Abstract:SUMMARYOncogene-induced senescence (OIS) is a form of stable cell cycle arrest elicited in cells as a response to oncogenic stimulation. OIS must be bypassed for transformation, but the mechanisms of OIS establishment and bypass remain poorly understood, especially at the post-transcriptional level. Here we show that the RNA binding protein UNR/CSDE1, previously involved in melanoma metastasis, unexpectedly enables OIS in primary mouse keratinocytes that have been challenged by over-expression of oncogenic H-R… Show more
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