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Structure and Function of the Murine Lymph Node.

机译:小鼠淋巴结的结构和功能。

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摘要

Lymph nodes (LNs) are dynamic organs responsible for providing a supportive and centralized environment for the generation of immune response. Utilizing a highly organized network of non-hematopoietic stromal cells, the LN serves as the context in which the immune system collects and presents antigen, promotes innate and adaptive immune interaction, and generates protective cell-mediated and humoral immunity. In this way, proper organization and function of the LN environment is a critical component of effective immunity, and understanding its complexity has direct impact on the ability to generate and modulate primary immune response to specific antigens. To this end, the LN architecture, underlying stromal networks, and environmental and cellular responses to influenza vaccination were investigated. Using novel approaches to conduit imaging, details of the collagen network that comprises the LN scaffolding have been integrated into current understandings of LN architecture. The cellular compartment responsible for the maintenance of that scaffolding, fibroblastic reticular cells (FRCs), have been studied using an induced diptheria toxin receptor model. By specifically ablating the FRC population in mice, their role in the maintenance of T cell homeostasis has been confirmed in vivo. More surprisingly, a disruption of the FRC network resulted in a loss of B cell follicle structure within LNs, and a reduction in humoral immunity to influenza vaccination. These findings led to the identification of a new subset of FRCs which reside in B cell follicles, and serve as a critical source of the B cell survival factor BAFF. Turning towards the hematopoietic response to influenza vaccination, a highly unexpected lymph node resident dendritic cell (LNDC) response has been identified following vaccine antigen deposition within specialized sites in the LN medulla. Rapid migration of LNDCs into these sites optimizes exposure of the population to viral antigen, and de novo synthesis of a CXCL10 chemokine gradient by activated LNDCs ensures efficient antigen specific CD4+ T cell response, and protective humoral immunity---independent of migratory dendritic cell status. Altogether, these studies highlight a highly dynamic, responsive LN environment with direct influence on primary immune response---the understanding of which has broad implications in vaccine biology.
机译:淋巴结(LN)是负责为免疫反应的产生提供支持和集中化环境的动态器官。 LN利用高度组织化的非造血基质细胞网络,是免疫系统收集和呈递抗原,促进先天性和适应性免疫相互作用并产生保护性细胞介导和体液免疫的环境。这样,LN环境的正确组织和功能是有效免疫力的关键组成部分,了解其复杂性直接影响产生和调节对特定抗原的初次免疫反应的能力。为此,研究了LN架构,底层基质网络以及环境和细胞对流感疫苗接种的反应。使用新颖的导管成像方法,包含LN支架的胶原蛋白网络的详细信息已集成到当前对LN体系结构的了解中。已经使用诱导的白喉毒素受体模型研究了负责维持该支架的细胞室,成纤维细胞网状细胞(FRC)。通过特异性消融小鼠的FRC种群,已在体内证实了它们在维持T细胞稳态中的作用。更令人惊讶的是,FRC网络的破坏导致LN内B细胞卵泡结构的丧失,以及针对流感疫苗的体液免疫力降低。这些发现导致鉴定出存在于B细胞滤泡中的FRC的新子集,并且其是B细胞存活因子BAFF的关键来源。转向对流感疫苗的造血反应,已在疫苗抗原沉积在LN延髓的特定部位后,发现了高度意外的淋巴结驻留树突状细胞(LNDC)反应。 LNDC迅速迁移到这些位点可优化人群对病毒抗原的暴露,并且活化的LNDC从头合成CXCL10趋化因子梯度可确保有效的抗原特异性CD4 + T细胞反应和保护性体液免疫-独立于迁移性树突状细胞状态。总而言之,这些研究强调了对原发性免疫反应有直接影响的高度动态,反应灵敏的LN环境-对疫苗生物学的理解具有广泛的意义。

著录项

  • 作者

    Woodruff, Matthew Charles.;

  • 作者单位

    Harvard University.;

  • 授予单位 Harvard University.;
  • 学科 Health Sciences Immunology.
  • 学位 Ph.D.
  • 年度 2014
  • 页码 111 p.
  • 总页数 111
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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