The role of CD28- cells in human Chagas' disease

CD28-细胞在人类恰加斯病中的作用

• 批准号: 7094836
• 负责人: Walderez O. Dutra
• 金额: $ 5.4万
• 依托单位: UNIVERSIDADE FEDERAL DE MINAS GERAIS
• 依托单位国家: 美国
• 财政年份: 2007
• 资助国家: 美国
• 起止时间: 2007-07-01 至 2010-06-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7094836
• 关键词: Address; Affect; Americas; Antigens; Apoptosis; Area; Autoantigens; Biological Assay; Blood Transfusion; Brazil; CD28 Antigens; CD28 gene; CD8B1 gene; Cardiac; Case Study; Cell Adhesion Molecules; Cells; Chagas Disease; Chronic; Clinical; Collaborations; Complex; Country; Data; Disease; Disease Marker; Evolution; Experimental Designs; Feces; Government; Grant; Heart; Heart Diseases; Human; Human Biology; ITGAM gene; Immune response; In Vitro; Incidence; Individual; Infection; Insecta; International; Intervention; Knowledge; Latin America; Lead; Methods; Molecular Profiling; Morbidity - disease rate; Nature; Numbers; Outcome; Parasites; Parasitic Diseases; Pathology; Patients; Pattern; Peripheral Blood Mononuclear Cell; Population; Prognostic Marker; Publishing; Research; Research Design; Research Personnel; Research Project Grants; Role; Series; Specialist; Specificity; Students; Surface; T-Lymphocyte; Tissues; Transcend; Trypanosoma; Trypanosoma cruzi; United States; Urine; Work; base; concept; cytokine; cytotoxic; cytotoxicity; design; disorder control; human disease; immunopathology; improved; migration; response; transmission process; vector

DESCRIPTION (provided by applicant): The long-term aim of this research project is to gain a better understanding of the involvement of defined T- cell subpopulations in the establishment of protective and/or pathogenic immune responses in human Chagas' disease, a prevalent and endemic parasitic disease caused by the infection with Trypanosoma cruzi. Through a series of comprehensive mechanistic studies we will dissect the role of CD4+ and CD8+ T cells with differential expression of CD28 in the dynamics of the immune response in human Chagas' disease. Specific aims are: 1.Determine the adhesion molecule expression by CD28+ and CD28- T cells from individuals with different clinical forms of Chagas' disease; 2. Determine the intensity and specificity of the cytotoxic function of CD28+ and CD28- T cells from individuals with different clinical forms of Chagas' disease; 3. Determine the regulatory function of CD28+ and CD28- T cells from individuals with different clinical forms of Chagas' disease. To perform these studies we will use peripheral blood mononuclear cells from a selected group of chagasic patients, carefully classified as belonging to the indeterminate or severe cardiac clinical forms. Cellular recruitment potential, cytotoxicity and regulatory functions will be evaluated ex vivo and after in vitro stimulation with parasite, as well as autologous antigens, through the analysis of expression of surface or intracellular molecules by FACS and by biological assays. These studies will greatly improve the knowledge on Chagas' disease immunopathology by clarifying how CD28+ and CD28- sub- populations relate to the differential clinical evolution of disease. We hope that the new concepts derived from our findings will allow for the identification of markers of disease evolution and/or morbidity, offering new possibilities of clinical intervention to benefit the 17 million infected people. Transcending the limits of Chagas' disease, our findings will add to our knowledge on the biology of human T cells with differential expression of CD28, opening new possibilities of studies in other human diseases. Finally, depending largely on a Brazilian scientific core of researchers and students, the implementation of these studies will also lead to increased research capacities in Brazil through intense collaborations with international and national specialists.

描述（由申请人提供）：本研究项目的长期目标是更好地了解确定的T细胞亚群在人类恰加斯病（一种由克氏锥虫感染引起的流行性和地方性寄生虫病）中建立保护性和/或致病性免疫应答中的作用。通过一系列的综合机制研究，我们将剖析CD 4+和CD 8 + T细胞与CD 28的差异表达在人类恰加斯病的免疫反应动力学中的作用。具体目标是：1.测定来自不同临床形式的恰加斯病个体的CD 28+和CD 28- T细胞的粘附分子表达; 2.确定来自具有不同临床形式的恰加斯病的个体的CD 28+和CD 28- T细胞的细胞毒性功能的强度和特异性; 3.确定来自不同临床形式的恰加斯病个体的CD 28+和CD 28- T细胞的调节功能。为了进行这些研究，我们将使用来自一组选定的chagglutamine患者的外周血单核细胞，仔细分类为属于不确定或严重的心脏临床形式。将通过FACS和生物测定分析表面或细胞内分子的表达，离体和用寄生虫以及自体抗原体外刺激后评价细胞募集潜力、细胞毒性和调节功能。这些研究将通过阐明CD 28+和CD 28-亚群如何与疾病的不同临床演变相关，极大地提高对恰加斯病免疫病理学的认识。我们希望，从我们的研究结果中得出的新概念将有助于确定疾病演变和/或发病率的标志物，为临床干预提供新的可能性，使1700万感染者受益。我们的发现超越了恰加斯病的局限性，将增加我们对CD 28差异表达的人类T细胞生物学的了解，为其他人类疾病的研究开辟新的可能性。最后，这些研究的实施在很大程度上取决于巴西研究人员和学生的科学核心，通过与国际和国内专家的密切合作，也将提高巴西的研究能力。