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Natural IgM Anti-leucocyte Autoantibodies (IgM-ALA) Regulate Inflammation Induced by Innate and Adaptive Immune Mechanisms
- 作者:Peter I. Lobo ; Kenneth L. Brayman ; Mark D. Okusa
- 关键词:Natural IgM ; anti ; leucocyte antibodies ; allograft rejection ; TH ; 17 ; renal IRI ; autoimmune insulitis
- 刊名:Journal of Clinical Immunology
- 出版年:2014
- 出版时间:July 2014
- 年:2014
- 卷:34
- 期:1-supp
- 页码:22-29
- 全文大小:4,192 KB
- 参考文献:1. Steele, EJ, Cunningham, AJ (1978) High proportion of Ig producing cells making autoantibody in normal mice. Nature 274: pp. 483-6 CrossRef
2. Dighiero, G, Guilbert, B, Fermand, JP, Lymberi, P, Danon, F, Avrameas, S (1983) Thirty-six human monoclonal immunoglobulins with antibody activity against cytoskeleton proteins, thyroglobulin, and native DNA: immunologic studies and clinical correlations. Blood 62: pp. 264-70
3. Hardy, RR, Hayakawa, K (1986) Development and physiology of Ly-1 B and its human homolog, Leu-1 B. Immunol Rev 93: pp. 53-79 CrossRef
4. Nakamura, M, Burastero, SE, Ueki, Y, Larrick, JW, Notkins, AL, Casali, P (1988) Probing the normal and autoimmune B cell repertoire with Epstein-Barr virus: frequency of B cells producing monoreactive high affinity autoantibodies in patients with Hashimoto’s disease and systemic lupus erythematosus. J Immunol 141: pp. 4165-72
5. Mouthon, L, Lacroix-Desmazes, S, Nobrega, A, Barreau, C, Coutinho, A, Kazatchkine, MD (1996) The self reactive antibody repertoire of normal human serum IgM is acquired in early childhood and remains conserved throughout life. Scand J Immunol 44: pp. 243-51 CrossRef
6. Clarke, SH, Arnold, LW (1998) B-1 cell development: evidence for an uncommitted immunoglobulin (Ig)M+ B cell precursor in B-1 cell differentiation. J Exp Med 187: pp. 1325-34 CrossRef
7. Casali, P, Burastero, SE, Nakamura, M, Inghirami, G, Notkins, AL (1987) Human lymphocytes making rheumatoid factor and antibody to ssDNA belong to Leu-1+ B-cell subset. Science 236: pp. 77-81 CrossRef
8. Hardy, RR, Hayakawa, K, Shimizu, M, Yamasaki, K, Kishimoto, T (1987) Rheumatoid factor secretion from human Leu-1+ B cells. Science 236: pp. 81-3 CrossRef
9. Kasaian, MT, Casali, P (1993) Autoimmunity-prone B-1 (CD5 B) cells, natural antibodies and self recognition. Autoimmunity 15: pp. 315-29 CrossRef
10. Rieben, R, Roos, A, Muizert, Y, Tinguely, C, Gerritsen, AF (1999) Daha M R Immunoglobulin M-enriched human intravenous immunoglobulin prevents complement activation in-vitro and in-vivo in a rat model of acute inflammation. Blood 93: pp. 942-8
11. Murakami, M, Tsubata, T, Shinkura, R, Nisitani, S, Okamoto, M, Yoshioka, H (1994) Oral administration of lipopolysaccharides activates B-1 cells in the peritoneal cavity and lamina propria of the gut and induces autoimmune symptoms in an autoantibody transgenic mouse. J Exp Med 180: pp. 111-21 CrossRef
12. Nisitani, S, Tsubata, T, Murakami, M, Honjo, T (1995) Administration of interleukin-5 or -10 activates peritoneal B-1 cells and induces autoimmune hemolytic anemia in anti-erythrocyte autoantibody-transgenic mice. Eur J Immunol 25: pp. 3047-52 CrossRef
13. Yang, Y, Tung, JW, Ghosn, EE, Herzenberg, LA (2007) Division and differentiation of natural antibody-producing cells in mouse spleen. Proc Natl Acad Sci U S A 104: pp. 4542-6 CrossRef
14. Ha, SA, Tsuji, M, Suzuki, K, Meek, B, Yasuda, N, Kaisho, T (2006) Regulation of B1 cell migration by signals through Toll-like receptors. J Exp Med 203: pp. 2541-50 CrossRef
15. Hayakawa, K, Asano, M, Shuiton, SA, Gui, M, Allman, D, Stewart, CL (1999) Positive selection of natural autoreactive B cells. Science 285: pp. 113-6 CrossRef
16. Baumgarth, N, Herman, OC, Jager, GC, Brown, L, Herzenberg, LA (1999) Innate and acquired humoral immunities to influenza virus are mediated by distinct arms of the immune system. Proc Natl Acad Sci U S A 96: pp. 2250-5
文摘
Little is known about the function of natural IgM autoantibodies, especially that of IgM anti-leukocyte autoantibodies (IgM-ALA). Natural IgM-ALA are present at birth and characteristically increase during inflammatory and infective conditions. Our prior clinical observations and those of other investigators showing fewer rejections in renal and cardiac allografts transplanted into recipients with high levels of IgM-ALA led us to investigate whether IgM-ALA regulate the inflammatory response. In this review, we show that IgM, in physiologic doses, inhibit pro-inflammatory cell function in-vitro. We also show in an IgM knockout murine model, with intact B cells and regulatory T cells, that there is more severe inflammation and loss of function in the absence of IgM after renal ischemia reperfusion injury and cardiac allograft rejection. Replenishing IgM in IgM knockout mice or increasing the levels of IgM-ALA in wild-type B6 mice significantly attenuated the inflammation in both of these inflammatory models that involve IFN-γ and IL-17. The protective effect on renal ischemia reperfusion injury Is mediated by IgM ALA as protection was lost when using IgM pre-adsorbed with leukocytes to remove IgM-ALA. We provide data to show that the anti-inflammatory effect of IgM is mediated, in part, by inhibiting TLR-4-induced NF-κB translocation into the nucleus and inhibiting differentiation of activated T cells into Th-1 and Th-17 cells. In additional studies, we also show that intra-peritoneal administration of IgM prevents NOD mice from developing autoimmune insulitis which also involves Th-1 and Th-17 cells. These observations highlight the importance of IgM-ALA in regulating excess inflammation mediated by both innate and adaptive immune mechanisms and where the inflammatory response involves Th-17 cells that are not effectively regulated by T regs, B regs, and IL-10. IgM-ALA may in part regulate inflammation by altering dendritic cell function, as dendritic cells pre-treated in-vitro with polyclonal IgM protected mice from renal IRI. The latter findings may have relevance for cell-based therapy.
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