| Literature DB >> 28504647 |
Utthara Nayar1, Jouliana Sadek1, Jonathan Reichel1, Denise Hernandez-Hopkins1, Gunkut Akar1, Peter J Barelli2, Michelle A Sahai3, Hufeng Zhou4, Jennifer Totonchy1, David Jayabalan1, Ruben Niesvizky5, Ilaria Guasparri1, Duane Hassane5, Yifang Liu1, Shizuko Sei6, Robert H Shoemaker7, J David Warren2, Olivier Elemento3, Kenneth M Kaye4, Ethel Cesarman1.
Abstract
Primary effusion lymphoma (PEL) is a largely incurable malignancy of B cell origin with plasmacytic differentiation. Here, we report the identification of a highly effective inhibitor of PEL. This compound, 6-ethylthioinosine (6-ETI), is a nucleoside analog with toxicity to PEL in vitro and in vivo, but not to other lymphoma cell lines tested. We developed and performed resistome analysis, an unbiased approach based on RNA sequencing of resistant subclones, to discover the molecular mechanisms of sensitivity. We found different adenosine kinase-inactivating (ADK-inactivating) alterations in all resistant clones and determined that ADK is required to phosphorylate and activate 6-ETI. Further, we observed that 6-ETI induces ATP depletion and cell death accompanied by S phase arrest and DNA damage only in ADK-expressing cells. Immunohistochemistry for ADK served as a biomarker approach to identify 6-ETI-sensitive tumors, which we documented for other lymphoid malignancies with plasmacytic features. Notably, multiple myeloma (MM) expresses high levels of ADK, and 6-ETI was toxic to MM cell lines and primary specimens and had a robust antitumor effect in a disseminated MM mouse model. Several nucleoside analogs are effective in treating leukemias and T cell lymphomas, and 6-ETI may fill this niche for the treatment of PEL, plasmablastic lymphoma, MM, and other ADK-expressing cancers.Entities:
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Year: 2017 PMID: 28504647 PMCID: PMC5451239 DOI: 10.1172/JCI83936
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808