CpG Stimulation of Primary Mouse B Cells Is Blocked by Inhibitory Oligodeoxyribonucleotides at a Site Proximal to NF-<i>κ</i>B Activation

Lenert, Petar; Stunz, Laura L.; Yi, Ae-Kyung; Krieg, Arthur Μ.; Ashman, Robert F.

doi:10.1089/108729001317022241

Cited by 104 publications

(92 citation statements)

References 51 publications

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“…3 and 4). Consistent with these findings, suppressive motifs were recently shown to down-regulate CpG-dependent NF-B and AP-1 induction (17,18). These observations suggest that CpG motifs must continuously signal receptive cells for triggering to persist.…”

Section: Discussionsupporting

confidence: 62%

Effect of Suppressive DNA on CpG-Induced Immune Activation

Yamada

Gürsel

Takeshita

et al. 2002

The Journal of Immunology

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Bacterial DNA and synthetic oligodeoxynucleotides (ODN) containing unmethylated CpG motifs stimulate a strong innate immune response. This stimulation can be abrogated by either removing the CpG DNA or adding inhibitory/suppressive motifs. Suppression is dominant over stimulation and is specific for CpG-induced immune responses (having no effect on LPS- or Con A-induced activation). Individual cells noncompetitively internalize both stimulatory and suppressive ODN. Studies using ODN composed of both stimulatory and suppressive motifs indicate that sequence recognition proceeds in a 5′→3′ direction, and that a 5′ motif can block recognition of immediately 3′ sequences. These findings contribute to our understanding of the immunomodulatory activity of DNA-based products and the rules that govern immune recognition of stimulatory and suppressive motifs.

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Section: Discussionsupporting

confidence: 62%

Effect of Suppressive DNA on CpG-Induced Immune Activation

Yamada

Gürsel

Takeshita

et al. 2002

The Journal of Immunology

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“…TCR ϭ T cell receptor. activation and may thus limit the pathologic changes caused by CpG-driven immune responses (10,13,25).…”

Section: Discussionmentioning

confidence: 99%

“…The mechanism by which suppressive ODNs inhibit the activity of CpG DNA is a matter of considerable interest. Recent studies suggest that suppressive ODNs interfere with CpG-mediated cell signaling upstream of nuclear factor B activation (11,25). However, suppressive ODNs do not block the cellular uptake of CpG DNA or binding to Toll-like receptor 9 (13).…”

Section: Discussionmentioning

confidence: 99%

Influence of stimulatory and suppressive DNA motifs on host susceptibility to inflammatory arthritis

Zeuner

Verthelyi

Gürsel

et al. 2003

Arthritis & Rheumatism

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Objective. To examine whether systemic administration of immunostimulatory and immunosuppressive oligodeoxynucleotides (ODNs) alter host susceptibility to inflammatory arthritis.Methods. Normal BALB/c mice were treated systemically with CpG ODNs or suppressive ODNs, and then challenged intraarticularly with CpG DNA. The onset and magnitude of the resulting inflammatory response was monitored.Results. Systemic delivery of CpG ODNs significantly increased susceptibility to local inflammation, whereas systemic treatment with suppressive ODNs reduced this susceptibility. CD11c؉ cells played a key role in mediating host sensitivity to arthritis. These cells were the dominant source of tumor necrosis factor ␣ production in CpG-stimulated animals and transferred resistance to arthritis from mice treated with suppressive ODNs.Conclusion. Systemic exposure to immunostimulatory and immunosuppressive DNA influences host susceptibility to local inflammatory challenge. Current findings raise the possibility that suppressive ODNs may be useful in the prevention/treatment of proinflammatory diseases.

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“…AO was used in double-stranded form by mixing with an equimolar amount of reverse activating ODN (RAO), heating to 65°C, and cooling slowly to room temperature. 2114L and 2088L are based on 2114 and 2088 (16), but lengthened and made as PO-ODN. LPS from Salmonella minnesota Re595 (Sigma-Aldrich) was dissolved in 0.1% triethylamine and sonicated.…”

Section: Methodsmentioning

confidence: 99%

“…Although a number of studies have shown an inhibitory action of viral (12) and vertebrate (13)(14)(15) DNA or specific ODN (12-14, 16 -20), there is no consensus in the literature about the nature of such motifs. The suggestions for inhibitory motifs include GC-rich sequences such as CCGG (12), GC-rich sequences when linked closely to CpG (21), methylated CpG motifs (15), certain G-rich sequences such as GGAGGGG (16,17), and deoxyguanosine (dG) homopolymer (13,14,22). In none of these cases is it known how an inhibitory effect is mediated, and competition for CpG DNA uptake has not always been eliminated as a mechanism.…”

mentioning

confidence: 99%

The Molecular Basis for the Lack of Immunostimulatory Activity of Vertebrate DNA

Stacey

Young

Clark

et al. 2003

The Journal of Immunology

165

193

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Macrophages and B cells are activated by unmethylated CpG-containing sequences in bacterial DNA. The lack of activity of self DNA has generally been attributed to CpG suppression and methylation, although the role of methylation is in doubt. The frequency of CpG in the mouse genome is 12.5% of Escherichia coli, with unmethylated CpG occurring at ∼3% the frequency of E. coli. This suppression of CpG alone is insufficient to explain the inactivity of self DNA; vertebrate DNA was inactive at 100 μg/ml, 3000 times the concentration at which E. coli DNA activity was observed. We sought to resolve why self DNA does not activate macrophages. Known active CpG motifs occurred in the mouse genome at 18% of random occurrence, similar to general CpG suppression. To examine the contribution of methylation, genomic DNAs were PCR amplified. Removal of methylation from the mouse genome revealed activity that was 23-fold lower than E. coli DNA, although there is only a 7-fold lower frequency of known active CpG motifs in the mouse genome. This discrepancy may be explained by G-rich sequences such as GGAGGGG, which potently inhibited activation and are found in greater frequency in the mouse than the E. coli genome. In summary, general CpG suppression, CpG methylation, inhibitory motifs, and saturable DNA uptake combined to explain the inactivity of self DNA. The immunostimulatory activity of DNA is determined by the frequency of unmethylated stimulatory sequences within an individual DNA strand and the ratio of stimulatory to inhibitory sequences.

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CpG Stimulation of Primary Mouse B Cells Is Blocked by Inhibitory Oligodeoxyribonucleotides at a Site Proximal to NF-κB Activation

Cited by 104 publications

References 51 publications

Effect of Suppressive DNA on CpG-Induced Immune Activation

Effect of Suppressive DNA on CpG-Induced Immune Activation

Influence of stimulatory and suppressive DNA motifs on host susceptibility to inflammatory arthritis

The Molecular Basis for the Lack of Immunostimulatory Activity of Vertebrate DNA

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