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抗CD40单克隆抗体与爱泼斯坦-巴尔病毒在人B淋巴细胞激活和转化中的协同作用。

Synergy between anti-CD40 MAb and Epstein-Barr virus in activation and transformation of human B lymphocytes.

作者信息

Tsuchiyama L, Kieran J, Boyle P, Wetzel G D

机构信息

Preclinical Biology Research, Bayer Corp., Berkeley, CA 94701, USA.

出版信息

Hum Antibodies. 1997;8(1):43-7.

PMID:9265505
Abstract

For human B lymphocytes, Epstein-Barr virus (EBV) is a polyclonal activator, inducing both proliferation and Ig secretion. It is also a transforming virus capable of generating immortalized B cell lines. These early and late functions of EBV are not apparently connected. The receptor for EBV, CD21, also serves as a receptor for some complement components and is called CR2. This molecule associates with CD19 and TAPA-1 on the surface of B cells. This complex is involved in signaling B cells and participates in many responses. We have observed that simultaneous ligation of CD40 and the CD21 complex, by exposure to anti-CD40 MAbs and EBV, enhances both the short-term proliferation as well as the long-term transformation rate of human B lymphocytes. B cell proliferation shows synergy between anti-CD40 MAb and EBV. CD19 also appears to be involved in the synergistic activation of B cells through CD40 and CD21, since ligation of CD19 with anti-CD19 MAbs, either prior to or concomitant with exposure to anti-CD40 and EBV, markedly inhibits both proliferation and subsequent B cell transformation. These observations do not elucidate the mechanisms of B cell transformation employed by EBV but the do suggest a relationship between early proliferation and later transformation induced by the virus. Anti-CD40 enhances both these effects and anti-CD19 is capable of inhibiting both.

摘要

对于人类B淋巴细胞而言,爱泼斯坦-巴尔病毒(EBV)是一种多克隆激活剂,可诱导细胞增殖和免疫球蛋白分泌。它也是一种能够产生永生化B细胞系的转化病毒。EBV的这些早期和晚期功能显然没有关联。EBV的受体CD21也是某些补体成分的受体,被称为CR2。该分子与B细胞表面的CD19和TAPA-1相关联。这一复合体参与B细胞信号传导,并参与多种反应。我们观察到,通过暴露于抗CD40单克隆抗体和EBV同时连接CD40和CD21复合体,可提高人类B淋巴细胞的短期增殖以及长期转化率。B细胞增殖显示出抗CD40单克隆抗体和EBV之间的协同作用。CD19似乎也通过CD40和CD21参与B细胞的协同激活,因为在暴露于抗CD40和EBV之前或同时用抗CD19单克隆抗体连接CD19,可显著抑制增殖和随后的B细胞转化。这些观察结果并未阐明EBV用于B细胞转化的机制,但确实提示了该病毒诱导的早期增殖与晚期转化之间的关系。抗CD40增强了这两种效应,而抗CD19能够抑制这两种效应。

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