J. Clin. Invest.

2007

DOI: 10.1172/jci28549

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Monocyte subsets differentially employ CCR2, CCR5, and CX3CR1 to accumulate within atherosclerotic plaques

¹

,

David Álvarez²,

Theodore Kaplan³

et al.

Abstract: Monocytes participate critically in atherosclerosis. There are 2 major subsets expressing different chemokine receptor patterns: CCR2 + CX3CR1 + Ly-6C hi and CCR2 -CX3CR1 ++ Ly-6C lo monocytes. Both C-C motif chemokine receptor 2 (CCR2) and C-X 3 -C motif chemokine receptor 1 (CX3CR1) are linked to progression of atherosclerotic plaques. Here, we analyzed mouse monocyte subsets in apoE-deficient mice and traced their differentiation and chemokine receptor usage as they accumulated within atherosclerotic plaque… Show more

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Mobilization and Recruitment Of Monocytes To Target Sites1

Cr1 Gene Expression In Mos Macs and Dcs1

Atherosclerosis Pathogenesis1

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Cited by 1,177 publications

(1,420 citation statements)

References 57 publications

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“…Injured muscle only recruits CX3CR1 lo /Ly-6C + MOs/MPs that subsequently switch into antiinfl ammatory CX3CR1 hi / Ly-6C − MOs/MPs and differentiate into MPs We labeled each circulating subset with fl uorescent latex beads (LXs) before injury, as previously described (12,15). Labeling of MOs does not alter their migratory capacities (12).…”

Section: Resultsmentioning

confidence: 99%

Inflammatory monocytes recruited after skeletal muscle injury switch into antiinflammatory macrophages to support myogenesis

et al. 2007

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No abstract

“…Injured muscle only recruits CX3CR1 lo /Ly-6C + MOs/MPs that subsequently switch into antiinfl ammatory CX3CR1 hi / Ly-6C − MOs/MPs and differentiate into MPs We labeled each circulating subset with fl uorescent latex beads (LXs) before injury, as previously described (12,15). Labeling of MOs does not alter their migratory capacities (12).…”

Section: Resultsmentioning

confidence: 99%

Inflammatory monocytes recruited after skeletal muscle injury switch into antiinflammatory macrophages to support myogenesis

et al. 2007

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No abstract

“…A major role in mobilization and recruitment of Ly6C high monocytes, under both homeostatic and pathological conditions, has been attributed to the chemokine receptor CCR2 (CD192), bound by the chemokines CCL2 and CCL7 [32][33][34]. CCL2 (monocyte chemotactic protein-1 or MCP-1) is expressed by many nucleated cell types in response to pro-inflammatory or microbial stimuli and the role of the CCL2-CCR2-axis in recruitment of Ly6C high monocytes to sites of inflammation has been demonstrated for various pathological conditions (such as infection, atherosclerosis and diabetes) [32][33][34][35][36]. In cancer, CCL2 was identified as the first tumor-derived factor (TDF) that induced chemotaxis in monocytes [37].…”

Section: Mobilization and Recruitment Of Monocytes To Target Sitesmentioning

confidence: 99%

Monocytes and Macrophages in Cancer: Development and Functions

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,

²

,

³

2012

Cancer Microenvironment

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Monocytes and tumor-associated macrophages are part of the myeloid family, a group of hematopoietic derived cells. Monocytes are direct precursors of hematopoietic stem cell-derived macrophages. After their recruitment into the tumor tissue, they can differentiate into tumor-associated macrophages, a very heterogeneous cell population in terms of phenotype and pro-tumor function, supporting tumor initiation, local progression and distant metastasis. Therefore, targeting monocytes and macrophages is a promising immunotherapeutic approach. This review will focus on the development of monocytes as macrophage precursors, the functions of tumorassociated macrophages and the possibility of interfering with tumor development and progression by targeting these myeloid cells.

“…15,23,[44][45][46][47][48][49][50] Under those conditions, CX 3 CL1 may facilitate the adhesion and transmigration of Mos. 51 Additionally, it has been recently proposed that a direct and evolutionary conserved role for CX 3 CR1-CX 3 CL1 interactions is involved in Mo survival. 43 Although chemokines were originally defined as chemoattractants, a growing body of evidence indicates their additional involvement in the control of cell survival.…”

Section: Cr1 Gene Expression In Mos Macs and Dcsmentioning

confidence: 99%

Differential expression of the fractalkine chemokine receptor (CX3CR1) in human monocytes during differentiation

¹

,

²

,

³

et al. 2014

Cell Mol Immunol

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Circulating monocytes (Mos) may continuously repopulate macrophage (MAC) or dendritic cell (DC) populations to maintain homeostasis. MACs and DCs are specialized cells that play different and complementary immunological functions. Accordingly, they present distinct migratory properties. Specifically, whereas MACs largely remain in tissues, DCs are capable of migrating from peripheral tissues to lymphoid organs. The aim of this work was to analyze the expression of the fractalkine receptor (CX 3 CR1) during the monocytic differentiation process. Freshly isolated Mos express high levels of both CX 3 CR1 mRNA and protein. During the Mo differentiation process, CX 3 CR1 is downregulated in both DCs and MACs. However, MACs showed significantly higher CX 3 CR1 expression levels than did DC. We also observed an antagonistic CX 3 CR1 regulation by interferon (IFN)-c and interleukin (IL)-4 during MAC activation through the classical and alternative MAC pathways, respectively. IFN-c inhibited the loss of CX 3 CR1, but IL-4 induced it. Additionally, we demonstrated an association between CX 3 CR1 expression and apoptosis prevention by soluble fractalkine (sCX 3 CL1) in Mos, DCs and MACs. This is the first report demonstrating sequential and differential CX 3 CR1 modulation during Mo differentiation. Most importantly, we demonstrated a functional link between CX 3 CR1 expression and cell survival in the presence of sCX 3 CL1.

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