Repair of O6-carboxymethylguanine adducts by O6-methylguanine-DNA methyltransferase in human colon epithelial cells

Abstract: The protein O6-methylguanine-DNA methyltransferase (MGMT) is able to repair the mutagenic O6-methylguanine adduct back to guanine. In this context, it may protect against colorectal cancer (CRC) formation associated with N-nitroso compounds. Such compounds may be endogenously formed by nitrosylation of amino acids, which can give rise to mutagenic O6-methylguanine (O6-MeG) and O6-carboxymethylguanine (O6-CMG) adducts. It is well-established that O6-MeG is repaired by MGMT. However, up to now, whether O6-CMG is… Show more

“…O 6 -alkG results from the reaction of electrophilic alkylating agents with the O 6 -position of guanine. O 6 -Carboxymethylguanosine (O 6 -CMG) and O 6 -methylguanosine (O 6 -MeG) ( Figure A), which are mutagenic and carcinogenic, are two intensively studied O 6 -alkG lesions. , Their occurrence in humans is found to be positively associated with the consumption of red or processed meat and may lead to colorectal cancer. − An AP site (Figure A), another common DNA lesion, is formed by alkylating agents via the initiation of the base excision repair (BER) pathway. , In this pathway, the AP site acts as an important intermediate generated via excision of the damaged nucleobases of DNA . In addition, the AP site can result from other endogenous and exogenous sources including spontaneous hydrolysis of nucleobases in DNA .…”

“…O 6 -Carboxymethylguanosine (O 6 -CMG) and O 6 -methylguanosine (O 6 -MeG) (Figure 1A), which are mutagenic and carcinogenic, are two intensively studied O 6 -alkG lesions. 12,13 Their occurrence in humans is found to be positively associated with the consumption of red or processed meat and may lead to colorectal cancer. 13−15 An AP site (Figure 1A), another common DNA lesion, is formed by alkylating agents via the initiation of the base excision repair (BER) pathway.…”

Discrimination between Different DNA Lesions by Monitoring Single-Molecule Polymerase Stalling Kinetics during Nanopore Sequencing

“…O 6 -alkG results from the reaction of electrophilic alkylating agents with the O 6 -position of guanine. O 6 -Carboxymethylguanosine (O 6 -CMG) and O 6 -methylguanosine (O 6 -MeG) ( Figure A), which are mutagenic and carcinogenic, are two intensively studied O 6 -alkG lesions. , Their occurrence in humans is found to be positively associated with the consumption of red or processed meat and may lead to colorectal cancer. − An AP site (Figure A), another common DNA lesion, is formed by alkylating agents via the initiation of the base excision repair (BER) pathway. , In this pathway, the AP site acts as an important intermediate generated via excision of the damaged nucleobases of DNA . In addition, the AP site can result from other endogenous and exogenous sources including spontaneous hydrolysis of nucleobases in DNA .…”

“…O 6 -Carboxymethylguanosine (O 6 -CMG) and O 6 -methylguanosine (O 6 -MeG) (Figure 1A), which are mutagenic and carcinogenic, are two intensively studied O 6 -alkG lesions. 12,13 Their occurrence in humans is found to be positively associated with the consumption of red or processed meat and may lead to colorectal cancer. 13−15 An AP site (Figure 1A), another common DNA lesion, is formed by alkylating agents via the initiation of the base excision repair (BER) pathway.…”

Discrimination between Different DNA Lesions by Monitoring Single-Molecule Polymerase Stalling Kinetics during Nanopore Sequencing

Meat and digestive cancers

A combination of direct reversion and nucleotide excision repair counters the mutagenic effects of DNA carboxymethylation