Adenosine Inhibits Tumor Cell Invasion via Receptor-Independent Mechanisms

Virtanen, Sanna S.; Kukkonen-Macchi, Anu; Vainio, Minna; Elima, Kati; Härkönen, Pirkko; Jalkanen, Sirpa; Yegutkin, Gennady G.

doi:10.1158/1541-7786.mcr-14-0302-t

Cited by 42 publications

(35 citation statements)

References 39 publications

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“…Importantly, these effects of adenosine were well within the adenosine concentration range that has been measured in the tumor microenvironment [48]. In line with these findings, Virtanen et al recently described an inhibitory effect of exogenous adenosine on cancer cell invasion and migration [18]. They suggested that receptor-independent mechanisms were responsible for this effect.…”

Section: Discussionsupporting

confidence: 63%

“…Cells were cultured for a maximum of 15 passages to minimize the risk of experimental variance due to mutations. This is particularly important as there are contradictory reports about the expression levels of adenosine receptor subtypes in breast cancer cell lines [18][19][20]. Prior to experiments, the cells were trypsinized and washed once with serum-containing medium and three times with serum-free medium containing 20 mM HEPES and 0.1 % bovine serum albumin (BSA).…”

Section: Cell Culturementioning

confidence: 99%

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Adenosine arrests breast cancer cell motility by A3 receptor stimulation

Ledderose

Hefti

Chen

et al. 2016

Purinergic Signalling

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In neutrophils, adenosine triphosphate (ATP) release and autocrine purinergic signaling regulate coordinated cell motility during chemotaxis. Here, we studied whether similar mechanisms regulate the motility of breast cancer cells. While neutrophils and benign human mammary epithelial cells (HMEC) form a single leading edge, MDA-MB-231 breast cancer cells possess multiple leading edges enriched with A3 adenosine receptors. Compared to HMEC, MDA-MB-231 cells overexpress the ectonucleotidases ENPP1 and CD73, which convert extracellular ATP released by the cells to adenosine that stimulates A3 receptors and promotes cell migration with frequent directional changes. However, exogenous adenosine added to breast cancer cells or the A3 receptor agonist IB-MECA dose-dependently arrested cell motility by simultaneous stimulation of multiple leading edges, doubling cell surface areas and significantly reducing migration velocity by up to 75 %. We conclude that MDA-MB-231 cells, HMEC, and neutrophils differ in the purinergic signaling mechanisms that regulate their motility patterns and that the subcellular distribution of A3 adenosine receptors in MDA-MB-231 breast cancer cells contributes to dysfunctional cell motility. These findings imply that purinergic signaling mechanisms may be potential therapeutic targets to interfere with the motility of breast cancer cells in order to reduce the spread of cancer cells and the risk of metastasis.

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Section: Discussionsupporting

confidence: 63%

Section: Cell Culturementioning

confidence: 99%

Adenosine arrests breast cancer cell motility by A3 receptor stimulation

Ledderose

Hefti

Chen

et al. 2016

Purinergic Signalling

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“…Moreover, the effect of the dCF on tumour invasion and migration was also clearly visible in more invasive human breast cancer cells, MDA‐MB‐231 and T47D. It has been shown previously, that this could be a receptor‐independent effect mediated by adenosine via inhibition of AMP‐activated protein kinase . However, based on our study, the significant role of adenosine receptors in these processes should also be noticed.…”

Section: Discussionmentioning

confidence: 99%

Adenosine deaminase inhibition suppresses progression of 4T1 murine breast cancer by adenosine receptor‐dependent mechanisms

Kutryb–Zajac

Koszałka

Mierzejewska

et al. 2018

J Cellular Molecular Medi

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The activity of a cell‐surface ecto‐adenosine deaminase (eADA) is markedly increased in the endothelial activation and vascular inflammation leading to decreased adenosine concentration and alterations in adenosine signalling. Depending on the specific pathway activated, extracellular purines mediate host cell response or regulate growth and cytotoxicity on tumour cells. The aim of this study was to test the effects of adenosine deaminase inhibition by 2′deoxycoformycin (dCF) on the breast cancer development. dCF treatment decreased a tumour growth and a final tumour mass in female BALB/c mice injected orthotopically with 4T1 cancer cells. dCF also counteracted cancer‐induced endothelial dysfunction in orthotopic and intravenous 4T1 mouse breast cancer models. In turn, this low dCF dose had a minor effect on immune stimulation exerted by 4T1 cell implantation. In vitro studies revealed that dCF suppressed migration and invasion of 4T1 cells via A2a and A3 adenosine receptor activation as well as 4T1 cell adhesion and transmigration through the endothelial cell layer via A2a receptor stimulation. Similar effects of dCF were observed in human breast cancer cells. Moreover, dCF improved a barrier function of endothelial cells decreasing its permeability. This study highlights beneficial effects of adenosine deaminase inhibition on breast cancer development. The inhibition of adenosine deaminase activity by dCF reduced tumour size that was closely related to the decreased aggressiveness of tumour cells by adenosine receptor‐dependent mechanisms and endothelial protection.

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“…In meduloblastoma cell lines, the metastatic potential is inversely correlated with CD73 expression and activity [35]. Pharmacological inhibition of CD73 reduces adhesion but increases the invasion/migration capacities in vitro [17, 36], and treatment with adenosine (produced by CD73) inhibits cell migration and invasion [37]. More recently, loss of CD73 has been involved in epithelial barrier misstructuration and endometrial tumor progression [17].…”

Section: Discussionmentioning

confidence: 99%

MiR-422a promotes loco-regional recurrence by targeting NT5E/CD73 in head and neck squamous cell carcinoma

et al. 2016

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At the time of diagnosis, 60% of patients with head and neck squamous cell carcinoma (HNSCC) present tumors in an advanced stage (III-IV) of disease and 80% will relapse within the first two years post-treatment, due to their frequent radio(chemo)resistance. To identify new molecular targets and companion biomarkers, we have investigated the miRNome of 75 stage III-IV oropharynx tumors without relapse (R) or with loco-regional relapse (non-responder, NR) within two years post-treatment. Interestingly, miR-422a was significantly downregulated in NR tumors, in agreement with the increase in cell proliferation and adhesion induced by miR-422a inhibition in vitro. Furthermore, we identified CD73/NT5E oncogene as target of miR-422a. Indeed, modulation of the endogenous level of miR-422a inversely influences the expression and the enzymatic activity of CD73. Moreover, knocking down CD73 mimics the effects of miR-422a upregulation. Importantly, in tumors, miR-422a and CD73 expression levels are inversely correlated, and both are predictive of relapse free survival - especially considering loco(regional) recurrence - in vitro two independent cohorts of advanced oropharynx or HNSCC (N=255) tumors. In all, we reported, for the first time, that MiR-422a and its target CD73 are involved in early loco(regional) recurrence of HNSCC tumors and are new targets for personalized medicine.

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Adenosine Inhibits Tumor Cell Invasion via Receptor-Independent Mechanisms

Cited by 42 publications

References 39 publications

Adenosine arrests breast cancer cell motility by A3 receptor stimulation

Adenosine arrests breast cancer cell motility by A3 receptor stimulation

Adenosine deaminase inhibition suppresses progression of 4T1 murine breast cancer by adenosine receptor‐dependent mechanisms

MiR-422a promotes loco-regional recurrence by targeting NT5E/CD73 in head and neck squamous cell carcinoma

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