4.7 Article

Rhodamine B conjugates of triterpenoic acids are cytotoxic mitocans even at nanomolar concentrations

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ELSEVIER FRANCE-EDITIONS SCIENTIFIQUES MEDICALES ELSEVIER
DOI: 10.1016/j.ejmech.2016.12.040

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Triterpenes; Maslinic acid; Mitocan; Cytotoxicity; Rhodamine B; Betulinic acid; Oleanolic acid; Ursolic acid; Platanic acid; Glycyrrhetinic acid

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  1. WissenschaftsCampus Halle WCH [W13004216]

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Triterpenoic acids 1-6 exhibited very low or no cytotoxicity at all, but their corresponding 2,3-di-Oacetyl-piperazinyl amides 13-18 showed low EC50 values for several human tumor cell lines. Their cytotoxicity, however, was also high for the non-malignant mouse fibroblasts NIH 3T3. A significant improvement was achieved by preparing the rhodamine B derivatives 19-24. While rhodamine B is not cytotoxic (up to a concentration of 30 mu M cut-off of the assay), the triterpenoid piperazine-spacered rhodamine B derivatives were cytotoxic in nano-molar concentration. Compound 24 (a diacetylated maslinic acid derivative) was most toxic for several human tumor cell lines but less toxic for mouse fibroblasts NIH 3T3. Staining and double-staining experiments revealed 24 to act as a mitocan. (C) 2016 Elsevier Masson SAS. All rights reserved.

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