Eotaxin-2 blockade ameliorates experimental autoimmune encephalomyelitis

被引:1
作者
Karin Mausner-Fainberg [1 ,2 ]
Arnon Karni [1 ,2 ]
Jacob George [3 ,2 ]
Michal Entin-Meer [4 ,2 ]
Arnon Afek [2 ,5 ]
机构
[1] Department of Neurology, The Neuroimmunology Laboratory,64239 Tel Aviv, Israel
[2] Department of Cardiology, Kaplan Medical Center,Rehovot, 64239 Tel Aviv, Israel
[3] Department of Cardiology, TASMC, 64239 Tel Aviv, Israel
来源
World Journal of Immunology | 2013年 / 01期
关键词
Multiple sclerosis; Experimental autoimmune encephalomyelitis; Eotaxin-2; Neutralizing monoMausner-Fainberg K et al.Eotaxin-2 blockade ameliorates EAE;
D O I
暂无
中图分类号
R744.51 [];
学科分类号
1002 ;
摘要
AIM: To study the effect of blocking the eo-2 pathwayon the development and severity of experimental autoimmune encephalomyelitis(EAE). METHODS: We produced m Ab directed against eo-2,named D8. MOG35-55 induced-EAE mice were dailyintravenously injected with either 25 μg or 100 μg D8,or with vehicle control alone [phosphate-buffered saline(PBS)], starting from day 0 post immunization and weremonitored for EAE clinical score(n = 10 in each group).Mice were sacrificed on day 58 and their sera were assessed for the presence of anti-myelin oligodendrocyteglycoprotein(anti-MOG) antibodies autoantibodies, aswell as for the profile of pro-inflammatory cytokines andchemokines. Histological analysis of brain sections wasperformed by hematoxylin and eosin staining.RESULTS: Daily treatment of EAE induced mice with D8 significantly decreased the severity of EAE symptoms. Treatment with both concentrations of D8 ameliorated EAE symptoms compared to PBS treated mice, starting from day 42 post immunization(0.89 ± 0.35 in D8 25 μg and D8 100 μg treated groups vs 2.11 ± 0.38 in the PBS treated group, P = 0.03). A significant improvement in EAE clinical score compared to total Ig G treated mice was observed with the higher concentration of D8(0.81 ± 0.38 in D8 100 μg treated group vs 2.11 ± 0.31 in Ig G1 treated group, on day 56 post immunization, P = 0.04). D8 treated mice with EAE did not significantly exhibit lower sera levels of anti-MOG autoantibodies compared to Ig G-treated mice. However, they expressed lower sera levels of the pro-inflammatory cytokines: tumor necrosis factor(7.8 ± 0.2 pg/m L in D8 100 μg treated mice vs 19.9 ± 3.4 pg/m L in Ig G treated mice, P = 0.005) and interferon-gamma(1.4 ± 0.6 pg/m L in D8 100 μg treated mice vs 3.6 ± 0.4 pg/m L in Ig G treated mice, P = 0.02), as well as reduced levels of the chemokine macrophage chemoattractant protein-1(27.2 ± 3.1 pg/m L in D8 100 μg treated mice vs 63.7 ± 12.3 pg/m L in Ig G treated mice, P = 0.03). These findings indicate that blocking the eo-2 pathway in EAE may affect not only eosinophil infiltration into the central nervous system(CNS), but also have an effect on monocytes and T cells, but not humoral, mediated responses. Histological analysis of the brains of D8 treated mice with EAE support that this treatment decreases immune cells infiltrates in the CNS.CONCLUSION: Taken together, these findings suggest a role for eo-2 in EAE pathogenesis and consequentially may support a therapeutic potential of anti-eo-2 neutralizing m Ab in multiple sclerosis.
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页码:7 / 14
页数:8
相关论文
共 37 条
[21]  
Expression of a Functional Eotaxin (CC Chemokine Ligand 11) Receptor CCR3 by Human Dendritic Cells. Sylvie Beaulieu,Davide F. Robbiani,Xixuan Du,Elaine Rodrigues,Ralf Ignatius,Yang Wei,Paul Ponath,James W. Young,Melissa Pope,Ralph M. Steinman,Svetlana Mojs. J. Immunol . 2002
[22]  
Augmentation of demyelination in rat acute allergic encephalomyelitis by circulating mouse monoclonal antibodies directed against a myelin/oligodendrocyte glycoprotein. Linington C,Bradl M,Lassmann H,Brunner C,Vass K. The American journal of pathology . 1988
[23]  
Cerebrospinal fluid eosinophilia. A manifestation of a disorder resembling multiple sclerosis in childhood. Snead O C,Kalavsky S M. The Journal of Pediatrics . 1976
[24]  
Inhibition of leukotriene B4-receptor interaction suppresses eosinophil infiltration and disease pathology in a murine model of experimental allergic encephalomyelitis. Gladue R P,Carroll L A,Milici A J,Scampoli D N,Stukenbrok H A,Pettipher E R,Salter E D,Contillo L,Showell H J. The Journal of experimental medicine . 1996
[25]  
Eotaxin-2 Generation Is Differentially Regulated by Lipopolysaccharide and IL-4 in Monocytes and Macrophages. Kimiko Watanabe,Peter J. Jose,Sara M. Rank. J. Immunol . 2002
[26]  
Absence of mono cyte chemoattractant protein 1 in mice leads to decreased local macropHage recruitment and antigen specific T helper cell type 1 immune response in experimental autoimmune encepHalomyelitis. Huang D R,Wang J,Kivisakk P,et al. The Journal of Experimental Medicine . 2001
[27]  
CNS-derived interleukin-4 is essential for the regulation of autoimmune inflammation and induces a state of alternative activation in microglial cells. Ponomarev Eugene D,Maresz Katarzyna,Tan Yanping,Dittel Bonnie N. The Journal of neuroscience : the official journal of the Society for Neuroscience . 2007
[28]  
IL-6 blockade inhibits the induction of myelin antigen-specific Th17 cells and Th1 cells in experimental autoimmune encephalomyelitis. Serada Satoshi,Fujimoto Minoru,Mihara Masahiko,Koike Nobuo,Ohsugi Yoshiyuki,Nomura Shintaro,Yoshida Hiroto,Nishikawa Teppei,Terabe Fumitaka,Ohkawara Tomoharu,Takahashi Tsuyoshi,Ripley Barry,Kimura Akihiro,Kishimoto Tadamitsu,Naka Tetsuji. Proceedings of the National Academy of Sciences of the United States of America . 2008
[29]  
IL-23 is critical in the induction but not in the effector phase of experimental autoimmune encephalomyelitis. Thakker P,Leach MW,Kuang W, et al. J Immunol . 2007
[30]  
Raine CS: Homing to central nervous system vasculature by antigen-specific lymphocytes.I. Localization of 14c-labeled cells during acute, chronic and relapsing experimental allergic encephalitis. Cross AH,Canella B,Brosnan CF. Laboratory Investigation . 1990
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