Mortalin sensitizes human cancer cells to MKT-077-induced senescence
Document Type
Article
Source Title
Cancer Letters
Volume
252
First Page
259
Last Page
269
Publication Date
2007
Abstract
Mortalin is a chaperone protein that functions in many cellular processes such as mitochondrial biogenesis, intracellular trafficking, cell proliferation and signaling. Its upregulation in many human cancers makes it a candidate target for therapeutic intervention by small molecule drugs. In continuation to our earlier studies showing mortalin as a cellular target of MKT-077, a mitochondrion-seeking delocalized cationic dye that causes selective death of cancer cells, in this work, we report that MKT-077 binds to the nucleotide-binding domain of mortalin, causes tertiary structural changes in the protein, inactivates its chaperone function, and induces senescence in human tumor cell lines. Interestingly, in tumor cells with elevated level of mortalin expression, fairly low drug doses were sufficient to induce senescence. Guided by molecular screening for mortalin in tumor cells, our results led to the idea that working at low doses of the drug could be an alternative senescence-inducing cancer therapeutic strategy that could, in theory, avoid renal toxicities responsible for the abortion of MKT-077 clinical trials. Our work may likely translate to a re-appraisal of the therapeutic benefits of low doses of several classes of anti-tumor drugs, even of those that had been discontinued due to adverse effects.
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Recommended Citation
Deocaris, C. C., Widodo, N., Shrestha, B. G., Kaur, K., Ohtaka, M., Yamasaki, K., Kaul, S. C., & Wadhwa, R. (2007). Mortalin sensitizes human cancer cells to MKT-077-induced senescence. Cancer Letters, 252, 259-269. Retrieved from https://animorepository.dlsu.edu.ph/faculty_research/5467
Disciplines
Biochemistry, Biophysics, and Structural Biology
Keywords
Molecular chaperones; Cancer cells; Aging—Molecular aspects
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