C-Reactive Protein Impairs Dendritic Cell Development, Maturation, and Function: Implications for Peripheral Tolerance

Jimenez, Rachel V.; Wright, Tyler; Jones, Nicholas; Wu, Jianming; Gibson, Andrew; Szalai, Alexander J.

doi:10.3389/fimmu.2018.00372

Cited by 40 publications

(42 citation statements)

References 40 publications

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“…The finding in this study that serum CRP levels are associated with overall survival in patients with stage IV melanoma treated with nivolumab or ipilimumab further support an immune suppressive role for CRP and possibly other APPs and suggest a novel mechanism for resistance to PD-1 blockade in melanoma that may be applicable to other cancers. CRP has been shown to alter DC maturation and function in murine models, 31 although it has not been previously shown to behave similarly with human DCs, and few investigations have explored the impact of high levels of CRP on human T cells.…”

Section: Crp Upregulates Il-1β In Expanded Mart-1specific T Cellsmentioning

confidence: 99%

C reactive protein impairs adaptive immunity in immune cells of patients with melanoma

Yoshida

Ichikawa

Giuroiu

et al. 2020

J Immunother Cancer

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BackgroundHigh C reactive protein (CRP) levels have been reported to be associated with a poor clinical outcome in a number of malignancies and with programmed cell death protein 1 immune checkpoint blockade in patients with advanced cancer. Little is known about the direct effects of CRP on adaptive immunity in cancer. Therefore, we investigated how CRP impacted the function of T cells and dendritic cells (DCs) from patients with melanoma.MethodsThe effects of CRP on proliferation, function, gene expression and phenotype of patient T cells and DCs, and expansion of MART-1 antigen-specific T cells were analyzed by multicolor flow cytometry and RNA-seq. Additionally, serum CRP levels at baseline from patients with metastatic melanoma treated on the Checkmate-064 clinical trial were assessed by a Luminex assay.ResultsIn vitro, CRP inhibited proliferation, activation-associated phenotypes and the effector function of activated CD4+ and CD8+ T cells from patients with melanoma. CRP-treated T cells expressed high levels of interleukin-1β, which is known to enhance CRP production from the liver. CRP also suppressed formation of the immune synapse and inhibited early events in T-cell receptor engagement. In addition, CRP downregulated the expression of costimulatory molecules on mature DCs and suppressed expansion of MART-1-specific CD8+ T cells in a dose-dependent manner by impacting on both T cells and antigen-presenting cells. High-serum CRP levels at baseline were significantly associated with a shorter survival in both nivolumab-treated and ipilimumab-treated patients.ConclusionsThese findings suggest that high levels of CRP induce an immunosuppressivemilieuin melanoma and support the blockade of CRP as a therapeutic strategy to enhance immune checkpoint therapies in cancer.Trial registration numberNCT01783938andNCT02983006.

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Section: Crp Upregulates Il-1β In Expanded Mart-1specific T Cellsmentioning

confidence: 99%

C reactive protein impairs adaptive immunity in immune cells of patients with melanoma

Yoshida

Ichikawa

Giuroiu

et al. 2020

J Immunother Cancer

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“…It remains to be investigated if the here described mechanism also contributes to the protection against experimental inflammation in animals overexpressing human CRP ( 25 – 28 ). Interestingly, CRP was recently shown to impair dendritic cell development, maturation and function ( 60 ). This anti-inflammatory mechanism involves the inhibitory Fcγ receptor IIB ( 60 ).…”

