The regulatory dendritic cell marker C1q is a potent inhibitor of allergic inflammation

Mascarell, Laurent; Airouche, Sabi; Berjont, Nathalie; Gary, C; Gueguen, Claire; Fourcade, Gwladys; Bellier, Bertrand; Togbé, Dieudonnée; Ryffel, Bernhard; Klatzmann, David; Baron‐Bodo, Véronique; Moingeon, Philippe

doi:10.1038/mi.2016.87

Cited by 33 publications

(19 citation statements)

References 27 publications

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“…Whereas the onset of autoimmunity in C1q -/mice is highly age dependent, we found early evidence for aberrant T cell activation, albeit milder, in 5-month-old mice. Short-term intraperitoneal injection of C1q in a model of allergic airway diseases failed to show a significant expansion of Treg cells in blood, the lungs, and the spleen (46). These findings are in contrast with chronic and lung-specific (e.g., intratracheal) administration of C1q results in potent upregulation of Tregs and decreased inflammation in the airways, suggesting localized induction of Tregs that control inflammation.…”

Section: Discussionmentioning

confidence: 81%

Cigarette smoke–induced reduction of C1q promotes emphysema

et al. 2019

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Section: Discussionmentioning

confidence: 81%

Cigarette smoke–induced reduction of C1q promotes emphysema

et al. 2019

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“…There are also other molecules that can be regarded as the biomarkers of Tol-DC. The complement subunit C1q was recently identified as a biomarker for monocyte-derived Tol-DC, which could suppress CD4 + T-cell activation via increasing IL-10 secretion ( 24 ). Immature DC are a rich source of active C1q, and the expression of C1q is downregulated when DC are approaching the mature state ( 25 ).…”

Section: The Characteristics and Biomarkers Of Tol-dcmentioning

confidence: 99%

Tolerogenic Dendritic Cells: The Pearl of Immunotherapy in Organ Transplantation

et al. 2020

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Over a half century, organ transplantation has become an effective method for the treatment of end-stage visceral diseases. Although the application of immunosuppressants (IS) minimizes the rate of allograft rejection, the common use of IS bring many adverse effects to transplant patients. Moreover, true transplant tolerance is very rare in clinical practice. Dendritic cells (DCs) are thought to be the most potent antigen-presenting cells, which makes a bridge between innate and adaptive immunity. Among their subsets, a small portion of DCs with immunoregulatory function was known as tolerogenic DC (Tol-DC). Previous reports demonstrated the ability of adoptively transferred Tol-DC to approach transplant tolerance in animal models. In this study, we summarized the properties, ex vivo generation, metabolism, and clinical attempts of Tol-DC. Tol-DC is expected to become a substitute for IS to enable patients to achieve immune tolerance in the future.

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“…Expression or secretion of molecules, such as C1q, can confer a potent direct anti-inflammatory function to regulatory DCs independent of their capacity for expanding the pool of Treg cells. 120 AIT combined with biological agents and probiotics Studies on the combination of biological agents with AIT seemed more and more frequent in recent years. A combined therapy comprising a probiotic together with peanut OIT was recently reported.…”

Section: New Findings On Regulation Of Allergen-specific Ige and Igg mentioning

confidence: 99%

Advances and highlights in allergen immunotherapy: On the way to sustained clinical and immunologic tolerance

Berings

Karaaslan

Altunbulakli

et al. 2017

Journal of Allergy and Clinical Immunology

103

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Allergen immunotherapy (AIT) is an effective treatment strategy for allergic diseases and has been used for more than 100 years. In recent years, however, the expectations on concepts, conduct, statistical evaluation, and reporting have developed significantly. Products have undergone dose-response and confirmative studies in adults and children to provide evidence for the optimal dosage, safety, and efficacy of AIT vaccines using subcutaneous and sublingual delivery pathways in large patient cohorts, ensuring solid conclusions to be drawn from them for the advantage of patients and societies alike. Those standards should be followed today, and products answering to them should be preferred over others lacking optimization and proof of efficacy and safety. Molecular and cellular mechanisms of AIT include early mast cell and basophil desensitization effects, regulation of T- and B-cell responses, regulation of IgE and IgG production, and inhibition of responses from eosinophils, mast cells, and basophils in the affected tissues. There were many developments to improve vaccination strategies, demonstration of new molecules involved in molecular mechanisms, and demonstration of new biomarkers for AIT during the last few years. The combination of probiotics, vitamins, and biological agents with AIT is highlighting current advances. Development of allergoids and recombinant and hypoallergenic vaccines to skew the immune response from IgE to IgG and regulation of dendritic cell, mast cell, basophil, innate lymphoid cell, T-cell, and B-cell responses to allergens are also discussed in detail.

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The regulatory dendritic cell marker C1q is a potent inhibitor of allergic inflammation

Cited by 33 publications

References 27 publications

Cigarette smoke–induced reduction of C1q promotes emphysema

Cigarette smoke–induced reduction of C1q promotes emphysema

Tolerogenic Dendritic Cells: The Pearl of Immunotherapy in Organ Transplantation

Advances and highlights in allergen immunotherapy: On the way to sustained clinical and immunologic tolerance

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