INSERM U563, Centre de Physiopathologie de Toulouse-Purpan, Toulouse, France.
J Invest Dermatol. 2010 May;130(5):1337-44. doi: 10.1038/jid.2009.433. Epub 2010 Jan 28.
Endogenous opioid peptides mainly produced by neurons are also released by immune cells. They bind to mu- (mu-opioid receptor, MOR), delta-, and kappa-opioid receptors. On the basis of studies on mice showing that MOR is the main mediator of the deleterious effects of opioids on immunity, we wondered whether MOR, absent under normal conditions, is expressed in some pathological situations such as lymphomas. mRNA expression for all three opioid receptors was examined in lymph node biopsy samples from patients with non-Hodgkin's B-cell and T-cell lymphomas. We found that MOR and one of its ligands (enkephalin) are simultaneously expressed almost exclusively in lymph nodes from patients with Sézary cutaneous T cell lymphoma. As MOR was undetectable in circulating malignant T lymphocytes and in normal immune cells, we hypothesized that tumor-released cytokines might induce MOR expression in non-neoplastic lymph node cells. The correlation between mRNA levels of MOR and interleukin-13 (IL-13) within lymph nodes from Sézary patients led us to investigate the ability of IL-13 to upregulate MOR expression in normal immune cell subsets. We found that IL-13 upregulates MOR in activated Langerhans cells. Thus, our data suggest that, under pathological conditions, IL-13 overexpression might allow immune-derived endogenous opioids to down-modulate immune response.
内源性阿片肽主要由神经元产生,也由免疫细胞释放。它们与 μ-(μ-阿片受体,MOR)、δ-和 κ-阿片受体结合。基于研究表明,MOR 是阿片类药物对免疫产生有害影响的主要介质,我们想知道在正常情况下不存在的 MOR 是否在某些病理情况下表达,例如淋巴瘤。在非霍奇金 B 细胞和 T 细胞淋巴瘤患者的淋巴结活检样本中,检查了所有三种阿片受体的 mRNA 表达。我们发现,MOR 和其配体之一(脑啡肽)几乎仅在患有蕈样真菌病皮肤 T 细胞淋巴瘤的患者的淋巴结中同时表达。由于循环恶性 T 淋巴细胞和正常免疫细胞中无法检测到 MOR,我们假设肿瘤释放的细胞因子可能诱导非肿瘤性淋巴结细胞中 MOR 的表达。Sézary 患者淋巴结中 MOR 和白细胞介素 13(IL-13)的 mRNA 水平之间的相关性促使我们研究 IL-13 是否能够上调正常免疫细胞亚群中 MOR 的表达。我们发现 IL-13 可上调活化的朗格汉斯细胞中的 MOR。因此,我们的数据表明,在病理条件下,IL-13 的过度表达可能允许免疫衍生的内源性阿片类物质下调免疫反应。
