Targeting Tyro3, Axl and MerTK (TAM receptors): implications for macrophages in the tumor microenvironment

Myers, K.; Amend, Sarah R.; Pienta, Kenneth J.

doi:10.1186/s12943-019-1022-2

Cited by 275 publications

(271 citation statements)

References 166 publications

(153 reference statements)

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“…Moreover, in OS, a key osteoblast transcription factor, the Runt Related Transcription Factor 2 (RUNX2), is usually overexpressed [6,7] and metalloprotease MMP-2, alone or with MMP-9, plays a pivotal role in OS metastases and OS patients' outcome [8,9]. Tumor microenvironment (TME) comprises a variety of infiltrating immune cells, including tumor-associated macrophages (TAMs), which are the most abundant [10][11][12][13]. TAMs and their alternative activation states greatly contribute to the progression of tumors [14][15][16][17].…”

Section: Introductionmentioning

confidence: 99%

Mifamurtide and TAM-like macrophages: effect on proliferation, migration and differentiation of osteosarcoma cells

et al. 2020

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Tumor-associated macrophages and their alternative activation states together with cytokines and growth factors trapped in tumor microenvironment contribute to the progression of OS. In contrast to other tumor types, M2 polarized macrophages, reduce metastasis and improve survival in osteosarcoma patients. Mifamurtide is an immunomodulatory drug given together with standard adjuvant chemotherapy in high-grade osteosarcoma to improve outcome. Macrophages obtained from peripheral blood mononucleated cells of healthy donors and MG63 cells were cultured alone and together, and treated with Mifamurtide. We analyzed the effects of Mifamurtide on macrophage polarization and on MG63 proliferation, migration and differentiation, evaluating the expression of M1/M2 and osteoblast markers and molecules involved in metastasis and proliferation pathways. Our data suggest that Mifamurtide, switching macrophage polarization towards a TAM-like intermediate M1/M2 phenotype, may modulate the delicate balance between pro-inflammatory and immunomodulatory macrophage functions. Moreover, Mifamurtide may inhibit the cellular proliferation and induce the tumor cell differentiation, probably through the down regulation of pSTAT3, pAKT and IL-17R.

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Section: Introductionmentioning

confidence: 99%

Mifamurtide and TAM-like macrophages: effect on proliferation, migration and differentiation of osteosarcoma cells

et al. 2020

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“…Macrophages not only reside in stroma but can also sequester in interstitial fluids and transudates . Activated monocytes recruited into the site of inflammation undergo monocyte‐to‐macrophage differentiation; nevertheless, there are no definite and distinctive markers that can be used for differential discrimination of these two cell types . Certain genes such as MERTK, CD64, AXL and TYRO3 have been acknowledged to be macrophage specific; low‐level expression of macrophage‐related markers is generally observed in monocytes as well .…”

Section: Discussionmentioning

confidence: 99%

PD‐L2⁺ wound zone macrophage‐like cells display M1/M2‐mixed activation and restrain the effector Th1 responses

et al. 2020

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Depending on the microenvironment conditions, macrophages display phenotypic and functional heterogeneity. This study characterized the programmed cell death-ligand 2 (PD-L2)-expressing macrophage-like cells drained from surgical wound zones, and investigated their influence on helper T (Th) cell responses. Although all CD14 + myeloid cells possessed macrophagelike features, CD206 + and CD163 + cells constituted a specific subpopulation with high PD-L2 expression. There was a modest correlation between the PD-L2 levels on CD206 + macrophages and the amount of interferon (IFN)-c in the drainage fluid. The adhesion-independent macrophages simultaneously presented both classically-activated M1 and alternatively-activated M2 characteristics. CD206 + and PD-L2 + cells were identified with high granularity and size, expressed arginase-1 and costimulatory molecules, had enhanced phagocytic activity and produced reactive oxygen species. The genes associated with macrophage differentiation (MERTK, AXL and TYRO3) were also upregulated. These cells provided costimulation to Th cells; yet, when PD-L2 was blocked, T-cell proliferation and IFNc production were enhanced. Under defined conditions devoid of activation stimuli and matrix adhesion, ex vivogenerated monocyte-derived macrophages displayed limited capacity to stimulate T cells. Upon exposure to IFNc, they significantly upregulated programmed death 1 ligands, especially PD-L2. These cells did not completely abrogate T-cell differentiation; however, PD-L2 checkpoint blockade restored Th1 proliferation and secretion of interleukin-2, tumor necrosis factor-a and IFNc. In conclusion, upregulation of PD-L2 on the wound zone macrophages may constitute a negative feedback loop that restrains the Th1 effector responses and avoids exacerbation of inflammation during tissue healing.

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“…Through the PI3K/Akt signaling axis, MerTK induces polarization of M2 macrophages while inhibiting polarization of M1 macrophages, and thereby resulting in the resolution of inflammation [58]. M2 macrophages play a crucial role in the cancer microenvironment by facilitating tumor progression and invasion due to their immunosuppressive characteristics [59]. In addition to innate immunity, MerTK is involved in the modulation in adaptive immunity as genetic ablation of MerTK parallels increased intratumoral CD8 + T lymphocytes and promoted lymphocyte proliferation [48].…”

Section: Tam Receptorsmentioning

confidence: 99%

Regulation of efferocytosis as a novel cancer therapy

et al. 2020

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Efferocytosis is a physiologic phagocytic clearance of apoptotic cells, which modulates inflammatory responses and the immune environment and subsequently facilitates immune escape of cancer cells, thus promoting tumor development and progression. Efferocytosis is an equilibrium formed by perfect coordination among "find-me", "eat-me" and "don't-eat-me" signals. These signaling pathways not only affect the proliferation, invasion, metastasis, and angiogenesis of tumor cells but also regulate adaptive responses and drug resistance to antitumor therapies. Therefore, efferocytosis-related molecules and pathways are potential targets for antitumor therapy. Besides, supplementing conventional chemotherapy, radiotherapy and other immunotherapies with efferocytosis-targeted therapy could enhance the therapeutic efficacy, reduce off-target toxicity, and promote patient outcome.

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Targeting Tyro3, Axl and MerTK (TAM receptors): implications for macrophages in the tumor microenvironment

Cited by 275 publications

References 166 publications

Mifamurtide and TAM-like macrophages: effect on proliferation, migration and differentiation of osteosarcoma cells

Mifamurtide and TAM-like macrophages: effect on proliferation, migration and differentiation of osteosarcoma cells

PD‐L2⁺ wound zone macrophage‐like cells display M1/M2‐mixed activation and restrain the effector Th1 responses

Regulation of efferocytosis as a novel cancer therapy

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Targeting Tyro3, Axl and MerTK (TAM receptors): implications for macrophages in the tumor microenvironment

Cited by 275 publications

References 166 publications

Mifamurtide and TAM-like macrophages: effect on proliferation, migration and differentiation of osteosarcoma cells

Mifamurtide and TAM-like macrophages: effect on proliferation, migration and differentiation of osteosarcoma cells

PD‐L2+ wound zone macrophage‐like cells display M1/M2‐mixed activation and restrain the effector Th1 responses

Regulation of efferocytosis as a novel cancer therapy

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PD‐L2⁺ wound zone macrophage‐like cells display M1/M2‐mixed activation and restrain the effector Th1 responses