A Retinoid/Butyric Acid Prodrug Overcomes Retinoic Acid Resistance in Leukemias by Induction of Apoptosis

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Molecular Cancer Research 1:903-912 (2003)
© 2003 American Association for Cancer Research

Cell Cycle, Cell Death, and Senescence

A Retinoid/Butyric Acid Prodrug Overcomes Retinoic Acid Resistance in Leukemias by Induction of Apoptosis¹

Koren K. Mann¹, Ada Rephaeli², April L. Colosimo¹, Zuanel Diaz¹, Abraham Nudelman³, Inesa Levovich²^,3, Yongkui Jing⁴, Samuel Waxman⁴ and Wilson H. Miller, Jr.¹

¹ Lady Davis Institute/SMBD Jewish General Hospital, Center for Translational Research in Cancer, McGill University, Montreal, Quebec, Canada;
² Felsenstein Medical Research Center, Sackler School of Medicine, Tel Aviv University, Petach Tikva, Israel;
³ Chemistry Department, Bar Ilan University, Ramat Gan, Israel; and
⁴ Division of Hematology/Oncology, Department of Medicine, Mount Sinai School of Medicine, New York, NY

Requests for reprints: Wilson H. Miller, Jr., Lady Davis Institute for Medical Research, Sir Mortimer B. Davis Jewish General Hospital, 3755 Cote Ste Catherine Road, Montreal, Quebec, H3T 1E2 Canada. Phone: (514) 340-8222 ext. 4365; Fax: (514) 340-7573. E-mail: wmiller{at}ldi.jgh.mcgill.ca

Some success in overcoming retinoic acid (RA)-resistance hasbeen reported for acute promyelocytic leukemia in cell linesand the clinic by combining histone deacetylase inhibitors,like sodium butyrate (NaB), with RA. This epigenetic therapycounteracts the effects of nuclear corepressors, causing a DNAconformation that facilitates RA-induced gene transcriptionand cell differentiation. In an effort to improve delivery ofeach drug, we have synthesized retinoyloxymethyl butyrate (RN1),a mutual prodrug of both RA and butyric acid. RN1 targets bothdrugs to the same cells or cellular compartments to achievedifferentiation at lower concentrations than using RA and NaBalone. In an RA-resistant cell line, which is not responsiveto RA and NaB given together at the same concentration, RN1inhibited growth substantially. This growth inhibition is causedby an increase in apoptosis and a minimal induction of differentiation,rather than the more complete granulocytic differentiation asseen in the RA-sensitive cell line. The different phenotypesinduced by RN1 in RA-sensitive versus RA-resistant cells arereflected by altered patterns of gene expression. In additionto acute promyelocytic leukemia cells, RN1 induces apoptosisof other RA-resistant leukemic cell lines with blocked transcriptionalpathways, but not normal human peripheral blood mononuclearcells. RN1, therefore, is a novel retinoid that may be morewidely active in hematologic malignancies than RA alone.