JCI Insight (Jun 2021)

Protein synthesis inhibitor omacetaxine is effective against hepatocellular carcinoma

  • Ling Li,
  • Gilad Halpert,
  • Michael G. Lerner,
  • Haijie Hu,
  • Peter Dimitrion,
  • Matthew J. Weiss,
  • Jin He,
  • Benjamin Philosophe,
  • Richard Burkhart,
  • William R. Burns,
  • Russell N. Wesson,
  • Andrew MacGregor Cameron,
  • Christopher L. Wolfgang,
  • Christos Georgiades,
  • Satomi Kawamoto,
  • Nilofer S. Azad,
  • Mark Yarchoan,
  • Stephen J. Meltzer,
  • Kiyoko Oshima,
  • Laura M. Ensign,
  • Joel S. Bader,
  • Florin M. Selaru

Journal volume & issue
Vol. 6, no. 12

Abstract

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Hepatocellular carcinoma (HCC) is the sixth most common and the fourth most deadly cancer worldwide. The development cost of new therapeutics is a major limitation in patient outcomes. Importantly, there is a paucity of preclinical HCC models in which to test new small molecules. Herein, we implemented potentially novel patient-derived organoid (PDO) and patient-derived xenografts (PDX) strategies for high-throughput drug screening. Omacetaxine, an FDA-approved drug for chronic myelogenous leukemia (CML), was found to be a top effective small molecule in HCC PDOs. Next, omacetaxine was tested against a larger cohort of 40 human HCC PDOs. Serial dilution experiments demonstrated that omacetaxine is effective at low (nanomolar) concentrations. Mechanistic studies established that omacetaxine inhibits global protein synthesis, with a disproportionate effect on short–half-life proteins. High-throughput expression screening identified molecular targets for omacetaxine, including key oncogenes, such as PLK1. In conclusion, by using an innovative strategy, we report — for the first time to our knowledge — the effectiveness of omacetaxine in HCC. In addition, we elucidate key mechanisms of omacetaxine action. Finally, we provide a proof-of-principle basis for future studies applying drug screening PDOs sequenced with candidate validation in PDX models. Clinical trials could be considered to evaluate omacetaxine in patients with HCC.

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