CCR6 Regulation of Intestinal T Lymphocyte Development

CCR6 对肠道 T 淋巴细胞发育的调节

• 批准号: 6875743
• 负责人: IFOR R WILLIAMS
• 金额: $ 30.29万
• 依托单位: EMORY UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-04-01 至 2008-03-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6875743
• 关键词: T lymphocyte; bone marrow; bromodeoxyuridine; cell differentiation; cell proliferation; chemokine receptor; gene targeting; genetically modified animals; interferon gamma; interleukin 10; laboratory mouse; protein structure function

DESCRIPTION (provided by applicant): The intestinal epithelium is home to specialized subsets of intraepithelial T lymphocytes (IEL) that provide essential regulatory and effector functions. Chemokines and chemokine receptors play pivotal roles in guiding the trafficking of T cells during their differentiation from precursors in lymphoid tissues and their subsequent migration to extralymphoid sites. Absence of the CC chemokine receptor 6 (CCR6) in mice leads to perturbations of mucosal immunity including an increase in the number of small intestinal IEL. IEL from CCR6 deficient mice display selective expansion of the alpha beta TCR IEL subsets expressing CD8alpha/alpha that can develop from precursors in intestinal cryptopatches through an extrathymic differentiation pathway. Preliminary studies using mutant mice with an EGFP knock in mutation at the CCR6 locus demonstrate that CCR6 is expressed on a majority of the IEL precursors found in cryptopatches, but is absent from mature IEL. The central objective of the proposed studies is to identify the mechanisms by which absence of CCR6 leads to dysregulated local T cell differentiation in the intestine. The differentiation potential of IEL precursors from CCR6 deficient and wild-type mice will be compared using a competitive adoptive transfer model in which both types of precursor cells are allowed to differentiate into mature IEL following transfer into mice that lack endogenous cryptopatches and intestinal IEL (CD132 null mice that lack the common gamma chain of the IL-2 receptor). The first specific aim is to determine the stage of IEL differentiation at which CCR6 deficient IEL precursors begin to show preferential expansion compared to wild-type IEL precursors. Functional properties (cytokine production, lytic activity, and proliferative rate) of IEL derived from CCR6 null or wild type precursors will also be compared. The second aim is to investigate the potential precursor-product relationship between CCR6+ and CCR6- c-kit+ intestinal lymphocyte precursors by comparing their relative maturity and differentiation potential. Mechanistic insights into the CCR6 dependent regulatory pathway that normally maintains homeostatic control over intestinal IEL may lead to identification of new types of chemokine receptor targeted pharmacological manipulations useful in the treatment of human inflammatory bowel disease.

描述（由申请人提供）：肠上皮是上皮内T淋巴细胞（IEL）特化亚群的家园，提供基本的调节和效应功能。趋化因子和趋化因子受体在引导T细胞从淋巴组织中的前体分化以及随后迁移到淋巴外位点期间的运输中起关键作用。 小鼠中CC趋化因子受体6（CCR 6）的缺失导致粘膜免疫的扰动，包括小肠IEL数量的增加。来自CCR 6缺陷小鼠的IEL显示表达CD 8 α/α的α β TCR IEL亚群的选择性扩增，其可以通过胸腺外分化途径从肠内隐睾中的前体发育。 使用在CCR 6基因座处具有EGFP敲入突变的突变小鼠的初步研究表明，CCR 6在大多数在cryptopatches中发现的IEL前体上表达，但在成熟IEL中不存在。拟议研究的中心目标是确定CCR 6缺失导致肠道局部T细胞分化失调的机制。将使用竞争性过继转移模型比较来自CCR 6缺陷型小鼠和野生型小鼠的IEL前体的分化潜力，在该模型中，允许两种类型的前体细胞在转移到缺乏内源性cryptopatches和肠IEL的小鼠（缺乏IL-2受体的共同γ链的CD 132缺失小鼠）中后分化成成熟IEL。第一个具体目的是确定与野生型IEL前体相比，CCR 6缺陷IEL前体开始显示优先扩增的IEL分化阶段。 还将比较源自CCR 6缺失或野生型前体的IEL的功能特性（细胞因子产生、裂解活性和增殖速率）。 第二个目的是通过比较CCR 6+和CCR 6- c-kit+肠淋巴细胞前体细胞的相对成熟度和分化潜能来研究它们之间潜在的受体-产物关系。对CCR 6依赖性调节途径的机制性见解通常维持对肠道IEL的稳态控制，这可能导致鉴定新型趋化因子受体靶向药理学操作，其可用于治疗人类炎症性肠病。