The Mincle-Activating Adjuvant TDB Induces MyD88-Dependent Th1 and Th17 Responses through IL-1R Signaling

Desel, Christiane; Werninghaus, Kerstin; Ritter, Manuel; Jozefowski, Katrin; Wenzel, Jens; Russkamp, Norman F.; Schleicher, Ulrike; Christensen, Dennis; Wirtz, Stefan; Kirschning, Carsten J.; Agger, Else Marie; Costa, Clarissa Prazeres da; Lang, Roland

doi:10.1371/journal.pone.0053531

Cited by 132 publications

(135 citation statements)

References 36 publications

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“…In contrast, we and others observed intact in vitro activation of macrophages or granulocytes by TDM or TDB in the absence of MYD88, arguing against a role for TLR (7,11,12). In vivo, glycolipid adjuvant activity depends on MYD88 signaling (3,6), which is at least partially due to IL-1R signaling but independent of TLR2/3/4/7/9 (13).…”

contrasting

confidence: 69%

“…TLRindependent functions of the MYD88 adapter protein can also contribute to TDB/TDM responses in vivo, as the adjuvant effect of TDB is independent of TLR2/3/4/7 but requires MYD88 (6). We recently tested the role of the MYD88-utilizing cytokines IL-1, IL-18, and IL-33 for adjuvanticity of TDB, and identified an important contribution of IL-1R signaling (13). Similar findings of TLR-independent, but IL-1R-Myd88-dependent, in vivo adjuvanticity have been reported by Sher's group (56) for CFA.…”

Section: Discussionmentioning

confidence: 99%

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Differential Control of Mincle-Dependent Cord Factor Recognition and Macrophage Responses by the Transcription Factors C/EBPβ and HIF1α

Schoenen

Huber

Sonda

et al. 2014

The Journal of Immunology

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Trehalose-6,6-dimycolate (TDM), the mycobacterial cord factor, and its synthetic analog Trehalose-6,6-dibehenate (TDB) bind to the C-type lectin receptors macrophage-inducible C-type lectin (Mincle) and Mcl to activate macrophages. Genetically, the transcriptional response to TDB/TDM has been defined to require FcRγ-Syk-Card9 signaling. However, TDB/TDM-triggered kinase activation has not been studied well, and it is largely unknown which transcriptional regulators bring about inflammatory gene expression. In this article, we report that TDB/TDM caused only weak Syk-phosphorylation in resting macrophages, consistent with low basal Mincle expression. However, LPS-priming caused MYD88-dependent upregulation of Mincle, resulting in enhanced TDB/TDM-induced kinase activation and more rapid inflammatory gene expression. TLR-induced Mincle expression partially circumvented the requirement for Mcl in the response to TDB/TDM. To dissect transcriptional responses to TDB/TDM, we mined microarray data and identified early growth response (Egr) family transcription factors as direct Mincle target genes, whereas upregulation of Cebpb and Hif1a required new protein synthesis. Macrophages and dendritic cells lacking C/EBPβ showed nearly complete abrogation of TDB/TDM responsiveness, but also failed to upregulate Mincle. Retroviral rescue of Mincle expression in Cebpb-deficient cells restored induction of Egr1, but not of G-CSF. This pattern of C/EBPβ dependence was also observed after stimulation with the Dectin-1 ligand Curdlan. Inducible expression of hypoxia-inducible factor 1α (HIF1α) also required C/EBPβ. In turn, HIF1α was not required for Mincle expression, kinase activation, and Egr1 or Csf3 expression, but critically contributed to NO production. Taken together, we identify C/EBPβ as central hub in Mincle expression and inflammatory gene induction, whereas HIF1α controls Nos2 expression. C/EBPβ also connects TLR signals to cord factor responsiveness through MYD88-dependent upregulation of Mincle.

