Miscoding and DNA Polymerase Stalling by Methoxyamine-Adducted Abasic Sites
Тип публикации: Journal Article
Дата публикации: 2022-01-28
scimago Q1
wos Q2
БС2
SJR: 0.957
CiteScore: 7.5
Impact factor: 3.8
ISSN: 0893228X, 15205010
PubMed ID:
35089032
General Medicine
Toxicology
Краткое описание
Apurinic/apyrimidinic (AP) sites appear in DNA spontaneously and as intermediates of base excision DNA repair. AP sites are noninstructive lesions: they strongly block DNA polymerases, and if bypassed, the nature of the incorporated dNMP is mostly guided by the interactions within the polymerase-DNA active site. Many DNA polymerases follow the "A-rule", preferentially incorporating dAMP opposite to natural AP sites. Methoxyamine (MX), a small molecule, efficiently reacts with the aldehyde moiety of natural AP sites, thereby preventing their cleavage by APEX1, the major human AP endonuclease. MX is currently regarded as a possible sensitizer of cancer cells toward DNA-damaging drugs. To evaluate the mutagenic potential of MX, we have studied the utilization of various dNTPs by five DNA polymerases of different families encountering MX-AP adducts in the template in comparison with the natural aldehydic AP site. The Klenow fragment of Escherichia coli DNA polymerase I strictly followed the A-rule with both natural AP and MX-adducted AP sites. Phage RB69 DNA polymerase, a close relative of human DNA polymerases δ and ε, efficiently incorporated both dAMP and dGMP. DNA polymerase β mostly incorporated dAMP and dCMP, preferring dCMP opposite to the natural AP site and dAMP opposite to the MX-AP site, while DNA polymerase λ was selective for dGMP, apparently via the primer misalignment mechanism. Finally, translesion DNA polymerase κ also followed the A-rule for MX-AP and additionally incorporated dCMP opposite to a natural AP site. Overall, the MX-AP site, despite structural differences, was similar to the natural AP site in terms of the dNMP misincorporation preference but was bypassed less efficiently by all polymerases except for Pol κ.
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Yudkina A. V., Zharkov D. O. Miscoding and DNA Polymerase Stalling by Methoxyamine-Adducted Abasic Sites // Chemical Research in Toxicology. 2022. Vol. 35. No. 2. pp. 303-314.
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Yudkina A. V., Zharkov D. O. Miscoding and DNA Polymerase Stalling by Methoxyamine-Adducted Abasic Sites // Chemical Research in Toxicology. 2022. Vol. 35. No. 2. pp. 303-314.
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TY - JOUR
DO - 10.1021/acs.chemrestox.1c00359
UR - https://doi.org/10.1021/acs.chemrestox.1c00359
TI - Miscoding and DNA Polymerase Stalling by Methoxyamine-Adducted Abasic Sites
T2 - Chemical Research in Toxicology
AU - Yudkina, Anna V
AU - Zharkov, Dmitry O
PY - 2022
DA - 2022/01/28
PB - American Chemical Society (ACS)
SP - 303-314
IS - 2
VL - 35
PMID - 35089032
SN - 0893-228X
SN - 1520-5010
ER -
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@article{2022_Yudkina,
author = {Anna V Yudkina and Dmitry O Zharkov},
title = {Miscoding and DNA Polymerase Stalling by Methoxyamine-Adducted Abasic Sites},
journal = {Chemical Research in Toxicology},
year = {2022},
volume = {35},
publisher = {American Chemical Society (ACS)},
month = {jan},
url = {https://doi.org/10.1021/acs.chemrestox.1c00359},
number = {2},
pages = {303--314},
doi = {10.1021/acs.chemrestox.1c00359}
}
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Yudkina, Anna V., et al. “Miscoding and DNA Polymerase Stalling by Methoxyamine-Adducted Abasic Sites.” Chemical Research in Toxicology, vol. 35, no. 2, Jan. 2022, pp. 303-314. https://doi.org/10.1021/acs.chemrestox.1c00359.