The miR-371∼373 Cluster Represses Colon Cancer Initiation and Metastatic Colonization by Inhibiting the TGFBR2/ID1 Signaling Axis

Ullmann, Pit; Rodriguez, Fabien; Schmitz, Martine; Meurer, Steffen K.; Qureshi-Baig, Komal; Felten, Paul; Ginolhac, Aurélien; Antunes, Laurent; Frasquilho, Sónia; Zügel, Nikolaus; Weiskirchen, Ralf; Haan, Serge; Letellier, Elisabeth

doi:10.1158/0008-5472.can-17-3003

Cited by 35 publications

(35 citation statements)

References 50 publications

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“…The miR-371-373 cluster can act either as tumor-suppressors (Langroudi et al, 2015;Ullmann et al, 2018) or potential oncogenes (Wei et al, 2015;Ghasemi et al, 2018) in various human malignancies. In HBV infection, the upregulation of miRs-372-373 has been shown to positively correlate with the number of HBV DNA copies.…”

Section: Microrna Signaling In Hbv Infectionmentioning

confidence: 99%

MicroRNA Involvement in Signaling Pathways During Viral Infection

Barbu

Condrat

Thompson

et al. 2020

Front. Cell Dev. Biol.

109

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Section: Microrna Signaling In Hbv Infectionmentioning

confidence: 99%

MicroRNA Involvement in Signaling Pathways During Viral Infection

Barbu

Condrat

Thompson

et al. 2020

Front. Cell Dev. Biol.

109

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“…In addition, TGFBR2 has also been identified as a novel regulator of GBM stemness, 29 which may be related to the platelet‐derived growth factor receptor inhibitor resistance in GBM treatment 30 . TGFBR2 exerted the tumour‐enhancing effects via targeting different downstream mediators such as inhibitor of DNA binding, 31 Smad2/3 32 and p53 33 in other types of cancers. Moreover, several miRNAs including miR‐181c, 34 miR‐373 35 and miR‐502c 36 suppressed GBM progression via the inhibition of TGFBR2 expression.…”

Section: Discussionmentioning

confidence: 99%

LncRNA MIR4435‐2HG potentiates the proliferation and invasion of glioblastoma cells via modulating miR‐1224‐5p/TGFBR2 axis

Zhang

Yang

et al. 2020

J Cellular Molecular Medi

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Glioblastoma (GBM) belongs to the high‐grade (IV) gliomas with extremely poor prognosis. Accumulating evidence uncovered the key roles of long non‐coding RNAs (lncRNAs) in GBM development. This study aimed to determine the biological actions and the clinical relevance of lncRNA MIR4435‐2 Host Gene (MIR4435‐2HG) in GBM. Data from GEPIA database showed that MIR4435‐2HG was up‐regulated in GBM tissues and high expression of MIR4435‐2HG correlated with shorter overall survival of GBM patients. Further experimental assays verified the up‐regulation of MIR4435‐2HG in GBM tissues and cell lines. In vitro cell studies and in vivo animal studies showed that knockdown of MIR4435‐2HG resulted in the inhibition of GBM cell proliferation and invasion and in vivo tumour growth, while MIR4435‐2HG overexpression driven GBM progression. Furthermore, MIR44435‐2HG was found to sponge miR‐1224‐5p and suppress miR‐1224‐5p expression; overexpression of miR‐1224‐5p attenuated the enhancement in GBM cell proliferation and invasion induced by MIR4435‐2HG overexpression. In a subsequent study, miR‐1224‐5p was found to target transforming growth factor‐beta receptor type 2 (TGFBR2) and repressed TGFBR2 expression, and in vitro assays showed that miR‐1224‐5p exerted tumour‐suppressive effects via targeting TGFBR2. More importantly, TGFRB2 knockdown antagonized hyper‐proliferation and invasion of GBM cells with MIR4435‐2HG overexpression. Clinically, the down‐regulation of miR‐1224‐5p and up‐regulation of TGFBR2 were verified in the GBM clinical samples. Taken together, the present study suggests the oncogenic role of MIR4435‐2HG in GBM and underlies the key function of MIR4435‐2HG‐driven GBM progression via targeting miR‐1224‐5p/TGFBR2 axis.

