Piperazine derivatives of butyric acid as differentiating agents in human leukemic cells |
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Authors: | Reynald Gillet P. Jeannesson Houcine Sefraoui Marie-Luce Arnould-Guérin Serge Kirkiacharian Jean-Claude Jardillier François Pieri |
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Affiliation: | (1) Laboratoire de Biochimie et Biologie Moléculaire, Faculté de Pharmacie, IFR 53, Centre des Biomolécules, 51 rue Cognacq-Jay, F-51096 Reims Cedex, France Tel.: +33 (0) 3 26 05 35 67 Fax: +33 (0) 3 26 05 37 30, FR;(2) Laboratoire de Pharmacologie, Faculté de Pharmacie, Université de Picardie, 1 rue des Louvels, F-88037 Amiens Cedex 1, France, FR;(3) Laboratoire de Chimie Thérapeutique, Faculté de Pharmacie, rue Jean-Baptiste Clément, F-92226 Chatenay-Malabry, France, FR |
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Abstract: | Butyric acid is a potent antineoplastic agent with a well-documented differentiation activity on a wide variety of tumor cells. However, its clinical development is strongly limited by its very short metabolic half-life. In this study we report on the in vitro effects of new original piperazine derivatives of butyric acid on the induction of differentiation and the growth inhibition of human erythroleukemia K562 cells and myeloid leukemia HL60 cells. 1-(2-hydroxyethyl) 4-(1-oxobutyl)-piperazine (HEPB) and [1-(2-hydroxyethyl) 4-(1-oxobutyl)-piperazine] butyrate (HEPDB) were efficient in acting on the differentiation and proliferation of both cell lines, whereas 1-phenyl 4-(1-oxobutyl)-piperazine (PPB) and 1-(3,4-methylene dioxybenzyl) 4-(1-oxobutyl)-piperazine (POB) acted only on proliferation rates. Such derivatives did not induce significant toxicity in mice. These preliminary results should enable, by the development of new series of piperazine derivatives, a better understanding of the mechanisms of action of butyric acid and its analogues on the coupling of growth and differentiation of neoplastic cells. Received: 1 June 1997 / Accepted: 23 July 1997 |
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Keywords: | : Butyric acid Differentiation Leukemia Piperazine derivatives Proliferation |
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