CpG-containing immunostimulatory DNA sequences elicit TNF-α–dependent toxicity in rodents but not in humans

Campbell, John D.; Cho, Yan; Foster, Martyn; Kanzler, Holger; Kachura, Melissa A.; Lum, Jeremy A.; Ratcliffe, Marianne J.; Sathe, Atul; Leishman, Andrew J.; Bahl, Ash; McHale, Mark; Coffman, Robert L.; Hessel, Edith M.

doi:10.1172/jci38294

Cited by 65 publications

(56 citation statements)

References 52 publications

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“…It is important to note that while flow cytometric analysis provides unambiguous data about the pDCs' phenotypic changes, the detected cytokines and chemokine could be released by diverse cell types responding to mtDNA treatment. In humans, TLR9 expression in mononuclear blood cells and lymphoid tissues is restricted to B cells and pDCs, whereas in mice, TLR9 expression has also been demonstrated in macrophages, myeloid DCs, and activated T cells in addition to pDCs and B cells [52]. Despite this fact, the results of our in vivo experiments correlate very well with those of cell culture assays.…”

Section: Discussionsupporting

confidence: 58%

Oxidative modification enhances the immunostimulatory effects of extracellular mitochondrial DNA on plasmacytoid dendritic cells

Pázmándi

Agod

Kumar

et al. 2014

Free Radical Biology and Medicine

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Oxidative modification enhances the immunostimulatory effects of extracellular mitochondrial DNA on plasmacytoid dendritic cells, Free Radical Biology and Medicine, http://dx.doi.org/10.1016/j. freeradbiomed. 2014.09.028 This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting galley proof before it is published in its final citable form. Please note that during the production process errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain.www.elsevier.com/locate/freeradbiomed Abbreviations: 7-AAD, 7-aminoactinomycin-D; 8-oxoG, 8-oxo-7,8-dihydroguanine; 8-oxodG, 8-oxo-7,8-dihydro-2'- well as increased TNF-Į and IL-8 production from the cells. These effects were more apparent when pDCs were exposed to oxidatively modified mtDNA. Neither native nor oxidized mtDNA molecules were able to induce interferon (IFN)-Į secretion from pDCs unless they formed a complex with human cathelicidin LL-37, an antimicrobial peptide.Interestingly, simultaneous administration of a Toll-like receptor (TLR)9 antagonist abrogated the effects of both native and oxidized mtDNAs on human pDCs. In a murine model, oxidized mtDNA also proved a more potent activator of pDCs compared to the native form, except for induction of IFN-Į production. Collectively, we demonstrate here for the first time that elevated levels of 8-oxoG bases in the extracellular mtDNA induced by oxidative stress increase the immunostimulatory capacity of mtDNA on pDCs. 3 HighlightsWe compared the immunostimulatory capacity of native and oxidized mtDNA on pDCs.8-Oxoguanin-containing mtDNA has a greater capacity to activate primary human pDCs.In vivo, oxidized mtDNA also proved a more potent activator of pDC than native mtDNA.

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Section: Discussionsupporting

confidence: 58%

Oxidative modification enhances the immunostimulatory effects of extracellular mitochondrial DNA on plasmacytoid dendritic cells

Pázmándi

Agod

Kumar

et al. 2014

Free Radical Biology and Medicine

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“…or i.t. [27][28][29] The anti-tumor activity of aerosol-delivered CpG-ODN was evaluated in two murine tumor models with different characteristics and behavior: the mammary carcinoma N202.1A is highly immunogenic due to overexpression of the heterologous rat neu oncogene, 25 while the B16 melanoma is poorly immunogenic and reportedly expresses very low levels of MHC I molecules. 42 These two tumors also differ in their sensitivity to immune effectors, with the neu-expressing mouse mammary tumor sensitive to cytotoxic activity of T but not NK cells, 43 while NK cells are required to counteract the growth of B16 melanomas.…”

Section: Discussionmentioning

confidence: 99%

“…Unlike i.n.-administered CpG-ODN, which induces lung tissue inflammation associated with weight loss in rodents, [27][28][29] prolonged repeated treatments at intervals of 72-96 hr with 1.5 mg CpG-ODN aerosol for 3 weeks were well tolerated. No effects on body weight and no histological changes in the structure of lungs, as indicated by histopathological examination of hematoxylin and eosin-stained sections of lung tissue, were observed in mice exposed to CpG-ODN aerosolization (data not shown).…”

