PLoS ONE (Jan 2020)

An iron-dependent metabolic vulnerability underlies VPS34-dependence in RKO cancer cells.

  • Marek J Kobylarz,
  • Jonathan M Goodwin,
  • Zhao B Kang,
  • John W Annand,
  • Sarah Hevi,
  • Ellen O'Mahony,
  • Gregory McAllister,
  • John Reece-Hoyes,
  • Qiong Wang,
  • John Alford,
  • Carsten Russ,
  • Alicia Lindeman,
  • Martin Beibel,
  • Guglielmo Roma,
  • Walter Carbone,
  • Judith Knehr,
  • Joseph Loureiro,
  • Christophe Antczak,
  • Dmitri Wiederschain,
  • Leon O Murphy,
  • Suchithra Menon,
  • Beat Nyfeler

DOI
https://doi.org/10.1371/journal.pone.0235551
Journal volume & issue
Vol. 15, no. 8
p. e0235551

Abstract

Read online

VPS34 is a key regulator of endomembrane dynamics and cargo trafficking, and is essential in cultured cell lines and in mice. To better characterize the role of VPS34 in cell growth, we performed unbiased cell line profiling studies with the selective VPS34 inhibitor PIK-III and identified RKO as a VPS34-dependent cellular model. Pooled CRISPR screen in the presence of PIK-III revealed endolysosomal genes as genetic suppressors. Dissecting VPS34-dependent alterations with transcriptional profiling, we found the induction of hypoxia response and cholesterol biosynthesis as key signatures. Mechanistically, acute VPS34 inhibition enhanced lysosomal degradation of transferrin and low-density lipoprotein receptors leading to impaired iron and cholesterol uptake. Excess soluble iron, but not cholesterol, was sufficient to partially rescue the effects of VPS34 inhibition on mitochondrial respiration and cell growth, indicating that iron limitation is the primary driver of VPS34-dependency in RKO cells. Loss of RAB7A, an endolysosomal marker and top suppressor in our genetic screen, blocked transferrin receptor degradation, restored iron homeostasis and reversed the growth defect as well as metabolic alterations due to VPS34 inhibition. Altogether, our findings suggest that impaired iron mobilization via the VPS34-RAB7A axis drive VPS34-dependence in certain cancer cells.