Aberrant DNA glycosylase-initiated repair pathway of free radicals induced DNA damage: implications for age-related diseases and natural aging

Matkarimov, B.; Saparbaev, M.

Aberrant DNA glycosylase-initiated repair pathway of free radicals induced DNA damage: implications for age-related diseases and natural aging

dc.contributor.author	Matkarimov, B.
dc.contributor.author	Saparbaev, M.
dc.date.accessioned	2017-08-09T09:33:43Z
dc.date.available	2017-08-09T09:33:43Z
dc.date.issued	2017
dc.description.abstract	Aerobic cellular respiration generates reactive oxygen species (ROS), which can damage macro-molecules including lipids, proteins and DNA. It was proposed that aging is a consequence of accumulation of naturally occurring unrepaired oxidative DNA damage. In human cells, approximately 2000 to 8000 DNA lesions occur per hour in each cell, i.e. 40000 to 200000 per cell per day. DNA repair systems are able to discriminate between regular and modified bases. For example, DNA glycosylases specifically recognize and excise damaged bases among vast majority of regular bases in the base excision repair (BER) pathway. However, mismatched pairs between two regular bases occur due to spontaneous conversion of 5-methylcytosine to thymine and DNA polymerase errors during replication. To counteract these mutagenic threats to genome stability, cells evolved special DNA repair systems that target the non-damaged DNA strand in a duplex to remove mismatched regular DNA bases. Base excision repair (BER) and mismatch repair (MMR) pathways initiated by mismatch-specific adenine- and thymine-DNA glycosylases (MutY/MUTYH and TDG/MBD4, respectively) can recognize and remove normal DNA bases in mismatched DNA duplexes. Under certain circumstances in DNA repair deficient cells bacterial MutY and human TDG can act in an aberrant manner: MutY and TDG remove Adenine and Thymine opposite to misincorporated 8-oxoguanine and damaged Adenine, respectively. These unusual activities lead either to mutations or futile DNA repair, thus indicating that the DNA repair pathways which target non-damaged DNA strand can act in an aberrant manner and introduce genome instability in the presence of unrepaired DNA lesions. Both accumulation of oxidative DNA damage in cells and the aberrant DNA repair can contribute to cancer, brain disorders and premature senescence.	ru_RU
dc.identifier.citation	Matkarimov, B. Saparbaev, M. (2017) Aberrant DNA glycosylase-initiated repair pathway of free radicals induced DNA damage: implications for age-related diseases and natural aging. Vol. 33. N 1. pp.3–23	ru_RU
dc.identifier.issn	0233-7657
dc.identifier.uri	doi: http://dx.doi.org/10.7124/bc.000943
dc.identifier.uri	http://nur.nu.edu.kz/handle/123456789/2534
dc.language.iso	en	ru_RU
dc.publisher	Biopolymers and Cell. doi: http://dx.doi.org/10.7124/bc.000943	ru_RU
dc.rights	Attribution-NonCommercial-ShareAlike 3.0 United States	*
dc.rights.uri	http://creativecommons.org/licenses/by-nc-sa/3.0/us/	*
dc.subject	oxidative DNA damage	ru_RU
dc.subject	crystal structure	ru_RU
dc.subject	base excision repair	ru_RU
dc.subject	nucleotide incision repair	ru_RU
dc.subject	AP endonuclease	ru_RU
dc.title	Aberrant DNA glycosylase-initiated repair pathway of free radicals induced DNA damage: implications for age-related diseases and natural aging	ru_RU
dc.type	Article	ru_RU