Role of CD45 in Hematopoiesis and Lymphomagenesis

CD45 在造血和淋巴瘤发生中的作用

• 批准号: 6682426
• 负责人: Michelle L. Hermiston
• 金额: $ 12.72万
• 依托单位: UNIVERSITY OF CALIFORNIA, SAN FRANCISCO
• 依托单位国家: 美国
• 财政年份: 2003
• 资助国家: 美国
• 起止时间: 2003-07-11 至 2006-06-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6682426
• 关键词: B lymphocyte; CD antigens; T lymphocyte; biological signal transduction; carcinogenesis; cell cell interaction; cell growth regulation; cell proliferation; comparative genomic hybridization; gene expression; genetic manipulation; genetically modified animals; hematopoiesis; laboratory mouse; leukocyte activation /transformation; lymphoma; microarray technology; neoplasm /cancer genetics; protein tyrosine phosphatase

DESCRIPTION (provided by applicant): Lymphocyte homeostasis requires the coordinate regulation of signaling cascades governing proliferation, differentiation, and death. Dysregulation of these processes is a necessary prerequisite for the development of lymphoid malignancies. Our lab recently reported a novel murine model containing a mutation that disrupts the negative regulation of the receptor-like protein tyrosine phosphatase CD45 during dimerization. These mice develop a profound lymphoproliferative disorder with polyclonal activation of T and B cells, massive splenomegaly, and premature death. A subset also develops stigmata of autoimmunity including anti-double stranded DNA antibody formation and immune complex-mediated glomerulonephritis. To define the cell type responsible for disease generation, the CD45 mutant mice were mated to mice deficient in T, B, or T and B cells. Genetic elimination of B cells, but not T cells results in ablation of the autoimmune and lymphoproliferative disorders. In contrast, absence of T cells resulted in a dramatic increase in the prevalence of lymphoma. These observations support the hypothesis that precise regulation of CD45 function by dimerization is essential for the maintenance of homeostasis within the hematopoietic system. Disruption of this function can have profound consequences leading to lymphoproliferation, autoimmunity, and malignancy. The goal of this proposal is to define the molecular and cellular basis for the breakdown of homeostasis and to identify the steps required for the development of lymphomas. The first aim tests B cell-intrinsic mechanisms that contribute to disease initiation. The second aim focuses on contributions from the microenvironment that may enhance B cell expansion and the mechanisms by which T cells inhibit lymphomagenesis. In the third aim, biochemical and gene expression analyses are used to address the molecular basis by which the CD45 mutation contributes to disease. Array CGH and ENU mutagenesis are used to begin to identify cooperating events that contribute to the progression from hyperproliferating to malignant state. These studies should provide important insights into the links between immune regulation, autoimmunity, and lymphoid malignancies as well as improve our understanding of the mechanisms governing immune surveillance.

描述（由申请人提供）： 淋巴细胞的稳态需要协调调节信号级联控制增殖，分化和死亡。 这些过程的失调是淋巴恶性肿瘤发展的必要前提。 我们的实验室最近报道了一种新的小鼠模型，该模型含有一种突变，该突变破坏了受体样蛋白酪氨酸磷酸酶CD45在二聚化过程中的负调控。 这些小鼠发展为严重的淋巴组织增生性疾病，伴有T和B细胞的多克隆活化、巨大的脾肿大和过早死亡。 一个亚群也发展自身免疫性红斑，包括抗双链DNA抗体形成和免疫复合物介导的肾小球肾炎。 为了确定导致疾病产生的细胞类型，将CD 45突变小鼠与T、B或T和B细胞缺陷的小鼠交配。 B细胞而不是T细胞的遗传消除导致自身免疫和淋巴增生性疾病的消除。 相反，T细胞的缺乏导致淋巴瘤患病率的急剧增加。 这些观察结果支持这样的假设，即通过二聚化精确调节CD45功能对于维持造血系统内的稳态是必不可少的。 这一功能的破坏可能产生深远的后果，导致淋巴细胞增生，自身免疫和恶性肿瘤。 这个建议的目标是确定破坏稳态的分子和细胞基础，并确定淋巴瘤发展所需的步骤。 第一个目的是测试有助于疾病起始的B细胞内在机制。 第二个目标集中在微环境的贡献，可能会提高B细胞的扩增和T细胞抑制淋巴瘤的机制。 在第三个目标中，生物化学和基因表达分析用于解决CD45突变导致疾病的分子基础。 阵列CGH和ENU诱变用于开始鉴定有助于从过度增殖发展到恶性状态的协同事件。 这些研究应该提供重要的见解，免疫调节，自身免疫和淋巴恶性肿瘤之间的联系，以及提高我们对免疫监视机制的理解。