Flagellin Treatment Protects against Chemicals, Bacteria, Viruses, and Radiation

Vijay‐Kumar, Matam; Aitken, Jesse D.; Sanders, Catherine J.; Frias, Amena H.; Sloane, Valerie; Xu, Jianguo; Neish, Andrew S.; Rojas, Mauricio; Gewirtz, Andrew T.

doi:10.4049/jimmunol.180.12.8280

Cited by 169 publications

(159 citation statements)

References 29 publications

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“…Moreover, TLR5 activation was not caused by contamination of PEI with bacterial or other protein source, as endotoxin was undetectable in the PEI preparation and PEI treated overnight with proteinase K - a procedure that completely ablates the activity of flagellin to activate TLR5 - induced the same dose-dependent TLR5 activation ( Figure 4B). In addition, intraperitoneal administration of linear PEI in WT mice, pretreated or not with proteinase K, induced the same serum cytokine secretion pattern reported for flagellin (30), with significant and selective upregulation of keratinocyte chemoattractant (KC) and IFN-inducible protein 10 (IP-10) 2 hours after injection ( Figure 4C and Supplemental Figure 4B). Most importantly, PEI-mediated KC and IP-10 upregulation was completely abrogated in Tlr5 -/-littermates ( Figure 4C), confirming that linear PEI is a TLR5 agonist, which we believe to be novel, with a range of activities similar to those of flagellin.…”

Section: Figurementioning

confidence: 67%

Polyethylenimine-based siRNA nanocomplexes reprogram tumor-associated dendritic cells via TLR5 to elicit therapeutic antitumor immunity

Cubillos-Ruiz¹,

Engle²,

Scarlett³

et al. 2009

J. Clin. Invest.

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132

207

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The success of clinically relevant immunotherapies requires reversing tumor-induced immunosuppression.Here we demonstrated that linear polyethylenimine-based (PEI-based) nanoparticles encapsulating siRNA were preferentially and avidly engulfed by regulatory DCs expressing CD11c and programmed cell death 1-ligand 1 (PD-L1) at ovarian cancer locations in mice. PEI-siRNA uptake transformed these DCs from immunosuppressive cells to efficient antigen-presenting cells that activated tumor-reactive lymphocytes and exerted direct tumoricidal activity, both in vivo and in situ. PEI triggered robust and selective TLR5 activation in vitro and elicited the production of hallmark TLR5-inducible cytokines in WT mice, but not in Tlr5 -/-littermates. Thus, PEI is a TLR5 agonist that, to our knowledge, was not previously recognized. In addition, PEI-complexed nontargeting siRNA oligonucleotides stimulated TLR3 and TLR7. The nonspecific activation of multiple TLRs (specifically, TLR5 and TLR7) reversed the tolerogenic phenotype of human and mouse ovarian tumor-associated DCs. In ovarian carcinoma-bearing mice, this induced T cell-mediated tumor regression and prolonged survival in a manner dependent upon myeloid differentiation primary response gene 88 (MyD88; i.e., independent of TLR3). Furthermore, gene-specific siRNA-PEI nanocomplexes that silenced immunosuppressive molecules on mouse tumor-associated DCs elicited discernibly superior antitumor immunity and enhanced therapeutic effects compared with nontargeting siRNA-PEI nanocomplexes. Our results demonstrate that the intrinsic TLR5 and TLR7 stimulation of siRNA-PEI nanoparticles synergizes with the gene-specific silencing activity of siRNA to transform tumor-infiltrating regulatory DCs into DCs capable of promoting therapeutic antitumor immunity.

