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进行性多发性硬化症中活化抑制细胞功能障碍

Activated suppressor cell dysfunction in progressive multiple sclerosis.

作者信息

Antel J P, Bania M B, Reder A, Cashman N

出版信息

J Immunol. 1986 Jul 1;137(1):137-41.

PMID:2940299
Abstract

Concanavalin A (Con A)-induced suppressor activity has previously been shown to be reduced in multiple sclerosis (MS) patients with active clinical disease. In this study, we demonstrate that OKT3, as well as Con A induced suppressor activity mediated by unfractionated peripheral blood mononuclear cells is reduced in patients with the progressive form of MS. By performing reconstitution experiments involving E+, T4+, or T8+ cells derived from either MS patients or controls, and normal allogeneic macrophages or E- cells, we sought to define the cellular basis for this suppressor defect. In both MS and control groups, E+ cells were required to obtain measurable levels of suppression. Suppressor levels induced by Con A-activated cultures containing E+ cells from MS patients were lower than those induced by those containing control donor E+ cells. Suppression mediated by T8+ cells from MS patients was also lower than for controls. In the control group, suppression mediated by T8+ cells exceeded that mediated by T4+ cells; such differences were not apparent in the MS group. These results suggest that although Con A-induced suppression can be mediated by a number of T and non-T cell subsets, the functional suppressor defect measured in the MS population does involve the T8+ cell subset.

摘要

刀豆球蛋白A(Con A)诱导的抑制活性先前已被证明在患有活动性临床疾病的多发性硬化症(MS)患者中降低。在本研究中,我们证明,在进行性MS患者中,OKT3以及由未分级外周血单个核细胞介导的Con A诱导的抑制活性降低。通过进行涉及来自MS患者或对照的E +、T4 +或T8 +细胞,以及正常同种异体巨噬细胞或E -细胞的重建实验,我们试图确定这种抑制缺陷的细胞基础。在MS组和对照组中,都需要E +细胞才能获得可测量的抑制水平。含有MS患者E +细胞的Con A激活培养物诱导的抑制水平低于含有对照供体E +细胞的培养物诱导的抑制水平。MS患者T8 +细胞介导的抑制也低于对照组。在对照组中,T8 +细胞介导的抑制超过T4 +细胞介导的抑制;在MS组中这种差异不明显。这些结果表明,尽管Con A诱导的抑制可由多种T细胞和非T细胞亚群介导,但在MS群体中测得的功能性抑制缺陷确实涉及T8 +细胞亚群。

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