Literature DB >> 18843207

A novel Bim-BH3-derived Bcl-XL inhibitor: biochemical characterization, in vitro, in vivo and ex-vivo anti-leukemic activity.

Raffaella Ponassi1, Barbara Biasotti, Valeria Tomati, Silvia Bruno, Alessandro Poggi, Davide Malacarne, Guido Cimoli, Annalisa Salis, Sarah Pozzi, Maurizio Miglino, Gianluca Damonte, Pietro Cozzini, Francesca Spyrakis, Francesca Spyraki, Barbara Campanini, Luca Bagnasco, Nicoletta Castagnino, Lorenzo Tortolina, Anna Mumot, Francesco Frassoni, Antonio Daga, Michele Cilli, Federica Piccardi, Ilaria Monfardini, Miriam Perugini, Gabriele Zoppoli, Cristina D'Arrigo, Raffaele Pesenti, Silvio Parodi.   

Abstract

BH3-only members of the Bcl-2 family exert a fundamental role in apoptosis induction. This work focuses on the development of a novel peptidic molecule based on the BH3 domain of Bim. The antiapoptotic molecule Bcl-X(L), involved in cancer development/progression and tumour resistance to cytotoxic drugs, is a target for Bim. According to a rational study of the structural interactions between wt Bim-BH3 and Bcl-X(L), we replaced specific residues of Bim-BH3 with natural and non-natural aminoacids and added an internalizing sequence, thus increasing dramatically the inhibitory activity of our modified Bim-BH3 peptide, called 072RB. Confocal microscopy and flow cytometry demonstrated cellular uptake and internalization of 072RB, followed by co-localization with mitochondria. Multiparameter flow cytometry demonstrated that the 072RB dose-dependent growth inhibition of leukaemia cell lines was due to apoptotic cell death. No effect was observed when cells were treated with the internalizing vector alone or a mutated control peptide (single aminoacid substitution L94A). Ex-vivo derived leukemic cells from acute myeloid leukaemia (AML) patients underwent cell death when cultured in vitro in the presence of 072RB. Conversely, no significant cytotoxic effect was observed when 072RB was administered to cultures of peripheral blood mononuclear cells, either resting or PHA-stimulated, and bone marrow cells of normal donors. Xenografts of human AML cells in NOD/SCID mice displayed a significant delay of leukemic cell growth upon treatment with 072RB administered intravenously (15 mg/Kg three times, 48 hours after tumour cell injection). Altogether, these observations support the therapeutic potentials of this novel BH3 mimetic.

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Year:  2008        PMID: 18843207     DOI: 10.4161/cc.7.20.6830

Source DB:  PubMed          Journal:  Cell Cycle        ISSN: 1551-4005            Impact factor:   4.534


  13 in total

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