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Biodistribution and Efficacy Studies of the Proteasome Inhibitor BSc2118 in a Mouse Melanoma Model.

Authors :
Mlynarczuk-Bialy I
Doeppner TR
Golab J
Nowis D
Wilczynski GM
Parobczak K
Wigand ME
Hajdamowicz M
Biały LP
Aniolek O
Henklein P
Bähr M
Schmidt B
Kuckelkorn U
Kloetzel PM
Source :
Translational oncology [Transl Oncol] 2014 Oct 24; Vol. 7 (5), pp. 570-9. Date of Electronic Publication: 2014 Oct 24 (Print Publication: 2014).
Publication Year :
2014

Abstract

Inhibition of the proteasome offers many therapeutic possibilities in inflammation as well as in neoplastic diseases. However, clinical use of proteasome inhibitors is limited by the development of resistance or severe side effects. In our study we characterized the anti-tumor properties of the novel proteasome inhibitor BSc2118. The sensitivity of tumor lines to BSc2118 was analyzed in comparison to bortezomib using crystal violet staining in order to assess cell viability. The In Vivo distribution of BSc2118 in mouse tissues was tracked by a fluorescent-modified form of BSc2118 (BSc2118-FL) and visualized by confocal microscopy. Inhibition of the 20S proteasome was monitored both in cultured cell lines and in mice, respectively. Finally, safety and efficacy of BSc2118 was evaluated in a mouse melanoma model. BSc2118 inhibits proliferation of different tumor cell lines with a similar potency as compared with bortezomib. Systemic administration of BSc2118 in mice is well tolerated, even when given in a dose of 60 mg/kg body weight. After systemic injection of BSc2118 or bortezomib similar proteasome inhibition patterns are observed within the murine organs. Detection of BSc2118-FL revealed correlation of distribution pattern of BSc2118 with inhibition of proteasomal activity in cells or mouse tissues. Finally, administration of BSc2118 in a mouse melanoma model shows significant local anti-tumor effects. Concluding, BSc2118 represents a novel low-toxic agent that might be alternatively used for known proteasome inhibitors in anti-cancer treatment.

Details

Language :
English
ISSN :
1936-5233
Volume :
7
Issue :
5
Database :
MEDLINE
Journal :
Translational oncology
Publication Type :
Academic Journal
Accession number :
25389452
Full Text :
https://doi.org/10.1016/j.tranon.2014.07.002