Cell Reports (Jan 2015)

P53 Mutations Change Phosphatidylinositol Acyl Chain Composition

  • Adam Naguib,
  • Gyula Bencze,
  • Dannielle D. Engle,
  • Iok I.C. Chio,
  • Tali Herzka,
  • Kaitlin Watrud,
  • Szilvia Bencze,
  • David A. Tuveson,
  • Darryl J. Pappin,
  • Lloyd C. Trotman

DOI
https://doi.org/10.1016/j.celrep.2014.12.010
Journal volume & issue
Vol. 10, no. 1
pp. 8 – 19

Abstract

Read online

Phosphatidylinositol phosphate (PIP) second messengers relay extracellular growth cues through the phosphorylation status of the inositol sugar, a signal transduction system that is deregulated in cancer. In stark contrast to PIP inositol head-group phosphorylation, changes in phosphatidylinositol (PI) lipid acyl chains in cancer have remained ill-defined. Here, we apply a mass-spectrometry-based method capable of unbiased high-throughput identification and quantification of cellular PI acyl chain composition. Using this approach, we find that PI lipid chains represent a cell-specific fingerprint and are unperturbed by serum-mediated signaling in contrast to the inositol head group. We find that mutation of Trp53 results in PIs containing reduced-length fatty acid moieties. Our results suggest that the anchoring tails of lipid second messengers form an additional layer of PIP signaling in cancer that operates independently of PTEN/PI3-kinase activity but is instead linked to p53.