AI Article Synopsis
- - The study reveals that the RNA editing protein ADAR1 is down-regulated during the metastatic transition of melanoma, which increases melanoma cell growth and tumor characteristics.
- - Knockdown of ADAR1 in melanoma cells leads to resistance against tumor infiltrating lymphocytes, indicating a significant role for ADAR1 in melanoma immune resistance through its effect on miR-222 and ICAM1 expression.
- - Higher levels of miR-222 in melanoma tissues correlate with poor clinical response to the drug ipilimumab, suggesting miR-222 could serve as a biomarker to predict treatment outcomes and inform personalized therapy.
Article Abstract
The blossom of immunotherapy in melanoma highlights the need to delineate mechanisms of immune resistance. Recently, we have demonstrated that the RNA editing protein, adenosine deaminase acting on RNA-1 (ADAR1) is down-regulated during metastatic transition of melanoma, which enhances melanoma cell proliferation and tumorigenicity. Here we investigate the role of ADAR1 in melanoma immune resistance.Importantly, knockdown of ADAR1 in human melanoma cells induces resistance to tumor infiltrating lymphocytes in a cell contact-dependent mechanism. We show that ADAR1, in an editing-independent manner, regulates the biogenesis of miR-222 at the transcription level and thereby Intercellular Adhesion Molecule 1 (ICAM1) expression, which consequently affects melanoma immune resistance. ADAR1 thus has a novel, pivotal, role in cancer immune resistance. Corroborating with these results, the expression of miR-222 in melanoma tissue specimens was significantly higher in patients who had no clinical benefit from treatment with ipilimumab as compared to patients that responded clinically, suggesting that miR-222 could function as a biomarker for the prediction of response to ipilimumab.These results provide not only novel insights on melanoma immune resistance, but also pave the way to the development of innovative personalized tools to enable optimal drug selection and treatment.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4745707 | PMC |
| http://dx.doi.org/10.18632/oncotarget.4905 | DOI Listing |
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