Molecular Cancer (Jan 2009)

The chromatin remodelling factor BRG1 is a novel binding partner of the tumor suppressor p16<sup>INK4a</sup>

  • Mann Graham J,
  • Reisman David N,
  • Scolyer Richard A,
  • Diefenbach Eve,
  • Frausto Monika,
  • Scurr Lyndee L,
  • Dijkstra Menno K,
  • Haferkamp Sebastian,
  • Becker Therese M,
  • Kefford Richard F,
  • Rizos Helen

DOI
https://doi.org/10.1186/1476-4598-8-4
Journal volume & issue
Vol. 8, no. 1
p. 4

Abstract

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Abstract Background CDKN2A/p16INK4a is frequently altered in human cancers and it is the most important melanoma susceptibility gene identified to date. p16INK4a inhibits pRb phosphorylation and induces cell cycle arrest, which is considered its main tumour suppressor function. Nevertheless, additional activities may contribute to the tumour suppressor role of p16INK4a and could help explain its specific association with melanoma predisposition. To identify such functions we conducted a yeast-two-hybrid screen for novel p16INK4a binding partners. Results We now report that p16INK4a interacts with the chromatin remodelling factor BRG1. We investigated the cooperative roles of p16INK4a and BRG1 using a panel of cell lines and a melanoma cell model with inducible p16INK4a expression and BRG1 silencing. We found evidence that BRG1 is not required for p16INK4a-induced cell cycle inhibition and propose that the p16INK4a-BRG1 complex regulates BRG1 chromatin remodelling activity. Importantly, we found frequent loss of BRG1 expression in primary and metastatic melanomas, implicating this novel p16INK4a binding partner as an important tumour suppressor in melanoma. Conclusion This data adds to the increasing evidence implicating the SWI/SNF chromatin remodelling complex in tumour development and the association of p16INK4a with chromatin remodelling highlights potentially new functions that may be important in melanoma predisposition and chemoresistance.