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contrasting

confidence: 69%

Section: Discussionmentioning

confidence: 99%

Differential Control of Mincle-Dependent Cord Factor Recognition and Macrophage Responses by the Transcription Factors C/EBPβ and HIF1α

Schoenen

Huber

Sonda

et al. 2014

The Journal of Immunology

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“…TDB induces strong T H 1 and T H 17 immune responses and the C-type lectin Mincle is the receptor for APC activation. The adjuvant effect also requires MyD88 and Schweneker and colleagues identified the Nlrp3 inflammasome as mediator for TDB-triggered induction of immune response [Werninghaus et al 2009;Desel et al 2013;Schweneker et al 2013]. Properties of cationic liposome-forming lipids were studied with rigid DDA or fluid dimethyldioleoylammonium (DODA) liposomes.…”

Section: Cationic Liposome Adjuvant Vaccinesmentioning

confidence: 99%

Liposomes as vaccine delivery systems: a review of the recent advances

Schwendener

2014

Therapeutic Advances in Vaccines

432

309

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Liposomes and liposome-derived nanovesicles such as archaeosomes and virosomes have become important carrier systems in vaccine development and the interest for liposome-based vaccines has markedly increased. A key advantage of liposomes, archaeosomes and virosomes in general, and liposome-based vaccine delivery systems in particular, is their versatility and plasticity. Liposome composition and preparation can be chosen to achieve desired features such as selection of lipid, charge, size, size distribution, entrapment and location of antigens or adjuvants. Depending on the chemical properties, water-soluble antigens (proteins, peptides, nucleic acids, carbohydrates, haptens) are entrapped within the aqueous inner space of liposomes, whereas lipophilic compounds (lipopeptides, antigens, adjuvants, linker molecules) are intercalated into the lipid bilayer and antigens or adjuvants can be attached to the liposome surface either by adsorption or stable chemical linking. Coformulations containing different types of antigens or adjuvants can be combined with the parameters mentioned to tailor liposomal vaccines for individual applications. Special emphasis is given in this review to cationic adjuvant liposome vaccine formulations. Examples of vaccines made with CAF01, an adjuvant composed of the synthetic immune-stimulating mycobacterial cordfactor glycolipid trehalose dibehenate as immunomodulator and the cationic membrane forming molecule dimethyl dioctadecylammonium are presented. Other vaccines such as cationic liposome-DNA complexes (CLDCs) and other adjuvants like muramyl dipeptide, monophosphoryl lipid A and listeriolysin O are mentioned as well. The field of liposomes and liposome-based vaccines is vast. Therefore, this review concentrates on recent and relevant studies emphasizing current reports dealing with the most studied antigens and adjuvants, and pertinent examples of vaccines. Studies on liposome-based veterinary vaccines and experimental therapeutic cancer vaccines are also summarized.

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“…Molecular mechanisms of TDB/TDM adjuvanticity were identified to be strictly Mincle-dependent and strong IL-17 production post immunization controls the generation of cellular immunity. 31,32 Desel et al 32 showed that adjuvanticity of TDM/TDB not only depends on Mincle, but also necessitates MyD88. Whereas in vitro studies identified MyD88 independence, in vivo adjuvanticity was strongly dependent on MyD88 signaling.…”

Section: Antigen Delivery and Immune-stimulationmentioning

confidence: 99%

A case-study investigating the physicochemical characteristics that dictate the function of a liposomal adjuvant

Perrie

Kastner

Kaur

et al. 2013

Human Vaccines & Immunotherapeutics

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The Mincle-Activating Adjuvant TDB Induces MyD88-Dependent Th1 and Th17 Responses through IL-1R Signaling

Cited by 132 publications

References 36 publications

Differential Control of Mincle-Dependent Cord Factor Recognition and Macrophage Responses by the Transcription Factors C/EBPβ and HIF1α

Differential Control of Mincle-Dependent Cord Factor Recognition and Macrophage Responses by the Transcription Factors C/EBPβ and HIF1α

Liposomes as vaccine delivery systems: a review of the recent advances

A case-study investigating the physicochemical characteristics that dictate the function of a liposomal adjuvant

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