International Journal of Molecular Sciences (Sep 2019)

Targeting Nuclear Exporter Protein XPO1/CRM1 in Gastric Cancer

  • Rachel Sexton,
  • Zaid Mahdi,
  • Rahman Chaudhury,
  • Rafic Beydoun,
  • Amro Aboukameel,
  • Husain Y. Khan,
  • Erkan Baloglu,
  • William Senapedis,
  • Yosef Landesman,
  • Anteneh Tesfaye,
  • Steve Kim,
  • Philip A. Philip,
  • Asfar S. Azmi

DOI
https://doi.org/10.3390/ijms20194826
Journal volume & issue
Vol. 20, no. 19
p. 4826

Abstract

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Gastric cancer remains an unmet clinical problem in urgent need of newer and effective treatments. Here we show that the nuclear export protein, Exportin 1 (XPO1, chromosome region maintenance 1 or CRM1), is a promising molecular target in gastric cancer. We demonstrate significant overexpression of XPO1 in a cohort of histologically diverse gastric cancer patients with primary and metastatic disease. XPO1 RNA interference suppressed gastric cancer cell growth. Anti-tumor activity was observed with specific inhibitor of nuclear export (SINE) compounds (selinexor/XPOVIO), second-generation compound KPT-8602/eltanexor, KPT-185 and +ve control Leptomycin B in three distinct gastric cancer cell lines. SINE compounds inhibited gastric cancer cell proliferation, disrupted spheroid formation, induced apoptosis and halted cell cycle progression at the G1/S phase. Anti-tumor activity was concurrent with nuclear retention of tumor suppressor proteins and inhibition of colony formation. In combination studies, SINE compounds enhanced the efficacy of nab-paclitaxel in vitro and in vivo. More significantly, using non-coding RNA sequencing studies, we demonstrate for the first time that SINE compounds can alter the expression of non-coding RNAs (microRNAs and piwiRNAs). SINE treatment caused statistically significant downregulation of oncogenic miR-33b-3p in two distinct cell lines. These studies demonstrate the therapeutic significance of XPO1 in gastric cancer that warrants further clinical investigation.

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