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人类酗酒者中T细胞黏附标志物以及CD45R和CD57抗原的调节

Modulation of T-cell adhesion markers, and the CD45R and CD57 antigens in human alcoholics.

作者信息

Cook R T, Ballas Z K, Waldschmidt T J, Vandersteen D, LaBrecque D R, Cook B L

机构信息

Department of Pathology, Veteran's Affairs Medical Center, Iowa City, Iowa 52246, USA.

出版信息

Alcohol Clin Exp Res. 1995 Jun;19(3):555-63. doi: 10.1111/j.1530-0277.1995.tb01548.x.

Abstract

Direct and indirect evidence indicates that T cells are altered in alcoholics. The most commonly reported changes under direct examination have been consistent with an increased level of activation as reflected by shifts in the ratio of common leukocyte antigen isoforms expressed at the cell surface, by increases in the expression of class II antigen, or by alterations in the expression of various adhesion molecules. Functional evidence for T-cell abnormality includes loss of delayed hypersensitivity and a number of findings attributed to dysregulation of B cells by alcoholic T cells; these include the widely reported distrubances of immunoglobulin production in vivo and a range of abnormal responses when T and B cells are combined in vitro. Detailed flow cytometric examination of T cells from alcoholics with or without active liver disease reveals a significant loss of L-selectin CD8+ T cells, but not usually of CD4+ T cells. There is an inverse increase in the expression of CD11b on the CD8+ cells that have decreased L-selectin+ percentages. Both CD8+ and CD4+ T cells in alcoholics display a significant loss of the CD45RA isoform and a gain of cells exhibiting the CD45RO isoform. Other surface alterations include increased expression of CD57, a marker most commonly associated on T cells with conditions of chronic increased antigenic exposure. It is argued that these and other T-cell alterations in alcoholics are cytokine-driven in part and result in T-cell differentiation states that are functionally inappropriate.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

直接和间接证据表明,酗酒者的T细胞发生了改变。直接检测中最常报告的变化与激活水平的提高一致,这表现为细胞表面表达的常见白细胞抗原异构体比例的变化、II类抗原表达的增加或各种黏附分子表达的改变。T细胞异常的功能证据包括迟发型超敏反应的丧失以及一些归因于酒精性T细胞对B细胞调节异常的发现;这些发现包括体内免疫球蛋白产生的广泛紊乱以及T细胞和B细胞在体外联合时的一系列异常反应。对患有或未患有活动性肝病的酗酒者的T细胞进行详细的流式细胞术检查发现,L-选择素CD8+ T细胞显著减少,但CD4+ T细胞通常没有减少。在L-选择素+百分比降低的CD8+细胞上,CD11b的表达呈反向增加。酗酒者的CD8+和CD4+ T细胞均显示CD45RA异构体显著减少,而表现出CD45RO异构体的细胞增加。其他表面变化包括CD57表达增加,CD57是一种最常与T细胞上慢性抗原暴露增加的情况相关的标志物。有人认为,酗酒者的这些以及其他T细胞改变部分是由细胞因子驱动的,并导致功能上不适当的T细胞分化状态。(摘要截选至250字)

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