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来那度胺抑制多发性硬化进展与CD4⁺/CD45RA⁺细胞上调及CD4⁺/CD45RO⁺细胞下调有关。

Inhibition of the progression of multiple sclerosis by linomide is associated with upregulation of CD4+/CD45RA+ cells and downregulation of CD4+/CD45RO+ cells.

作者信息

Lehmann D, Karussis D, Mizrachi-Koll R, Linde A S, Abramsky O

机构信息

Department of Neurology and Laboratory of Neuroimmunology, Hadassah-Hebrew University Hospital, Jerusalem, IL-91120, Israel.

出版信息

Clin Immunol Immunopathol. 1997 Nov;85(2):202-9. doi: 10.1006/clin.1997.4444.

Abstract

In a recent double-blind, phase II study, conducted in our department, we showed that Linomide-treated MS patients had significantly less active lesions (in serial monthly MRI tests) and a tendency for clinical stabilization. Here we present the immunological evaluation of the patients who participated in this study and propose a novel mechanism by which Linomide downregulates autoreactivity. Peripheral blood leukocytes (PBLs), serum, and CSF samples were obtained at two to four time points over the 6 months of the trial. Flow cytometric analysis (FACS) of the CD5/CD19, CD4/CD8, CD14/CD3, CD16/CD3, CD45RA/CD4, and CD45RO/CD4 surface markers on PBLs was performed and the levels of the IL-1beta, IL-2, IL-4, IL-6, IL-10, TNF-alpha, IFN-gamma, and IL-2R were also examined. White blood counts of Linomide-treated patients were consistently elevated throughout the treatment period (P = 0.002-0.04). Cytokines levels in serum and CSF were highly fluctuating and we could not detect any clear trend as a result of Linomide treatment. FACS analysis showed that Linomide treatment significantly increased the percentage of the CD4+/CD45RA+ cells (from 35.5% at baseline to 42.3% at week 24; P = 0.02), and decreased CD4+/CD45RO+ lymphocytes (62.6% at baseline vs 53.7% at week 24, P = 0.02). Linomide also induced a transient increase in the NK-cells, the NK 1.1 cells, and the CD5 B-cells (P = 0.02). Upregulation of naive CD45RA T-lymphocytes and parallel downregulation of memory CD45RO cells seems to be one of the main mechanisms by which Linomide inhibits MS activity and may represent an alternative immunomodulating approach for the treatment of MS and autoimmunity in general.

摘要

在我们科室最近进行的一项双盲II期研究中,我们发现接受利诺米德治疗的多发性硬化症(MS)患者的活动性病灶显著减少(在每月进行的系列MRI检查中),并且有临床病情稳定的趋势。在此,我们展示了参与本研究患者的免疫学评估结果,并提出了一种利诺米德下调自身反应性的新机制。在试验的6个月期间,于两到四个时间点采集外周血白细胞(PBL)、血清和脑脊液样本。对PBL上的CD5/CD19、CD4/CD8、CD14/CD3、CD16/CD3、CD45RA/CD4和CD45RO/CD4表面标志物进行流式细胞术分析(FACS),并检测IL-1β、IL-2、IL-4、IL-6、IL-10、TNF-α、IFN-γ和IL-2R的水平。接受利诺米德治疗的患者在整个治疗期间白细胞计数持续升高(P = 0.002 - 0.04)。血清和脑脊液中的细胞因子水平波动很大,我们未能检测到利诺米德治疗带来的任何明显趋势。FACS分析显示,利诺米德治疗显著增加了CD4+/CD45RA+细胞的百分比(从基线时的35.5%增至第24周时的42.3%;P = 0.02),并减少了CD4+/CD45RO+淋巴细胞(基线时为62.6%,第24周时为53.7%,P = 0.02)。利诺米德还使自然杀伤细胞、NK 1.1细胞和CD5 B细胞短暂增加(P = 0.02)。幼稚CD45RA T淋巴细胞的上调以及记忆CD45RO细胞的平行下调似乎是利诺米德抑制MS活动的主要机制之一,并且可能代表了一种用于治疗MS及一般自身免疫性疾病的替代免疫调节方法。

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