CCL2 and CCR2 regulate pain-related behaviour and early gene expression in post-traumatic murine osteoarthritis but contribute little to chondropathy

Zarebska, J; Chanalaris, Anastasios; Driscoll, Clare; Burleigh, Annika; Miller, Rachel E.; Malfait, A.-M.; Stott, B.; Vincent, Tonia L.

doi:10.1016/j.joca.2016.10.008

Cited by 105 publications

(102 citation statements)

References 37 publications

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“…The present study was designed to determine if using a combination of a well-established model of chronic pain and alcohol preference/consumption in mice – surgical destabilization of the medial meniscus (DMM) [7; 9; 14; 16] and the two-bottle ethanol choice [2], respectively – is appropriate for studying chronic pain-induced ethanol intake. A positive outcome would allow further investigation of this approach as an appropriate avenue to investigate the basis of the co-morbidity of pain and alcohol intake that results in alcohol abuse clinically.…”

Section: Introductionmentioning

confidence: 99%

A mouse model for chronic pain-induced increase in ethanol consumption

Butler

Knapp

Ulici

et al. 2016

Pain

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Chronic pain conditions are often co-morbid with alcohol abuse. "Self-medication" with alcohol introduces a host of problems associated with the abuse of alcohol which over time has the potential of exacerbating the painful condition. Despite the prevalence of chronic pain being associated with alcohol abuse, rodent models which mimic the co-morbid conditions are lacking. In the present study, we model osteoarthritis (OA) in C57BL/6J mice by surgically destabilizing the medial meniscus (DMM). Sham operated mice served as controls. Thirteen weeks after surgery, DMM but not sham operated mice exhibited pronounced incapacitance of the surgicallymanipulated hindlimb compared to the non-surgically manipulated hindlimb. At this time, the mice were exposed to the two-bottle ethanol choice, beginning with 2.5% with a gradual increasing to 20%. Compared to sham controls, DMM mice consumed more EtOH and preferred EtOH over water at the 20% EtOH concentration. Histological analysis verified that the DMM mice exhibited significant damage to the articular cartilage and osteophyte growth compared to sham controls and these measures of the severity of OA correlated with the amount of ethanol * Correspondence: Dr. George R. Breese, Bowles Center for Alcohol Studies, Thurston Bowles Building, The University of North Carolina at Chapel Hill, Chapel Hill, NC 27599-7178, USA. Declaration of interestThe authors report no conflicts of interest. The authors alone are responsible for the content and writing of the paper. intake. Thus, the combination of the DMM model of OA with the enhanced two-bottle ethanol choice is a potential preclinical approach in mice by which the basis of the co-morbid association of alcohol abuse and chronic pain conditions can be explored. HHS Public Access

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Section: Introductionmentioning

confidence: 99%

A mouse model for chronic pain-induced increase in ethanol consumption

Butler

Knapp

Ulici

et al. 2016

Pain

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“…When a small number of Ccr2 null mice were first tested in a surgical model of OA induced by destabilization of the medial meniscus (DMM), these mutant mice developed similar cartilage damage as wild-types over an 8-week period [7]. In the largest study yet, two independent laboratories recently confirmed an absence of protection from cartilage damage in Ccr2 null mice 8 weeks after DMM, while there was a slight trend toward chondroprotection at 12,16, and 20 weeks [8]. In contrast, a recent study reported partial protection from cartilage damage and synovitis, 20 weeks after DMM [9]; notably, this study was conducted in 20-week old mice, which resulted in more severe joint damage in wild-type mice by week 20 compared to surgery in 10-week old mice [8, 9].…”

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confidence: 99%

“…In the largest study yet, two independent laboratories recently confirmed an absence of protection from cartilage damage in Ccr2 null mice 8 weeks after DMM, while there was a slight trend toward chondroprotection at 12,16, and 20 weeks [8]. In contrast, a recent study reported partial protection from cartilage damage and synovitis, 20 weeks after DMM [9]; notably, this study was conducted in 20-week old mice, which resulted in more severe joint damage in wild-type mice by week 20 compared to surgery in 10-week old mice [8, 9]. While the protective effect was statistically significant, Ccr2 null mice still developed significant joint damage in this study [9].…”

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confidence: 99%

“…Thus, it could be hypothesized that CCR2 signaling may be crucial for recruiting cells that are involved in resolving acute post-injury inflammation and/or promoting repair, which may partly explain the absent or modest joint protective effects of Ccr2 ablation or sustained pharmacological CCR2 blockade, as well as the dependency of the effect size on the severity of the model. In this respect, Miotla Zarebska et al found distinctly altered inflammatory responses in whole-joint extracts from Ccr2 null mice compared to wild-types, 6 hours and 7 days after destabilization [8]. Notably, in wild-type mice, one of the most strongly induced genes – besides the CCR2 ligand, Ccl2 – was Arg1 , the gene encoding arginase 1, which is expressed in macrophages and partly defines the M2 macrophage phenotype [14].…”

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confidence: 99%

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Can we target CCR2 to treat osteoarthritis? The trick is in the timing!

Miller

Malfait

2017

Osteoarthritis and Cartilage

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“…Chemokines also play an important role in the pathology of RP [6]. In particular, chemokine (C-C motif) ligand 2 (CCL2) directs microglia to the site of injury or infection [7, 8]. Vascular cell adhesion molecule 1 (VCAM-1), an adhesion molecule, also plays a role in chemotaxis [9, 10].…”

Section: Introductionmentioning

confidence: 99%

Curcumin Delays Retinal Degeneration by Regulating Microglia Activation in the Retina of rd1 Mice

Wang

Yin

Gao

et al. 2017

Cell Physiol Biochem

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Background/Aims: Retinitis pigmentosa (RP) is characterized by degeneration of photoreceptors, and there are currently no effective treatments for this disease. However, curcumin has shown neuroprotectant efficacy in a RP rat and swine model, and thus, may have neuroprotective effects in this disease. Methods: Immunofluorescence staining, electroretinogram recordings, and behavioral tests were used to analyze the effects of curcumin and the underlying mechanism in retinal degeneration 1 (rd1) mice. Results: The number of apoptotic cells in the retina of rd1 mice at postnatal day 14 significantly decreased with curcumin treatment and visual function was improved. The activation of microglia and secretion of chemokines and matrix metalloproteinases in the retina were inhibited by curcumin. These effects were also observed in a co-culture of BV2 microglial cells and retina-derived 661W cells. Conclusions: Curcumin delayed retinal degeneration by suppressing microglia activation in the retina of rd1 mice. Thus, it may be an effective treatment for neurodegenerative disorders such as RP.

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CCL2 and CCR2 regulate pain-related behaviour and early gene expression in post-traumatic murine osteoarthritis but contribute little to chondropathy

Cited by 105 publications

References 37 publications

A mouse model for chronic pain-induced increase in ethanol consumption

A mouse model for chronic pain-induced increase in ethanol consumption

Can we target CCR2 to treat osteoarthritis? The trick is in the timing!

Curcumin Delays Retinal Degeneration by Regulating Microglia Activation in the Retina of rd1 Mice

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