Sullivan D A, Edwards J A
Schepens Eye Research Institute, Harvard Medical School, Boston, MA 02114, USA.
J Steroid Biochem Mol Biol. 1997 Feb;60(3-4):237-45. doi: 10.1016/s0960-0760(96)00190-2.
Sjögren's syndrome, an autoimmune disease that occurs primarily in women, causes extensive inflammation and significant dysfunction in the lacrimal gland, and is one of the leading causes of dry eye syndromes throughout the world. Recently, our research has shown that androgen treatment causes a significant suppression of the immunopathological lesions in lacrimal tissues of female mouse models (MRL/Mp-lpr/lpr [MRL/lpr] and NZB/NZW F1 [F1]) of Sjögren's syndrome. To extend these findings, the objective of the present study was to determine whether this androgen-induced anti-inflammatory action may be paralleled by an increase in the functional activity of lacrimal glands in these autoimmune mice. Towards this end, we measured the tear levels of immunoglobulin A (IgA), which originates from lacrimal tissue and whose concentration is known to be diminished in mucosal sites in Sjögren's syndrome. For comparative purposes, we also evaluated whether the administration of other steroid hormones or immunosuppressive agents might duplicate possible androgen effects on the secretory function of lacrimal tissue. Female MRL/lpr and F1, as well as non-autoimmune BALB/c, mice were treated with vehicle, steroids or immunosuppressive compounds for 17 to 54 days after the onset of disease. Lacrimal glands, tears and sera were collected immediately before (pretreatment), or after, therapy and processed for the analysis of either tear IgA (enzyme-linked immunosorbent assay; ELISA) and protein content or the magnitude of lymphocyte infiltration (computer-assisted image analysis). Our findings demonstrated that testosterone treatment stimulated a significant increase in the concentration and total amount of tear IgA, as well as tear protein, compared to levels in pretreatment or placebo controls. This hormone action was reproduced by exposure to a diverse array of "anabolic" and "androgenic" androgen analogues, but not by treatment with estradiol, danazol, cyclosporine A, dexamethasone or cyclophosphamide. In contrast, only dexamethasone increased serum IgA concentrations. Of particular interest is the fact that the androgen control of IgA output by the lacrimal gland appeared to be independent of this steroid's suppression of lymphocyte infiltration in lacrimal tissue. Overall, these results show that androgen therapy enhances the functional activity of the lacrimal gland in mouse models of Sjögren's syndrome.
干燥综合征是一种主要发生于女性的自身免疫性疾病,会导致泪腺广泛炎症和严重功能障碍,是全球干眼症综合征的主要病因之一。最近,我们的研究表明,雄激素治疗可显著抑制干燥综合征雌性小鼠模型(MRL/Mp-lpr/lpr [MRL/lpr]和NZB/NZW F1 [F1])泪腺组织中的免疫病理损伤。为了拓展这些发现,本研究的目的是确定这种雄激素诱导的抗炎作用是否可能伴随着这些自身免疫小鼠泪腺功能活性的增加。为此,我们测量了泪液中免疫球蛋白A(IgA)的水平,IgA源自泪腺组织,已知其浓度在干燥综合征的黏膜部位会降低。为了进行比较,我们还评估了给予其他类固醇激素或免疫抑制剂是否可能复制雄激素对泪腺组织分泌功能的潜在影响。雌性MRL/lpr和F1小鼠以及非自身免疫性BALB/c小鼠在疾病发作后17至54天接受载体、类固醇或免疫抑制化合物治疗。在治疗前(预处理)或治疗后立即收集泪腺、泪液和血清,并进行处理,以分析泪液IgA(酶联免疫吸附测定;ELISA)和蛋白质含量,或淋巴细胞浸润程度(计算机辅助图像分析)。我们的研究结果表明,与预处理或安慰剂对照组的水平相比,睾酮治疗可显著提高泪液IgA的浓度和总量以及泪液蛋白质含量。这种激素作用可通过接触多种“合成代谢”和“雄激素”类雄激素类似物重现,但用雌二醇、达那唑、环孢素A、地塞米松或环磷酰胺治疗则无法重现。相比之下,只有地塞米松会增加血清IgA浓度。特别值得关注的是,雄激素对泪腺IgA分泌的控制似乎与该类固醇对泪腺组织中淋巴细胞浸润的抑制作用无关。总体而言,这些结果表明雄激素治疗可增强干燥综合征小鼠模型中泪腺的功能活性。