Section: Discussionmentioning

confidence: 99%

C-Reactive Protein Stimulates Nicotinic Acetylcholine Receptors to Control ATP-Mediated Monocytic Inflammasome Activation

et al. 2018

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Blood levels of the acute phase reactant C-reactive protein (CRP) are frequently measured as a clinical marker for inflammation, but the biological functions of CRP are still controversial. CRP is a phosphocholine (PC)-binding pentraxin, mainly produced in the liver in response to elevated levels of interleukin-1β (IL-1β) and of the IL-1β-dependent cytokine IL-6. While both cytokines play important roles in host defense, excessive systemic IL-1β levels can cause life-threatening diseases such as trauma-associated systemic inflammation. We hypothesized that CRP acts as a negative feedback regulator of monocytic IL-1β maturation and secretion. Here, we demonstrate that CRP, in association with PC, efficiently reduces ATP-induced inflammasome activation and IL-1β release from human peripheral blood mononuclear leukocytes and monocytic U937 cells. Effective concentrations are in the range of marginally pathologic CRP levels (IC50 = 4.9 µg/ml). CRP elicits metabotropic functions at nicotinic acetylcholine (ACh) receptors (nAChRs) containing subunits α7, α9, and α10 and suppresses the function of ATP-sensitive P2X7 receptors in monocytic cells. Of note, CRP does not induce ion currents at conventional nAChRs, suggesting that CRP is a potent nicotinic agonist controlling innate immunity without entailing the risk of adverse effects in the nervous system. In a prospective study on multiple trauma patients, IL-1β plasma concentrations negatively correlated with preceding CRP levels, whereas inflammasome-independent cytokines IL-6, IL-18, and TNF-α positively correlated. In conclusion, PC-laden CRP is an unconventional nicotinic agonist that potently inhibits ATP-induced inflammasome activation and might protect against trauma-associated sterile inflammation.

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“…Dendritic cells are fundamental players of both innate and adaptive immunity and could induce a tolerogenic effect on biomaterials by releasing interleukin-10 (Franz et al, 2011) following native CRP stimulation ( Figure 5). It has been recently proposed that native CRP down-regulates dendritic cell development and activation/maturation through Fc gamma receptor IIB (Fcγ RIIB), so it acts as a stopper on T cell mediated immunity, shifting the balance toward tolerance (Jimenez et al, 2018) (Figure 5). Inducing tolerogenic capabilities of biomaterials appears a promising strategy to down-regulate the host immune responses and resolve inflammation.…”

Section: Minimizing Thrombosis and Inflammation In Biomaterialsmentioning

confidence: 99%

Thrombogenic and Inflammatory Reactions to Biomaterials in Medical Devices

Labarrere

Dabiri

Kassab

2020

Front. Bioeng. Biotechnol.

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Blood-contacting medical devices of different biomaterials are often used to treat various cardiovascular diseases. Thrombus formation is a common cause of failure of cardiovascular devices. Currently, there are no clinically available biomaterials that can totally inhibit thrombosis under the more challenging environments (e.g., low flow in the venous system). Although some biomaterials reduce protein adsorption or cell adhesion, the issue of biomaterial associated with thrombosis and inflammation still exists. To better understand how to develop more thrombosis-resistant medical devices, it is essential to understand the biology and mechano-transduction of thrombus nucleation and progression. In this review, we will compare the mechanisms of thrombus development and progression in the arterial and venous systems. We will address various aspects of thrombosis, starting with biology of thrombosis, mathematical modeling to integrate the mechanism of thrombosis, and thrombus formation on medical devices. Prevention of these problems requires a multifaceted approach that involves more effective and safer thrombolytic agents but more importantly the development of novel thrombosis-resistant biomaterials mimicking the biological characteristics of the endothelium and extracellular matrix tissues that also ameliorate the development and the progression of chronic inflammation as part of the processes associated with the detrimental generation of late thrombosis and neo-atherosclerosis. Until such developments occur, engineers and clinicians must work together to develop devices that require minimal anticoagulants and thrombolytics to mitigate thrombosis and inflammation without causing serious bleeding side effects.

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C-Reactive Protein Impairs Dendritic Cell Development, Maturation, and Function: Implications for Peripheral Tolerance

Cited by 40 publications

References 40 publications

C reactive protein impairs adaptive immunity in immune cells of patients with melanoma

C reactive protein impairs adaptive immunity in immune cells of patients with melanoma

C-Reactive Protein Stimulates Nicotinic Acetylcholine Receptors to Control ATP-Mediated Monocytic Inflammasome Activation

Thrombogenic and Inflammatory Reactions to Biomaterials in Medical Devices

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