用产生了高度耐受性。同样,身体依赖性也发展起来,表现为突然出现的、纳曲酮诱发的戒断综合征迹象。植入吗啡药粒导致脾脏和胸腺重量及细胞数量显著减少,戒断组动物的减少程度最大。吗啡耐受性与体外刺激后B细胞增殖受抑制以及T细胞产生白细胞介素-2(IL-2)和白细胞介素-4有关。在有或没有IL-2的情况下孵育24小时后,吗啡耐受小鼠的自然杀伤细胞活性显著降低,但吗啡戒断小鼠没有。相比之下,在吗啡戒断动物中,细胞毒性T细胞的体外诱导显著降低,但吗啡耐受动物没有。通过肿瘤坏死因子的产生评估,接触吗啡对巨噬细胞功能的影响显然有限。这些研究表明,吗啡耐受和戒断过程对免疫效应和调节机制有不同的影响。

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