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用单克隆抗I-A抗体进行体内治疗后B细胞的消失与再现。

Disappearance and reappearance of B cells after in vivo treatment with monoclonal anti-I-A antibodies.

作者信息

Waldor M K, Hardy R R, Hayakawa K, Steinman L, Herzenberg L A, Herzenberg L A

出版信息

Proc Natl Acad Sci U S A. 1984 May;81(9):2855-8. doi: 10.1073/pnas.81.9.2855.

Abstract

Previous studies have shown that treatment with antibodies to the murine I-A antigen encoded in the major histocompatibility complex attenuates experimental allergic encephalitis and experimental autoimmune myasthenia gravis. These studies were conducted with SJL mice, an inbred strain that is highly susceptible to the induction of these diseases. Here we show that injection of monoclonal anti-I-A antibody in the amounts used for the above studies rapidly depletes B cells. Fluorescence-activated cell sorter (FACS) multiparameter analysis of the B-cell subpopulations in treated animals shows that maximum depletion occurs around 5 days after treatment and that recovery of some subpopulations i still incomplete 1 month later. SJL mice are more sensitive to this B-cell depletion and recover more slowly than putatively normal C3H.Ighb (CKB) mice. Some components of the primary, secondary and tertiary IgG antibody responses are reduced in anti-I-A-treated SJL animals immunized after the first and second anti-I-A injections. The persistence of some antibody response impairment well beyond the time when anti-I-A disappears raises a note of caution concerning human therapy protocols based on the injection of anti-Ia antibodies.

摘要

先前的研究表明,用针对主要组织相容性复合体中编码的鼠I-A抗原的抗体进行治疗,可减轻实验性变应性脑脊髓炎和实验性自身免疫性重症肌无力。这些研究是在SJL小鼠身上进行的,SJL小鼠是一种近交系,对诱导这些疾病高度敏感。在此我们表明,以上述研究中使用的剂量注射单克隆抗I-A抗体可迅速耗尽B细胞。对经处理动物的B细胞亚群进行荧光激活细胞分选仪(FACS)多参数分析显示,处理后约5天出现最大程度的细胞耗竭,且1个月后一些亚群仍未完全恢复。SJL小鼠对这种B细胞耗竭更敏感,且比假定正常的C3H.Ighb(CKB)小鼠恢复得更慢。在首次和第二次注射抗I-A后进行免疫的经抗I-A处理的SJL动物中,初次、二次和三次IgG抗体反应的某些成分有所降低。某些抗体反应损害在抗I-A消失后的很长时间内仍然持续,这对基于注射抗Ia抗体的人类治疗方案提出了警示。

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