Contamination of DNase Preparations Confounds Analysis of the Role of DNA in Alum-Adjuvanted Vaccines

Noges, Laura; White, Janicé; Cambier, John C.; Kappler, John W.; Marrack, Philippa

doi:10.4049/jimmunol.1501565

Cited by 15 publications

(11 citation statements)

References 48 publications

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“…When injected in the absence of virus infection, dsDNA from splenocytes recapitulated many but not all of the exacerbating effects of RV on asthma-related outcomes in mice, suggesting that more complex structures containing dsDNA, rather than dsDNA alone, were responsible for the full aggravating effects. This assumption was concordant with the fact that the commercially available DNase that we used degrades not only dsDNA but also DNA-associated proteins19,30–33. We therefore postulated that NETs, which contain both dsDNA and proteins/peptides, were the main source of airway dsDNA elicited by RV infection.…”

Section: Discussionsupporting

confidence: 76%

Host DNA released by NETosis promotes rhinovirus-induced type-2 allergic asthma exacerbation

Toussaint

Jackson

Swieboda

et al. 2017

Nat Med

266

244

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Respiratory viral infections represent the most common cause of allergic asthma exacerbations. Amplification of type 2 immune response is strongly implicated in asthma exacerbation, but how virus infection boosts type 2 responses is poorly understood. We report a significant correlation between release of host double stranded DNA (dsDNA) following rhinovirus infection and exacerbation of type 2 allergic inflammation in humans. In a mouse model of allergic airway hypersensitivity, we show that rhinovirus infection triggers dsDNA release associated with neutrophil extracellular traps (NETs) formation (NETosis). We further demonstrate that inhibiting NETosis by blocking neutrophil elastase, or degrading NETs with DNase protects mice from type 2 immunopathology. Furthermore, injection of mouse genomic DNA alone is sufficient to recapitulate many features of rhinovirus-induced type 2 immune responses and asthma pathology. Thus, NETosis and its associated extracellular dsDNA contribute to the pathogenesis and may represent potential therapeutic targets of rhinovirus-induced asthma exacerbations.

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Section: Discussionsupporting

confidence: 76%

Host DNA released by NETosis promotes rhinovirus-induced type-2 allergic asthma exacerbation

Toussaint

Jackson

Swieboda

et al. 2017

Nat Med

266

244

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“…It is difficult to evaluate the contributions of NETs since it is difficult to eliminate them entirely from injected alum. As for the accompanying chromatin, a couple of papers have suggested that host DNA may indeed increase alum’s effects but host DNA is certainly not the only intrinsic adjuvant induced by alum ([29–31] but see [32]). Alum may also act simply as a particle, lysing lysosome and releasing lysosomal enzymes into the cytoplasm [33–35] or by distorting the plasma membrane of antigen presenting cells [36] and/or somehow by its ability to rapidly induce production if cytokines and chemokines [37,38].…”

Section: Insoluble Salts and Other Particulate Adjuvantsmentioning

confidence: 99%

Old and new adjuvants

McKee

Marrack

2017

Current Opinion in Immunology

Self Cite

169

126

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“…Some studies suggested that the release of dsDNA from damaged and dying host cells, which is induced by alum injection, may contribute to priming of Th2 CD4 + T cells (4,5) and enhance MHC class II-mediated Ag presentation, prolonging CD4 + T cell interactions with DCs (5). However, a recent report by Noges et al (6) showed that some of the DNase preparations used in the above studies are contaminated by proteases, casting doubt on the significance of dsDNA in responses to alum.…”

mentioning

confidence: 98%

The Syk–NFAT–IL-2 Pathway in Dendritic Cells Is Required for Optimal Sterile Immunity Elicited by Alum Adjuvants

Khameneh

Spreafico

et al. 2017

The Journal of Immunology

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Despite a long history and extensive usage of insoluble aluminum salts (alum) as vaccine adjuvants, the molecular mechanisms underpinning Ag-specific immunity upon vaccination remain unclear. Dendritic cells (DCs) are crucial initiators of immune responses, but little is known about the molecular pathways used by DCs to sense alum and, in turn, activate T and B cells. In this article, we show that alum adjuvanticity requires IL-2 specifically released by DCs, even when T cell secretion of IL-2 is intact. We demonstrate that alum, as well as other sterile particulates, such as uric acid crystals, induces DCs to produce IL-2 following initiation of actin-mediated phagocytosis that leads to Src and Syk kinase activation, Ca 2+ mobilization, and calcineurin-dependent activation of NFAT, the master transcription factor regulating IL-2 expression. Using chimeric mice, we show that DC-derived IL-2 is required for maximal Ag-specific proliferation of CD4 + T cells and optimal humoral responses following alum-adjuvanted immunization. These data identify DC-derived IL-2 as a key mediator of alum adjuvanticity in vivo and the Src-Syk pathway as a potential leverage point in the rational design of novel adjuvants.

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Contamination of DNase Preparations Confounds Analysis of the Role of DNA in Alum-Adjuvanted Vaccines

Cited by 15 publications

References 48 publications

Host DNA released by NETosis promotes rhinovirus-induced type-2 allergic asthma exacerbation

Host DNA released by NETosis promotes rhinovirus-induced type-2 allergic asthma exacerbation

Old and new adjuvants

The Syk–NFAT–IL-2 Pathway in Dendritic Cells Is Required for Optimal Sterile Immunity Elicited by Alum Adjuvants

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