Discordant effects of anti–VLA-4 treatment before and after onset of relapsing experimental autoimmune encephalomyelitis
Bradley E. Theien, … , Vijay K. Kuchroo, Stephen D. Miller
Bradley E. Theien, … , Vijay K. Kuchroo, Stephen D. Miller
Published April 15, 2001
Citation Information: J Clin Invest. 2001;107(8):995-1006. https://doi.org/10.1172/JCI11717.
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Article

Discordant effects of anti–VLA-4 treatment before and after onset of relapsing experimental autoimmune encephalomyelitis

Abstract

Initial migration of encephalitogenic T cells to the central nervous system (CNS) in relapsing experimental autoimmune encephalomyelitis (R-EAE), an animal model of multiple sclerosis (MS), depends on the interaction of the α4 integrin (VLA-4) expressed on activated T cells with VCAM-1 expressed on activated cerebrovascular endothelial cells. Alternate homing mechanisms may be employed by infiltrating inflammatory cells after disease onset. We thus compared the ability of anti–VLA-4 to regulate proteolipid protein (PLP) 139-151–induced R-EAE when administered either before or after disease onset. Preclinical administration of anti–VLA-4 either to naive recipients of primed encephalitogenic T cells or to mice 1 week after peptide priming, i.e., before clinical disease onset, inhibited the onset and severity of clinical disease. In contrast, Ab treatment either at the peak of acute disease or during remission exacerbated disease relapses and increased the accumulation of CD4+ T cells in the CNS. Most significantly, anti–VLA-4 treatment either before or during ongoing R-EAE enhanced Th1 responses to both the priming peptide and endogenous myelin epitopes released secondary to acute tissue damage. Collectively, these results suggest that treatment with anti–VLA-4 Ab has multiple effects on the immune system and may be problematic in treating established autoimmune diseases such as MS.

Authors

Bradley E. Theien, Carol L. Vanderlugt, Todd N. Eagar, Cheryl Nickerson-Nutter, Remederios Nazareno, Vijay K. Kuchroo, Stephen D. Miller

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Figure 1

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Anti–VLA-4 inhibits induction of, but exacerbates, ongoing clinical R-EA...
Anti–VLA-4 inhibits induction of, but exacerbates, ongoing clinical R-EAE. The indicated numbers of SJL mice were treated with rat control Ig or anti–VLA-4 (PS/2) beginning at day 7 (preclinical treatment), day 14 (acute-phase treatment), or day 24 (remission treatment) relative to priming with PLP139-151/CFA on day 0. Three treatments per week for 3 consecutive weeks were administered. (a and c) Short-term experiments from which animals were taken after three treatments and after nine treatments for immune assays (see Figures 46). Animals in experiments shown in b, d, e, and f also received nine treatments but were observed for a longer period of time. The data are expressed as mean clinical score versus day after priming (a, c, and e) and as the long-term relapse rate (b, d, and f). Data shown are representative of two to three separate experiments. AValues for the PS/2-treated mice are either significantly above or below those of the control Ig-treated mice; P < 0.05.