IN-VITRO AND IN-VIVO INHIBITION OF MITOGEN-DRIVEN T-CELL ACTIVATION BY RECOMBINANT INTERFERON-BETA

被引：98

作者：

RUDICK, RA

CARPENTER, CS

COOKFAIR, DL

TUOHY, VK

RANSOHOFF, RM

机构：

[1] CLEVELAND CLIN EDUC FDN, DEPT GEN MED SCI, CLEVELAND, OH 44106 USA

[2] SUNY BUFFALO, DEPT SOCIAL & PREVENT MED, BUFFALO, NY 14260 USA

[3] SUNY BUFFALO, DEPT NEUROL, BUFFALO, NY 14260 USA

[4] CLEVELAND CLIN EDUC FDN, DEPT MOLEC BIOL, CLEVELAND, OH 44106 USA

来源：

NEUROLOGY | 1993年 / 43卷 / 10期

关键词：

D O I：

10.1212/WNL.43.10.2080

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Recombinant interferon beta (rIFNbeta) is being tested as experimental immunotherapy for exacerbating-remitting MS. To clarify the possible mechanisms of a therapeutic response to rIFNbeta in MS patients, we conducted studies on the effects of rIFNbeta on mitogen-driven T-cell activation by stimulating peripheral blood mononuclear cells (PBMC) with concanavalin A (ConA) or with anti-CD3 monoclonal antibodies in the presence or absence of rIFNbeta. We monitored T-cell activation using proliferation assays or by expression of surface activation markers detected by flow cytometry. In vitro rIFNbeta, in concentrations greater-than-or-equal-to 10 U/ml, inhibited PBMC proliferation or surface expression of interleukin-2 receptor (IL-2R), transferrin receptor, or CD2. In contrast, rIFNgamma augmented mitogen-driven IL-2R expression. PBMC isolated from normal volunteers or MS patients responded to ConA and rIFNbeta in a similar manner. We conducted pilot in vivo studies in exacerbating-remitting MS patients participating in a double-blind placebo-controlled clinical trial of rIFNbeta. PBMC were isolated from study participants immediately before and 24 hours after a weekly study injection. IL-2R expression by T cells was determined following a ConA stimulus. While there was no significant change following placebo injection, rIFNbeta recipients showed significantly reduced ConA-driven IL-2R expression following study injection. The results document in vitro and in vivo inhibition of mitogen-driven T-cell activation by rIFNbeta. This suggests a possible mechanism underlying a therapeutic response to rIFNbeta in MS patients.

引用

页码：2080 / 2087

页数：8

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