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本文引用的文献

1
Molecular analysis of double isotype expression in IgA switching.IgA类别转换中双同种型表达的分子分析
J Immunol. 1993 Feb 15;150(4):1338-47.
2
T cell-derived B cell differentiation factor(s). Effect on the isotype switch of murine B cells.T细胞衍生的B细胞分化因子。对小鼠B细胞同种型转换的影响。
J Exp Med. 1982 Mar 1;155(3):734-48. doi: 10.1084/jem.155.3.734.
3
Expression of lymphocyte surface IgE does not require switch recombination.淋巴细胞表面IgE的表达不需要类别转换重组。
Nature. 1982 Jun 24;297(5868):697-9. doi: 10.1038/297697a0.
4
Rearrangement of immunoglobulin gamma 1-chain gene and mechanism for heavy-chain class switch.免疫球蛋白γ1链基因重排及重链类别转换机制
Proc Natl Acad Sci U S A. 1980 Feb;77(2):919-23. doi: 10.1073/pnas.77.2.919.
5
Antibodies of the secondary response can be expressed without switch recombination in normal mouse B cells.在正常小鼠B细胞中,二次免疫应答的抗体可以在不发生类别转换重组的情况下表达。
Proc Natl Acad Sci U S A. 1984 Nov;81(22):7189-93. doi: 10.1073/pnas.81.22.7189.
6
Inducible production of c-fos antisense RNA inhibits 3T3 cell proliferation.c-fos反义RNA的诱导产生抑制3T3细胞增殖。
Proc Natl Acad Sci U S A. 1986 Jul;83(13):4794-8. doi: 10.1073/pnas.83.13.4794.
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Oligodeoxynucleotides as inhibitors of gene expression: a review.作为基因表达抑制剂的寡脱氧核苷酸:综述
Cancer Res. 1988 May 15;48(10):2659-68.
8
IL-4 induces co-expression of intrinsic membrane IgG1 and IgE by murine B cells stimulated with lipopolysaccharide.白细胞介素-4可诱导经脂多糖刺激的小鼠B细胞共表达内在膜免疫球蛋白G1和免疫球蛋白E。
J Immunol. 1988 Jul 15;141(2):489-98.
9
The role of IL-5 in IgA B cell differentiation.白细胞介素-5在IgA B细胞分化中的作用。
J Immunol. 1988 May 1;140(9):3033-9.
10
Differential regulation of IgG1 and IgE synthesis by interleukin 4.白细胞介素4对IgG1和IgE合成的差异调节
J Exp Med. 1988 Jan 1;167(1):183-96. doi: 10.1084/jem.167.1.183.

生殖系转录本下调对免疫球蛋白A同种型分化的影响。

Effect of downregulation of germline transcripts on immunoglobulin A isotype differentiation.

作者信息

Wakatsuki Y, Strober W

机构信息

Mucosal Immunity Section, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

J Exp Med. 1993 Jul 1;178(1):129-38. doi: 10.1084/jem.178.1.129.

DOI:10.1084/jem.178.1.129
PMID:8315375
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2191091/
Abstract

In this study we determined the role of immunoglobulin (Ig) germline transcripts in the isotype switch differentiation of the cloned lymphoma B cell line CH12.LX. In initial studies, we showed that addition of transforming growth factor beta (TGF-beta) and interleukin 4 (IL-4), either alone or in combination, augment switching from membrane (m)IgM+ to mIgA+ cells, and that increased switching is preceded and paralleled by an increase in the steady-state level of alpha germline transcripts (alpha GLT). Interestingly, TGF-beta and IL-4 affect switching in different ways, as shown by the fact that IL-4 increases and TGF-beta decreases the number of dual-positive (mIgM+/mIgA+) cells; in addition, TGF-beta and IL-4 have different effects on the time course of induction of alpha GLT. In subsequent studies, we established that we could downregulate alpha GLT levels in CH12.LX B cells by transfecting an expression vector that can be induced to produce transcripts antisense to the I alpha exon. Using this approach we downregulated alpha GLT in CH12.LX B cells undergoing switching in the presence of TGF-beta and IL-4 and showed that such downregulation led to decreased switching, as evidenced by decreased appearance of dual-positive B cells as well as decreased IgA synthesis relative to IgM synthesis. This result was corroborated by the fact that incubation of CH12.LX cells with phosphorothio-oligo antisense DNA to I alpha sequence also led to a decrease in the number of dual-positive cells and in the IgA/IgM secretion ratio. In summary, IgA isotype differentiation in CH12.LX B cell, particularly the steps necessary for the elaboration of mIgM+/mIgA+ switch intermediate cells, is inhibited by downregulation of alpha GLT; it is therefore apparent that alpha GLT plays a key role in the initial stage of isotype switch differentiation.

摘要

在本研究中,我们确定了免疫球蛋白(Ig)种系转录本在克隆的淋巴瘤B细胞系CH12.LX的同种型转换分化中的作用。在初步研究中,我们发现单独或联合添加转化生长因子β(TGF-β)和白细胞介素4(IL-4)可增强从膜(m)IgM⁺细胞向mIgA⁺细胞的转换,并且在转换增加之前及同时,α种系转录本(αGLT)的稳态水平会升高。有趣的是,TGF-β和IL-4以不同方式影响转换,如下所示:IL-4增加而TGF-β减少双阳性(mIgM⁺/mIgA⁺)细胞的数量;此外,TGF-β和IL-4对αGLT诱导的时间进程有不同影响。在后续研究中,我们证实通过转染一种可诱导产生与Iα外显子反义转录本的表达载体,能够下调CH12.LX B细胞中的αGLT水平。使用这种方法,我们在TGF-β和IL-4存在的情况下,对正在进行转换的CH12.LX B细胞中的αGLT进行了下调,并表明这种下调导致转换减少,这可通过双阳性B细胞出现减少以及相对于IgM合成而言IgA合成减少来证明。用针对Iα序列的硫代磷酸寡核苷酸反义DNA孵育CH12.LX细胞也导致双阳性细胞数量和IgA/IgM分泌比率降低,这一事实证实了该结果。总之,CH12.LX B细胞中的IgA同种型分化,特别是形成mIgM⁺/mIgA⁺转换中间细胞所需的步骤,会因αGLT的下调而受到抑制;因此很明显,αGLT在同种型转换分化的初始阶段起着关键作用。