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循环中的CD20dim T淋巴细胞随年龄增长而增加:记忆性细胞毒性表型的证据。

Circulating CD20dim T-lymphocytes increase with age: evidence for a memory cytotoxic phenotype.

作者信息

Storie I, Wilson G A, Granger V, Barnett D, Reilly J T

机构信息

Department of Haematology, Northern General Hospital, Sheffield, UK.

出版信息

Clin Lab Haematol. 1995 Dec;17(4):323-8.

PMID:8697727
Abstract

The CD20 antigen has been regarded as a B lineage specific, 35 kDa, non-glycosylated membrane phosphoprotein, which functions as either a Ca2+ ion channel or as a regulatory protein of such a channel. Weak expression of CD20 (CD20dim), however, has recently been reported on a sub-population of T lymphocytes. We present results which confirm the existence of a CD20dim T lymphocyte population and show that such cells have a reduced antibody-binding capacity, when compared to CD20bright B-cells (10337 +/- 642 and 346311 +/- 24264 respectively). In addition, CD20dim cell counts vary with age, with the highest levels occurring in octogenarians: cord blood 0.3 +/- 0.1% (n = 13), 20-60 year-old group 2.1 +/- 1.1% (n = 18) and individuals > or = 61 years of age 6.9 +/- 3.2% (n = 10) (P < 0.001). Further characterization of CD20dim T cells, using three colour flow cytometry, demonstrated a predominantly memory cytotoxic phenotype, in that the cells were CD8+CD28+CD45RO+T-CR alpha beta +CD38-HLA-DR-.

摘要

CD20抗原一直被认为是一种B淋巴细胞特异性的、35 kDa的非糖基化膜磷蛋白,其功能为钙离子通道或此类通道的调节蛋白。然而,最近有报道称在T淋巴细胞亚群上存在CD20弱表达(CD20dim)。我们展示的结果证实了CD20dim T淋巴细胞群体的存在,并表明与CD20高表达的B细胞相比(分别为10337±642和346311±24264),此类细胞的抗体结合能力降低。此外,CD20dim细胞计数随年龄变化,在八旬老人中水平最高:脐血为0.3±0.1%(n = 13),20 - 60岁组为2.1±1.1%(n = 18),61岁及以上个体为6.9±3.2%(n = 10)(P < 0.001)。使用三色流式细胞术对CD20dim T细胞进行进一步表征,结果显示其主要为记忆性细胞毒性表型,即细胞为CD8 + CD28 + CD45RO + T - CRαβ + CD38 - HLA - DR - 。

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