Section: Effects Of Cpg-odn Aerosolization In Bal Fluidmentioning

confidence: 99%

Anti‐tumor activity of CpG‐ODN aerosol in mouse lung metastases

Sfondrini

Sommariva

Tortoreto

et al. 2013

Intl Journal of Cancer

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Studies in preclinical models have demonstrated the superior anti-tumor effect of CpG oligodeoxynucleotides (CpG-ODN) when administered at the tumor site rather than systemically. We evaluated the effect of aerosolized CpG-ODN on lung metastases in mice injected with immunogenic N202.1A mammary carcinoma cells or weakly immunogenic B16 melanoma cells. Upon reaching the bronchoalveolar space, aerosolized CpG-ODN activated a local immune response, as indicated by production of IL-12p40, IFN-c and IL-1b and by recruitment and maturation of DC cells in bronchoalveolar lavage fluid of mice. Treatment with aerosolized CpG-ODN induced an expansion of CD41 cells in lung and was more efficacious than systemic i.p. administration against experimental lung metastases of immunogenic N202.1A mammary carcinoma cells, whereas only i.p. delivery of CpG-ODN provided anti-tumor activity, which correlated with NK cell expansion in the lung, against lung metastases of the poorly immunogenic B16 melanoma. The inefficacy of aerosol therapy to induce NK expansion was related to the presence of immunosuppressive macrophages in B16 tumor-bearing lungs, as mice depleted of these cells by clodronate treatment responded to aerosol CpG-ODN through expansion of the NK cell population and significantly reduced numbers of lung metastases. Our results indicate that tumor immunogenicity and the tumor-induced immunosuppressive environment are critical factors to the success of CpG therapy in the lung, and point to the value of routine sampling of the lung immune environment in defining an optimal immunotherapeutic strategy.

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“…8 CpG given in this manner has caused tumor necrosis factor-␣-dependent toxicity in rodents. 53 In the present study, CpG therapy was optimized (ie, systemic administration of a nontoxic dose of 5 g) with the addition of subtherapeutic amounts of anti-ST2L mAb. All features of allergic asthma were markedly attenuated by this combination therapeutic approach, and prominent induction of IL-12p70 and MIG/CXCL9 was observed in whole lung and isolated asthmatic DCs.…”

Section: Discussionmentioning

confidence: 99%

Targeting ST2L Potentiates CpG-Mediated Therapeutic Effects in a Chronic Fungal Asthma Model

Ramaprakash

Shibata

Duffy³

et al. 2011

The American Journal of Pathology

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IL-33 and its soluble receptor and cell-associated receptor (ST2L) are all increased in clinical and experimental asthma. The present study addressed the hypothesis that ST2L impairs the therapeutic effects of CpG in a fungal model of asthma. C57BL/6 mice were sensitized to Aspergillus fumigatus and challenged via i.t. instillation with live A. fumigatus conidia. Mice were treated with IgG alone, anti-ST2L monoclonal antibody (mAb) alone, CpG alone, IgG plus CpG, or anti-ST2L mAb plus CpG every other day from day 14 to day 28 and investigated on day 28 after conidia. Lung ST2L and toll-like receptor 9 protein expression levels concomitantly increased in a time-dependent manner during fungal asthma. Therapeutic blockade of ST2L with an mAb attenuated key pathological features of this model. At subtherapeutic doses, neither anti-ST2L mAb nor CpG alone affected fungal asthma severity. However, airway hyperresponsiveness, mucus cell metaplasia, peribronchial fibrosis, and fungus retention were markedly reduced in asthmatic mice treated with the combination of both. Whole lung CXCL9 levels were significantly elevated in the combination group but not in the controls. Furthermore, in asthmatic mice treated with the combination therapy, dendritic cells generated significantly greater IL-12p70 with CpG in vitro compared with control dendritic cells. The combination of anti-ST2L mAb with CpG significantly attenuated experimental asthma, suggesting that targeting ST2L might enhance the therapeutic efficacy of CpG during allergic inflammation.

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CpG-containing immunostimulatory DNA sequences elicit TNF-α–dependent toxicity in rodents but not in humans

Cited by 65 publications

References 52 publications

Oxidative modification enhances the immunostimulatory effects of extracellular mitochondrial DNA on plasmacytoid dendritic cells

Oxidative modification enhances the immunostimulatory effects of extracellular mitochondrial DNA on plasmacytoid dendritic cells

Anti‐tumor activity of CpG‐ODN aerosol in mouse lung metastases

Targeting ST2L Potentiates CpG-Mediated Therapeutic Effects in a Chronic Fungal Asthma Model

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