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“…In metastasisderived tumor initiated cells (TICs), TGFβ receptor 2 (TGFBR2), an identified target of miR-371-3, were repressed and the miR-371-3/TGFBR2/inhibitor of DNA binding 1 signaling pathway showed credible connection to self-renewal of TIC. 7 MiR-373 regulated tumor cell proliferation and growth by prohibiting or enhancing multiple target genes expression, including large tumor suppressor homolog 2 (LATS2), 12,36 CD44, 14 nuclear factor I/B (NFIB), 37 and estrogen receptor (ER). 38 Moreover, the stemness of CRC cells was enhanced by miR-372/373 via repressing differentiationrelated pathways, such as NFκB, MAPK/Erk, and VDR.…”

Section: Discussionmentioning

confidence: 99%

“…MicroRNA-371-3 (miR-371-3) cluster locates on chromosome 19 and has three members, miR-371, MiR-372 and miR-373. MiR-371-3 cluster has been discussed to be involved in several diseases, such as canine visceral leishmaniasis, 4 stroke, 5 Kawasaki diseases, 6 colon cancer, 7 and moreover, it's role in the pathology of cancers is currently being focused on in several studies. [8][9][10][11] MiR-372 and miR-373 were reported to have the capacity to activate wild-type p53, counteract p53-mediated CDK inhibition and nourish oncogenic RAS to promote testicular germ cell cancerous process, 12 and up regulated miR-371-3p could reverse the acquired drug resistance and improve overall survival of cancer patients.…”

Section: Introductionmentioning

confidence: 99%

<p>MicroRNA-371-3 cluster as biomarkers for the diagnosis and prognosis of cancers</p>

Pan¹,

He²,

Xu³

et al. 2019

CMAR

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To date, increasing evidences have demonstrated that the aberrant expression of miR-371-3 cluster has been verified in various cancers and could be potentially used as a biomarker for tumor diagnosis and prognosis. To explore the role of miR-371-3 cluster in tumor diagnosis and prognosis, we conducted this study based on the published data. Methods: We searched electronic databases (PubMed, EMBASE and Web of Science databases) (Jan 1, 2007 to Jun 1, 2018). The pooled sensitivity, specificity and area under the curve (AUC) of summary receiver operator characteristic (SROC) curve were used for diagnostic values, meanwhile the pooled hazard ration (HR) and 95% CI were used to explore the prognosis capacity of miR-372 and miR-373. In addition, the publication bias of the enrolled studies was tested and a sensitivity analysis of each study was performed to evaluate the stability of the pooled result. Results: A total of eleven eligible studies containing six eligible studies containing 870 participants for diagnosis and 1218 cancer cases for prognosis were selected for this study. For diagnosis, the pooled results revealed that the miR-371 (sensitivity: 0.85, specificity: 0.92, AUC: 0.92) and miR-373 (sensitivity: 0.81, specificity: 0.93, AUC: 0.93) could be used as diagnostic biomarkers. For prognosis, we observed that elevated miR-372 indicated poor prognosis (HR=2.31, 95% CI: 1.04-5.14), especially in the cutoff value subgroup of median (HR=2.62, 95% CI: 1.54-4.46). In addition, pooled results showed that expression of miR-373 was not related to prognosis because of the significant heterogeneity, and the high miR-373 expression presented favorable prognosis in Asians (HR=0.34, 95% CI: 0.23-0.50) after omitting the study of heterogeneity origin. Conclusion: The current studies demonstrated that miR-371 and miR-373 could be predictive tumor diagnostic biomarkers and the expression of miR-372 and miR-373 may indicate prognosis of cancer patients.

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The miR-371∼373 Cluster Represses Colon Cancer Initiation and Metastatic Colonization by Inhibiting the TGFBR2/ID1 Signaling Axis

Cited by 35 publications

References 50 publications

MicroRNA Involvement in Signaling Pathways During Viral Infection

MicroRNA Involvement in Signaling Pathways During Viral Infection

LncRNA MIR4435‐2HG potentiates the proliferation and invasion of glioblastoma cells via modulating miR‐1224‐5p/TGFBR2 axis

<p>MicroRNA-371-3 cluster as biomarkers for the diagnosis and prognosis of cancers</p>

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