| Literature DB >> 25565207 |
An S Tan1, James W Baty1, Lan-Feng Dong2, Ayenachew Bezawork-Geleta2, Berwini Endaya2, Jacob Goodwin2, Martina Bajzikova3, Jaromira Kovarova3, Martin Peterka3, Bing Yan2, Elham Alizadeh Pesdar2, Margarita Sobol4, Anatolyj Filimonenko4, Shani Stuart5, Magdalena Vondrusova3, Katarina Kluckova3, Karishma Sachaphibulkij2, Jakub Rohlena3, Pavel Hozak4, Jaroslav Truksa3, David Eccles1, Larisa M Haupt5, Lyn R Griffiths5, Jiri Neuzil6, Michael V Berridge7.
Abstract
We report that tumor cells without mitochondrial DNA (mtDNA) show delayed tumor growth, and that tumor formation is associated with acquisition of mtDNA from host cells. This leads to partial recovery of mitochondrial function in cells derived from primary tumors grown from cells without mtDNA and a shorter lag in tumor growth. Cell lines from circulating tumor cells showed further recovery of mitochondrial respiration and an intermediate lag to tumor growth, while cells from lung metastases exhibited full restoration of respiratory function and no lag in tumor growth. Stepwise assembly of mitochondrial respiratory (super)complexes was correlated with acquisition of respiratory function. Our findings indicate horizontal transfer of mtDNA from host cells in the tumor microenvironment to tumor cells with compromised respiratory function to re-establish respiration and tumor-initiating efficacy. These results suggest pathophysiological processes for overcoming mtDNA damage and support the notion of high plasticity of malignant cells.Entities:
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Year: 2015 PMID: 25565207 DOI: 10.1016/j.cmet.2014.12.003
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287