Cancers (Oct 2021)

High Expression of <i>PPM1D</i> Induces Tumors Phenotypically Similar to <i>TP53</i> Loss-of-Function Mutations in Mice

  • Jelena Milosevic,
  • Susanne Fransson,
  • Miklos Gulyas,
  • Thale K. Olsen,
  • Gabriel Gallo-Oller,
  • Diana Treis,
  • Lotta H. M. Elfman,
  • Margareta Wilhelm,
  • Tommy Martinsson,
  • Ninib Baryawno,
  • Per Kogner,
  • John Inge Johnsen

DOI
https://doi.org/10.3390/cancers13215493
Journal volume & issue
Vol. 13, no. 21
p. 5493

Abstract

Read online

PPM1D is a negative regulator of p53 and genomic aberrations resulting in increased activity of PPM1D have been observed in cancers of different origins, indicating that PPM1D has oncogenic properties. We established a transgenic mouse model overexpressing PPM1D and showed that these mice developed a wide variety of cancers. PPM1D-expressing mice developed tumors phenotypically and genetically similar to tumors in mice with dysfunctional p53. T-cell lymphoblastic lymphoma was the most frequent cancer observed in these mice (55%) followed by adenocarcinomas (24%), leukemia (12%) and other solid tumors including neuroblastoma. Characterization of T-cell lymphomas in mice overexpressing PPM1D demonstrates Pten-deletion and p53-accumulation similar to mice with p53 loss-of-function. Also, Notch1 mutations which are recurrently observed in T-cell acute lymphoblastic lymphoma (T-ALL) were frequently detected in PPM1D-transgenic mice. Hence, PPM1D acts as an oncogenic driver in connection with cellular stress, suggesting that the PPM1D gene status and expression levels should be investigated in TP53 wild-type tumors.

Keywords