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多发性硬化症中CD45阳性T细胞亚群对髓鞘碱性蛋白的不同反应。

Differential responses of CD45+ve T-cell subsets to MBP in multiple sclerosis.

作者信息

Ponsford M, Mazza G, Coad J, Campbell M J, Zajicek J, Wraith D C

机构信息

Department of Pathology and Microbiology, School of Medical Sciences, University of Bristol, Bristol, UK.

出版信息

Clin Exp Immunol. 2001 May;124(2):315-22. doi: 10.1046/j.1365-2249.2001.01507.x.

Abstract

The proliferative response of preparations of whole PBMC populations from 20 healthy individuals and 28 multiple sclerosis (MS) patients to purified protein derivative (PPD) and myelin basic protein (MBP) was monitored in a kinetic assay over a period of up to 10 days. PPD produced a classical secondary response in both groups, the magnitude being significantly reduced in the MS cohort. The magnitude and pattern of response to MBP did not differ between the two populations. The kinetic profile characteristic of a primary response was observed in both groups. Enrichment of the CD45RO+ve and CD45RA+ve T-cell subsets in PBMC led to a secondary response to PPD in the RO+ve and primary response in the RA+ve population in both groups. The response to MBP in both RO+ve and RA+ve populations exhibited primary kinetics in both MS patients and healthy individuals. However, the use of T-cell subset enriched populations allowed a finer dissection of the response to MBP which highlighted the more active role of RO-positive cells in MS patients. The most striking difference between patients and healthy individuals occurred on day 4 of culture when a greater response to MBP occurred in the CD45RO enriched population, paralleling the response to PPD, in the majority of patients. Futhermore in 4/8 patients and only 1/8 healthy individuals the response in the RO+ve cultures was maintained at a higher level than that seen in the corresponding RA+ve cultures throughout the culture period. This data indicates that a measurable memory response to MBP exists in MS patients implying prior activation of MBP reactive T lymphocytes during the course of disease.

摘要

在一项长达10天的动力学分析中,监测了来自20名健康个体和28名多发性硬化症(MS)患者的全外周血单个核细胞(PBMC)群体制剂对纯化蛋白衍生物(PPD)和髓鞘碱性蛋白(MBP)的增殖反应。PPD在两组中均产生了典型的二次反应,MS队列中的反应强度显著降低。两组对MBP的反应强度和模式没有差异。在两组中均观察到了初级反应的动力学特征。PBMC中CD45RO+阳性和CD45RA+阳性T细胞亚群的富集导致两组中RO+阳性群体对PPD产生二次反应,RA+阳性群体产生初级反应。RO+阳性和RA+阳性群体对MBP的反应在MS患者和健康个体中均表现出初级动力学。然而,使用富集T细胞亚群的群体可以更精细地剖析对MBP的反应,这突出了RO阳性细胞在MS患者中更积极的作用。患者和健康个体之间最显著的差异出现在培养的第4天,此时在大多数患者中,CD45RO富集群体对MBP的反应更大,与对PPD的反应相似。此外,在4/8的患者中,只有1/8的健康个体,RO+阳性培养物中的反应在整个培养期间维持在高于相应RA+阳性培养物的水平。这些数据表明,MS患者中存在对MBP的可测量记忆反应,这意味着在疾病过程中MBP反应性T淋巴细胞先前被激活。

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