AI Article Synopsis

  • Theileria annulata is a parasite that infects bovine macrophages, leading to tropical theileriosis, a disease resembling leukemia.
  • Using advanced RNA sequencing, researchers found that infection triggers specific microRNAs, including miR-126-5p, which play a critical role in the malignancy of transformed macrophages.
  • The study highlights how changes in miR-126-5p levels, influenced by the phosphorylation status of a protein called AGO2, affect the behavior of macrophages, differentiating between virulent and non-virulent strains in terms of their tumor-disseminating abilities.

Article Abstract

Theileria annulata is an apicomplexan parasite that infects and transforms bovine macrophages that disseminate throughout the animal causing a leukaemia-like disease called tropical theileriosis. Using deep RNAseq of T. annulata-infected B cells and macrophages we identify a set of microRNAs induced by infection, whose expression diminishes upon loss of the hyper-disseminating phenotype of virulent transformed macrophages. We describe how infection-induced upregulation of miR-126-5p ablates JIP-2 expression to release cytosolic JNK to translocate to the nucleus and trans-activate AP-1-driven transcription of mmp9 to promote tumour dissemination. In non-disseminating attenuated macrophages miR-126-5p levels drop, JIP-2 levels increase, JNK1 is retained in the cytosol leading to decreased c-Jun phosphorylation and dampened AP-1-driven mmp9 transcription. We show that variation in miR-126-5p levels depends on the tyrosine phosphorylation status of AGO2 that is regulated by Grb2-recruitment of PTP1B. In attenuated macrophages Grb2 levels drop resulting in less PTP1B recruitment, greater AGO2 phosphorylation, less miR-126-5p associated with AGO2 and a consequent rise in JIP-2 levels. Changes in miR-126-5p levels therefore, underpin both the virulent hyper-dissemination and the attenuated dissemination of T. annulata-infected macrophages.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5892942PMC
http://dx.doi.org/10.1371/journal.ppat.1006942DOI Listing

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