Gruschwitz M S, Moormann S, Krömer G, Sgonc R, Dietrich H, Boeck G, Gershwin M E, Boyd R, Wick G
Institute for General and Experimental Pathology, University of Innsbruck, Medical School, Austria.
J Autoimmun. 1991 Aug;4(4):577-93. doi: 10.1016/0896-8411(91)90178-f.
University of California at Davis line 200 (UCD-200) chickens develop a hereditary connective tissue disease characterized by severe lymphocytic infiltration, vascular occlusion and fibrosis of skin and internal organs. To identify cellular immunological abnormalities in the acute inflammatory disease stage of this animal model for progressive systemic sclerosis (PSS) we investigated the phenotypic characteristics and function of peripheral blood lymphocytes (PBL), spleen cells and thymocytes in comparison with skin infiltrating cells. Immunofluorescence and immunohistochemical analysis using monoclonal antibodies revealed the overwhelming majority of skin infiltrating mononuclear cells in the deeper dermis and subcutaneous tissue to be T cell receptor alpha/beta (TcR2)+/CD3+/CD4+/class II+ cells, a small portion (5-10%) of which were interleukin 2 (IL-2) receptor positive. In contrast, the inflammatory infiltrate in perivascular areas of the papillary dermis was constituted of mainly TcR gamma/delta (TcR1)+/class II- lymphocytes. Only few B cells (T/B cell ratio greater than 5) were detected. These diseased chickens showed significantly reduced percentages and numbers of circulating peripheral T cells exhibiting TcR1, TcR2, CD3, CD4 or IL-2-receptor, probably owing to an increased influx into lymphoid organs and affected tissues. In contrast to healthy chickens, the thymi of UCD-200 animals revealed fewer cells expressing TcR1, TcR2 and class II antigen, suggesting an altered intrathymic maturation of the T cell lineage. Functional in vitro studies showed a significantly decreased T cell mitogen-induced proliferation rate associated with a decreased capacity to produce IL-2 and to express IL-2 receptors. In contrast to the deficient in vitro IL-2 production the sera of UCD-200 chickens contained significant levels of IL-2 bioactivity. The alteration of T lymphocyte physiology in UCD-200 chickens adds, at least in part, to the parallels between this animal model and its human counterpart. These data confirm our hypothesis that the PSS-like disease of UCD-200 chickens includes a numeric and/or functional alteration of peripheral T cell subsets, especially of TcR1 positive cells, in contrast to the pronounced accumulation in the afflicted tissues.
加利福尼亚大学戴维斯分校200系(UCD - 200)鸡会患上一种遗传性结缔组织疾病,其特征为严重的淋巴细胞浸润、血管闭塞以及皮肤和内脏器官纤维化。为了确定这种进行性系统性硬化症(PSS)动物模型在急性炎症疾病阶段的细胞免疫异常情况,我们将外周血淋巴细胞(PBL)、脾细胞和胸腺细胞的表型特征及功能与皮肤浸润细胞进行了比较研究。使用单克隆抗体的免疫荧光和免疫组织化学分析显示,在真皮深层和皮下组织中,绝大多数皮肤浸润单核细胞为T细胞受体α/β(TcR2)+/CD3+/CD4+/II类分子+细胞,其中一小部分(5 - 10%)白细胞介素2(IL - 2)受体呈阳性。相比之下,乳头层真皮血管周围区域的炎性浸润主要由TcRγ/δ(TcR1)+/II类分子-淋巴细胞构成。仅检测到少量B细胞(T/B细胞比率大于5)。这些患病鸡的循环外周T细胞中,表现出TcR1、TcR2、CD3、CD4或IL - 2受体的细胞百分比和数量显著降低,这可能是由于流入淋巴器官和受影响组织的数量增加所致。与健康鸡相比,UCD - 200动物的胸腺中表达TcR1、TcR2和II类抗原的细胞较少,这表明T细胞谱系的胸腺内成熟发生了改变。体外功能研究显示,T细胞丝裂原诱导的增殖率显著降低,同时产生IL - 2和表达IL - 2受体的能力也下降。与体外IL - 2产生不足相反,UCD - 200鸡的血清中含有显著水平的IL - 2生物活性。UCD - 200鸡中T淋巴细胞生理学的改变至少部分地解释了这种动物模型与其人类对应物之间的相似之处。这些数据证实了我们的假设,即UCD - 200鸡的PSS样疾病包括外周T细胞亚群,尤其是TcR1阳性细胞的数量和/或功能改变,这与患病组织中明显的细胞积聚形成对比。
