Comparison of CpG s-ODNs, chromatin immune complexes, and dsDNA fragment immune complexes in the TLR9-dependent activation of rheumatoid factor B cells

Ann Marshak-Rothstein; Liliana Busconi; Christina M. Lau; Abigail S. Tabor; Elizabeth A. Leadbetter; Shizuo Akira; Arthur M. Krieg; Grayson B. Lipford; Gregory A. Viglianti; Ian R. Rifkin

doi:10.1179/096805104225005850

Comparison of CpG s-ODNs, chromatin immune complexes, and dsDNA fragment immune complexes in the TLR9-dependent activation of rheumatoid factor B cells

Ann Marshak-Rothstein, Liliana Busconi, Christina M. Lau, Abigail S. Tabor, Elizabeth A. Leadbetter, Shizuo Akira, Arthur M. Krieg, Grayson B. Lipford, Gregory A. Viglianti, Ian R. Rifkin

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Resumen

Synthetic single-stranded oligodeoxynucleotides (15-30 bp) containing CpG motifs and phosphorothioate backbones (CpG s-ODN), immune complexes consisting of anti-nucleosome mAbs and mammalian chromatin (chromatin IC), and immune complexes consisting of anti-hapten mAbs and haptenated-double stranded DNA fragments (∼600 bp) can all effectively stimulate transgenic B cells expressing a rheumatoid factor receptor by a TLR9-dependent process. However, differential sensitivity to both s-ODN and small molecule inhibitors suggests that stimulatory CpG sODN and chromatin IC may either access TLR9 via different routes or depend on discrete activation parameters. These data have important implications regarding the therapeutic application of TLR9 inhibitors to the treatment of systemic autoimmune diseases.

Idioma original	English (US)
Páginas (desde-hasta)	247-251
Número de páginas	5
Publicación	Journal of Endotoxin Research
Volumen	10
N.º	4
DOI	https://doi.org/10.1179/096805104225005850
Estado	Published - 2004
Publicado de forma externa	Sí

ASJC Scopus subject areas

Infectious Diseases
Molecular Biology
Cell Biology
Microbiology
Immunology

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10.1179/096805104225005850

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Marshak-Rothstein, A., Busconi, L., Lau, C. M., Tabor, A. S., Leadbetter, E. A., Akira, S., Krieg, A. M., Lipford, G. B., Viglianti, G. A., & Rifkin, I. R. (2004). Comparison of CpG s-ODNs, chromatin immune complexes, and dsDNA fragment immune complexes in the TLR9-dependent activation of rheumatoid factor B cells. Journal of Endotoxin Research, 10(4), 247-251. https://doi.org/10.1179/096805104225005850

Marshak-Rothstein, A, Busconi, L, Lau, CM, Tabor, AS, Leadbetter, EA, Akira, S, Krieg, AM, Lipford, GB, Viglianti, GA & Rifkin, IR 2004, 'Comparison of CpG s-ODNs, chromatin immune complexes, and dsDNA fragment immune complexes in the TLR9-dependent activation of rheumatoid factor B cells', Journal of Endotoxin Research, vol. 10, n.º 4, pp. 247-251. https://doi.org/10.1179/096805104225005850

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title = "Comparison of CpG s-ODNs, chromatin immune complexes, and dsDNA fragment immune complexes in the TLR9-dependent activation of rheumatoid factor B cells",

abstract = "Synthetic single-stranded oligodeoxynucleotides (15-30 bp) containing CpG motifs and phosphorothioate backbones (CpG s-ODN), immune complexes consisting of anti-nucleosome mAbs and mammalian chromatin (chromatin IC), and immune complexes consisting of anti-hapten mAbs and haptenated-double stranded DNA fragments (∼600 bp) can all effectively stimulate transgenic B cells expressing a rheumatoid factor receptor by a TLR9-dependent process. However, differential sensitivity to both s-ODN and small molecule inhibitors suggests that stimulatory CpG sODN and chromatin IC may either access TLR9 via different routes or depend on discrete activation parameters. These data have important implications regarding the therapeutic application of TLR9 inhibitors to the treatment of systemic autoimmune diseases.",

keywords = "Autoreactive B cells, Bafilomycin A, Chromatin immune complexes, Inhibitory s-ODN, Toll-like receptor 9",

author = "Ann Marshak-Rothstein and Liliana Busconi and Lau, {Christina M.} and Tabor, {Abigail S.} and Leadbetter, {Elizabeth A.} and Shizuo Akira and Krieg, {Arthur M.} and Lipford, {Grayson B.} and Viglianti, {Gregory A.} and Rifkin, {Ian R.}",

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AU - Lau, Christina M.

AU - Tabor, Abigail S.

AU - Leadbetter, Elizabeth A.

AU - Akira, Shizuo

AU - Krieg, Arthur M.

AU - Lipford, Grayson B.

AU - Viglianti, Gregory A.

AU - Rifkin, Ian R.

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AB - Synthetic single-stranded oligodeoxynucleotides (15-30 bp) containing CpG motifs and phosphorothioate backbones (CpG s-ODN), immune complexes consisting of anti-nucleosome mAbs and mammalian chromatin (chromatin IC), and immune complexes consisting of anti-hapten mAbs and haptenated-double stranded DNA fragments (∼600 bp) can all effectively stimulate transgenic B cells expressing a rheumatoid factor receptor by a TLR9-dependent process. However, differential sensitivity to both s-ODN and small molecule inhibitors suggests that stimulatory CpG sODN and chromatin IC may either access TLR9 via different routes or depend on discrete activation parameters. These data have important implications regarding the therapeutic application of TLR9 inhibitors to the treatment of systemic autoimmune diseases.

KW - Autoreactive B cells

KW - Bafilomycin A

KW - Chromatin immune complexes

KW - Inhibitory s-ODN

KW - Toll-like receptor 9

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Comparison of CpG s-ODNs, chromatin immune complexes, and dsDNA fragment immune complexes in the TLR9-dependent activation of rheumatoid factor B cells

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