Inflammation and Cancer: Extra- and Intracellular Determinants of Tumor-Associated Macrophages as Tumor Promoters

Szebeni, Gábor J.; Vízler, Csaba; Kitajka, Klára; Puskás, László G.

doi:10.1155/2017/9294018

Cited by 168 publications

(154 citation statements)

References 137 publications

(162 reference statements)

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“…The expression of several molecules can help determine Mϕ phenotype . On the cell surface, we chose to evaluate the expression of CD14, a typical Mϕ/monocyte protein and co‐receptor to TLR, and CD64, one of the receptors for Fcγ, HLA‐DR, and CD86, both involved in Ag presentation to T cells and CD206, a scavenger receptor associated with the alternative phenotype in Mϕs.…”

Section: Resultsmentioning

confidence: 99%

Lactate secreted by cervical cancer cells modulates macrophage phenotype

Stone

Rossetti

Alvarez

et al. 2019

Journal of Leukocyte Biology

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Cervical cancer continues to be a public health problem in developing countries. Previous studies have shown that cervical cancer cells display markers of aerobic glycolysis, indicating that these tumors are likely to secrete lactate. Mostly, lactate is recognized as a molecule capable of suppressing immune responses, through inhibition of T cells, Mϕs, and dendritic cells. We and others have previously shown that Mϕs are frequent cells infiltrating cervical cancers with the ability to inhibit antitumor immune responses and promote tumor growth through angiogenesis. Here, we have tested the hypothesis that lactate, secreted by cervical cancer cells, can modulate Mϕ phenotype. First, we showed higher lactate plasma concentrations in patients with increasing cervical lesion grades, with maximum concentration in the plasma of cancer patients, which supported our hypothesis. We then inhibited lactate production in tumor cell spheroids established from cervical cancer derived cell lines, using the lactate dehydrogenase inhibitor, oxamate, prior to co‐culture with monocytes. Lactate mediated part of the crosstalk between tumor cells and Mϕs, promoting secretion of IL‐1β, IL‐10, IL‐6, and up‐regulation of hypoxia induced factor‐1α expression, and down‐regulation of p65‐NFκB phosphorylation in Mϕs. We also showed that Mϕs from co‐cultures treated with oxamate were better inducers of T cell activation. Of note, experiments performed with inhibition of the monocarboxylate transporters rendered similar results. Our data confirms the hypothesis that lactate, secreted by cervical tumor cells, influences the phenotype of tumor Mϕs, promoting a suppressive phenotype.

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Section: Resultsmentioning

confidence: 99%

Lactate secreted by cervical cancer cells modulates macrophage phenotype

Stone

Rossetti

Alvarez

et al. 2019

Journal of Leukocyte Biology

View full text Add to dashboard Cite

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“…It has been reported that the chemokine CXCL12 (SDF‐1), together with CXCR4, was important for recruitment of CXCR4 + monocytes/macrophages into the CXCL12‐rich tissue area (Szebeni et al, ). SDF‐1 was down‐regulated by miR‐454 in PDAC cells, resulting in less migration of macrophages (CD86 + ) in vitro , and macrophage density was positively correlated with high SDF‐1 protein levels in vivo (Fan et al, ).…”

Section: Discussionmentioning

confidence: 99%

MicroRNA‐342 inhibits tumor growth via targeting chemokine CXCL12 involved in macrophages recruitment/activation

et al. 2018

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MicroRNAs (miRNAs) play important roles in initiation, development, progression and metastasis of tumors. MiR‐342 has been reported as a tumor suppressor or an onco‐miRNA based on functions or expression changes in various types of cancers. However, the biological roles and underlying molecular mechanisms of miR‐342 in tumorigenesis remain largely unknown. Here, we found that miR‐342 was expressed significantly less in a murine MS‐K tumor cell line that showed riched blood vessels. Over‐expression of miR‐342 in MS‐K cells inhibited cell proliferation, colony formation, reduced frequency of S phase population in vitro and suppressed tumor growth in vivo. Moreover, increasing miR‐342 impeded blood vessels formation and accumulation of macrophages (CD11b+) in tumors. By bioinformatic analysis and dual‐luciferase reporter assays, chemokine CXCL12 was identified as a direct target of miR‐342. Restored Cxcl12 expression in MS‐K‐miR‐342 cells could rescue cell proliferation in vitro. In MS‐K‐miR‐342 tumor‐infiltrated macrophages, expression of proangiogenic genes (Vegf‐A and Thbs1) and M2‐subtype macrophage markers (Cd163, Dectin1 and Ym1) was significantly down‐regulated compared with controls. Moreover, lower level of Cxcl12 and its receptor Cxcr4 was observed in the macrophages of MS‐K‐miR‐342 tumors, and MS‐K‐miR‐342 derived miR‐342, but not endogenous miR‐342, might contribute to Cxcl12 suppression in TAM. These results suggest that miR‐342 is involved in MS‐K tumor growth as a tumor suppressor by targeting chemokine CXCL12.

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“…264 In many cell types, though, especially in normal macrophage cells, TFEB is mutually antagonistic to STAT3 activity, and would thereby limit the protection of a tumor by macrophages. 269 Therefore, an intervention that differentially targets malignant cells from macrophages could have an added value. 266 Activation of TFEB by CQ can induce antitumor M1 macrophage activity.…”

Section: Feasibility Of Treating Malignant Tumors With Cq: Strengthsmentioning

confidence: 99%

Dissecting pharmacological effects of chloroquine in cancer treatment: interference with inflammatory signaling pathways

2019

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Chloroquines are 4-aminoquinoline-based drugs mainly used to treat malaria. At pharmacological concentrations, they have significant effects on tissue homeostasis, targeting diverse signaling pathways in mammalian cells. A key target pathway is autophagy, which regulates macromolecule turnover in the cell. In addition to affecting cellular metabolism and bioenergetic flow equilibrium, autophagy plays a pivotal role at the interface between inflammation and cancer progression. Chloroquines consequently have critical effects in tissue metabolic activity and importantly, in key functions of the immune system. In this article, we will review the work addressing the role of chloroquines in the homeostasis of mammalian tissue, and the potential strengths and weaknesses concerning their use in cancer therapy.

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Inflammation and Cancer: Extra- and Intracellular Determinants of Tumor-Associated Macrophages as Tumor Promoters

Cited by 168 publications

References 137 publications

Lactate secreted by cervical cancer cells modulates macrophage phenotype

Lactate secreted by cervical cancer cells modulates macrophage phenotype

MicroRNA‐342 inhibits tumor growth via targeting chemokine CXCL12 involved in macrophages recruitment/activation

Dissecting pharmacological effects of chloroquine in cancer treatment: interference with inflammatory signaling pathways

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