miR-217 is an oncogene that enhances the germinal center reaction.

نویسندگان

  • Virginia G de Yébenes
  • Nahikari Bartolomé-Izquierdo
  • Rubén Nogales-Cadenas
  • Pablo Pérez-Durán
  • Sonia M Mur
  • Nerea Martínez
  • Lorena Di Lisio
  • Davide F Robbiani
  • Alberto Pascual-Montano
  • Marta Cañamero
  • Miguel A Piris
  • Almudena R Ramiro
چکیده

microRNAs are a class of regulators of gene expression that have been shown critical for a great number of biological processes; however, little is known of their role in germinal center (GC) B cells. Although the GC reaction is crucial to ensure a competent immune response, GC B cells are also the origin of most human lymphomas, presumably due to bystander effects of the immunoglobulin gene remodeling that takes place at these sites. Here we report that miR-217 is specifically upregulated in GC B cells. Gain- and loss-of-function mouse models reveal that miR-217 is a positive modulator of the GC response that increases the generation of class-switched antibodies and the frequency of somatic hypermutation. We find that miR-217 down-regulates the expression of a DNA damage response and repair gene network and in turn stabilizes Bcl-6 expression in GC B cells. Importantly, miR-217 overexpression also promotes mature B-cell lymphomagenesis; this is physiologically relevant as we find that miR-217 is overexpressed in aggressive human B-cell lymphomas. Therefore, miR-217 provides a novel molecular link between the normal GC response and B-cell transformation.

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عنوان ژورنال:
  • Blood

دوره 124 2  شماره 

صفحات  -

تاریخ انتشار 2014