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Analysis of CD27 surface expression on T cell subsets in MS patients and control individuals.

作者信息

Hintzen R Q, Fiszer U, Fredrikson S, Rep M, Polman C H, van Lier R A, Link H

机构信息

Department of Neurology, Free University Hospital, Amsterdam, Netherlands.

出版信息

J Neuroimmunol. 1995 Jan;56(1):99-105. doi: 10.1016/0165-5728(94)00137-d.

DOI:10.1016/0165-5728(94)00137-d
PMID:7822487
Abstract

Within the peripheral blood, CD4+CD27- T cells only reside within the CD45RA- (memory or primed) T cell subset. Cells with this phenotype have characteristics of specialized effector T cells according to their cytokine secretion profiles and the expression of tissue-specific adhesion molecules. This subset was previously found to be increased in certain diseases that are associated with immune activation. Therefore we analyzed CD27 expression of peripheral blood and CSF T cells in MS patients. Within the CD4+ T cell subset no differences were seen between MS patients and controls in proportions of CD45RA-CD27- cells. However, when the CD3+ T cell compartment was analyzed, CD27- cells were also found within the CD45RA+ subset. These cells, most likely CD8+, are significantly reduced in PBL and CSF of MS patients as compared with OND patients. In MS and OND groups the level of CD27- cells in peripheral blood correlated significantly with that in CSF, indicating a balanced migration of CD27- cells between the two compartments. In OIND patients, however, this equilibrium was lost. The correlation of the level of CD27+ cells with the amount of intrathecally produced IgG in MS patients may suggest that CD27+ cells are responsible for B cell help in this disease.

摘要

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