S-adenosylmethionine and methylthioadenosine inhibit cancer metastasis by targeting microRNA 34a/b-methionine adenosyltransferase 2A/2B axis

Tomasi, Maria Lauda; Cossu, Carla; Spissu, Ylenia; Floris, Andrea; Ryoo, Minjung; Iglesias–Ara, Ainhoa; Wang, Qiang; Pandol, Stephen J.; Bhowmick, Neil A.; Seki, Ekihiro; Posadas, Edwin M.; Lu, Shelly C.

doi:10.18632/oncotarget.20234

Cited by 31 publications

(42 citation statements)

References 30 publications

(75 reference statements)

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“…In a chemically induced hepatocarcinogenesis rat model, both endogenous and exogenous MTA levels were found to be negatively correlated with preneoplastic liver lesions and DNA synthesis 27, 29. Similar inhibitory effects of MTA have also been observed in cultured HCT116 human colon cancer cells, colorectal cancer cells, HeLa cervical cancer cells, Daudi and Raji lymphoma cells, erythroleukemia cells, promyelocytic cells and mitogen stimulated human peripheral blood lymphocytes 8, 31-35.…”

Section: Mta and Tumorsupporting

confidence: 72%

“…It is noteworthy that most of these studies indicate that MTA had the opposite effect on the apoptosis of normal versus cancerous cells. In vitro , it enhances the apoptosis of human RKO and SW620 colon cancer cells 35, 41 and of HuH7 liver cancer cells 42. However, it does not have such effects on normal colon epithelial cells or even has anti-apoptotic effects on normal hepatocytes 41, 42.…”

Section: Mta and Tumormentioning

confidence: 99%

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5'-Methylthioadenosine and Cancer: old molecules, new understanding

Li¹,

Wang²,

Wu³

2019

J. Cancer

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While the metabolic changes in cancer tissues were first observed by Warburg Otto almost a century ago, altered metabolism has recently returned as a focus of cancer research. 5'-Methylthioadenosine (MTA) is a naturally occurring sulfur-containing nucleoside found in numerous species. While MTA was first isolated several decades ago, a lack of sensitive and specific analytical methodologies designed for its direct quantification has hampered the study of its physiological and pathophysiological features. Many studies indicate that MTA suppresses tumors by inhibiting tumor cell proliferation, invasion, and the induction of apoptosis while controlling the inflammatory micro-environments of tumor tissue. In this review, we assessed the effects of MTA and of related materials on the growth and functions of normal and malignant cells.

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Section: Mta and Tumorsupporting

confidence: 72%

Section: Mta and Tumormentioning

confidence: 99%

5'-Methylthioadenosine and Cancer: old molecules, new understanding

Li¹,

Wang²,

Wu³

2019

J. Cancer

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“…These discrepancies might be due to the different cellular context and tumor types and remain to be elucidated. Interestingly, while this article was in preparation, Tomasi et al reported that overexpression of MAT2A promoted ERK activation and cell migration in prostate and pancreatic cancer cells which do not express MAT1A. Taken our and Tomasi's data together, it is suggested that the liver‐specific MAT1A may play a critical role in metastasis of liver cancer and both increasing MAT2A and decreasing MAT1A are necessary for HCC metastasis.…”

Section: Discussionmentioning

confidence: 56%

A novel mechanism of the M1‐M2 methionine adenosyltransferase switch‐mediated hepatocellular carcinoma metastasis

Wang

Jin

Yao

et al. 2018

Molecular Carcinogenesis

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Hepatocellular carcinoma (HCC) manifests as a highly metastatic cancer with extremely poor prognosis. However, mechanisms underlying metastasis of HCC are not fully understood. Here, we showed that switching gene expression from MAT1A to MAT2A (M1-M2 switch) promoted cancer invasion and metastasis. Reversion of the M1-M2 switch repressed, whereas enhancing the M1-M2 switch promoted the ability of HCC cells to metastasize. Moreover, we provided clinical data showing that tipping the balance between MAT1A and MAT2A expression correlated with increased metastasis and inferior recurrence-free survival in HCC patients. Molecular pathways analysis showed that downregulation of MAT1A, which augmented osteopontin (OPN) expression through decreasing methylation of the OPN promoter, and MAT2A upregulation, which induced integrin β3 (ITGB3) expression by binding to ITGB3 promoter, collaboratively triggered ERK signaling and thereby promoted metastasis. Thus, the simultaneous downregulation of MAT1A and upregulation of MAT2A are necessary and sufficient for HCC metastasis in the process of M1-M2 switch. Our findings provide novel mechanistic insights into cancer metastasis. Inhibition and prevention of the M1-M2 switch would offer a novel therapeutic option for treatment of HCC.

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“…Over-expression of miR-34a or miR-34b lead to the low expression level of MAT2B, mainly in the protein expression level of CWR22Rv-1 and MIA PaCa-2 cells [ 65 ]. Using microRNA microarray, Lo TF et al [ 66 ] found that after berberine treatment, the expression of miR-21-3p (previously named miR-21) up-regulated in HepG2 human hepatoma cell line.…”

Section: Discussionmentioning

confidence: 99%

The biological functions of target genes in pan-cancers and cell lines were predicted by miR-375 microarray data from GEO database and bioinformatics

et al. 2018

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BackgroundMicroRNA is endogenous non-coding small RNA that negative regulate and control gene expression, and increasing evidence links microRNA to oncogenesis and the pathogenesis of cancer. The goal of this study was to explore the potential molecular mechanism of miR-375 in various cancers.MethodsMiR-375 overexpression in different tumor cell lines was probed with microarray data from Gene Expression Omnibus (GEO). The common target genes of miR-375 were obtained by Robust Rank Aggregation (RRA), and identified by miRWalk2.0 software for target gene prediction. Additionally, we directed in silico analysis including Protein-Protein Interactions (PPI) analysis, gene ontology (GO) enrichment analysis and Kyoto Encyclopedia of Genes and Genomes (KEGG) pathways annotations to provide a summary of the function of miR-375 in various carcinomas. Eventually, data was obtained from The Cancer Genome Atlas (TCGA) were utilized for a validation in 7 cancers.ResultsThe nine miR-375 related chips were acquired by the GEO data. The 5 down regulated genes came from 9 available microarray datasets, which overlapped with the potential target genes predicted by miRWalk2.0 software. The target genes were intensely enriched in amino acid biosynthetic and metabolic process from biological process (GO) and Cysteine and methionine metabolism (KEGG analysis). In view of these approaches, VASN, MAT2B, HERPUD1, TPAPPC6B and TAT are probably the most important miR-375 targets. In addition, miR-375 was negatively correlated with MAT2B, which was verified in 5 tumors of TCGA.ConclusionIn summary, this study based on common target genes provides an innovative perspective for exploring the molecular mechanism of miR-375 in human tumors.

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S-adenosylmethionine and methylthioadenosine inhibit cancer metastasis by targeting microRNA 34a/b-methionine adenosyltransferase 2A/2B axis

Cited by 31 publications

References 30 publications

5'-Methylthioadenosine and Cancer: old molecules, new understanding

5'-Methylthioadenosine and Cancer: old molecules, new understanding

A novel mechanism of the M1‐M2 methionine adenosyltransferase switch‐mediated hepatocellular carcinoma metastasis

The biological functions of target genes in pan-cancers and cell lines were predicted by miR-375 microarray data from GEO database and bioinformatics

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