首页> 外文期刊>Blood: The Journal of the American Society of Hematology >The endogenous danger signal, crystalline uric acid, signals for enhanced antibody immunity.
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The endogenous danger signal, crystalline uric acid, signals for enhanced antibody immunity.

机译:内源性危险信号结晶尿酸可增强抗体免疫力。

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摘要

Studies have shown that the immune system can recognize self-antigens under conditions (eg, cell injury) in which the self-tissue might elaborate immune-activating endogenous danger signals. Uric acid (UA) is an endogenous danger signal recently identified to be released from dying cells. Prior work has shown that UA activates immune effectors of both the innate and adaptive immune system, including neutrophils and cytotoxic T-cell immunity. However, it was unclear whether UA could enhance antibody immunity, which was examined in this study. When added to dying tumor cells or with whole protein antigen, UA increased IgG1-based humoral immunity. Further, UA blocked growth of tumor in subsequent tumor challenge experiments, which depended on CD4, but not CD8, T cells. Sera derived from UA-treated animals enhanced tumor growth, suggesting it had little role in the antitumor response. UA did not signal for T-cell expansion or altered tumor-infiltrating leukocyte populations. Consistent with the lack of T-cell expansion, when applied to dendritic cells, UA suppressed T-cell growth factors but up-regulated B cell-activating cytokines. Understanding the nature of endogenous danger signals released from dying cells may aid in a better understanding of mechanisms of immune recognition of self.
机译:研究表明,免疫系统可以在自身组织可能细化免疫激活内源性危险信号的条件下(例如细胞损伤)识别自身抗原。尿酸(UA)是最近被确定从垂死的细胞中释放出来的内源性危险信号。先前的研究表明,UA激活先天性和适应性免疫系统的免疫效应物,包括嗜中性粒细胞和细胞毒性T细胞免疫。但是,尚不清楚UA是否可以增强抗体免疫性,这项研究对此进行了研究。当添加到垂死的肿瘤细胞或全蛋白抗原中时,UA会增加基于IgG1的体液免疫。此外,UA在随后的肿瘤攻击实验中阻断了肿瘤的生长,该实验依赖于CD4 T细胞,而不依赖CD8 T细胞。 UA处理过的动物的血清可促进肿瘤生长,表明它在抗肿瘤反应中几乎没有作用。 UA并未提示T细胞扩增或肿瘤浸润性白细胞数量改变。与缺乏T细胞扩增一致,当应用于树突状细胞时,UA抑制T细胞生长因子,但上调B细胞激活细胞因子。了解垂死细胞释放的内源性危险信号的性质可能有助于更好地了解自身的免疫识别机制。

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