Literature DB >> 28346427

MiR-21 is required for anti-tumor immune response in mice: an implication for its bi-directional roles.

W He1, C Wang2, R Mu1, P Liang1, Z Huang1, J Zhang1,3, L Dong1.   

Abstract

Here we show that miR-21, a microRNA known for its oncogenic activity, is also essential for mediating immune responses against tumor. Knockout of miR-21 in mice slowed the proliferation of both CD4+ and CD8+ cells, reduced their cytokine production and accelerated the grafted tumor growth. Further investigations indicated that miR-21 could activate CD4+ and CD8+ T cells via the PTEN/Akt pathway in response to stimulations. Taken together, these data suggest the key functions of miR-21 in mediating anti-tumor immune response and thereby uncover a bi-directional role of this traditionally known 'oncomiR' in tumorigenesis. Our study may provide new insights for the design of cancer therapies targeting microRNAs, with an emphasis on the dynamic and possibly unexpected role of these molecules.

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Year:  2017        PMID: 28346427     DOI: 10.1038/onc.2017.62

Source DB:  PubMed          Journal:  Oncogene        ISSN: 0950-9232            Impact factor:   9.867


  62 in total

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5.  Mathematical model of tumor-immune surveillance.

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8.  Over-expressing Akt in T cells to resist tumor immunosuppression and increase anti-tumor activity.

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Review 2.  Circulating MicroRNAs as a Tool for Diagnosis of Liver Disease Progression in People Living with HIV-1.

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Review 5.  microRNA-based diagnostic and therapeutic applications in cancer medicine.

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Review 6.  Control of Immunoregulatory Molecules by miRNAs in T Cell Activation.

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7.  circRIP2 accelerates bladder cancer progression via miR-1305/Tgf-β2/smad3 pathway.

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8.  A Two-Step Process of Effector Programming Governs CD4+ T Cell Fate Determination Induced by Antigenic Activation in the Steady State.

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9.  miR-21 sustains CD28 signalling and low-affinity T-cell responses at the expense of self-tolerance.

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10.  Suppressing miR-21 activity in tumor-associated macrophages promotes an antitumor immune response.

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