EXPRESSION OF THE FC RECEPTOR FOR IGG (FC-GAMMA-RII/CDW32) BY HUMAN CIRCULATING T-LYMPHOCYTES AND B-LYMPHOCYTES

被引：0

作者：

MANTZIORIS, BX

BERGER, MF

SEWELL, W

ZOLA, H

机构：

[1] FLINDERS UNIV S AUSTRALIA,MED CTR,DEPT CLIN IMMUNOL,BEDFORD PK,SA 5042,AUSTRALIA

[2] FLINDERS UNIV S AUSTRALIA,BEDFORD PK,SA 5042,AUSTRALIA

[3] ST VINCENTS HOSP,CTR IMMUNOL,SYDNEY,NSW 2010,AUSTRALIA

[4] UNIV NEW S WALES,SYDNEY,NSW 2010,AUSTRALIA

来源：

JOURNAL OF IMMUNOLOGY | 1993年 / 150卷 / 11期

关键词：

D O I：

暂无

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Tissue-specific isoforms of the human FcR for IgG FcgammaRII (CDw32) have previously been described by using mAb. These mAb were shown to exhibit different patterns of reactivity with lymphocytes. Among human PBL, FcgammaRII has been detected on B cells but not T cells when assessed by flow cytometry and microscopy with the use of mAb KB61 and 41H16. Although KB61 and 41H16 were found to react with B cells, the mAb IV.3, CIKM5, and 2E1 did not react with any PBL subset. In this study, we show that KB61 and 41H16 react strongly with the majority (93-96%) of B cells (CD20+), and weakly with a proportion (18-42%) of T cells (CD3+), including 10 to 14% of CD4+ and 27 to 69% of CD8+ cells. In addition, mRNA for FcgammaRII was detected in purified CD3+CD8high+ lymphocytes by polymerase chain reaction. KB61 and 41H16 also reacted with a majority of CD3-CD16/CD56+ cells, and CD3-CD20- cells. These findings indicate that a subset of T cells and non-T/non-B cells express FcgammaRII, and are of interest in the light of previous studies which postulate that human FcgammaR+ cells and FcgammaRII+ murine T cells suppress the B cell immune response.

引用

页码：5175 / 5184

页数：10

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