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吗啡诱导脾细胞向中枢神经系统迁移。

Morphine induces splenocyte trafficking into the CNS.

机构信息

Department of Pediatrics, University of Minnesota, Minneapolis, MN 55455, USA.

出版信息

J Neuroimmune Pharmacol. 2012 Jun;7(2):436-43. doi: 10.1007/s11481-011-9307-2. Epub 2011 Aug 20.

Abstract

Opioids significantly alter functional responses of lymphocytes following activation. The opiate Morphine, alters the Th1 to Th2 response and modulates functional responses such as cytolytic activity and T-cell proliferation. Although there has been extensive research involving morphine's effects on lymphocytes, little is known about the effects morphine has on lymphocyte trafficking. The objective of the study was to use in vivo bioluminescent imaging to determine morphine's effect on the trafficking pattern of splenocytes systemically and into the CNS either in a naïve state or following a neuroinflammatory stimulus. A neuroinflammatory response was induced by intracerebrally administering a DNA IFN-γ DNA plasmid into morphine-dependent or placebo wildtype mice. Mice with or without a neurostimulus received adoptively transferred firefly luciferase transgenic splenocytes and imaged. Morphine dependence significantly altered the inherent ability of splenocytes to traffic into the spleen, and lead to non-directed chaotic trafficking throughout the animal, including into the CNS. The morphine-mediated effects on trafficking were blocked by the antagonist naltrexone. Morphine dependence intensified splenocyte infiltration into the CNS following neuroinflammation induced by IFN-γ gene transfer. The study precented determined that morphine severely altered the ability of non-activated splenocytes to home to the spleen, inducing extrasplenic trafficking thoughout the animal. In addition to altering the ability of naive splenocyte to traffic to the spleen, this study demonstrated that morphine profoundly exacerbated lymphocyte infiltration into the CNS following a neurostimulus.

摘要

阿片类药物在激活后显著改变淋巴细胞的功能反应。阿片类药物吗啡改变了 Th1 向 Th2 的反应,并调节了细胞毒性活性和 T 细胞增殖等功能反应。尽管已经有大量涉及吗啡对淋巴细胞影响的研究,但对于吗啡对淋巴细胞迁移的影响知之甚少。本研究的目的是使用体内生物发光成像来确定吗啡对脾细胞在全身和中枢神经系统中的迁移模式的影响,无论是在未受刺激的状态下还是在神经炎症刺激后。通过向吗啡依赖或安慰剂野生型小鼠脑内给予 DNA IFN-γ DNA 质粒来诱导神经炎症反应。有或没有神经刺激的小鼠接受了荧光素酶转基因脾细胞的过继转移,并进行了成像。吗啡依赖显著改变了脾细胞进入脾脏的固有能力,并导致整个动物(包括中枢神经系统)出现无定向的混乱迁移。纳曲酮拮抗剂阻断了吗啡对迁移的介导作用。吗啡依赖加剧了 IFN-γ 基因转移诱导的神经炎症后脾细胞向中枢神经系统的浸润。该研究确定吗啡严重改变了非激活脾细胞归巢到脾脏的能力,诱导整个动物的脾外迁移。除了改变未刺激的脾细胞向脾脏迁移的能力外,本研究还表明,吗啡在神经刺激后强烈加剧了淋巴细胞向中枢神经系统的浸润。

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