Role of Mast Cells in Inflammation and Immunity

肥大细胞在炎症和免疫中的作用

• 批准号: 7202896
• 负责人: Stephen Joseph Galli
• 金额: $ 39.96万
• 依托单位: STANFORD UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 1996
• 资助国家: 美国
• 起止时间: 1996-08-20 至 2011-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7202896
• 关键词: angiogenesis; cell proliferation; cellular immunity; cytokine; epithelium; fibrosis; gene targeting; genetically modified animals; growth factor; inflammation; laboratory mouse; mast cell; microarray technology

DESCRIPTION (provided by applicant): The secretion of diverse mediators & cytokines by mast cells (MCs) activated by Fc-epsilon-RI-bound IgE & specific antigen (Ag) is widely regarded to be the main process by which MCs contribute significantly to allergic disorders such as atopic dermatitis & atopic asthma. However, there is strong evidence that effector T cells also have important roles in these disorders. In other settings, including cutaneous contact hypersensitivity (CHS), T cells clearly have critical roles but the contributions of the MC have been less certain, with different studies indicating that MCs can either enhance or have no effect on individual features of CHS responses. During the last period of support, we think that we have shed light on some of the factors which may importantly influence the roles of MCs in T cell-dependent host responses & diseases, including CHS. Our findings support the general hypothesis that: 1. Depending on the circumstances, MCs can importantly contribute to the development, magnitude and, remarkably, the resolution of several features of the pathology of T cell-dependent CHS responses; and 2. MCs can have these apparently paradoxical effects by exerting both direct & indirect actions on multiple recruited or resident cell types which participate in these reactions. Specifically, we found that, depending on the specific details of hapten sensitization & challenge, MCs can either markedly enhance or significantly limit the development, extent & duration of several features of the pathology associated with CHS in the mouse. We also reported evidence that: 1. the MC's ability to influence certain biological responses, including some which are relevant to CHS, may depend on occupancy of MC Fc-epsilon-RI by Ag-non-specific IgE; and 2. MCs can enhance the proliferation & cytokine production of multiple subsets of T cells in vitro, by mechanisms which either do or do not depend on IgE+Ag signaling via Fc-epsilon-RI, MC secretion of TNF, MC-T cell proximity or MC expression of co-stimulatory molecules (e.g., OX40L). Finally, we characterized in detail a new model for investigating MC function in vivo: c-kit mutant C57QUQ-Kit h/w/sh ("W sash") mice which have been selectively "repaired" of their MC deficiency by engraftment of in vitro-derived WT MCs or MCs with defined genetic abnormalities. We now wish to capitalize on these recent insights into the complex factors which can positively or negatively regulate MC functions during immune responses by pursuing the following aims: 1: Define the mechanisms by which MCs can modulate T cell proliferation & function; 2: Define the mechanisms by which MCs can enhance the elicitation phase & the pathological consequences of cutaneous CHS responses in vivo; & 3: Define the mechanisms by which MCs can limit the magnitude & duration of CHS responses. This work promises to improve our understanding of the complex potential roles of MCs, and IgE, in health & disease, as well as to improve our understanding of the pathology of CHS, a common occupational illness.

描述（由申请人提供）：被fc -epsilon- ri结合的IgE和特异性抗原（Ag）激活的肥大细胞（MCs）分泌多种介质和细胞因子被广泛认为是MCs在过敏性疾病（如特应性皮炎和特应性哮喘）中起重要作用的主要过程。然而，有强有力的证据表明效应T细胞在这些疾病中也起着重要作用。在其他情况下，包括皮肤接触过敏（CHS）， T细胞显然具有关键作用，但MC的贡献不太确定，不同的研究表明，MC可以增强或不影响CHS反应的个体特征。在最后的支持期间，我们认为我们已经阐明了一些可能重要影响MCs在T细胞依赖性宿主反应和疾病（包括CHS）中的作用的因素。我们的发现支持一般假设：1。根据具体情况，MCs可以重要地促进T细胞依赖性CHS反应病理的发展、大小和显著的几个特征的解决；和2。MCs可以通过对参与这些反应的多种募集或常驻细胞类型施加直接和间接的作用来产生这些明显矛盾的效果。具体来说，我们发现，根据半抗原致敏和激发的具体细节，MCs可以显著增强或显著限制小鼠中与CHS相关的几种病理特征的发展、程度和持续时间。我们还报告了以下证据：1。MC影响某些生物反应的能力，包括一些与CHS相关的生物反应，可能取决于ag非特异性IgE对MC Fc-epsilon-RI的占用；和2。MCs可以在体外增强多种T细胞亚群的增殖和细胞因子的产生，其机制可能依赖于或不依赖于IgE+Ag信号通过Fc-epsilon-RI、MC分泌TNF、MC-T细胞接近或MC共刺激分子（如OX40L）的表达。最后，我们详细描述了一种用于研究体内MC功能的新模型：c-kit突变体C57QUQ-Kit h/w/sh（“w带状”）小鼠，通过植入体外来源的WT MCs或具有明确遗传异常的MCs，选择性地“修复”了其MC缺陷。现在，我们希望利用这些最新的见解，通过追求以下目标，对免疫应答过程中可以积极或消极调节MC功能的复杂因素进行研究：1 .确定MC调节T细胞增殖和功能的机制；2：明确MCs在体内增强皮肤CHS反应引发期和病理后果的机制；& 3：定义MCs可以限制CHS反应的强度和持续时间的机制。这项工作有望提高我们对MCs和IgE在健康和疾病中的复杂潜在作用的理解，并提高我们对CHS（一种常见的职业病）病理的理解。