Publication | Open Access
<i>miR-146a</i> is a significant brake on autoimmunity, myeloproliferation, and cancer in mice
858
Citations
40
References
2011
Year
ImmunologyImmune RegulationPathologyInnate ImmunityImmune SystemTargeted DeletionImmune DysregulationInflammationLong Non-coding RnaAutoimmune DiseaseImmune SurveillanceAutoimmunitySelf-toleranceInappropriate ActivationImmune FunctionMicrorna DetectionEpigenetic RegulationCell BiologySignificant BrakeImmune Cell DevelopmentSmall RnaMedicineCell DevelopmentNon-coding Rna
Excessive or inappropriate activation of the immune system can be deleterious to the organism, warranting multiple molecular mechanisms to control and properly terminate immune responses. MicroRNAs (miRNAs), ∼22-nt-long noncoding RNAs, have recently emerged as key posttranscriptional regulators, controlling diverse biological processes, including responses to non-self. In this study, we examine the biological role of miR-146a using genetically engineered mice and show that targeted deletion of this gene, whose expression is strongly up-regulated after immune cell maturation and/or activation, results in several immune defects. Collectively, our findings suggest that miR-146a plays a key role as a molecular brake on inflammation, myeloid cell proliferation, and oncogenic transformation.
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