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松果体激素褪黑素对人单核细胞的激活作用。

Activation of human monocytes by the pineal hormone melatonin.

作者信息

Morrey K M, McLachlan J A, Serkin C D, Bakouche O

机构信息

Department of Molecular Pharmacology and Biologic Chemistry, Northwestern University Medical School, Chicago, IL 60611.

出版信息

J Immunol. 1994 Sep 15;153(6):2671-80.

PMID:8077674
Abstract

To determine the effects of the pineal hormone melatonin on human monocytes, human monocytes were activated by different concentrations of melatonin. Above the activation threshold of 5 x 10(-11) M, melatonin was able to induce the cytotoxicity of human monocytes, the secretion of IL-1, and the production of reactive oxygen intermediates. Melatonin and LPS seemed to have a synergistic effect on human monocyte activation. Indeed, below their respective monocyte activation threshold (5 x 10(-11) M and 0.625 ng/ml), melatonin (10(-12) M) in association with LPS (0.2 ng/ml) was able to induce cytotoxicity, IL-1 secretion, and reactive oxygen intermediates production. Melatonin alone at 10(-12) M or LPS alone at 0.2 ng/ml did not activate monocytes. Furthermore, melatonin was able to prime the monocytes for a subsequent activation by LPS. When monocytes were activated by LPS (0.25 ng/ml) at the time that they were plated and then activated by melatonin (10(-12) M) 8 h later, no IL-1 secretion and no cytotoxicity were detected. However, when the cells were first activated by melatonin (10(-12) M), and then 8 h later by LPS (0.25 ng/ml), IL-1 secretion and monocyte cytotoxicity were observed. Above its monocyte activation threshold, melatonin induces both cell-associated IL-1 alpha and IL-1 beta activities. Below this activation threshold, i.e., at 10(-12) M, melatonin does not induce the cell-associated IL-1 alpha and IL-1 beta activities, but does induce the mRNA for both IL-1 (alpha and beta). It seems that melatonin activates monocytes through protein kinase C. These data suggest that melatonin activates monocytes and induces their cytotoxic properties, along with the IL-1 secretion.

摘要

为了确定松果体激素褪黑素对人单核细胞的影响,用不同浓度的褪黑素激活人单核细胞。高于5×10⁻¹¹ M的激活阈值时,褪黑素能够诱导人单核细胞的细胞毒性、IL-1的分泌以及活性氧中间体的产生。褪黑素和脂多糖(LPS)似乎对人单核细胞的激活具有协同作用。实际上,在它们各自的单核细胞激活阈值(5×10⁻¹¹ M和0.625 ng/ml)以下,褪黑素(10⁻¹² M)与LPS(0.2 ng/ml)联合能够诱导细胞毒性、IL-1分泌以及活性氧中间体的产生。单独的10⁻¹² M褪黑素或单独的0.2 ng/ml LPS均不能激活单核细胞。此外,褪黑素能够使单核细胞对随后的LPS激活产生预刺激作用。当单核细胞在接种时被LPS(0.25 ng/ml)激活,然后在8小时后被褪黑素(10⁻¹² M)激活时,未检测到IL-1分泌和细胞毒性。然而,当细胞首先被褪黑素(10⁻¹² M)激活,然后在8小时后被LPS(0.25 ng/ml)激活时,观察到了IL-1分泌和单核细胞毒性。高于其单核细胞激活阈值时,褪黑素诱导细胞相关的IL-1α和IL-1β活性。在该激活阈值以下,即10⁻¹² M时,褪黑素不诱导细胞相关的IL-1α和IL-1β活性,但确实诱导IL-1(α和β)的mRNA。似乎褪黑素通过蛋白激酶C激活单核细胞。这些数据表明,褪黑素激活单核细胞并诱导其细胞毒性特性以及IL-1分泌。

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