Prep1 (pKnox1)-deficiency leads to spontaneous tumor development in mice and accelerates EmuMyc lymphomagenesis: a tumor suppressor role for Prep1.

نویسندگان

  • E Longobardi
  • G Iotti
  • P Di Rosa
  • S Mejetta
  • F Bianchi
  • L C Fernandez-Diaz
  • N Micali
  • P Nuciforo
  • E Lenti
  • M Ponzoni
  • C Doglioni
  • M Caniatti
  • P P Di Fiore
  • F Blasi
چکیده

The Prep1 homeodomain transcription factor is essential for embryonic development. 25% of hypomorphic Prep1(i/i) embryos, expressing the gene at 2% of the normal levels, survive pregnancy and live a normal-length life. Later in life, however, these mice develop spontaneous pre-tumoral lesions or solid tumors (lymphomas and carcinomas). In addition, transplantation of E14.5 fetal liver (FL) Prep1(i/i) cells into lethally irradiated mice induces lymphomas. In agreement with the above data, haploinsufficiency of a different Prep1-deficient (null) allele accelerates EmuMyc lymphoma growth. Therefore Prep1 has a tumor suppressor function in mice. Immunohistochemistry on tissue micrroarrays (TMA) generated from three distinct human cohorts comprising a total of some 1000 human tumors revealed that 70% of the tumors express no or extremely low levels of Prep1, unlike normal tissues. Our data in mice are thus potentially relevant to human cancer.

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عنوان ژورنال:
  • Molecular oncology

دوره 4 2  شماره 

صفحات  -

تاریخ انتشار 2010