Translesion synthesis past acrolein-derived DNA adducts by human mitochondrial DNA polymerase γ

Abstract:

Acrolein, a mutagenic aldehyde, is produced endogenously by lipid ...
Acrolein, a mutagenic aldehyde, is produced endogenously by lipid peroxidation and exogenously by combustion of organic materials, including tobacco products. Acrolein reacts with DNA bases forming exocyclic DNA adducts, such as γ-hydroxy-1,N2-propano-2'-deoxyguanosine (γ-HOPdG) and γ-hydroxy-1,N6-propano-2'-deoxyadenosine (γ-HOPdA). The bulky γ-HOPdG adduct blocks DNA synthesis by replicative polymerases but can be bypassed by translesion synthesis polymerases in the nucleus. Although acrolein-induced adducts are likely to be formed and persist in mitochondrial DNA, animal cell mitochondria lack specialized TLS polymerases to tolerate these lesions. Thus, it is important to understand how pol γ, the sole mitochondrial DNA polymerase in human cells, acts on acrolein-adducted DNA. To address this question, we investigated the ability of pol γ to bypass the minor-groove γ-HOPdG and major-groove γ-HOPdA adducts using single nucleotide incorporation and primer extension analyses. The efficiency of pol γ-catalyzed bypass of γ-HOPdG was low and surprisingly, pol γ preferred to incorporate purine nucleotides opposite the adduct. Pol γ also exhibited ~2-fold lower rates of excision of the misincorporated purine nucleotides opposite γ-HOPdG compared to the corresponding nucleotides opposite dG. Extension of primers from the termini opposite γ-HOPdG was accomplished only following error-prone purine nucleotide incorporation. However, pol γ preferentially incorporated dT opposite the γ-HOPdA adduct and efficiently extended primers from the correctly paired terminus, indicating that γ-HOPdA is probably non-mutagenic. In summary, our data suggest that acrolein-induced exocyclic DNA lesions can be bypassed by mitochondrial DNA polymerase but in the case of the minor-groove γ-HOPdG adduct, at the cost of unprecedentedly high mutation rates.

Polymerases:

Topics:

Nucleotide Analogs / Template Lesions, Fidelity

Status:

new topics/pols set partial results complete validated

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