Neutrophil extracellular traps (NETs) emerge from the cell as a DNA scaffold associated with cytoplasmic and granular proteins, able to immobilize and kill pathogens. This association occurs following nuclear and granular membrane disintegration, allowing contact with the decondensed chromatin. Thus, it is reasonable to speculate that the DNA can also mix with miRNAs and carry them in NETs. Here, we report for the first time the presence of the miRNA carriers associated with NETs and miRNAs present in NET-enriched supernatants (NET-miRs), thus adding a novel class of molecules and new proteins that can be released and transported in the NET platform. We observed that the majority of NET-miRs were common to all four stimuli used (PMA, interleukin-8, amyloid fibrils and Leishmania), and that miRNA-142-3p carried by NETs down-modulates protein kinase Cα and regulates tnf-α production in macrophages upon NET interaction with these cells. Our findings unveil a novel role for NETs in the cell communication processes, allowing the conveyance of miRNA from neutrophils to neighboring cells. Neutrophils are pivotal cells of the innate immune response, as they are the first leukocytes to reach infected or injured tissues. Neutrophils are endowed with powerful microbicidal properties, such as phagocytosis, degranulation and extrusion of neutrophil extracellular traps (NETs) 1. NETs are scaffold of chromatin decorated with cytoplasmic and granular proteins released to the extracellular milieu that are able to immobilize and kill pathogens by means of toxic molecules such as elastase and histone 2. NET release is triggered by different stimuli, such as pathogens (bacteria, fungi, viruses, parasites) 2 , endogenous molecules (e.g., interleukin [IL]-8 and amyloid fibrils) 2,3 , and inorganic compounds, such as phorbol myristate acetate (PMA) 1. The NET extrusion process is initiated with the loss of the classical nuclear morphology and chromatin decondensation, followed by the disappearance of all internal membranes, allowing the assembly of NET components 4. Many granular and cytoplasmatic proteins have been identified as NET cargos 5 , but the complete NET components remain to be defined. Thus, we asked whether other molecules, such as microRNAs (miRNAs), could be associated with NET scaffolds. miRNAs are short (19-24 nucleotides in length) non-coding RNAs, found intracellularly and outside the cells, and that regulate messenger RNA (mRNA) or protein levels either by promoting mRNA degradation or by attenuating protein translation. Despite accumulating evidence of extracellular miRNAs 6,7 , their presence associated with NETs has not yet been described.