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Section: Figurementioning

confidence: 67%

Polyethylenimine-based siRNA nanocomplexes reprogram tumor-associated dendritic cells via TLR5 to elicit therapeutic antitumor immunity

Cubillos-Ruiz¹,

Engle²,

Scarlett³

et al. 2009

J. Clin. Invest.

Self Cite

132

207

View full text Add to dashboard Cite

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“…Flagellin-mediated protection of rodents and nonhuman primates against lethal irradiation was associated with CSF3-mediated granulopoiesis and the antiapoptotic effect of superoxide dismutase 2 (47). Flagellin treatment has been linked to resistance against inflammatory colitis and gut infections (40,48). The TLR5-induced circulating and local production of IL-17/IL-22 may be the main driving force behind these protective effects.…”

Section: Discussionmentioning

confidence: 99%

TLR5 Signaling Stimulates the Innate Production of IL-17 and IL-22 by CD3negCD127+ Immune Cells in Spleen and Mucosa

Maele

Carnoy

Cayet

et al. 2010

The Journal of Immunology

124

117

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“…23 An additional study did not observe the same side effects using 25-50 mg/mouse. 16 This is one reason why we analyzed the dose-dependent effects of flagellin on the development of liver injury in mice and tested doses of 0-200 mg. The current data suggest that the gross lesions in liver and significant increase in serum ALT/AST levels usually occurred 12 h after the intraperitoneal treatment with 100 or 200 mg, but not with lower doses.…”

Section: Discussionmentioning

confidence: 99%

“…15 Furthermore, flagellin has the potential to be used as a biological protectant against both major acute radiation syndrome during cancer radiotherapy and a mitigator of radiation emergencies. 6 Vijay-Kumar et al 16 demonstrated that the systemic administration of flagellin might be a relatively safe means of providing temporary nonspecific protection against chemical, bacterial, viral and radiation challenge. However, in contrast, several studies have shown that flagellin not only triggers a prototypical systemic inflammatory response in mice, including the induction and secretion of pro-inflammatory cytokines in the lungs, small intestine, liver and kidney, 17 but also plays an important pathophysiological role in certain inflammatory diseases.…”

Section: Introductionmentioning

confidence: 99%

Over-activation of TLR5 signaling by high-dose flagellin induces liver injury in mice

et al. 2014

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Flagellin is a potent activator of a broad range of cell types that are involved in innate and adaptive immunity. Therefore, it is a good adjuvant candidate for vaccines, and it might function as a biological protectant against both major acute radiation syndrome during cancer radiotherapy and a mitigator of radiation emergencies. However, accumulating evidence has implicated flagellin in the occurrence of some inflammatory diseases, such as acute lung inflammation, cardiovascular collapse and inflammatory bowel disease. The aim of this study was to elucidate whether only flagellin-TLR5 signaling activation plays a role in the pathophysiology of liver or whether some other flagellin activity also contributes to liver injury either via bacterial infections or during clinical applications. Recombinant flagellin proteins with or without TLR5-stimulating activity were used to evaluate the role of flagellin-TLR5 signaling in liver injury in wild-type and TLR5 KO mice. Gross lesions and large areas of hepatocellular necrosis were observed in liver tissue 12 h after the intraperitoneal administration of 100 or 200 mg flagellin (FliC) in a dose-and time-dependent manner in wild-type mice, but not in TLR5 KO mice. Deletion of the N-terminal or TLR5 binding domain of flagellin inhibited flagellin-induced inflammatory responses and the subsequent acute liver function abnormality and damage. These data confirmed that flagellin is an essential determinant of liver injury and demonstrated that the over-activation of TLR5 signaling by high-dose flagellin caused acute inflammatory responses, neutrophil accumulation and oxidative stress in the liver, which contributes to the progression and severity of flagellin-induced liver injury.

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Flagellin Treatment Protects against Chemicals, Bacteria, Viruses, and Radiation

Cited by 169 publications

References 29 publications

Polyethylenimine-based siRNA nanocomplexes reprogram tumor-associated dendritic cells via TLR5 to elicit therapeutic antitumor immunity

Polyethylenimine-based siRNA nanocomplexes reprogram tumor-associated dendritic cells via TLR5 to elicit therapeutic antitumor immunity

TLR5 Signaling Stimulates the Innate Production of IL-17 and IL-22 by CD3negCD127+ Immune Cells in Spleen and Mucosa

Over-activation of TLR5 signaling by high-dose flagellin induces liver injury in mice

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