[免疫球蛋白产生的调节:细胞受体对这些分子Fc部分的作用]。

Annales d'immunologie Pub Date : 1982-09-01
J P Revillard, L T Lê Thi Bich-Thuy
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引用次数: 0

摘要

本文旨在综述Ig Fc部分受体在人B淋巴细胞多克隆活化中的作用。IgG Fc片段被单核细胞消化成肽,引发b细胞分化并释放一种称为Fc TRF的t细胞替代因子。在PWM和单核细胞存在的情况下,未结合的聚集IgG抑制了b细胞向IgG合成细胞的分化。这种抑制不是同型特异性的。在结合聚集的IgG后,T细胞能够对PWM诱导的b细胞分化表现出同型限制性抑制。最后,从T淋巴细胞或B淋巴细胞或中性粒细胞释放的可溶性Fc γ R被发现抑制IgG的合成和B细胞成熟为IgM或Ig a分泌细胞。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
[Regulation of immunoglobulin production: role of the cellular receptors for the Fc portion of these molecules].

The aim of this paper was to review the action of the receptors for the Fc portion of Ig on the polyclonal activation of human B lymphocytes. The IgG Fc fragments were shown to be digested by monocytes into peptides which triggered B-cell differentiation and the release of a T-cell replacing factor termed (Fc)TRF. In the presence of PWM and monocytes, unbound aggregated IgG suppressed B-cell differentiation into Ig-synthesizing cells. This suppression was not isotype-specific. After having bound aggregated IgG, T cells were able to display an isotype-restricted suppression of B-cell differentiation induced by PWM. Finally, soluble Fc gamma R released from T or B lymphocytes or neutrophils were found to inhibit both the synthesis of IgG and the maturation of B cells into IgM or Ig A-secreting cells.

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