A CCR2 macrophage endocytic pathway mediates extravascular fibrin clearance in vivo

Summary Physiologic turnover of interstitial collagen is mediated by a sequential pathway, in which collagen is fragmented by pericellular collagenases, endocytosed by collagen receptors, and routed to lysosomes for degradation by cathepsins. Here, we used intravital microscopy to investigate if malignant tumors, which are characterized by high rates of extracellular matrix turnover, utilize a similar collagen degradation pathway. Tumors of epithelial, mesenchymal, or neural crest origin all displayed vigorous endocytic collagen degradation. The cells engaged in this process were identified as tumor-associated macrophage (TAM)-like cells that degraded collagen in a mannose receptor-dependent manner. Accordingly, mannose receptor-deficient mice displayed increased intra-tumoral collagen. Whole transcriptome profiling uncovered a distinct extracellular matrix-catabolic signature of these collagen-degrading TAMs. Lineage-ablation studies revealed that collagen-degrading TAMs originated from circulating CCR2+ monocytes. The study identifies a function of TAMs in altering the tumor microenvironment through endocytic collagen turnover and establishes macrophages as centrally engaged in tumor-associated collagen degradation.

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“…The degradation of such non-collagenous ECM proteins may also involve endocytosis (Motley et al, 2016). …”

Section: Discussionmentioning

confidence: 99%

Tumor-Associated Macrophages Derived from Circulating Inflammatory Monocytes Degrade Collagen through Cellular Uptake

et al. 2017

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“…Much evidence showing that macrophages can respond to CCL2 also comes from studies done on osteoclasts, which are tissue-resident macrophages (102)(103)(104)(105). Concluding, it seems that macrophages represent a wide spectrum of differently polarized cells wherein some subsets do express CCR2 and are able to respond to CCL2 while others do not (171)(172)(173). Regulation of cell expression of this chemokine receptor may represent a neat way of controlling site-specific macrophage responses to CCL2.…”

Section: Considerations Regarding Ccl2's Impact On Myeloid Cellsmentioning

confidence: 99%

“…When investigating BMDMs (M-CSF derived) and BMDCs (GM-CSF derived) generated from CCL2 knockout and CCR2 knockout mice, Chen et al found reduced phagocytosis (of Escherichia coli) and endocytosis (of dextran) compared to BMDMs of wild-type mice (108). Furthermore, the CCL2/CCR2 axis seems to be essential for macrophage-mediated endocytosis of collagen and fibrin (111,171). This ECM turnover is critical during tissue remodeling and repair (197).…”

Section: Increase Of Phagocytosis Efferocytosis and Endocytosis Ofmentioning

confidence: 99%

More Than Just Attractive: How CCL2 Influences Myeloid Cell Behavior Beyond Chemotaxis

2019

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Monocyte chemoattractant protein-1 (MCP-1/CCL2) is renowned for its ability to drive the chemotaxis of myeloid and lymphoid cells. It orchestrates the migration of these cell types both during physiological immune defense and in pathological circumstances, such as autoimmune diseases including rheumatoid arthritis and multiple sclerosis, inflammatory diseases including atherosclerosis, as well as infectious diseases, obesity, diabetes, and various types of cancer. However, new data suggest that the scope of CCL2's functions may extend beyond its original characterization as a chemoattractant. Emerging evidence shows that it can impact leukocyte behavior, influencing adhesion, polarization, effector molecule secretion, autophagy, killing, and survival. The direction of these CCL2-induced responses is context dependent and, in some cases, synergistic with other inflammatory stimuli. The involvement of CCL2 signaling in multiple diseases renders it an interesting therapeutic target, although current targeting strategies have not met early expectations in the clinic. A better understanding of how CCL2 affects immune cells will be pivotal to the improvement of existing therapeutic approaches and the development of new drugs. Here, we provide an overview of the pleiotropic effects of CCL2 signaling on cells of the myeloid lineage, beyond chemotaxis, and highlight how these actions might help to shape immune cell behavior and tumor immunity.

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“…In healing wounds, the plasma-derived ECM is cleared through extracellular proteolysis by fibrinolytic enzymes (59) and through endocytosis by CCR2 + macrophages (60). In the healing infarct, clearance of the fibrin-based provisional matrix by the plasminogen/plasmin system is an important part of the reparative response.…”

Section: Ecm During the Proliferative Phase Of Infarct Healingmentioning

confidence: 99%

The extracellular matrix in myocardial injury, repair, and remodeling

Frangogiannis¹

2017

Journal of Clinical Investigation

390

318

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A CCR2 macrophage endocytic pathway mediates extravascular fibrin clearance in vivo

Cited by 37 publications

References 88 publications

Tumor-Associated Macrophages Derived from Circulating Inflammatory Monocytes Degrade Collagen through Cellular Uptake

Tumor-Associated Macrophages Derived from Circulating Inflammatory Monocytes Degrade Collagen through Cellular Uptake

More Than Just Attractive: How CCL2 Influences Myeloid Cell Behavior Beyond Chemotaxis

The extracellular matrix in myocardial injury, repair, and remodeling

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