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抗白细胞介素-10治疗小鼠的免疫状态改变

Modified immunological status of anti-IL-10 treated mice.

作者信息

Ishida H, Hastings R, Thompson-Snipes L, Howard M

机构信息

DNAX Research Institute, Palo Alto 94304.

出版信息

Cell Immunol. 1993 May;148(2):371-84. doi: 10.1006/cimm.1993.1119.

Abstract

We have shown that continuous treatment of mice from birth to adulthood with neutralizing anti-IL-10 antibodies leads to specific depletion of Ly1 B cells, while conventional B cells remain normal in terms of number, phenotype, and function. Extending our characterization of these animals, we show here that anti-IL-10 treated mice can be distinguished from untreated or isotype control treated mice by several other criteria. Anti-IL-10 treated mice contained substantially elevated levels of circulating TNF-alpha, and in many cases circulating IL-6, and were profoundly susceptible to death by LPS-induced shock, a monokine mediated inflammatory reaction. Analysis of serum immunoglobulin levels in anti-IL-10 treated mice revealed a decrease in serum IgA levels to accompany the previously reported reduction in serum IgM, plus a striking increase in IgG2a and IgG2b levels. Further investigation of the Ly1 B cell depletion of anti-IL-10 treated mice revealed that this effect was transient as evidenced by the return of Ly1 B cells in normal numbers 8 weeks after anti-IL-10 treatment was discontinued. The Ly1 B cell depletion that occurred during anti-IL-10 treatment was found to be compensated by an increase in peritoneal T cells and granulocytes. Finally, while anti-IL-10 treated mice were unable to produce antibodies to phosphorylcholine and alpha 1,3-dextran, they developed normal antibody responses following intraperitoneal injections of TNP-Ficoll, suggesting the existence of subcategories within the family of thymus independent type II polysaccharide antigens. These data are discussed within the context of their implications for the roles of IL-10 and Ly1 B cells in the immune system.

摘要

我们已经表明,从出生到成年持续用中和性抗IL-10抗体处理小鼠会导致Ly1 B细胞特异性耗竭,而传统B细胞在数量、表型和功能方面保持正常。在扩展对这些动物的特征描述时,我们在此表明,抗IL-10处理的小鼠可通过其他几个标准与未处理或同型对照处理的小鼠区分开来。抗IL-10处理的小鼠循环TNF-α水平大幅升高,在许多情况下循环IL-6水平也升高,并且极易死于LPS诱导的休克,这是一种单因子介导的炎症反应。对抗IL-10处理的小鼠血清免疫球蛋白水平的分析显示,血清IgA水平降低,同时伴有先前报道的血清IgM降低,以及IgG2a和IgG2b水平显著升高。对抗IL-10处理的小鼠Ly1 B细胞耗竭的进一步研究表明,这种效应是短暂的,抗IL-10处理停止8周后Ly1 B细胞数量恢复正常即证明了这一点。发现在抗IL-10处理期间发生的Ly1 B细胞耗竭由腹膜T细胞和粒细胞的增加所补偿。最后,虽然抗IL-10处理的小鼠不能产生针对磷酸胆碱和α1,3-葡聚糖的抗体,但在腹腔注射TNP-菲可后它们产生了正常的抗体反应,这表明胸腺非依赖性II型多糖抗原家族中存在亚类。将在这些数据对IL-10和Ly1 B细胞在免疫系统中的作用的影响的背景下讨论这些数据。

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