Effect of endonuclease G depletion on plasmid DNA uptake and levels of homologous recombination in hela cells
- Authors: Misic V.1, El-Mogy M.1,2, Geng S.1,3, Haj-Ahmad Y.1
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Affiliations:
- Department of Biological Sciences
- Molecular Biology Department
- Montreal Neurological Institute
- Issue: Vol 50, No 2 (2016)
- Pages: 252-261
- Section: Molecular Cell Biology
- URL: https://journal-vniispk.ru/0026-8933/article/view/162587
- DOI: https://doi.org/10.1134/S0026893316020175
- ID: 162587
Cite item
Abstract
Endonuclease G (EndoG) is a mitochondrial apoptosis regulator that also has roles outside of programmed cell death. It has been implicated as a defence DNase involved in the degradation of exogenous DNA after transfection of mammalian cells and in homologous recombination of viral and endogenous DNA. In this study, we looked at the effect of EndoG depletion on plasmid DNA uptake and the levels of homologous recombination in HeLa cells. We show that the proposed defence role of EndoG against uptake of non-viral DNA vectors does not extend to the cervical carcinoma HeLa cells, as targeting of EndoG expression by RNA interference failed to increase intracellular plasmid DNA levels. However, reducing EndoG levels in HeLa cells resulted in a statistically significant reduction of homologous recombination between two plasmid DNA substrates. These findings suggest that non-viral DNA vectors are also substrates for EndoG in its role in homologous recombination.
Keywords
About the authors
V. Misic
Department of Biological Sciences
Author for correspondence.
Email: vanjamisic.bu@gmail.com
Canada, St. Catharines, ON
M. El-Mogy
Department of Biological Sciences; Molecular Biology Department
Email: vanjamisic.bu@gmail.com
Canada, St. Catharines, ON; Dokki, Giza
S. Geng
Department of Biological Sciences; Montreal Neurological Institute
Email: vanjamisic.bu@gmail.com
Canada, St. Catharines, ON; Montreal, Quebec
Y. Haj-Ahmad
Department of Biological Sciences
Email: vanjamisic.bu@gmail.com
Canada, St. Catharines, ON
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