Why CCR2 and CCR5 Blockade Failed and Why CCR1 Blockade Might Still Be Effective in the Treatment of Rheumatoid Arthritis

Lebre, Maria C.; Vergunst, Clarissa E.; Choi, IY; Aarrass, Saida; Formas-Oliveira, A. S.; Wyant, Tim; Horuk, Richard; Reedquist, Kris A.; Tak, Paul P.

doi:10.1371/journal.pone.0021772

Cited by 78 publications

(67 citation statements)

References 34 publications

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“…The use of antibodies against CCR2 and CCR5 was recently reported to have failed in inhibiting synovial fluidinduced monocyte chemotaxis. Interestingly the use of either an anti-CCR1 Ab or a CCR1 antagonist (BX471) inhibited synovial fluid-induced monocyte chemotaxis, highlighting this receptor as a potential target in reducing monocyte recruitment to RA synovium (Lebre et al, 2011). In terms of animal models, conflicting evidence surrounding CC chemokine receptors has been reported.…”

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confidence: 99%

CC Chemokine Receptors and Chronic Inflammation—Therapeutic Opportunities and Pharmacological Challenges

2013

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confidence: 99%

CC Chemokine Receptors and Chronic Inflammation—Therapeutic Opportunities and Pharmacological Challenges

2013

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“…A range of therapeutic agents that target CCR2 or CCL2 are being developed (6)(7)(8), although initial trial results for CCR2 blockade in RA patients have been disappointing (9). Nevertheless, CCR2/CCL2 inhibition may ultimately find utility in the treatment of a range of conditions (6)(7)(8).…”

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confidence: 99%

CCR2 Deficiency Promotes Exacerbated Chronic Erosive Neutrophil-Dominated Chikungunya Virus Arthritis

Poo

Nakaya

Gardner

et al. 2014

J Virol

122

143

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Chikungunya virus (CHIKV) is a member of a globally distributed group of arthritogenic alphaviruses that cause weeks to months of debilitating polyarthritis/arthralgia, which is often poorly managed with current treatments. Arthritic disease is usually characterized by high levels of the chemokine CCL2 and a prodigious monocyte/macrophage infiltrate. Several inhibitors of CCL2 and its receptor CCR2 are in development and may find application for treatment of certain inflammatory conditions, including autoimmune and viral arthritides. Here we used CCR2 ؊/؊ mice to determine the effect of CCR2 deficiency on CHIKV infection and arthritis. Although there were no significant changes in viral load or RNA persistence and only marginal changes in antiviral immunity, arthritic disease was substantially increased and prolonged in CCR2 ؊/؊ mice compared to wild-type mice. The monocyte/macrophage infiltrate was replaced in CCR2 ؊/؊ mice by a severe neutrophil (followed by an eosinophil) infiltrate and was associated with changes in the expression levels of multiple inflammatory mediators (including CXCL1, CXCL2, granulocyte colony-stimulating factor [G-CSF], interleukin-1␤ [IL-1␤], and IL-10). The loss of anti-inflammatory macrophages and their activities (e.g., efferocytosis) was also implicated in exacerbated inflammation. Clear evidence of cartilage damage was also seen in CHIKV-infected CCR2 ؊/؊ mice, a feature not normally associated with alphaviral arthritides. Although recruitment of CCR2 ؉ monocytes/macrophages can contribute to inflammation, it also appears to be critical for preventing excessive pathology and resolving inflammation following alphavirus infection. Caution might thus be warranted when considering therapeutic targeting of CCR2/CCL2 for the treatment of alphaviral arthritides. IMPORTANCEHere we describe the first analysis of viral arthritis in mice deficient for the chemokine receptor CCR2. CCR2 is thought to be central to the monocyte/macrophage-dominated inflammatory arthritic infiltrates seen after infection with arthritogenic alphaviruses such as chikungunya virus. Surprisingly, the viral arthritis caused by chikungunya virus in CCR2-deficient mice was more severe, prolonged, and erosive and was neutrophil dominated, with viral replication and persistence not being significantly affected. Monocytes/macrophages recruited by CCL2 thus also appear to be important for both preventing even worse pathology mediated by neutrophils and promoting resolution of inflammation. Caution might thus be warranted when considering the use of therapeutic agents that target CCR2/CCL2 or inflammatory monocytes/macrophages for the treatment of alphaviral (and perhaps other viral) arthritides. Individuals with diminished CCR2 responses (due to drug treatment or other reasons) may also be at risk of exacerbated arthritic disease following alphaviral infection.

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“…CCR1 has been demonstrated to play a key role in diseases associated with inappropriate leukocyte infiltration and activation, such as multiple sclerosis (23,24), rheumatoid arthritis (25,26), progressive kidney disease (27)(28)(29), and transplant rejection (20,30,31). Many attempts have been made to develop small molecule drugs that effectively inhibit receptor signaling, but thus far all have failed during clinical trials primarily due to lack of efficacy (32)(33)(34). Despite its biomedical relevance, relatively little has been reported on the molecular pharmacology of the receptor in its apo (i.e.…”

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confidence: 99%

The Chemokine Receptor CCR1 Is Constitutively Active, Which Leads to G Protein-independent, β-Arrestin-mediated Internalization

Gilliland

Salanga

Kawamura

et al. 2013

Journal of Biological Chemistry

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Background: CCR1 is a chemokine receptor of significant importance in human health, yet little is known about its ligand-independent behavior. Results: CCR1 exhibits constitutive activity leading to basal signaling and ␤-arrestin-mediated receptor internalization. Conclusion: Constitutive activity may enable CCR1 to engage in dual functions of canonical signaling and non-canonical chemokine scavenging. Significance: This may suggest a new function for CCR1 and avenue for drug development.

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Why CCR2 and CCR5 Blockade Failed and Why CCR1 Blockade Might Still Be Effective in the Treatment of Rheumatoid Arthritis

Cited by 78 publications

References 34 publications

CC Chemokine Receptors and Chronic Inflammation—Therapeutic Opportunities and Pharmacological Challenges

CC Chemokine Receptors and Chronic Inflammation—Therapeutic Opportunities and Pharmacological Challenges

CCR2 Deficiency Promotes Exacerbated Chronic Erosive Neutrophil-Dominated Chikungunya Virus Arthritis

The Chemokine Receptor CCR1 Is Constitutively Active, Which Leads to G Protein-independent, β-Arrestin-mediated Internalization

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