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爱泼斯坦-巴尔病毒引起的免疫球蛋白产生与永生化之间的关系。

Relationship between immunoglobulin production and immortalization by Epstein Barr virus.

作者信息

Tosato G, Blaese R M, Yarchoan R

出版信息

J Immunol. 1985 Aug;135(2):959-64.

PMID:2989369
Abstract

After infection with Epstein Barr virus (EBV), human B lymphocytes actively secrete immunoglobulin (Ig) and are immortalized to become long-term cell lines. In these studies, we investigated the relationship between these virally induced processes utilizing limiting dilution culture techniques, and asked whether all B cells stimulated by EBV to secrete Ig are also immortalized. The activation of B cells by EBV resulting in Ig production and immortalization involved a single precursor cell, required live viral particles, and was independent of immunity to EBV by the lymphocyte donor. However, the precursor frequency of B cells activated to secrete Ig (mean 4.7%) was higher than the precursor frequency of B cells activated to long-term in vitro growth (mean 2.1%). When examined at a single cell level, it appeared that although the vast majority of the immortalized B cells also secrete Ig, only approximately 50% of the B cell precursors induced by EBV to secrete Ig go on to form long-term cell lines. In addition, although immortalized B cell clones producing all major classes of Ig were detected, IgM-committed precursors were more likely to become immortal than were precursors committed to IgG or IgA production. In contrast to these findings in B cells freshly infected with EBV, Ig production was almost always associated with evidence of long-term growth when B cells from previously established EBV-induced B cell lines were tested in identical limiting dilution cultures. Thus, after infection with EBV, human B cells can either become transiently activated to proliferate and to secrete Ig, or become transformed into long-term cell lines most of which produce Ig.

摘要

感染爱泼斯坦-巴尔病毒(EBV)后,人类B淋巴细胞会积极分泌免疫球蛋白(Ig)并永生化,成为长期细胞系。在这些研究中,我们利用有限稀释培养技术研究了这些病毒诱导过程之间的关系,并询问是否所有受EBV刺激分泌Ig的B细胞也会永生化。EBV激活B细胞导致Ig产生和永生化涉及单个前体细胞,需要活病毒颗粒,并且与淋巴细胞供体对EBV的免疫力无关。然而,被激活分泌Ig的B细胞的前体频率(平均4.7%)高于被激活进行长期体外生长的B细胞的前体频率(平均2.1%)。在单细胞水平上进行检测时,似乎虽然绝大多数永生化的B细胞也分泌Ig,但由EBV诱导分泌Ig的B细胞前体中只有约50%会继续形成长期细胞系。此外,虽然检测到了产生所有主要Ig类别的永生化B细胞克隆,但IgM定向的前体比IgG或IgA产生定向的前体更有可能永生化。与新鲜感染EBV的B细胞中的这些发现相反,当在相同的有限稀释培养中测试来自先前建立的EBV诱导的B细胞系的B细胞时,Ig产生几乎总是与长期生长的证据相关。因此,感染EBV后,人类B细胞要么被短暂激活以增殖并分泌Ig,要么转化为大多数产生Ig的长期细胞系。

相似文献

1
Relationship between immunoglobulin production and immortalization by Epstein Barr virus.爱泼斯坦-巴尔病毒引起的免疫球蛋白产生与永生化之间的关系。
J Immunol. 1985 Aug;135(2):959-64.
2
Heterogeneity of EBV-transformable human B lymphocyte populations.EB病毒转化的人B淋巴细胞群体的异质性。
J Immunol. 1986 Jan;136(1):106-12.
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Stimulation of EBV-activated human B cells by monocytes and monocyte products. Role of IFN-beta 2/B cell stimulatory factor 2/IL-6.单核细胞及单核细胞产物对EB病毒激活的人B细胞的刺激作用。干扰素-β2/ B细胞刺激因子2/白细胞介素-6的作用
J Immunol. 1988 Jun 15;140(12):4329-36.
4
Patterns of isotype commitment in human B cells: limiting dilution analysis of Epstein Barr virus-infected cells.人类B细胞中的同种型定向模式:对爱泼斯坦-巴尔病毒感染细胞的有限稀释分析
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Phenotype, frequency, and EBV responsiveness of human marrow B and pre-B cells.人类骨髓B细胞和前B细胞的表型、频率及EB病毒反应性
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Ig isotypes produced by EBV-transformed B cells as a function of age and tissue distribution.EB病毒转化的B细胞产生的免疫球蛋白同种型与年龄及组织分布的关系。
J Immunol. 1988 Jun 1;140(11):3887-92.
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Limiting dilution analysis of the B cell compartment in human bone marrow.人骨髓中B细胞区室的有限稀释分析。
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In vitro regulation of IgA subclass production. III. Selective transformation of IgA1 producing cells by Epstein-Barr virus.体外IgA亚类产生的调节。III. 爱泼斯坦-巴尔病毒对产生IgA1细胞的选择性转化
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Immortalization of EBV-infected B cells is not influenced by exogenous signals acting on B cell proliferation. Effects of mutant EL-4 thymoma cells and transforming growth factor-beta.EB病毒感染的B细胞永生化不受作用于B细胞增殖的外源性信号影响。突变EL-4胸腺瘤细胞和转化生长因子-β的作用
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10
[Analysis of Epstein-Barr virus transformation of human lymphocytes: susceptibility of B lymphocyte subpopulations and differentiation stage of the transformed cells].[爱泼斯坦-巴尔病毒对人淋巴细胞的转化分析:B淋巴细胞亚群的易感性及转化细胞的分化阶段]
Hokkaido Igaku Zasshi. 1985 Sep;60(5):724-34.

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