UNIQUE ENDOTHELIAL MOLECULES IN AUTOIMMUNE INFLAMMATION

自身免疫性炎症中独特的内皮分子

• 批准号: 6080497
• 负责人: SARA A MICHIE
• 金额: $ 9.79万
• 依托单位: STANFORD UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 1999
• 资助国家: 美国
• 起止时间: 1999-09-30 至 2002-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6080497
• 关键词: NOD mouse; Sjogren's syndrome; autoimmune disorder; cell adhesion molecules; cell migration; cellular pathology; chemokine; cytokine receptors; dissection; enzyme linked immunosorbent assay; gene expression; high endothelial venule; immunocytochemistry; in situ hybridization; inflammation; insulin dependent diabetes mellitus; lacrimal apparatus; leukocyte activation /transformation; lymphocyte; pancreatic islets; polymerase chain reaction; salivary glands; video microscopy

The migration of autoreactive and effector lymphocytes from blood into target organs is a key event in the initiation and maintenance of target organ damage in autoimmune diseases. This migration involves a complex adhesion cascade with sequential lymphocyte/endothelial adhesion and activation events. Our goals are to identify adhesion triggering chemokines and novel activating and adhesion molecules expressed by high endothelial venules (HEV) in sites of autoimmune-mediated inflammation and tissue destruction, and to define the roles of these molecules in lymphocyte migration to these sites. We will use nonobese diabetic (NOD) mice, a well-characterized model for human insulin dependent diabetes mellitus (IDDM) and Sjogren's syndrome, as a model to define the unique endothelial molecules involved in lymphocyte migration to inflamed pancreatic islets, salivary gland and lacrimal gland. In Specific Aim 1, we shall use laser capture microdissection (LCM) and gene analysis techniques to define the patterns of chemokine expression by HEV endothelial cells in inflamed islets, salivary gland and lacrimal gland. The roles of these chemokines (and their receptors) in lymphocyte migration to inflamed tissues will be assessed in functional studies, including in vitro assays of lymphocyte adhesion and in vivo migration studies with mAb- inhibition or chemokine desensitization. Under Specific Aim 2, we shall use LCM and gene microarray analyses to identify and characterize genes that are expressed in a tissue-selective or inflammation-specific manner by HEV in sites of autoimmune- mediated target organ damage. We are most interested in genes encoding novel adhesion or activating molecules that may mediate lymphocyte migration into inflamed pancreatic islets and salivary and lacrimal gland. These studies will define novel therapeutic targets for the prevention of inflammation and target organ damage in autoimmune diseases including IDDM and Sjogren's syndrome.

自身反应性淋巴细胞和效应淋巴细胞从血液向靶器官的迁移是自身免疫性疾病中靶器官损伤的启动和维持的关键事件。 这种迁移涉及复杂的粘附级联反应，具有顺序的淋巴细胞/内皮细胞粘附和激活事件。 我们的目标是确定粘附触发趋化因子和新的激活和粘附分子表达的高内皮微静脉（HEV）在网站的自身免疫介导的炎症和组织破坏，并确定这些分子在淋巴细胞迁移到这些网站的作用。 我们将使用非肥胖糖尿病（NOD）小鼠，一个良好的特征模型，为人类胰岛素依赖型糖尿病（IDDM）和干燥综合征，作为一个模型，以确定独特的内皮细胞分子参与淋巴细胞迁移到发炎的胰岛，唾液腺和泪腺。在具体目标1中，我们将使用激光捕获显微切割（LCM）和基因分析技术来确定炎症胰岛，唾液腺和泪腺中HEV内皮细胞表达趋化因子的模式。 将在功能研究中评估这些趋化因子（及其受体）在淋巴细胞迁移至炎症组织中的作用，包括淋巴细胞粘附的体外测定和mAb抑制或趋化因子脱敏的体内迁移研究。 在特定目标2下，我们将使用LCM和基因微阵列分析来鉴定和表征在自身免疫介导的靶器官损伤位点中由HEV以组织选择性或炎症特异性方式表达的基因。 我们最感兴趣的是编码新的粘附或激活分子的基因，这些分子可能介导淋巴细胞迁移到发炎的胰岛、唾液腺和泪腺。 这些研究将确定新的治疗目标，用于预防炎症和靶器官损伤的自身免疫性疾病，包括胰岛素依赖性糖尿病和干燥综合征。