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抗IgD抗体对小鼠免疫系统的多克隆激活。VIII. IgD分泌的刺激。

Polyclonal activation of the murine immune system by an antibody to IgD. VIII. Stimulation of IgD secretion.

作者信息

Mountz J D, Smith J, Snapper C M, Mushinski J F, Finkelman F D

机构信息

Department of Medicine, Uniformed Services University of the Health Sciences, Bethesda, MD 20814.

出版信息

J Immunol. 1987 Oct 1;139(7):2172-8.

PMID:3498752
Abstract

The low levels of serum IgD found in mice and the lack of a typical DNA switch sequence between C delta and C mu raise the possibility that the generation of murine IgD-secreting cells results from a chance "mistake" rather than a controlled process. The recent observation that injection of mice with purified IgD upregulates IgD receptor expression on helper T cells and enhances the ability of these T cells to induce B cells to differentiate into antibody secreting cells led us to look for evidence of controlled differentiation of B cells into IgD-secreting cells. To do this, we injected mice with a goat antibody to IgD (GaM delta), because this antibody stimulates large increases in IgM, IgG1, IgG2a, and IgE secretion. Mice injected with GaM delta demonstrated a large increase in splenic content of mRNA specific for the secreted form of delta-chain, as well as a greater than 100-fold increase in the percentage of splenic IgD-containing plasmablasts. The secretory IgD response was totally T-dependent. Production of the secretory form of IgD was not seen until 7 days after GaM delta injection, and peaked sharply on day 8, whereas by day 6 IgM secretion had already peaked and IgG1 and IgG2 secretion had attained substantial levels. This observation suggests that: 1) either cells that synthesize large quantities of the secretory form of delta-chain, unlike cells that synthesize large quantities of the secretory forms of gamma-, epsilon-, or alpha-chains, do this without deleting C mu, or, despite the absence of a typical DNA switch sequence between C mu and C delta, controls must exist to effect the C mu deletion and VDJ-C delta joining; and 2) if secreted IgD has a role in the regulation of a humoral immune response it most likely is involved in later processes, such as memory cell generation or response termination, rather than in relatively early processes, such as helper T cell activation.

摘要

在小鼠体内发现的血清IgD水平较低,以及Cδ和Cμ之间缺乏典型的DNA转换序列,这使得小鼠产生分泌IgD的细胞可能是由于偶然的“错误”而非受控过程。最近的观察发现,给小鼠注射纯化的IgD会上调辅助性T细胞上的IgD受体表达,并增强这些T细胞诱导B细胞分化为抗体分泌细胞的能力,这促使我们寻找B细胞受控分化为分泌IgD细胞的证据。为此,我们给小鼠注射了抗IgD的山羊抗体(GaMδ),因为这种抗体能刺激IgM、IgG1、IgG2a和IgE分泌大幅增加。注射了GaMδ的小鼠脾脏中分泌型δ链特异性mRNA含量大幅增加,含IgD的脾成浆细胞百分比增加了100多倍。分泌型IgD反应完全依赖T细胞。直到注射GaMδ后7天才出现分泌型IgD的产生,并在第8天急剧达到峰值,而到第6天IgM分泌已经达到峰值,IgG1和IgG2分泌也已达到相当水平。这一观察结果表明:1)与合成大量γ、ε或α链分泌形式的细胞不同,合成大量分泌型δ链的细胞在不删除Cμ的情况下就能做到这一点,或者,尽管Cμ和Cδ之间没有典型的DNA转换序列,但必然存在控制机制来实现Cμ的删除和VDJ-Cδ连接;2)如果分泌型IgD在体液免疫反应调节中起作用,它很可能参与后期过程,如记忆细胞的产生或反应终止,而不是相对早期的过程,如辅助性T细胞激活。

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