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MicroRNA-142 controls thymocyte proliferation.

Alexander MildnerElik ChapnikDiana VarolTegest AychekNardi LamplNatalia RivkinAnita BringmannFranziska PaulSigalit Boura-HalfonYifat Segal HayounZohar Barnett-ItzhakiIdo AmitEran HornsteinSteffen Jung
Published in: European journal of immunology (2017)
T-cell development is a spatially and temporally regulated process, orchestrated by well-defined contributions of transcription factors and cytokines. Here, we identify the noncoding RNA miR-142 as an additional regulatory layer within murine thymocyte development and proliferation. MiR-142 deficiency impairs the expression of cell cycle-promoting genes in mature mouse thymocytes and early progenitors, accompanied with increased levels of cyclin-dependent kinase inhibitor 1B (Cdkn1b, also known as p27Kip1 ). By using CRISPR/Cas9 technology to delete the miR-142-3p recognition element in the 3'UTR of cdkn1b, we confirm that this gene is a novel target of miR-142-3p in vivo. Increased Cdkn1b protein expression alone however was insufficient to cause proliferation defects in thymocytes, indicating the existence of additional critical miR-142 targets. Collectively, we establish a key role for miR-142 in the control of early and mature thymocyte proliferation, demonstrating the multifaceted role of a single miRNA on several target genes.
Keyphrases
  • cell proliferation
  • cell cycle
  • long non coding rna
  • long noncoding rna
  • signaling pathway
  • transcription factor
  • crispr cas
  • poor prognosis
  • genome wide
  • genome editing
  • pi k akt
  • gene expression
  • replacement therapy