| Literature DB >> 29769289 |
Kevin J Frankowski1, Chen Wang2, Samarjit Patnaik3, Frank J Schoenen1, Noel Southall3, Dandan Li4, Yaroslav Teper4, Wei Sun3, Irawati Kandela5, Deqing Hu6, Christopher Dextras3, Zachary Knotts4, Yansong Bian4, John Norton2, Steve Titus3, Marzena A Lewandowska2, Yiping Wen2, Katherine I Farley7, Lesley Mathews Griner3, Jamey Sultan3, Zhaojing Meng8, Ming Zhou8, Tomas Vilimas9, Astin S Powers10, Serguei Kozlov9, Kunio Nagashima11, Humair S Quadri4, Min Fang12, Charles Long2, Ojus Khanolkar2, Warren Chen2, Jinsol Kang2, Helen Huang2, Eric Chow2, Esthermanya Goldberg2, Coral Feldman2, Romi Xi2, Hye Rim Kim13, Gary Sahagian12, Susan J Baserga7, Andrew Mazar5, Marc Ferrer3, Wei Zheng3, Ali Shilatifard6, Jeffrey Aubé1, Udo Rudloff14, Juan Jose Marugan15, Sui Huang16.
Abstract
Metastasis remains a leading cause of cancer mortality due to the lack of specific inhibitors against this complex process. To identify compounds selectively targeting the metastatic state, we used the perinucleolar compartment (PNC), a complex nuclear structure associated with metastatic behaviors of cancer cells, as a phenotypic marker for a high-content screen of over 140,000 structurally diverse compounds. Metarrestin, obtained through optimization of a screening hit, disassembles PNCs in multiple cancer cell lines, inhibits invasion in vitro, suppresses metastatic development in three mouse models of human cancer, and extends survival of mice in a metastatic pancreatic cancer xenograft model with no organ toxicity or discernable adverse effects. Metarrestin disrupts the nucleolar structure and inhibits RNA polymerase (Pol) I transcription, at least in part by interacting with the translation elongation factor eEF1A2. Thus, metarrestin represents a potential therapeutic approach for the treatment of metastatic cancer.Entities:
Mesh:
Substances:
Year: 2018 PMID: 29769289 PMCID: PMC6176865 DOI: 10.1126/scitranslmed.aap8307
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956