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由人白血病 Jurkat T 细胞系合成的褪黑素与白细胞介素 -2 的产生有关。

Melatonin synthesized by Jurkat human leukemic T cell line is implicated in IL-2 production.

作者信息

Lardone Patricia J, Carrillo-Vico Antonio, Naranjo María C, De Felipe Beatriz, Vallejo Alejandro, Karasek Michal, Guerrero Juan M

机构信息

Department of Medical Biochemistry and Molecular Biology, School of Medicine and Virgen Macarena Hospital, University of Seville, Seville, Spain.

出版信息

J Cell Physiol. 2006 Jan;206(1):273-9. doi: 10.1002/jcp.20461.

Abstract

Human lymphocytes have recently been described as an important physiological source of melatonin (N-acetyl-5-methoxytryptamine), which could be involved in the regulation of the human immune system. On the other hand, stimulation of IL-2 production by exogenous melatonin has been shown in the Jurkat human lymphocytic cell line. Furthermore, both melatonin membrane and nuclear receptors are present in these cells. In this study, we show that the necessary machinery to synthesize melatonin is present and active in resting and stimulated Jurkat cells. Accordingly, we have found that cells synthesize and release melatonin in both conditions. Therefore, we investigated whether endogenous melatonin produced by Jurkat cells was involved in the regulation of IL-2 production. When melatonin membrane and nuclear receptors were blocked using specific antagonists, luzindole and CGP 55644, respectively, we found that IL-2 production decreased, and this drop was reverted by exogenous melatonin. Additionally, PHA activation of Jurkat cells changed the profile of melatonin nuclear receptor mRNA expression. A previous study showed that exogenous melatonin is able to counteract the decrease in IL-2 production caused by prostaglandin E2 (PGE2) in human lymphocytes via its membrane receptor. In our model, when we blocked the melatonin membrane receptor with luzindole, the inhibitory effect of PGE2 on IL-2 production was higher. Therefore, we have demonstrated the physiological role of endogenous melatonin in this cell line. These findings indicate that endogenous melatonin synthesized by human T cells would contribute to regulation of its own IL-2 production, acting as an intracrine, autocrine, and/or paracrine substance.

摘要

人类淋巴细胞最近被描述为褪黑素(N-乙酰-5-甲氧基色胺)的重要生理来源,褪黑素可能参与人类免疫系统的调节。另一方面,在外源褪黑素刺激下,Jurkat人淋巴细胞系中白细胞介素-2(IL-2)的产生已得到证实。此外,这些细胞中同时存在褪黑素膜受体和核受体。在本研究中,我们发现合成褪黑素所需的机制在静息和受刺激的Jurkat细胞中均存在且有活性。相应地,我们发现细胞在这两种情况下均能合成并释放褪黑素。因此,我们研究了Jurkat细胞产生的内源性褪黑素是否参与IL-2产生的调节。当分别使用特异性拮抗剂鲁辛朵和CGP 55644阻断褪黑素膜受体和核受体时,我们发现IL-2的产生减少,而外源性褪黑素可逆转这种下降。此外,Jurkat细胞经植物血凝素(PHA)激活后,褪黑素核受体mRNA表达谱发生改变。先前的一项研究表明,外源性褪黑素能够通过其膜受体抵消前列腺素E2(PGE2)对人类淋巴细胞中IL-2产生的抑制作用。在我们的模型中,当用鲁辛朵阻断褪黑素膜受体时,PGE2对IL-2产生的抑制作用增强。因此,我们证明了内源性褪黑素在该细胞系中的生理作用。这些发现表明,人类T细胞合成的内源性褪黑素作为一种内分泌、自分泌和/或旁分泌物质,有助于调节其自身IL-2的产生。

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